Blueprint
FORM 6-K
SECURITIES
AND EXCHANGE COMMISSION
Washington,
D.C. 20549
Report
of Foreign Issuer
Pursuant
to Rule 13a-16 or 15d-16 of
the
Securities Exchange Act of 1934
For the
month of May
2018
Commission
File Number: 001-11960
AstraZeneca PLC
1
Francis Crick Avenue
Cambridge
Biomedical Campus
Cambridge
CB2 0AA
United
Kingdom
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by check mark whether the registrant files or will file annual
reports under cover of Form 20-F or Form 40-F.
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by check mark whether the registrant by furnishing the information
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AstraZeneca PLC
INDEX
TO EXHIBITS
AstraZeneca PLC
18 May
2018 07:00
Q1 2018 Results
Encouraging launches and the performance of newer medicines
underpin reiterated guidance
As
expected, the Product Sales performance benefitted from strong
launches and the continued growth of newer medicines and China,
offset by the erosion of Crestor sales. Progress was made on
overall cost discipline, while the level of Externalisation
Revenue, divestment timing and investment in launches impacted the
overall results. Patients continued to benefit from the progress of
the pipeline and AstraZeneca’s plans remain on track, with
the Company continuing to anticipate Product Sales growth this
year, weighted to the second half.
Financial Highlights
|
Q1 2018
|
$m
|
% change
|
|
Actual
|
CER1
|
Total
Revenue
|
5,178
|
(4)
|
(9)
|
Product Sales
|
4,985
|
3
|
(2)
|
Externalisation Revenue
|
193
|
(66)
|
(67)
|
|
|
|
|
Reported
Operating Profit2
|
696
|
(24)
|
(21)
|
Core
Operating Profit3
|
896
|
(46)
|
(47)
|
|
|
|
|
Reported
Earnings Per Share (EPS)
|
$0.27
|
(37)
|
(29)
|
Core
EPS
|
$0.48
|
(51)
|
(51)
|
●
Product Sales increased by 3% (down by 2% at CER).
Strong performance of China and newer medicines across all therapy
areas was offset by the decline of Crestor sales in Europe and Japan. Total Revenue declined
by 4% (9% at CER) to $5,178m, reflecting the level of
Externalisation Revenue in the quarter
●
The Reported Gross Margin declined by five
percentage points (four at CER) to 77.3%, a result of the
favourable impact of manufacturing variances realised in Q1 2017,
as well as the agreement on Lynparza with MSD4;the
Core Gross Margin fell by five percentage points (four at CER) to
78.8%
●
Good
progress on overall cost discipline - Reported Operating Expenses
were stable (down by 5% at CER) at $3,817m; Core Operating Expenses
increased by 3% (but declined by 1% at CER) to $3,349m. Reported
R&D costs declined by 12% (16% at CER) to $1,279m;Core R&D
costs declined by 7% (12% at CER) to $1,240m, driven by efficiency
savings. Reported SG&A costs increased by 7% (2% at CER) to
$2,457m; Core SG&A costs increased by 11% (6% at CER) to
$2,028m, reflecting investment in China and new medicine
launches
●
Reported Other Operating Income & Expense
increased by 99% (97% at CER) to $469m, a result of a legal
settlement; Core Other Operating Income & Expense declined by
63% (64% at CER) to $124m, impacted by the timing of
divestments
●
Reported
EPS of $0.27 and Core EPS of $0.48
●
Capital
expenditure reduced to $213m (Q1 2017: $286m). Restructuring costs
reduced to $95m (Q1 2017: $312m), supporting an anticipated decline
over the full year
●
FY
2018 guidance reiterated and unchanged
Pascal Soriot, Chief Executive Officer, commenting on the results
said:
“Encouraging
launches and strong performances from our newer generation of
medicines made a significant contribution to Product Sales in the
quarter, paving the way for our anticipated return to growth in
2018. The performance was in line with our expectations and
guidance for the year is unchanged. We delivered strong results for
Lynparza, Tagrisso and Imfinzi in Oncology, Brilinta and Farxiga in CVRM and a successful launch
of Fasenra in Respiratory.
Our China sales continued to surpass expectations and we expect
that the effects of the Crestor patent expiries in Europe and
Japan will recede materially in the second half.
AstraZeneca’s
pipeline continued to bring significant benefits for patients, most
recently with the expanded US approval of Tagrisso for lung cancer and
Lynparza for breast cancer.
With our transformation coming into sharper commercial focus as the
year progresses, we are confident of delivering on our
goals.”
Commercial Highlights
Newer medicines5
generated more than $0.4bn in
additional sales at CER in the quarter. Product Sales highlights
were:
●
Oncology:
sales growth of 39% in the quarter (33% at CER) to $1,230m,
including:
- Lynparza sales of $119m, growth of 109% (100% at CER),
driven by regulatory approvals in the US
-Tagrisso sales of $338m, growth of 98% (89% at CER)
reflecting growth as the new standard of care in the treatment of
2nd-line EGFR6
T790M-mutated7
NSCLC8. Approved
in the US in April 2018 in the 1st-line setting
- Imfinzi sales of $62m (FY 2017: $19m), a result of the
recent US approval for the treatment of unresectable, Stage III
NSCLC
●
New CVRM9:
13% growth (8% at CER) to $900m, including:
- Brilinta sales of $293m, growth of
31% (24% at CER) due to continued market penetration in acute
coronary syndrome (ACS) and high-risk periprocedural myocardial infarction
(HR PMI)
- Farxiga sales of $299m, growth of 44%
(39% at CER) as the medicine continued to lead the market by
volume
- Bydureon sales of $139m, a decline of
9% (11% at CER). An encouraging BCise device launch, outweighed by the
impact of price pressures in the US
●
Respiratory:
stable sales of $1,181m (a decline of 6% at CER),
including:
- A Symbicort sales decline of 6% (12% at CER) to $634m, as
competitive class pressures in the US continued
- Pulmicort
sales growth of 3% (down by 3% at CER)
to $346m, reflecting the inflated level of demand in China in Q4
2017 and a supply delay in China
- Fasenra sales of $21m. A very strong launch and
uptake, especially in the US and
Germany
●
Emerging
Markets: the largest region by Product Sales, with growth of 13%
(8% at CER) to $1,765m, including:
- A China sales increase of 31% (22% at CER) to
$1,025m. For the first time, quarterly sales of more than $1bn were
achieved, underpinned by the launch of Tagrisso
-
An ex-China sales decline of 5% (7% at CER) to $740m. A robust
performance, outweighed by the impact of divested Product Sales and
a Russia sales decline of 38% (40% at CER) to $34m
Pipeline Highlights
The
table below highlights significant developments in the late-stage
pipeline since the prior results announcement:
Regulatory
Approvals
|
- Lynparza - ovarian cancer (2nd line;
tablets) (EU)
- Tagrisso - lung cancer (1st line)
(US)
- Imfinzi - lung cancer (Stage III)
(US)
- Lokelma (ZS-9) -
hyperkalaemia(EU)
|
Regulatory
Submissions and/or Acceptances
|
- Lynparza - breast cancer
(EU)
- moxetumomab
pasudotox - hairy cell leukaemia (3rd line) (US)
- Forxiga - type-1 diabetes
(EU)
|
Major
Phase III Data Readouts or Other Major Developments
|
- Tagrisso - lung cancer (1st line) -
priority review status (JP)
- Imfinzi + tremelimumab - lung cancer
(3rd line) (ARCTIC trial) - did not meet primary endpoints in
PDL1-low/neg. patients
- moxetumomab
pasudotox - hairy cell leukaemia (3rd line) - Priority Review
(US)
- selumetinib -
neurofibromatosis type 1 (NF1) - Orphan Drug Designation
(US)
- Fasenra - COPD (GALATHEA trial) - did
not meet primary endpoint
|
Guidance
Guidance
for FY 2018 is reiterated and unchanged. All measures in this
section are at CER. Company guidance is on Product Sales and Core
EPS only.
Product Sales
|
A low
single-digit percentage increase
|
Core EPS
|
$3.30
to $3.50
|
The
aforementioned anticipated growth in Product Sales is weighted
towards the second half of the year. This reflects the remaining
impact of generic competition, namely Crestor in Europe and Japan, as well as
the growing contribution from newer medicines.
Variations
in performance between quarters can be expected to continue. The
Company is unable to provide guidance and indications on a Reported
basis because the Company cannot reliably forecast material
elements of the Reported result, including the fair-value
adjustments arising on acquisition-related liabilities,
intangible-asset impairment charges and legal-settlement
provisions. Please refer to the section ‘Cautionary
Statements Regarding Forward-Looking Statements’ at the end
of this announcement.
Additional Commentary
Outside
of guidance, the Company today reiterates its additional
indications for FY 2018 vs. the prior year:
●
The sum of
Externalisation Revenue and Other Operating Income & Expense is
anticipated to decline vs. the prior year. As part of its long-term
growth strategy, the Company remains committed to focusing on
appropriate cash-generating and value-accretive externalisation
activities that reflect the ongoing productivity of the pipeline.
It is also committed to the continued management of its portfolio
through divestments and to increasing the focus on its three main
therapy areas over time
●
Core R&D costs
in FY 2018 are anticipated to be in the range of a low single-digit
percentage decline to stable. This expectation includes the
favourable impact on development costs from the MSD
collaboration
●
The Company
maintains its focus on reducing operational and infrastructure
costs. Total Core SG&A costs are, however, expected to increase
by a low to mid single-digit percentage in FY 2018, reflecting
targeted support for medicine launches, including Imfinzi in Oncology and Fasenra in Respiratory. The
Company also anticipates a reduction in restructuring costs in FY
2018 vs. the prior year
●
A Core Tax Rate of
16-20% (FY 2017: 14%)
Currency Impact
Based
only on average exchange rates in the three months to 31 March 2018
and the Company’s published currency sensitivities, there
would be a low single-digit favourable impact from currency
movements on Product Sales and Core EPS in FY 2018. Details on
currency sensitivities are contained within the Operating and
Financial Review.
Sustainability
AstraZeneca
is committed to being a valued and trusted partner to its
stakeholders over the long term. There is a distinct connection
between maintaining a strong business and making a positive impact
to a fairer, safer and healthier world. AstraZeneca is dedicated to
pushing the boundaries of science to deliver sustainable health
that transforms the lives of patients around the
world.
AstraZeneca’s
sustainability ambition is founded on making science accessible and
operating in a way that recognises the interconnection between
business growth, the needs of society and the limitations of the
planet. The Company’s sustainability ambition is reinforced
by its purpose and values, which are intrinsic to its business
model and ensures that the delivery of its strategy broadens access
to medicines, minimises the environmental footprint of medicines
and processes and ensures that all business activities are
underpinned by the highest levels of ethics and
transparency.
A full
update on the Company’s sustainability progress is shown
later in this announcement.
Notes
The
following notes refer to pages 1-3:
1.
Constant exchange
rates. These are non-GAAP financial measures because they remove
the effects of currency movements from Reported
results.
2.
Reported financial
measures are the financial results presented in accordance with
IFRS.
3.
Core financial
measures. These are non-GAAP financial measures because, unlike
Reported performance, they cannot be derived directly from the
information in the Group Financial Statements. See the Operating
and Financial Review for a definition of Core financial measures
and a reconciliation of Core to Reported financial
measures.
4.
Merck & Co.,
Inc., Kenilworth, NJ, US, known as MSD outside the US and
Canada.
5.
Here, Lynparza, Tagrisso, Imfinzi, Calquence, Brilinta, Farxiga, Lokelma, Bevespi and Fasenra.
6.
Epidermal growth
factor receptor.
7.
Substitution of
threonine (T) with methionine (M) at position 790 of exon 20
mutation.
8.
Non-small cell lung
cancer.
9.
New Cardiovascular,
Renal and Metabolism, incorporating Brilinta, Diabetes medicines and
Lokelma.
The
performance shown in this announcement covers the three-month
period to 31 March 2018 (the quarter or Q1 2018) compared to the
three-month period to 31 March 2017 (the prior quarter or Q1 2017),
unless stated otherwise.
Pipeline - Forthcoming Major News Flow
Innovation
is critical to addressing unmet patient needs and is at the heart
of the Company’s growth strategy. The focus on research and
development is designed to yield strong results from the
pipeline.
Q2
2018
|
Lynparza - ovarian cancer (1st line): data
readout10
Tagrisso - lung cancer: regulatory decision
(EU)
Lokelma - hyperkalaemia: regulatory decision
(US)
Duaklir - COPD: regulatory submission (US)
Fasenra - COPD (TERRANOVA): data readout
|
H2
2018
|
Lynparza - breast cancer: regulatory decision
(JP)
Lynparza - ovarian cancer (1st line): regulatory
submission
Tagrisso - lung cancer: regulatory decision
(JP)
Imfinzi - lung cancer (Stage III): regulatory decision (EU,
JP)
Imfinzi +/- treme - lung cancer (1st line) (MYSTIC): data
readout (final OS11), regulatory submission
Imfinzi +/- treme - head & neck cancer (1st line)
(KESTREL): data readout
Imfinzi +/- treme head & neck cancer (2nd line)
(EAGLE): data readout, regulatory submission
selumetinib
- thyroid cancer: data readout, regulatory submission
moxetumomab
pasudutox - hairy cell leukaemia (3rd line): regulatory decision
(US)
Farxiga - type-2 diabetes (DECLARE): data
readout
Bydureon autoinjector - type-2 diabetes: regulatory
decision (EU)
roxadustat
- anaemia: data readout
Bevespi - COPD: regulatory decision (EU)
Bevespi - COPD: regulatory submission (JP)
PT010 -
COPD: regulatory submission
Fasenra - COPD: regulatory submission
anifrolumab
- lupus: data readout
|
2019
|
Lynparza - breast cancer: regulatory decision
(EU)
Lynparza - pancreatic cancer: data readout, regulatory
submission
Imfinzi - lung cancer (PACIFIC): data readout (final
OS)
Imfinzi +/- treme - head & neck cancer (1st line)
(KESTREL): regulatory submission
Imfinzi + treme - lung cancer (NEPTUNE): data readout,
regulatory submission
Imfinzi +/- treme - lung cancer (POSEIDON): data readout,
regulatory submission
Imfinzi +/- treme - small-cell lung cancer (CASPIAN): data
readout, regulatory submission
Imfinzi +/- treme - bladder cancer (DANUBE): data readout,
regulatory submission
Calquence - Chronic lymphocytic leukaemia (CLL): data
readout, regulatory submission
Brilinta - Coronary artery disease (CAD) / type-2 diabetes:
data readout, regulatory submission
Farxiga - type-2 diabetes (DECLARE): regulatory
submission
Farxiga - heart failure: data readout
roxadustat
- anaemia: regulatory submission (US)
anifrolumab
- lupus: regulatory submission
lanabecestat
- Alzheimer's disease: data readout
|
Conference Call
A live
presentation and webcast for investors and analysts, hosted by
management, will begin at 12pm UK time today. Details can be
accessed via astrazeneca.com.
Reporting Calendar
The
Company intends to publish its first-half and second-quarter
financial results on Thursday, 26 July 2018.
About AstraZeneca
AstraZeneca
is a global, science-led biopharmaceutical company that focuses on
the discovery, development and commercialisation of prescription
medicines, primarily for the treatment of diseases in three therapy
areas - Oncology, CVRM and Respiratory. The Company also is
selectively active in the areas of autoimmunity, neuroscience and
infection. AstraZeneca operates in over 100 countries and its
innovative medicines are used by millions of patients
worldwide.
For
more information, please visit astrazeneca.com
and follow us on Twitter @AstraZeneca.
Investor
Relations
|
|
|
Thomas
Kudsk Larsen
|
|
+44 203
749 5712
|
Craig
Marks
|
Finance;
Fixed Income; M&A
|
+44
7881 615 764
|
Henry
Wheeler
|
Oncology
|
+44 203
749 5797
|
Mitchell
Chan
|
Oncology;
Other
|
+1 240
477 3771
|
Christer
Gruvris
|
Brilinta; Diabetes
|
+44 203
749 5711
|
Nick
Stone
|
Respiratory;
Renal
|
+44 203
749 5716
|
US toll
free
|
|
+1 866
381 7277
|
Media
Relations
|
|
|
Gonzalo
Viña
|
UK/Global
|
+44 203
749 5916
|
Karen
Birmingham
|
UK/Global
|
+44 203
749 5634
|
Rob
Skelding
|
UK/Global
|
+44 203
749 5821
|
Matt
Kent
|
UK/Global
|
+44 203
749 5906
|
Jacob
Lund
|
Sweden
|
+46
8 553 260 20
|
Michele
Meixell
|
US
|
+1 302
885 2677
|
Operating And Financial Review
All
narrative on growth and results in this section is based on actual
exchange rates, unless stated otherwise. Financial figures are in
US$ millions ($m). The performance shown in this announcement
covers the three-month period to 31 March 2018 (the quarter or Q1
2018) compared to the three-month period to 31 March 2017 (the
prior quarter or Q1 2017, respectively). All commentary in the
Operating and Financial Review relates to the quarter, unless
stated otherwise.
Core
financial measures, EBITDA, Net Debt, Initial Externalisation
Revenue and Ongoing Externalisation Revenue are non-GAAP financial
measures because they cannot be derived directly from the Group
Condensed Consolidated Financial Statements. Management believes
that these non-GAAP financial measures, when provided in
combination with Reported results, will provide investors and
analysts with helpful supplementary information to better
understand the financial performance and position of the Company on
a comparable basis from period to period. These non-GAAP financial
measures are not a substitute for, or superior to, financial
measures prepared in accordance with GAAP. Core financial measures
are adjusted to exclude certain significant items, such
as:
●
Amortisation and
impairment of intangible assets, including impairment reversals but
excluding any charges relating to IT assets
●
Charges and
provisions related to global restructuring programmes, which
includes charges that relate to the impact of global restructuring
programmes on capitalised IT assets
●
Other specified
items, principally comprising acquisition-related costs, which
include fair-value adjustments and the imputed finance charge
relating to contingent consideration on business combinations,
legal settlements and foreign-exchange gains and losses on certain
non-structural intra-group loans
Details
on the nature of Core financial measures are provided on page 68 of
the Annual
Report and Form
20-F Information 2017. Reference should be made to the
reconciliation of Core to Reported financial information and the
Reconciliation of Reported to Core Financial Measures table
included in the Financial Performance section of this
announcement.
EBITDA
is defined as Reported Profit Before Tax after adding back Net
Finance Expense, results from Joint Ventures and Associates and
charges for depreciation, amortisation and impairment. Reference
should be made to the Reconciliation of Reported Profit Before Tax
to EBITDA included in the Financial Performance section of this
announcement.
Net
Debt is defined as interest-bearing loans and borrowings net of
cash and cash equivalents, other investments and net derivative
financial instruments. Reference should be made to the
Reconciliation of Interest-Bearing Loans and Borrowings to Net Debt
included in the Cash Flow and Balance Sheet section of this
announcement.
Ongoing
Externalisation Revenue is defined as Externalisation Revenue
excluding Initial Externalisation Revenue (which is defined as
Externalisation Revenue that is recognised at the date of
completion of an agreement or transaction, in respect of upfront
consideration). Ongoing Externalisation Revenue comprises, among
other items, royalties, milestone revenue and profit-sharing income. Reference
should be made to the Breakdown of Externalisation Revenue table in
this Operating and Financial Review.
The
Company strongly encourages investors and analysts not to rely on
any single financial measure, but to review AstraZeneca’s
financial statements, including the notes thereto, and other
available Company reports, carefully and in their
entirety.
Table 1: Total Revenue
|
Q1 2018
|
$m
|
% change
|
Actual
|
CER
|
Total Revenue
|
5,178
|
(4)
|
(9)
|
|
|
|
|
Product
Sales
|
4,985
|
3
|
(2)
|
Externalisation
Revenue
|
193
|
(66)
|
(67)
|
Table 2: Product Sales
|
Q1 2018
|
$m
|
|
% change
|
Actual
|
CER
|
Oncology
|
1,230
|
25
|
39
|
33
|
New
CVRM
|
900
|
18
|
13
|
8
|
Respiratory
|
1,181
|
24
|
-
|
(6)
|
Other
|
1,674
|
34
|
(15)
|
(19)
|
|
|
|
|
|
Total
|
4,985
|
100
|
3
|
(2)
|
Table 3: Breakdown Of Externalisation Revenue
Ongoing
Externalisation Revenue of $91m represented 47% of total
Externalisation Revenue (Q1 2017: $181m, 32%). The Company
anticipates that Ongoing Externalisation Revenue will grow as a
proportion of Externalisation Revenue over time. A breakdown of
Externalisation Revenue is shown below:
|
$m
|
% of total
|
% change
|
Actual
|
CER
|
Royalties
|
8
|
4
|
(83)
|
(84)
|
|
83
|
43
|
(39)
|
(38)
|
|
|
|
|
|
Ongoing Externalisation Revenue
|
91
|
47
|
(50)
|
(49)
|
|
|
|
|
|
Initial
Externalisation Revenue
|
102
|
53
|
(73)
|
(75)
|
|
|
|
|
|
Total Externalisation Revenue
|
193
|
100
|
(66)
|
(67)
|
Table 4: Initial Externalisation Revenue
Where
AstraZeneca retains a significant ongoing interest in medicines or
potential new medicines, revenue arising from externalisation
agreements is reported as Externalisation Revenue in the
Company’s financial statements. A breakdown of Initial
Externalisation Revenue is shown below:
Medicine
|
Partner
|
Region
|
$m
|
Crestor
|
Almirall,
S.A. (Almirall)
|
Spain
|
61
|
Other
|
|
|
41
|
|
|
|
|
Total
|
|
|
102
|
Table 5: Ongoing Externalisation Revenue
A
breakdown of Ongoing Externalisation Revenue in the quarter is
shown below:
Medicine
|
Partner
|
Region
|
$m
|
Lynparza
|
MSD -
milestone revenue (breast cancer regulatory approval)
|
Global
|
70
|
Other
|
|
|
21
|
|
|
|
|
Total
|
|
|
91
|
Table 6: Externalised And Divested Medicines
Several
AstraZeneca medicines were externalised or divested after Q1 2017,
thus adversely impacting the Product Sales
performance:
Completion
|
Medicine
|
Region
|
|
Q1 2017
|
Difference
|
Adverse Impact on
Q1 2018
Product Sales
|
$m
|
$m
|
$m
|
|
June
2017
|
Seloken
|
Europe
|
6
|
21
|
(15)
|
|
June
2017
|
Zomig
|
Global
(excl. Japan)
|
7
|
19
|
(12)
|
|
October
2017
|
|
Global
|
19
|
85
|
(66)
|
|
January
2018
|
Crestor
|
Spain
|
3
|
22
|
(19)
|
|
|
|
|
|
|
|
|
|
Total
|
|
35
|
147
|
(112)
|
2%
|
Table 7: Ongoing Externalisation Revenue Agreements
Examples
of transactions that include Ongoing Externalisation Revenue are
shown below:
Completion
|
Medicine
|
Partner
|
Region
|
Externalisation Revenue
|
July
2017
|
Lynparza
|
MSD
|
Global
|
● Initial $1.0bn
revenue
● Up to $0.75bn for
certain licence options, including $0.25bn paid in Q4
2017
● Up to $6.15bn in
regulatory and sales milestones
|
March
2017
|
MEDI8897
|
Sanofi
Pasteur, Inc.
|
Global
|
● Initial €120m
revenue
● Up to €495m
in sales and development-related milestones
|
March
2017
|
Zoladex
|
TerSera
Therapeutics LLC (TerSera)
|
US and
Canada
|
● Initial $250m
revenue
● Up to $70m in
sales-related milestones
● Mid-teen percentage
royalties on sales
|
Product Sales
The
performance of major medicines is shown below, with a geographical
split shown in Note 6.
Table 8: Therapy Area And Medicine Performance
Therapy Area
|
Medicine
|
Q1 2018
|
$m
|
|
% change
|
Actual
|
CER
|
Oncology
|
Tagrisso
|
338
|
7
|
98
|
89
|
Iressa
|
132
|
3
|
6
|
(1)
|
Lynparza
|
119
|
2
|
109
|
100
|
Imfinzi
|
62
|
1
|
n/m
|
n/m
|
Calquence
|
8
|
-
|
n/m
|
n/m
|
Legacy:
|
|
|
|
|
Faslodex
|
254
|
5
|
19
|
14
|
Zoladex
|
184
|
4
|
(1)
|
(6)
|
Arimidex
|
54
|
1
|
4
|
(2)
|
Casodex
|
52
|
1
|
(7)
|
(13)
|
Others
|
27
|
1
|
4
|
(4)
|
Total Oncology
|
1,230
|
25
|
39
|
33
|
CVRM
|
Brilinta
|
293
|
6
|
31
|
24
|
Farxiga
|
299
|
6
|
44
|
39
|
Onglyza
|
129
|
3
|
(16)
|
(19)
|
Bydureon
|
139
|
3
|
(9)
|
(11)
|
Byetta
|
31
|
1
|
(33)
|
(35)
|
Symlin
|
9
|
-
|
(36)
|
(36)
|
Legacy:
|
|
|
|
|
Crestor
|
389
|
8
|
(38)
|
(42)
|
Seloken/Toprol-XL
|
200
|
4
|
8
|
3
|
Atacand
|
71
|
1
|
(5)
|
(9)
|
Others
|
85
|
2
|
(4)
|
(10)
|
Total CVRM
|
1,645
|
33
|
(8)
|
(12)
|
Respiratory
|
Symbicort
|
634
|
13
|
(6)
|
(12)
|
Pulmicort
|
346
|
7
|
3
|
(3)
|
Daliresp/Daxas
|
38
|
1
|
(14)
|
(16)
|
Tudorza/Eklira
|
34
|
1
|
(8)
|
(16)
|
Duaklir
|
28
|
1
|
47
|
26
|
Fasenra
|
21
|
-
|
n/m
|
n/m
|
Bevespi
|
5
|
-
|
n/m
|
n/m
|
Others
|
75
|
2
|
12
|
3
|
Total Respiratory
|
1,181
|
24
|
-
|
(6)
|
Other
|
Nexium
|
448
|
9
|
(3)
|
(7)
|
Synagis
|
224
|
4
|
(3)
|
(3)
|
Losec/Prilosec
|
69
|
1
|
1
|
(6)
|
Seroquel XR
|
53
|
1
|
(21)
|
(25)
|
Movantik/Moventig
|
28
|
1
|
(7)
|
(7)
|
Others
|
107
|
2
|
(25)
|
(29)
|
Total Other
|
929
|
19
|
(7)
|
(10)
|
|
Total Product Sales
|
4,985
|
100
|
3
|
(2)
|
Product Sales Summary
ONCOLOGY
Product
Sales of $1,230m; an increase of 39% (up 33% at CER). Oncology
Product Sales represented 25% of total Product Sales, up from 18%
in Q1 2017.
Lynparza
Product
Sales of $119m; an increase of 109% (100% at CER). The strong
performance was spread across the region and was particularly
noticeable in the US. To date, the medicine has received regulatory
approval in over 50 countries, with reviews underway in a number of
additional markets and for new uses.
US
sales grew by 144% to $66m; the performance partly reflected the H2
2017 launch of Lynparza
tablets and regulatory approval as a 2nd-line treatment for ovarian
cancer, regardless of
BRCA
status. The Company announced
more recently the approval of Lynparza in the US as a treatment for
patients with germline BRCA-mutated breast cancer; this
approval was reflected in sequential quarterly US sales growth of
22%, from $54m in Q4 2017. At the end of Q1 2018, Lynparza was the leading medicine in
the poly ADP ribose polymerase (PARP)-inhibitor class in the US, as
measured by total prescription volumes.
Sales
in Europe increased by 68% (44% at CER) to $42m, reflecting high
BRCA-testing rates, a
number of successful launches and encouraging levels of
reimbursement. Lynparza
sales in Europe in the quarter were for the treatment of ovarian
cancer, in capsule formulation. On 8 May 2018, the Company
announced that the European Medicines Agency (EMA) had approved Lynparza tablets (300mg twice daily) as a 2nd-line
treatment for ovarian cancer, regardless of BRCA status.
In July
2017, AstraZeneca and MSD announced a global strategic oncology
collaboration to co-develop Lynparza and the potential medicine
selumetinib for multiple cancer types as monotherapies and in
combinations. The integration of development and commercial
activities is progressing well, with both companies co-promoting
Lynparza.
Lung Cancer
Tagrisso
Product
Sales of $338m; an increase of 98% (89% at CER), partly driven by
increased testing rates, led by Japan and the US. The medicine has
received regulatory approval in more than 75
countries.
Sales in the US grew by 63% to $147m, reflecting an increase in
EGFR T790M-mutation testing rates. Sequential quarterly sales
increased by 15% from $128m in Q4 2017. In September 2017, US
National Comprehensive Cancer Network (NCCN) clinical-practice
guidelines were updated to include the use of Tagrisso as a 1st-line treatment of patients with
metastatic EGFR-mutated NSCLC. Tagrisso was approved by the US FDA in this setting in
April 2018.
Within Emerging Markets, Tagrisso sales were $71m (Q1 2017: $6m). Growth in Emerging
Markets was led by China, where an encouraging testing rate was
observed. Tagrisso was approved in China in March 2017 as the first
AstraZeneca medicine under the China FDA’s priority-review
pathway; China has a relatively-high prevalence of patients with an
EGFR mutation.
In Europe, sales of $69m represented growth of 97% (74% at CER),
driven by strong levels of demand, positive reimbursement decisions
and further growth in testing rates. Tagrisso was reimbursed in more than 15 European markets at
the end of the quarter and was under reimbursement review in a
number of additional European countries, with positive decisions
anticipated in H2 2018. A regulatory decision on
Tagrisso
as a 1st-line treatment for
EGFR-mutated NSCLC is also expected in the coming
weeks.
Sales in Japan increased by 26% (21% at CER) to $49m. Sequential
quarterly sales, however, declined from $61m in Q4 2017, driven by
a decline in T790M ctDNA testing rates from c.90% in Q4 2017 to
c.70% in Q1 2018. This followed the mandated expiry of free ctDNA
testing in 2017, which was concluded after the start of
reimbursement and the fulfilment of the bolus of late-line
patients. A regulatory decision on Tagrisso as a 1st-line treatment for EGFR-mutated NSCLC is
expected in the second half of the year.
Imfinzi
Product
Sales of $62m;Imfinzi was
approved under the US FDA’s Accelerated-Approval pathway in
May 2017 and launched on the same day as a fast-to-market, limited
commercial opportunity, indicated for the 2nd-line treatment of
patients with locally-advanced or metastatic urothelial carcinoma
(bladder cancer).
In February 2018, immediately following US regulatory approval, the
Company launched Imfinzi for the treatment of patients with unresectable,
Stage III NSCLC whose disease has not progressed following
concurrent platinum-based chemotherapy and radiation therapy (CRT).
The approval followed the award of Priority Review status in 2017.
The majority of Imfinzi sales in the quarter were for the treatment of
unresectable, Stage III NSCLC.
Iressa
Product
Sales of $132m; an increase of 6% (down by 1% at CER).
Emerging
Markets sales increased by 16% (8% at CER) to $71m. China sales
increased by 29% (21% at CER) to $44m; Iressa was included on the National
Reimbursement Drug List (NRDL) in 2017. Sales in the US were stable
at $8m and increased in Europe by 15% (4% at CER) to
$30m.
Other Oncology Medicines
Calquence
Product
Sales of $8m;Calquence was
approved and launched in the US on 31 October 2017. The medicine
delivered a promising performance in the quarter, illustrated by
the number of new-patient starts in previously-treated mantle cell
lymphoma (MCL). The medicine was included within NCCN MCL
guidelines on 15 November 2017, which helped to facilitate
reimbursement.
Legacy: Faslodex
Product
Sales of $254m; an increase of 19% (14% at CER).
Emerging
Markets sales grew by 44% (41% at CER) to $39m. China sales grew by
100% (83% at CER) to $12m.
US
sales increased by 14% to $134m, mainly reflecting a continued
strong uptake of the combination with palbociclib, a medicine
approved for the treatment of hormone-receptor-positive breast
cancer.
Europe
sales increased by 9% (down by 6% at CER) to $59m, reflecting the
impact of generic entrants in certain markets. In June 2017, a
label extension, based upon the FALCON trial in the 1st-line
setting was approved in Japan, where sales grew by 50% (43% at CER)
to $21m.
Legacy: Zoladex
Product
Sales of $184m; a decline of 1% (6% at CER).
Emerging
Markets sales increased by 16% (10% at CER) to $101m. Sales in
Europe increased by 6% (down by 3% at CER) to $34m. In the
Established Rest Of World (ROW) region, sales declined by 17% (21%
at CER) to $48m, driven by the effects of increased competition. On
31 March 2017, the Company completed an agreement with TerSera for
the sale of the commercial rights to Zoladex in the US and
Canada.
CVRM
New
CVRM sales increased by 13% (8% at CER) to $900m, comprising 18% of
total Product Sales. There were further strong performances from
Brilinta and Farxiga, after each attained
blockbuster-sales status in FY 2017.
Total
CVRM sales, which includes Crestor and other legacy medicines,
amounted to $1,645m and represented a decline of 8% (12% at
CER);total CVRM comprised 33% of total Product Sales, down from 37%
in Q1 2017.
Brilinta
Product
Sales of $293m; an increase of 31% (24% at CER).
Emerging
Markets sales of Brilinta
grew by 27% (20% at CER) to $76m, reflecting a continued
outperformance of branded oral anti-platelet medicines. Encouraging
results were delivered in a number of markets.
US
sales of Brilinta, at $115m, represented an increase
of 32%. The performance was driven primarily by an increase in the
average duration of therapy and strong growth in the number of
patients sent home from hospital with Brilinta. Furthermore, Brilinta achieved a record
total-prescription market share at the end of the quarter;
days-of-therapy volume market-share data was particularly
encouraging.
Sales
of Brilique in Europe
increased by 32% (15% at CER) to $86m, reflecting indication
leadership across a number of markets and bolstered by the
inclusion within HR PMI guidelines by the European Society of
Cardiology in 2017. Improvements were delivered across the major
markets; Brilique continued
to outperform branded oral anti-platelet medicines in the quarter
and gained further reimbursement in key markets in its HR PMI
indication with the 60mg dose.
Farxiga
Product
Sales of $299m; an increase of 44% (39% at CER). Farxiga consolidated its global
leadership position within the sodium-glucose co-transporter 2
(SGLT2) inhibitor class.
Emerging
Markets sales increased by 64% (62% at CER) to $69m, reflecting
ongoing launches and improved levels of patient access. In March
2017, Forxiga became the
first SGLT2-inhibitor medicine to be approved in China, with
encouraging initial results in access and performance.
US
sales increased by 32% to $127m. The performance in Q1 2017 was
adversely impacted by the Company’s level of participation in
affordability programmes; subsequent changes to the Company’s
approach to these programmes, however, helped to deliver a
much-improved performance in Q1 2018. Despite slower growth in the
US, the SGLT2 class continued to be scientifically underpinned by
growing evidence around cardiovascular (CV) benefits, including
data from the CVD-REAL series of studies, first published in May
2017.
Sales
in Europe increased by 48% (30% at CER) to $74m as the medicine
continued to gain overall market share; it also retained leadership
in a class that had the strongest growth among innovative oral
diabetes medicines in 2017. In Japan, where Ono Pharmaceutical Co.,
Ltd is a partner and records in-market sales, sales to the partner
amounted to $11m, representing growth of 57% (43% at
CER).
Bydureon
Product
Sales of $139m; a decline of 9% (11% at CER). Sales in the US
declined by 13% to $111m, reflecting pricing headwinds that offset
an encouraging performance from the recently-launched BCise device. Favourable sales volumes
were driven by continued growth in the glucagon-like peptide-1
(GLP-1) class, at the expense of insulin, for more-advanced forms
of type-2 diabetes.
Bydureon sales in Europe increased by 5% (stable at CER) to
$23m, partly reflecting market growth.
Onglyza
Product
Sales of $129m, a decline of 16% (19% at CER). The performance
reflected adverse pressures on the dipeptidyl peptidase-4 (DPP-4)
class and an acceleration of ongoing Diabetes market dynamics,
where patients are moving to medicines and classes of medicines
with documented CV benefits. Given the significant future potential
of Farxiga, the Company
continues to prioritise commercial support for Farxiga.
Sales
in Emerging Markets increased by 33% (27% at CER) to $40m.
Onglyza, after entry onto
the NRDL in China in 2017, led the Emerging Markets sales growth at
167% (150% at CER) to $16m. Sales in Europe declined by 15% (26% at
CER) to $23m, reflecting the broader trend of a shift away from the
DPP-4 class.
Legacy: Crestor
Product
Sales of $389m; a decline of 38% (42% at CER).
Sales
in China grew by 39% (30% at CER) to $145m, a result of underlying
demand and an element of benefit from the removal of the 2nd-line
usage restriction. Despite the effect of favourable managed-market
adjustments, US sales declined by 59% to $46m, reflecting the
impact of multiple Crestor
generic medicines. In Europe, sales declined by 67% (70% at CER) to
$65m, driven by the effect of generic medicines in various markets.
This impact on Europe sales is anticipated to continue in 2018,
predominantly weighted to the first half of the year.
In
Japan, where Shionogi Co. Ltd is a partner, sales declined by 76%
(77% at CER) to $26m, reflecting the recent entry of multiple
Crestor competitors in the
market in the second half of 2017, plus the effect of government
incentives for the increased adoption of generic medicines. This
impact on Japan sales is anticipated to be broadly in line with the
aforementioned timing in Europe.
RESPIRATORY
Product
Sales of $1,181m;stable (down by 6% at CER). Respiratory Product
Sales represented 24% of total Product Sales, unchanged vs. Q1
2017.
Symbicort
Product
Sales of $634m; a decline of 6% (12% at CER). Symbicort continued to lead the global
market by volume within the inhaled corticosteroid (ICS) /
Long-Acting Beta Agonist (LABA) class.
Emerging
Markets sales grew by 14% (10% at CER) to $128m, partly reflecting
growth in China of 38% (29% at CER) to $66m. In contrast, US sales
declined by 28% to $183m, reflecting pricing pressure and the
timing of government buying. The performance was in line with
expectations, with challenging market conditions expected to
continue.
In
Europe, sales increased by 6% (down by 7% at CER) to $212m; the
performance reflected the level of competition from other branded
and Symbicort-analogue
medicines. Symbicort,
however, continued to retain its class-leadership position and
stabilise its volume market share in the class. In Japan, where
Astellas Pharma Co. Ltd assists as a promotional partner, sales
declined by 2% (6% at CER) to $50m.
Pulmicort
Product
Sales of $346m; an increase of 3% (down by 3% at CER).
Emerging
Markets sales increased by 8% (2% at CER) to $270m, reflecting an
inflated level of demand in China in Q4 2017; strong underlying
volume growth in China, Middle East & Africa and Asia Pacific
was unchanged in Q1 2018; growth in China, however, was limited by
the impact of a temporary constraint in supply. Emerging Markets
represented 78% of global sales.
Sales
in the US and Europe declined by 29% to $29m and increased by 4%
(down by 8% at CER) to $27m, respectively, a consequence of the
medicine’s legacy status in these markets.
Daliresp/Daxas
Product
Sales of $38m; a decline of 14% (16% at CER).
US
sales, representing 76% of global sales, declined by 24% to $29m,
driven by a reduced adoption of the medicine. It is the only oral,
selective, long-acting inhibitor of phosphodiesterase-4, an
inflammatory enzyme associated with COPD. Sales in Europe increased
by 40% (20% at CER) to $7m.
Tudorza/Eklira
Product
Sales of $34m; a decline of 8% (16% at CER).
Sales
in the US declined by 27% to $11m, reflecting lower levels of use
of inhaled monotherapy medicines for the treatment of COPD. On 17
March 2017, AstraZeneca announced that it had entered a strategic
collaboration with Circassia Pharmaceuticals plc (Circassia) for
the development and commercialisation of Tudorza in the US. Circassia began its
promotion of Tudorza in the
US in May 2017, where AstraZeneca books Product Sales.
Sales
in Europe were stable (down by 10% at CER) to $20m, impacted by the
decline of the overall LAMA-monotherapy class.
Duaklir
Product Sales of $28m; an increase of 47% (26% at
CER).
Duaklir, the Company’s first inhaled dual
bronchodilator medicine, is now available for patients in
over 25 countries, with almost all sales emanating from Europe. The
growth in sales was favourably impacted by the performances in
Germany and the UK, as well as the recent launch in
Italy. The LAMA/LABA
class continued to grow strongly, albeit below expectations.
Duaklir is expected to be
submitted for US regulatory review in Q2 2018; the US trademark is
to be confirmed. Duaklir is
a registered trademark in certain European countries.
Bevespi
Product
Sales of $5m; launched in the US in Q1 2017.
Prescriptions
in the period tracked in line with other LAMA/LABA launches. The
overall class in the US, however, continues to grow more slowly
than anticipated. Bevespi
was the first medicine launched using the Company’s
Aerosphere Delivery
Technology delivered in a pressurised metered-dose
inhaler.
Fasenra
Product
Sales of $21m.
In
November 2017, the Company received approval for Fasenra as a treatment for patients
with severe, eosinophilic asthma; the approval was followed
immediately by the launch of the medicine. IQVIA new-to-brand
prescription data showed that Fasenra, a third-to-market medicine,
tracked in-line or ahead of prior biologic-medicine launches in
asthma. Initial feedback from physicians and patients was
particularly encouraging.
In
Europe and Japan, AstraZeneca received regulatory approval in
January 2018, respectively, on a similar basis to that in the US.
In Europe, a number of launches were executed, including, the
Netherlands, Austria, Denmark and Sweden; the launch and uptake of
Fasenra in Germany was
especially successful.
OTHER
Product
Sales of $929m; a decline of 7% (10% at CER). Other Product Sales
represented 19% of total Product Sales, down from 21% in Q1
2017.
Nexium
Product
Sales of $448m; a decline of 3% (7% at CER).
Emerging
Markets sales increased by 4% (down by 1% at CER) to $182m. Despite
the benefit of favourable managed-market adjustments, sales in the
US declined by 26% to $100m in the quarter. Sales in Europe were
stable (down by 13% at CER) at $61m. In Japan, where Daiichi Sankyo
is a partner, sales increased by 31% (25% at CER) to
$89m.
Synagis
Product
Sales of $224m; a decline of 3%.
US
sales declined by 15% to $134m, impacted by the prevailing
guidelines from the American Academy of Pediatrics Committee on
Infectious Diseases, which restrict the number of patients eligible
for preventative therapy with Synagis. Product Sales to AbbVie Inc.
(AbbVie), responsible for the commercialisation of Synagis in over 80 countries outside
the US, increased by 22% to $90m.
Seroquel XR
Product
Sales of $53m; a decline of 21% (25% at CER).
Sales
of Seroquel XR in the US,
where several competitors launched generic Seroquel XR medicines from November
2016, declined by 33% to $16m. Sales of Seroquel XR in Europe declined by 27%
(32% at CER) to $16m, also reflecting the impact of
generic-medicine competition.
Regional Product Sales
Table 9: Regional Product Sales
|
Q1 2018
|
$m
|
|
% change
|
Actual
|
CER
|
Emerging
Markets17
|
1,765
|
35
|
13
|
8
|
|
China
|
1,025
|
21
|
31
|
22
|
|
Ex. China
|
740
|
15
|
(5)
|
(7)
|
|
|
|
|
|
US
|
1,487
|
30
|
-
|
-
|
|
|
|
|
|
Europe
|
1,121
|
22
|
(1)
|
(12)
|
|
|
|
|
|
Established
ROW
|
612
|
12
|
(8)
|
(12)
|
|
Japan
|
399
|
8
|
(11)
|
(15)
|
|
Canada
|
126
|
3
|
1
|
(4)
|
|
Other Established ROW
|
87
|
2
|
(5)
|
(10)
|
|
|
|
|
|
Total
|
4,985
|
100
|
3
|
(2)
|
Emerging Markets
Product
Sales of $1,765m; an increase of 13% (8% at CER).
China
sales grew by 31% (22% at CER) to $1,025m, representing 58% of
total Emerging Markets sales. Onglyza and Iressa were included on the NRDL in
China in 2017, as were Brilinta, Faslodex and Seroquel XR; the benefits of this
inclusion are anticipated to impact Product Sales favourably in
2018. Crestor also had its
2nd-line usage restriction removed at that time and Zoladex was reclassified from the
hormone and endocrine classification to oncology, which is expected
to continue to support growth. Tagrisso was launched in China in early
2017.
Emerging
Markets sales excluding China, however, declined by 5% (7% at CER)
to $740m in Q1 2018, partly driven by the aforementioned impact
from externalised or divested Product Sales, as well as the decline
in Russia sales of 38% (40% at CER) to $34m that resulted from the
effect of government intervention in the management of healthcare
costs in 2017.
US
Product
Sales of $1,487m;stable.
The
performance reflected successful ongoing Oncology launches,
including Tagrisso and
Imfinzi, plus strong sales
of Farxiga and Brilinta, offset by the impact of
continued competitive intensity on sales of Symbicort, which declined by 28% to
$183m. Unfavourable managed-care pricing and generic-medicine
launches also had adverse effects on overall US sales. Oncology
sales in the US grew by 69% to $426m, primarily driven by
encouraging Tagrisso sales
growth of 63% to $147m.
Europe
Product
Sales of $1,121m; a decline of 1% (12% at CER).
Crestor sales declined by 67% (70% at CER) to $65m,
reflecting the entry of generic medicines in various markets in
2017. Excluding sales of Crestor, Europe sales grew by 13%
(stable at CER) to $1,056m.
The
newer medicines delivered an encouraging performance in the
quarter. Oncology sales in Europe grew by 33% (18% at CER) to
$249m, partly driven by Tagrisso sales growth of 97% (74% at
CER) to $69m. Lynparza
sales of $42m represented growth of 68% (44% at CER). Brilique growth of 32% (15% at CER) to
$86m was accompanied
by Forxiga sales growth of
48% (30% at CER) to $74m.
Established ROW
Product
Sales of $612m;a decline of 8% (12% at CER).
Japan sales declined by 11% (15% at CER) to $399m. The first
generic competitor to Crestor was launched in Japan in Q3 2017 and further
generic competition entered the market in the final quarter.
Crestor
sales in Japan declined by 76% (77% at
CER) to $26m. Excluding sales of Crestor, Japan sales grew by 9% (5% at CER) to
$373m.
As seen in other regions, newer medicines delivered an encouraging
performance in the quarter. Tagrisso sales in Japan increased by 26% (21% at CER) to
$49m due to an increase in demand; sequential quarterly sales
of Tagrisso, however, declined from $61m in Q4 2017, driven
by a decline in T790M ctDNA testing rates from c.90% in Q4 2017 to
c.70% in Q1 2018. This followed the mandated expiry of free ctDNA
testing in 2017, which was concluded after the start of
reimbursement and the fulfilment of the bolus of late-line
patients.
Faslodex sales in Japan were
favourably impacted by a new label in 2017, with sales increasing
by 50% (43% at CER) to $21m.
On 19 January 2018, the Company announced that Lynparza tablets, approved as maintenance treatment for
women with platinum-sensitive relapsed ovarian cancer regardless
of BRCA-mutation status, were approved in Japan and
launched in April 2018. A regulatory decision for
Lynparza
as treatment for breast cancer is
anticipated in the second half of the year.
Biennial
mandated price reductions became effective in Japan from 1 April
2018.
Financial Performance
Table 10: Reported Profit And Loss
|
Reported
|
Q1 2018
|
Q1 2017
|
% change
|
$m
|
$m
|
Actual
|
CER
|
Total
Revenue
|
5,178
|
5,405
|
(4)
|
(9)
|
Product Sales
|
4,985
|
4,843
|
3
|
(2)
|
Externalisation Revenue
|
193
|
562
|
(66)
|
(67)
|
|
|
|
|
|
Cost of
Sales
|
(1,134)
|
(894)
|
27
|
14
|
|
|
|
|
|
Gross
Profit
|
4,044
|
4,511
|
(10)
|
(13)
|
|
77.3%
|
82.3%
|
-5
|
-4
|
|
|
|
|
|
Distribution
Expense
|
(81)
|
(77)
|
6
|
(2)
|
% Total Revenue
|
1.6%
|
1.4%
|
-
|
-
|
R&D
Expense
|
(1,279)
|
(1,453)
|
(12)
|
(16)
|
% Total Revenue
|
24.7%
|
26.9%
|
+2
|
+2
|
SG&A
Expense
|
(2,457)
|
(2,300)
|
7
|
2
|
% Total Revenue
|
47.5%
|
42.6%
|
-5
|
-5
|
Other
Operating Income & Expense
|
469
|
236
|
99
|
97
|
% Total Revenue
|
9.1%
|
4.4%
|
+5
|
+5
|
|
|
|
|
|
Operating
Profit
|
696
|
917
|
(24)
|
(21)
|
% Total Revenue
|
13.4%
|
17.0%
|
-4
|
-2
|
Net
Finance Expense
|
(308)
|
(322)
|
(4)
|
(11)
|
Joint
Ventures and Associates
|
(14)
|
(13)
|
10
|
10
|
Profit
Before Tax
|
374
|
582
|
(36)
|
(27)
|
Taxation
|
(58)
|
(70)
|
|
|
Tax
Rate
|
16%
|
12%
|
|
|
Profit
After Tax
|
316
|
512
|
(38)
|
(30)
|
|
|
|
|
|
Earnings Per
Share
|
$0.27
|
$0.42
|
(37)
|
(29)
|
Table 11: Reconciliation Of Reported Profit Before Tax To
EBITDA19
|
Q1 2018
|
|
$m
|
% change
|
Actual
|
CER
|
Reported Profit
Before Tax
|
374
|
(36)
|
(27)
|
Net
Finance Expense
|
308
|
(4)
|
(11)
|
Joint
Ventures and Associates
|
14
|
10
|
10
|
Depreciation,
Amortisation and Impairment
|
709
|
8
|
3
|
|
|
|
|
EBITDA
|
1,405
|
(11)
|
(10)
|
Table 12: Reconciliation Of Reported To Core Financial
Measures
Q1
2018
|
Reported
|
Restructuring
|
Intangible Asset
Amortisation & Impairments
|
Diabetes Alliance
|
Other20
|
Core21
|
Core
|
% change
|
$m
|
$m
|
$m
|
$m
|
$m
|
$m
|
Actual
|
CER
|
Gross
Profit
|
4,044
|
32
|
45
|
-
|
-
|
4,121
|
(10)
|
(13)
|
Gross Margin22
|
77.3%
|
-
|
-
|
-
|
-
|
78.8%
|
-5
|
-4
|
|
|
|
|
|
|
|
|
|
Distribution
Expense
|
(81)
|
-
|
-
|
-
|
-
|
(81)
|
6
|
(2)
|
R&D
Expense
|
(1,279)
|
27
|
12
|
-
|
-
|
(1,240)
|
(7)
|
(12)
|
SG&A
Expense
|
(2,457)
|
36
|
349
|
107
|
(63)
|
(2,028)
|
11
|
6
|
Other
Operating Income & Expense
|
469
|
-
|
1
|
-
|
(346)
|
124
|
(63)
|
(64)
|
|
|
|
|
|
|
|
|
|
Operating
Profit
|
696
|
95
|
407
|
107
|
(409)
|
896
|
(46)
|
(47)
|
% Total Revenue
|
13.4%
|
-
|
-
|
-
|
-
|
17.3%
|
-14
|
-13
|
|
|
|
|
|
|
|
|
|
Net
Finance Expense
|
(308)
|
-
|
-
|
84
|
53
|
(171)
|
(2)
|
(7)
|
Taxation
|
(58)
|
(20)
|
(80)
|
(41)
|
72
|
(127)
|
(51)
|
(52)
|
|
|
|
|
|
|
|
|
|
Earnings Per
Share
|
$0.27
|
$0.06
|
$0.26
|
$0.11
|
$(0.22)
|
$0.48
|
(51)
|
(51)
|
Profit And Loss Commentary
Gross Profit
Reported
Gross Profit declined by 10% (13% at CER) to $4,044m; Core Gross
Profit declined by 10% (13% at CER) to $4,121m. The declines
reflected the movement in the Gross Margin, as well as the
aforementioned level of Externalisation Revenue.
The
Reported Gross Margin declined by five percentage points (four at
CER) to 77.3%. The Core Gross Margin declined by five percentage
points (four at CER) to 78.8%. The movements were a result of the
favourable impact of manufacturing variances realised in Q1 2017
and the inclusion of the profit share on the aforementioned
collaboration with MSD, as well as the effect of losses of
exclusivity on Crestor
sales in Europe and Japan.
The calculation
of Reported and Core Gross Margin excludes the impact of
Externalisation Revenue, thereby reflecting the underlying
performance of Product Sales.
Operating Expenses
Reported
Operating Expenses were stable (down by 5% at CER) at $3,817m. Core
Operating Expenses increased by 3% (down by 1% at CER) to
$3,349m.
Reported
R&D costs declined by 12% (16% at CER) to $1,279m, with the
Company continuing to focus on resource prioritisation and cost
discipline. Core R&D costs declined by 7% (12% at CER) to
$1,240m, reflecting productivity improvements across every therapy
area and the favourable impact on development costs from the MSD
collaboration. Targeted investment in the Company’s R&D
programme is a consistent priority; the level of activity was
unchanged in the quarter and Core R&D costs represented 24% of
Total Revenue.
Highlights
of the progress made included:
●
Moving
late-stage-execution roles to lower-cost locations
●
Optimising
protocols, including a review of the number of procedures,
countries involved and in-sourcing a larger proportion of clinical
trials
Reported
SG&A costs increased by 7% (2% at CER) to $2,457m. This
reflected investment in medical-affairs capability and capacity in
order to support launches and extensions of the newer medicines,
including Lynparza,
Tagrisso, Imfinzi, Calquence and Fasenra, as well as additional
investment to support sales growth in China.
Core
SG&A costs increased by 11% (6% at CER) to $2,028m, reflecting
the investment in the launches, as well as the significant
reduction in Core SG&A costs in the comparative period. Q1 2017
was a period when the Company delivered its lowest level of Core
SG&A investment for a number of years.
Other Operating Income & Expense
Where
AstraZeneca does not retain a significant ongoing interest in
medicines or potential new medicines, income from divestments is
reported within Other Operating Income & Expense in the
Company’s financial statements. Reported Other Operating
Income & Expense increased by 99% (97% at CER) to $469m and
included:
●
$346m, resulting from a legal
settlement
●
$63m, representing a gain on the
spin-out of six molecules from MedImmune’s early-stage
inflammation and autoimmunity programmes into an independent
biotech company, as announced on 28
February 2018
Core
Other Operating Income & Expense declined by 63% (64% at CER)
to $124m, with the difference to Reported Other Operating Income
& Expense reflecting the aforementioned legal
settlement.
Operating Profit
Reported
Operating Profit declined by 24% (21% at CER) to $696m, driven by
the declines in Total Revenue and the Reported Gross Margin, as
well as the increase in Reported SG&A costs. The Reported
Operating Profit margin declined by four percentage points (two at
CER) to 13% of Total Revenue. Core Operating Profit declined by 46%
(47% at CER) to $896m, driven by the aforementioned factors, as
well as the timing of divestments in FY 2018. The Core Operating
Profit margin declined by 14 percentage points (13 at CER) to 17%
of Total Revenue.
Net Finance Expense
Reported
Net Finance Expense declined by 4% (11% at CER) to $308m,
reflecting reduced levels of discount unwind on the put option over
the non-controlling interest in Acerta Pharma B.V. (Acerta Pharma).
Excluding the discount-unwind on acquisition-related liabilities,
Core Net Finance Expense declined by 2% (7% at CER) to
$171m.
Profit Before Tax
Reported
Profit Before Tax declined by 36% (27% at CER) to $374m, reflecting
the level of Externalisation Revenue, the lower Reported Gross
Margin and the increase in Reported SG&A costs.
Taxation
The Reported and Core tax rates for the quarter were 16% and 18%
respectively. These tax rates were lower than the UK Corporation
Tax Rate of 19%, mainly due to the impact of the geographical mix
of profits. The net cash tax paid was $117m, representing 31% of
Reported Profit Before Tax. The Reported and Core tax rates for the
comparative period were 12% and 17% respectively. The cash tax paid
for the comparative period was $62m, which was 11% of Reported
Profit Before Tax.
Earnings Per Share (EPS)
Reported
EPS of $0.27 represented a decline of 37% (29% at CER). The
performance reflected a decline in Total Revenue, the Reported
Gross Margin and increased Reported SG&A costs. Core EPS
declined by 51% to $0.48, impacted by the aforementioned factors as
well as the decline in Core Other Operating Income &
Expense.
Table 13: Cash Flow
|
Q1 2018
|
Q1 2017
|
Change
|
$m
|
$m
|
$m
|
Reported operating
profit
|
696
|
917
|
(221)
|
Depreciation,
amortisation and impairment
|
709
|
658
|
51
|
|
|
|
|
(Increase)/decrease
in working capital and short-term provisions
|
(993)
|
(887)
|
(106)
|
(Gains)/losses on
disposal of intangible assets
|
(65)
|
(52)
|
(13)
|
Non-cash and other
movements
|
(242)
|
(297)
|
55
|
Interest
paid
|
(128)
|
(189)
|
61
|
Tax
paid
|
(117)
|
(62)
|
(55)
|
|
|
|
|
Net
cash (outflow)/inflow from operating activities
|
(140)
|
88
|
(228)
|
The
Company saw a net cash outflow from operating activities of $140m
in the quarter, compared with an inflow of $88m in Q1 2017. The
increase in the movement of working-capital and short-term
provisions partly reflected launch support for newer
medicines.
Net
cash inflows from investing activities were $273m, compared with
outflows of $146m in Q1 2017. The difference partly reflected the
timing of receipts on disposals of intangible assets, as well as a
reduction in capital expenditure. The cash payment of contingent
consideration in respect of the BMS share of the global Diabetes
alliance amounted to $62m.
Net
cash outflows from financing activities were $663m in the quarter,
compared to $2,042m in Q1 2017, reflecting higher short-term
borrowings in Q1 2018.
Capital Expenditure
Capital
expenditure amounted to $213m in the quarter compared to $286m in
Q1 2017, which included investment in the new global headquarters
in Cambridge, UK, as well as strategic biotech manufacturing
capacity in Sweden.
Table 14: Debt And Capital Structure
|
At 31 March 2018
|
At 31 Dec 2017
|
At 31 March 2017
|
$m
|
$m
|
$m
|
Cash
and cash equivalents
|
3,005
|
3,324
|
3,129
|
Other
investments
|
868
|
1,300
|
548
|
Net
derivatives
|
565
|
504
|
215
|
|
|
|
|
Cash,
short-term investments and derivatives
|
4,438
|
5,128
|
3,892
|
|
|
|
|
Overdrafts and
short-term borrowings
|
(2,776)
|
(845)
|
(1,000)
|
Finance
leases
|
-
|
(5)
|
(80)
|
Current
instalments of loans
|
(1,394)
|
(1,397)
|
(1,762)
|
Loans
due after one year
|
(15,684)
|
(15,560)
|
(14,560)
|
|
|
|
|
Interest-bearing
loans and borrowings (Gross Debt)
|
(19,854)
|
(17,807)
|
(17,402)
|
|
|
|
|
Net
Debt
|
(15,416)
|
(12,679)
|
(13,510)
|
Capital Allocation
The
Board’s aim is to continue to strike a balance between the
interests of the business, financial creditors and the
Company’s shareholders. After providing for investment in the
business, supporting the progressive dividend policy and
maintaining a strong, investment-grade credit rating, the Board
will keep under review potential investment in immediately
earnings-accretive, value-enhancing opportunities.
Foreign Exchange
The
Group’s transactional currency exposures on working-capital
balances, which typically extend for up to three months, are hedged
where practicable using forward foreign-exchange contracts against
the individual Group Companies’ reporting currency. In
addition, the Group’s external dividend payments, paid
principally in pounds sterling and Swedish krona, are fully hedged
from announcement to payment date. Foreign-exchange gains and
losses on forward contracts for transactional hedging are taken to
profit.
Table 15: Currency Sensitivities
The
Company provides the following currency-sensitivity
information:
|
Average Exchange Rates vs. USD
|
|
Annual Impact Of 5% Strengthening in Exchange Rate vs. USD
($m)23
|
Currency
|
Primary Relevance
|
FY 2017
|
Q1 201824
|
% change
|
Product Sales
|
Core Operating Profit
|
EUR
|
Product
Sales
|
0.89
|
0.81
|
+10
|
+136
|
+57
|
JPY
|
Product
Sales
|
112.18
|
106.03
|
+6
|
+96
|
+66
|
CNY
|
Product
Sales
|
6.75
|
6.32
|
+7
|
+180
|
+98
|
SEK
|
Operating
Expenses
|
8.54
|
8.24
|
+4
|
+4
|
-70
|
GBP
|
Operating
Expenses
|
0.78
|
0.72
|
+8
|
+25
|
-75
|
Other25
|
|
|
|
|
+88
|
+44
|
Corporate And Business Development Update
a) MedImmmune Spin-Out - Early-Stage Inflammation And Autoimmunity
Programmes
On 28
February 2018, AstraZeneca announced that its global biologics
research and development arm, MedImmune, would spin out six
molecules from its early-stage inflammation and autoimmunity
programmes into an independent biotech company, Viela Bio. The new
company is focusing on developing medicines for severe autoimmune
diseases, by targeting the underlying causes of each
disease.
MedImmune
contributed three clinical and three pre-clinical potential new
medicines. This included inebilizumab, currently in Phase II trial
development for the treatment of neuromyelitis optica, a rare
condition that affects the optic nerve and spinal cord in
approximately five in 100,000 people. It was granted Orphan Drug
Designation by the US FDA in 2016 and by the EMA in 2017. Viela Bio
is be based in Gaithersburg, Maryland. It was funded with $250m
from a consortium of investors led by Boyu Capital, 6 Dimensions
Capital and Hillhouse Capital. AstraZeneca is the largest
non-controlling shareholder of Viela Bio.
The
Company realised a $63m gain in Q1 2018, reflected in the
Company’s financial statements within Other Operating Income
& Expense.
b) Divestment Of Seroquel
And
Seroquel
XR
On 8 May 2018, AstraZeneca announced that it had entered into an
agreement with Luye Pharma Group, Ltd. (Luye Pharma)
for the sale and licence of the rights
to Seroquel and Seroquel XR
in the UK, China and other
international markets. Seroquel, used primarily to treat the
disorders schizophrenia and bipolar, has lost its compound patent
protection globally; the Seroquel XR formulation patents have also
expired in the vast majority of its markets.
Luye
Pharma will pay $538m in consideration, including $260m immediately
following closure of the transaction. The total consideration,
adjusted for time value, will be recorded in Q2 2018 in Other
Operating Income & Expense within the Company’s financial
statements, subject to the timing of closure of the agreement. This
will include a milestone payable on the successful transition of
certain activities to Luye Pharma. AstraZeneca will continue to
manufacture and supply Seroquel and Seroquel XR to Luye Pharma during a
transition period.
The
transaction is expected to close by the end of Q2 2018, subject to
customary closing conditions and regulatory clearances. In FY 2017, Seroquel generated sales of $85m in the markets covered by this agreement,
while Seroquel XR generated $63m.
Sustainability Update
AstraZeneca’s
sustainability ambition has three priority areas, aligned with the
Company’s purpose and business strategy:
●
Environmental
Protection
●
Ethics and
Transparency
These
priorities were determined, along with a set of nine foundational
areas, through a materiality assessment with external and internal
stakeholders, respectively. Combined, they ensure the maximum
benefit to patients, the Company, broader society and the planet.
Progress against the three priorities is reported
below:
a) Access To Healthcare
Healthy
Heart Africa (HHA) is an innovative programme committed to tackling
hypertension and the increasing burden of CV disease across Africa.
In Q1 2018, the programme was ahead of its target for
blood-pressure screenings. Since launching in Kenya 2014 and in
Ethiopia 2016 respectively, HHA has conducted more than 5.5m
blood-pressure screenings.
The
AstraZeneca Young Health Programme (YHP) is a non-communicable
disease (NCD) prevention programme, developed in partnership with
John Hopkins Bloomberg School of Public Health and Plan
International in the US that has reached 2.25m young patients since
its launch in 2010. It aims to reduce the uptake of unhealthy
behaviours in young patients to improve their health outcomes as
adults and help address the growing burden of NCDs on health
systems. During the period, AstraZeneca launched several new
three-year programmes:
●
YHP Brazil, which
aims to reach more than 740,000 direct and indirect
beneficiaries
●
YHP Serbia, which
aims to reach 200,000 school children with advocacy and educational
programming on tobacco use
●
YHP Australia,
which aims to provide food and nutrition education to 10 secondary
schools in Victoria and New South Wales
Additionally,
YHP health camps in India, in partnership with Plan International,
delivered engaged employee volunteers and provided screening for
diabetes, hypertension, anaemia and respiratory disorders to more
than 1,000 patients from marginalised communities in Bangalore,
India.
During
the period, YHP was selected by Global Child Forum, a Swedish
not-for-profit foundation, as the subject of a ‘Deep
Dive’. Global Child Forum is focused on the advancement of
children’s rights, in accordance with the UN Convention on
the Rights of the Child. Its aim is to provide businesses with an
understanding of how and where their business may impact children.
On 11 April 2018, AstraZeneca presented a YHP case study at the
10th Global Child Forum at the Stockholm Royal Palace, Sweden; this
was subsequently followed by the publication of the YHP Deep
Dive.
b) Environmental Protection
AstraZeneca
is committed to managing its environmental impact across all
business activities, with a focus on Greenhouse Gas (GHG)
emissions, energy consumption, waste production and water use. The
Company’s approach focuses on science-based targets, mapped
to each of the environmental strategic priorities:
●
Reducing GHG
emissions to combat climate change
●
Protecting natural
resources through energy, waste and water management
●
Leading the way to
minimise Pharmaceuticals in the Environment
●
Preserving
biodiversity
During
the period, the Company received recognition from The Climate
Group, an international non-profit organisation, focused on
accelerating climate action for its increase in renewable energy
usage. AstraZeneca was identified as ‘Biggest Achiever’
for its 300% increase in renewable electricity in a single year. In
addition, AstraZeneca was also commended for its use of renewable
energy, as one of 122 multinational businesses which have made the
RE100 commitment, a collaborative, global initiative uniting
influential businesses that are committed to 100% renewable
electricity.
In
Cambridge, UK, the new R&D centre and global headquarters
achieved an ‘Excellent’ rating from the world-leading
Building Research Establishment Environmental Assessment
Methodology (BREEAM) assessment; AstraZeneca also received a credit
for innovation. BREEAM assesses a building’s environmental,
social and economic sustainability performance. AstraZeneca’s
rating status reflected best practice in a number of areas and the
Company’s accreditation recognised the efforts to ensure the
new site becomes an environment that will not only enhance staff
well-being, but also help protect natural resources.
c) Ethics And Transparency
During
the period, the Third Party Risk Management process, designed to
ensure that AstraZeneca can identify and manage risks associated
with third-party activities as early and effectively as possible,
increased coverage to 79%. In February 2018, a new Counterfeit
Medicines Partnership with Chinese company Tencent Holdings Limited
was established. The programme involved the development of online
tracking systems to fight counterfeit medicines, a particular
challenge in China. The Company also implemented an organisational
change to bring the functions of Global Compliance, Safety, Health
and Environment and the Sustainability Strategy and Engagement team
under a new umbrella function called Global Sustainability. The
changes signal AstraZeneca’s commitment to
sustainability.
Other Developments
During
the period, AstraZeneca was recognised for its commitment to
sustainability with two new external accolades. The Company was
listed as one of the 100 most sustainable companies in the world by
Corporate Knights, the Toronto-based media and investment advisory
firm. During the period, AstraZeneca also received certification
from the Top Employers Institute, in recognition of excellent
People Management and HR processes across several European markets.
The Institute assessed leadership, corporate & social
responsibility commitments and how the Company delivers on its
commitment to colleague diversity.
On 6
March 2018, the Company published its annual Sustainability Report
2017, which shares the results of AstraZeneca’s efforts in
the aforementioned priority areas. The report highlighted examples
of employee sustainability projects contributing to the
Company’s global goals.
On 20
March 2018, AstraZeneca published its first gender pay-gap report,
providing gender-pay information on the Company in the UK and
outlining the Company’s support for women, as well as its
focus on diversity and inclusion. AstraZeneca reported a median gap
in hourly pay of 13.5%, compared to an overall UK median gap of
18.4%. The reporting of the gender pay gap is an annual requirement
for all companies in the UK with 250 or more
employees.
During
the period, the Company commenced a robust programme of training
for key areas of the organisation that are responsible for data
privacy in preparation for the General Data Protection Regulation
(GDPR). GDPR is a new EU regulation, taking effect from 25 May
2018, giving EU and European Economic Area (EEA) citizens and
residents better control of their personal data, with one set of
data protection rules applicable to all organisations that hold
personal data relating to EU/EEA citizens and
residents.
Research And Development Update
A
comprehensive data pack comprising AstraZeneca’s pipeline of
medicines in human trials can be found in the clinical-trials
appendix available on astrazeneca.com.
Highlights of developments in the Company’s late-stage
pipeline since the prior results announcement are shown
below:
Table 16: Update From The Late-Stage Pipeline
Regulatory
Approvals
|
4
|
- Lynparza - ovarian cancer (2nd line;
tablets) (EU)
- Tagrisso - lung cancer (1st line)
(US)
- Imfinzi - lung cancer (Stage III)
(US)
- Lokelma - hyperkalaemia
(EU)
|
Regulatory
Submissions and/or Acceptances
|
3
|
- Lynparza - breast cancer
(EU)
- moxetumomab
pasudotox - hairy cell leukaemia (3rd line) (US)
- Farxiga - type-1 diabetes
(EU)
|
Major
Phase III
Data
Readouts or Other Major Developments
|
5
|
- Tagrisso - lung cancer (1st line) -
priority review status (JP)
- Imfinzi + tremelimumab - lung cancer
(3rd line) (ARCTIC trial) - did not meet primary endpoints in
PDL1-low/neg. patients
- moxetumomab
pasudotox - hairy cell leukaemia (3rd line) - Priority Review
(US)
- selumetinib - NF1 -
Orphan Drug Designation (US)
- Fasenra - COPD (GALATHEA trial) - did
not meet primary endpoint
|
New
Molecular Entitiesand Major Lifecycle Medicines in Phase III Trials
or Under Regulatory Review
|
15
|
Oncology
- Lynparza - multiple cancers26
- Tagrisso - lung cancer26
- Imfinzi - multiple cancers26
- Calquence - blood cancers
- moxetumomab
pasudotox - leukaemia26
- tremelimumab -
multiple cancers
- selumetinib -
thyroid cancer
- savolitinib -
kidney cancer
CVRM
- Lokelma - hyperkalaemia26
- roxadustat -
anaemia26
Respiratory
- Fasenra - COPD
- PT010 - COPD,
asthma
- tezepelumab -
severe, uncontrolled asthma
Other
- anifrolumab -
lupus
- lanabecestat -
Alzheimer’s disease
|
Total
Projects in Clinical Pipeline
|
130
|
|
ONCOLOGY
AstraZeneca
has a deep-rooted heritage in Oncology and offers a new generation
of medicines that have the potential to transform patients’
lives and the Company’s future. At least six Oncology
medicines are expected to be launched between 2014 and 2020, of
which Lynparza,
Tagrisso, Imfinzi and Calquence are already benefitting
patients. An extensive pipeline of small-molecule and biologic
medicines is in development and the Company is committed to
advancing Oncology, primarily focused on the treatment of lung,
ovarian, breast and blood cancers.
In
April 2018, at the American Association for Cancer Research annual
meeting, the Company presented data from the portfolios of DNA
Damage Response (DDR), Immuno-Oncology (IO) and Tumour Drivers
& Resistance.
The
Company presented data on its expanded portfolio of potential
medicines that exploit DDR dependencies to selectively kill cancer
cells across multiple tumour types. The Company reported
Lynparza OS data from the
pivotal OlympiAD trial in BRCA-mutated, metastatic breast cancer.
Data exploring the clinical properties of Lynparza and four other PARP inhibitors
were also presented to illustrate clinical efficacy and safety
profiles. Data on AZD6738, an Ataxia Telangiectasia and
Rad3-related (ATR) inhibitor and AZD0156, an Ataxia Telangiectasia
Mutated (ATM) inhibitor, were also presented.
The
Company also presented data and shared
new insights into the science of Imfinzi, including IO-IO combination data from Study 006 in
2nd-line NSCLC and Study 10 in 2nd-line bladder cancer.
Beyond Imfinzi, the Company presented data on a novel
bi-specific antibody, MEDI5752, designed to target dual checkpoints
on immune cells and use the potential synergies of combined
mechanisms in immunotherapy.
Finally,
the Company presented data on AZD4573, a cyclin-dependent kinase 9
(CDK9) inhibitor, which demonstrated rapid cell-death induction in
haematological-tumour models through depletion of myeloid leukemia
cell differentiation protein Mcl-1. Furthermore, early monotherapy
and combination data on the novel extracellular signal-regulated
kinase inhibitor
AZD0364 showed effects on
KRAS-mutated tumours, when used in combination with
selumetinib.
a) Lynparza
(multiple
cancers)
On 8
May 2018, the Company announced that the EMA had approved Lynparza tablets (300mg twice daily) for use as a
maintenance therapy for patients with platinum-sensitive relapsed high-grade, epithelial
ovarian, fallopian tube, or primary peritoneal cancer who are in
complete response or partial response to platinum-based
chemotherapy, regardless of BRCA status. The approval was based on two
randomised trials, SOLO-2 and Study 19, which showed
that Lynparza reduced the risk of
disease progression or death for platinum-sensitive, relapsed
patients, compared to placebo.
On 3 April 2018, the Company announced that the EMA had
validated for review the Marketing Authorisation
Application (MAA) for Lynparza for use as a treatment of patients with
deleterious or suspected deleterious BRCA-mutated, HER2-negative, metastatic breast cancer,
who have been previously treated with chemotherapy in the
neoadjuvant, adjuvant or metastatic setting.
At the
Society for Gynecological Oncology (SGO) annual meeting in New
Orleans, US in March 2018, ovarian-cancer cohort data from the
Lynparza + Imfinzi trial, MEDIOLA, was presented,
showing promising efficacy and a favourable side-effect profile for
the combination of Lynparza
+ Imfinzi in
platinum-sensitive, recurrent (PSR) ovarian-cancer patients. The
objective response rate was particularly high among patients who
had received one prior line of chemotherapy (77%).
Table 17: Key Lynparza
Combination Trials
Name
|
Phase
|
Population
|
Design
|
Timelines
|
Status
|
PAOLA-127
|
III
|
Stage
IV, 1st-line ovarian cancer
|
Lynparza maintenance + bevacizumab vs.
bevacizumab
maintenance
|
FPCD28
Q2 2015
First
data anticipated 2019
|
Recruitment
ongoing
|
DuO-O
|
III
|
Stage
IV, 1st-line ovarian cancer
|
Lynparza + Imfinzi
|
-
|
Planning(announced
at the aforementioned SGO meeting)
|
MEDIOLA
|
I/II
|
Advanced,
2nd-line gBRCA-mutated
ovarian cancer
Stage
IV, 1st to 3rd-line gBRCA-mutated, HER2-negative breast
cancer
Stage
IV, 2nd-line small cell lung cancer (SCLC)
Stage
IV, 2nd-line gastric cancer
|
Lynparza + Imfinzi
|
FPCD Q2
2016
|
Recruitment
ongoingInitial data from lung, breast, prostate and ovarian-cancer
cohorts presented in 2017 and 2018
|
VIOLETTE
|
II
|
Stage
IV, advanced, triple-negative breast cancer:
-HRRm
(Non-BRCA)
-Non-HRRm
|
Lynparza + ATR (AZD6738)
Lynparza + Wee1 (AZD1775)
Lynparza
|
FPCD Q4
2017
|
Recruitment
ongoing
|
Study
8
|
II
|
Stage
IV, advanced, castration-resistant prostate cancer
|
Lynparza + abiraterone vs. abiraterone
|
FPCD Q3
2014
|
Data to
be presented at American Society Of Clinical Oncology annual
meeting in June 2018
|
BAYOU
|
II
|
Stage
IV, 1st line cis-platinum chemotherapy-ineligible urothelial
bladder cancer
|
Lynparza + Imfinzi
vs. Imfinzi
|
FPCD Q1
2018
|
Recruitment
ongoing
|
b) Tagrisso
(lung
cancer)
On 18 April 2018, AstraZeneca announced that the US FDA had
approved Tagrisso as a 1st-line treatment for patients with
metastatic NSCLC whose tumours have EGFR mutations, as detected by
an approved test. The approval was based on results from the
1st-line NSLCLC Phase III FLAURA
trial, which showed that patients’ progression-free
survival (PFS) nearly doubled when treated with Tagrisso, compared to patients treated
with current standard of care (SoC) EGFR - tyrosine kinase
inhibitors (TKIs). Prior to
this, Tagrisso
received its first regulatory approval as a 1st-line treatment for
patients with metastatic EGFR-mutated NSCLC in Brazil.
On 27
April 2018, AstraZeneca announced that the CHMP had adopted a
positive opinion, recommending a change to the terms of the MAA for
Tagrisso to include the
1st-line treatment of adult patients with locally-advanced or
metastatic NSCLC with EGFR mutations. A regulatory decision by the
EMA is anticipated in Q2 2018, vs. the prior expectation of H2
2018.
On 5
February 2018, the Company announced that Tagrisso was granted priority
review status, based on the results from the FLAURA trial, by the
Ministry of Health, Labor and Welfare in Japan. In March
2016, Tagrisso was approved in Japan for
the treatment of EGFR-TKI resistant, EGFR T790M mutation-positive
inoperable or relapsed NSCLC. A supplementary new drug application
was submitted in November 2017 to expand indications to
include 1st-line treatment of EGFR mutation-positive NSCLC
patients, regardless of the presence of a T790M
mutation.
c) Imfinzi
(lung and other
cancers)
The
Company continues to advance multiple monotherapy trials of
Imfinzi and combination
trials of Imfinzi with
tremelimumab and other potential new medicines:
Lung Cancer
During
the period, the Company announced that the US FDA had approved
Imfinzi for the treatment
of patients with unresectable, Stage III NSCLC whose disease had
not progressed following concurrent platinum-based CRT; this was
the second indication approved for Imfinzi. CRT, followed by monitoring
for disease progression, has been the SoC in this setting for over
two decades and multiple trials have failed to improve upon this.
The approval of Imfinzi was
based on positive PFS data from the Phase III PACIFIC trial, in
which Imfinzi demonstrated
an improvement in median PFS of 11.2 months compared to placebo,
representing a 48% reduction in relative risk of progression or
death vs. placebo in all patients, regardless of PD-L1
status.
In May
2018, Health Canada also approved Imfinzi for the treatment of patients
with unresectable, Stage III NSCLC whose disease has not progressed
following concurrent platinum-based chemotherapy and radiation
therapy. The approval was granted under Health Canada’s
accelerated approval framework and was the second global approval
for Imfinzi for the
treatment of unresectable, Stage III NSCLC. Regulatory submissions,
based on the PACIFIC-trial data, are currently under review in both
the EU and Japan, where the Company anticipates regulatory
decisions in H2 2018. The PACIFIC trial is ongoing, evaluating OS
in unresectable, Stage III NSCLC, with data availability
anticipated in 2019.
The
Company recently announced an updated timeline for the final
analysis of the Phase III MYSTIC trial of Imfinzi as a potential monotherapy and
in combination with tremelimumab, vs. platinum-based SoC
chemotherapy in previously-untreated patients with metastatic
(Stage IV), 1st-line NSCLC. An increased number of events, required
for the OS analysis, means that final OS data is now expected to be
available in the second half of 2018, vs. the prior expectation of
H1 2018.
During
the period, the Company also reassessed timelines for the final
analysis of data from the Phase III NEPTUNE trial of Imfinzi in combination with
tremelimumab, versus platinum-based, SoC chemotherapy in
previously-untreated patients with metastatic (Stage IV) 1st-line
NSCLC. The trial is now expected to achieve an increased number of
required events for OS analysis to be available in 2019, vs. the
prior expectation of H2 2018. As previously communicated, the
Company has the flexibility to include novel biomarkers in the
NEPTUNE statistical-analysis plan.
Continued
emerging scientific evidence supports the use of OS over PFS as the
key, relevant primary endpoint, to characterise correctly the
clinical benefit of IO medicines. Accordingly, the Company recently
amended trials in the 1st-line NSCLC setting to increase the
emphasis on and robustness of OS as a primary endpoint, including
the Phase III PEARL trial (Imfinzi monotherapy), which will now
focus the primary-efficacy analysis on OS, rather than
PFS.
In the
Stage IV, 3rd-line setting, the Company recently reported data from
the Phase III ARCTIC trial in patients with locally-advanced or
metastatic NSCLC, who have received at least two prior treatments.
This randomised, open-label, multi-centre trial assessed the
efficacy and safety of the combination of Imfinzi plus tremelimumab, as well as
Imfinzi and tremelimumab
monotherapies, versus SoC chemotherapy in patients with
PDL1-low/negative NSCLC (sub-study B) and Imfinzi monotherapy versus SoC in
patients with PDL1-high NSCLC (sub-study A). In sub-study B, the
combination of Imfinzi plus
tremelimumab in patients with PD-L1 low/negative NSCLC did not meet
the primary endpoints of a statistically-significant and
clinically-meaningful improvement in PFS and OS, compared to SoC.
Activity and safety data from other arms within sub-study B were
consistent with prior published data. Sub-study A was not powered
for statistical significance;Imfinzi monotherapy, however, showed a
clinically-meaningful reduction in the risk of death, compared to
chemotherapy. Full data from the ARCTIC trial will be presented at
a forthcoming medical meeting.
Table 18: Ongoing Key IO Lung Cancer Late-Stage Trials
Name
|
Phase
|
Population
|
Design
|
Timelines
|
Status
|
Monotherapy
|
ADJUVANT
(BR 31)31
|
III
|
Stage
Ib-IIIa NSCLC
|
Imfinzi vs. placebo
|
FPCD Q1
2015
First
data anticipated 2020
|
Recruitment
ongoing
|
PACIFIC
|
III
|
Unresectable,
Stage III NSCLC
|
Imfinzi vs. placebo
|
FPCD Q2
2014
LPCD Q2
2016
Final
OS data anticipated 2019
|
Recruitment
completed
PFS
primary endpoint met
|
PACIFIC-2
|
III
|
Unresectable,
Stage III NSCLC
|
Concurrent
chemoradiation +/- Imfinzi
|
FPCD Q2
2018
First
data anticipated 2021
|
Recruitment
ongoing
|
PEARL
|
III
|
Stage
IV, 1st line NSCLC (Asia)
|
Imfinzi vs. SoC chemotherapy
|
FPCD Q1
2017
First
data anticipated 2020
|
Recruitment
ongoing
|
Combination therapy
|
MYSTIC
|
III
|
Stage
IV, 1st line NSCLC
|
Imfinzi, Imfinzi +
treme vs. SoC chemotherapy
|
FPCD Q3
2015
LPCD Q3
2016
Final
OS data anticipated H2 2018
|
Recruitment
completed
PFS
primary endpoint not met
|
NEPTUNE
|
III
|
Stage
IV, 1st line NSCLC
|
Imfinzi + treme vs. SoC chemotherapy
|
FPCD Q4
2015
LPCD Q2
2017
First
data anticipated 2019
|
Recruitment
completed
|
POSEIDON
|
III
|
Stage
IV, 1st line NSCLC
|
Imfinzi + SoC, Imfinzi + treme + SoC vs. SoC
chemotherapy
|
FPCD Q2
2017
First
data anticipated 2019
|
Recruitment
ongoing
|
CASPIAN
|
III
|
Stage
IV, 1st line small-cell lung cancer
|
Imfinzi + SoC, Imfinzi + treme + SoC vs. SoC
chemotherapy
|
FPCD Q1
2017
First
data anticipated 2019
|
Recruitment
ongoing
|
Other Cancers
During
the period, the Pharmaceutical Administration, the Medical Devices
Department and the Food & Nutrition Services of the Israel
Ministry of Health authority granted approval to Imfinzi as a treatment for patients
with locally-advanced or metastatic bladder cancer who have
suffered disease progression during or following
platinum-containing chemotherapy or who have suffered disease
progression within 12 months of neoadjuvant or adjuvant treatment
with platinum-containing chemotherapy. Imfinzi’s approval, based on
Phase Ib/II clinical-trial data, was received only 10 months after
submission, reflecting the importance of a new treatment option for
patients and compelling clinical data. Along with the approval in
Israel, Imfinzi is now
approved as a 2nd-line treatment for bladder cancer in the US,
Canada and Brazil, with a review ongoing in Australia.
During
the period, the Company amended the Phase III KESTREL trial by
focusing the primary-efficacy analysis on OS only, as the primary
endpoint. Accordingly, and based on current predictions, the first
data are now expected to be available in H2 2018, vs. the prior
expectation of H1 2018. Similarly, the timeline for the
availability of the first data anticipated for the Phase III EAGLE
trial recently moved to H2 2018 vs. the prior expectation of H1
2018.
Table 19: Key IO Non-Lung Cancer Late-Stage Trials
Name
|
Phase
|
Population
|
Design
|
Timelines
|
Status
|
DANUBE
|
III
|
Stage
IV, 1st line cisplatin chemotherapy- eligible/
ineligible
bladder cancer
|
Imfinzi, Imfinzi +
treme vs. SoC chemotherapy
|
FPCD Q4
2015
LPCD Q1
2017
First
data anticipated 2019
|
Recruitment
completed
|
KESTREL
|
III
|
Stage
IV, 1st line head and neck squamous cell carcinoma (HNSCC, head and
neck cancer)
|
Imfinzi, Imfinzi +
treme vs. SoC
|
FPCD Q4
2015
LPCD Q1
2017
First
data anticipated H2 2018
|
Recruitment
completed
|
EAGLE
|
III
|
Stage
IV, 2nd-line HNSCC
|
Imfinzi, Imfinzi +
treme vs. SoC
|
FPCD Q4
2015
LPCD Q3
2017
First
data anticipated H2 2018
|
Recruitment
completed
|
HIMALAYA
|
III
|
Stage
IV, 1st line hepatocellular carcinoma (HCC, liver
cancer)
|
Imfinzi, Imfinzi +
treme (two dosing regimens) vs. sorafenib
|
FPCD Q4
2017
First
data anticipated 2020
|
Recruitment
ongoing
|
d) Calquence
On 13
February 2018, the NCCN added Calquence as a category-2A recommended
treatment for relapsed / refractory CLL / small lymphocytic
lymphoma.
e) Moxetumomab Pasudotox
On 3
April 2018, the Company announced that the US FDA had accepted the
Biologics License Application (BLA) for moxetumomab pasudotox, an
investigational anti-CD22 recombinant immunotoxin and potential new
medicine for the treatment of adult patients with hairy cell
leukaemia who have received at least two prior lines of therapy.
The US FDA granted the moxetumomab pasudotox BLA Priority Review
status, with a Prescription Drug User Fee Act action date in the
third quarter of 2018.
f) Selumetinib
On 15
February 2018, the Company announced that the US FDA had granted
Orphan Drug Designation for selumetinib, a MEK 1/2 inhibitor, for
the treatment of NF1. This is an incurable genetic condition that
affects one in 3,000 births, with highly-variable symptoms,
including skin, neurological and skeletal manifestations. It can
cause secondary complications, including learning difficulties,
visual impairment, pain, disfigurement, twisting and curvature of
the spine, high blood pressure and epilepsy. NF1 is a devastating
condition that can lead to life-threatening complications. There is
no known cure for NF1 and there are limited treatment options to
manage symptoms.
Selumetinib
is being investigated by the US National Cancer Institute in a
Phase I/II trial, SPRINT, in paediatric patients with symptomatic,
NF1-related Plexiform neurofibromas; data is anticipated in Q2
2018.
CVRM
CV,
renal and metabolic diseases are key areas of focus as the Company
sets the challenge to better understand how its portfolio of
medicines might be used to help address multiple risk factors or
co-morbidities. Today, AstraZeneca is delivering life-changing
results in the main CV-disease areas and their complications. The
Company is investing in science to demonstrate CV and mortality
benefits, by slowing the underlying progression of CV-related
diseases and protecting the organs of the CV system. Ultimately,
AstraZeneca is looking to do more than just slow CV-related
disease, by modifying or even halting the natural course of the
disease itself and regenerate organs. The net result is a strong,
continued commitment to new CVRM-treatment options that have the
potential to deliver improved outcomes to hundreds of millions of
patients.
a) Brilinta
(CV
disease)
AstraZeneca
presented results of a new analysis of the PLATO (A Study of
PLATelet Inhibition and Patient Outcomes) trial at the ACC
(American College of Cardiology) meeting in Orlando, US in March
2018, showing that there were fewer deaths in patients suffering
from ACS who were treated with Brilinta within seven days prior to
having heart bypass surgery (coronary artery bypass graft),
compared to those treated with clopidogrel. For patients treated
with Brilinta, total
mortality was reduced by 51% and CV death was reduced by 48%, in
comparison to patients treated with clopidogrel.
At the
meeting, the Company also announced initial results from TREAT
(Ticagrelor in Patients With ST Elevation Myocardial Infarction
(STEMI) Treated With Pharmacological Thrombolysis), a Phase III,
investigator-initiated and academically-led trial, financially
supported by AstraZeneca, investigating the safety of Brilinta 90mg compared to clopidogrel
75mg for heart-attack patients treated with pharmacological
thrombolysis. The trial demonstrated comparable safety
profiles in thrombolysed STEMI patients, as measured by major
bleeding at 30 days, between Brilinta and clopidogrel (P<0.001
for non-inferiority). Rates of major CV events were similar between
Brilinta and clopidogrel at
30 days, although due to the low number of events, statistical
power to assess superiority was limited. Further assessment of
safety and efficacy data is planned at 12 months.
In
February 2018, new data was published in the Journal of the American College of
Cardiology. The new data suggested that treatment with
Brilinta 60mg significantly
reduces the risk of a major adverse cardiac event (MACE) by 19% and
coronary death by 36%, in patients who have survived a heart attack
and are living with multi-vessel-disease (MVD). The findings from
this pre-specified sub-analysis of the PEGASUS-TIMI 54 trial
suggested that this high-risk population may benefit from extended,
preventative anti-platelet therapy beyond the initial 12-month,
post-event period. This sub-analysis also highlighted the increased
risk of cardiac events among patients with MVD who have already
experienced a heart attack.
b) Farxiga
(diabetes)
AstraZeneca
presented results of its CVD-REAL 2 study at the aforementioned ACC
meeting. This new analysis assessed data from more than 400,000
patients, 74% of whom did not have a history of established CV
disease. Results showed that, across this broad population of
patients with type-2 diabetes, treatment with an SGLT2 inhibitor
(Farxiga, empagliflozin,
ipragliflozin, canagliflozin, tofogliflozin or luseogliflozin) was
associated with a 49% lower risk of acute coronary death (ACD), 36%
lower risk of hospitalisation for heart failure (hHF), 19% lower
risk of MI and 32% lower risk of stroke (P≤0.001 for all),
compared to other type-2 diabetes medicines. There was also a 40%
lower risk of the composite endpoint of hHF or ACD
(P<0.001). This data was consistent with the data from
CVD-REAL study presented at the American Diabetes Association
annual meeting in 2017.
During
the period, the Company announced submission acceptance from the
EMA for Forxiga for use as
an oral adjunct treatment to insulin in adults with type-1
diabetes. The submission acceptance was based on Phase III data
from the DEPICT (Dapagliflozin Evaluation in Patients
with Inadequately Controlled Type 1 diabetes)
clinical programme. The safety profile of Forxiga in the DEPICT clinical
programme to date was consistent with its established profile in
type-2 diabetes, with the exception of a higher number of diabetic
ketoacidosis (DKA) events in dapagliflozin-treated patients vs.
placebo in these type-1 diabetes trials. DKA is a known
complication for patients with diabetes that affects those with
type-1 diabetes more frequently than those with type-2
diabetes.
c) Bydureon
(type-2
diabetes)
On 3 April 2018, AstraZeneca announced that the US FDA had
approved Bydureon for injectable suspension as an add-on therapy to
basal insulin in adults with type-2 diabetes with inadequate
glycemic control. The approval was based on the DURATION-7 trial
showing significant HbA1c reduction when Bydureon was added to insulin glargine therapy vs. insulin
glargine alone.
During
the period, the Company received EMA acceptance for Bydureon, based on the CV outcome
trial, EXSCEL. This Phase IIIb/IV trial (EXenatide Study
of Cardiovascular Event Lowering) compared the
effect of once-weekly Bydureon (exenatide
extended-release) vs. placebo, when added to usual type-2 diabetes
treatments, on the risk of a MACE, a composite endpoint of CV
death, non-fatal myocardial infarction (MI) or non-fatal stroke, in
adults with type-2 diabetes at a wide range of CV risk. The trial
met its primary safety objective of non-inferiority for MACE. Fewer
CV events were observed in the Bydureon arm of the trial; the
efficacy objective of a superior reduction in MACE, however, did
not reach statistical significance.
d) Lokelma
(hyperkalaemia)
On 22
March 2018, AstraZeneca announced that the EMA had granted the
marketing authorisation for Lokelma (formerly ZS-9, sodium
zirconium cyclosilicate) for the treatment of adults with
hyperkalaemia.
During
the period, the Company also completed enrolment in the Phase III
HARMONIZE global trial. The trial was designed, alongside other
country specific trials, to evaluate the safety and efficacy of
Lokelma in patients with
hyperkalaemia in Japan, South Korea, Russia and Taiwan. It will,
along with other trials, support the registration of Lokelma in these
countries.
e) Roxadustat (anaemia)
During
the period, the Company and its partner FibroGen Inc. (Fibrogen)
announced an update to roxadustat’s Phase III programme. Data
is now anticipated in H2 2018, vs. the prior expectation of H1
2018;a US regulatory submission is anticipated in 2019, vs. the
prior expectation of H2 2018.
In
China, roxadustat was granted priority review by China FDA and the
Company continues to anticipate a regulatory decision in H2 2018.
If approved, roxadustat will be a first-in-class medicine, with
China being the first approval country.
Under
the terms of the agreement, Fibrogen and AstraZeneca will develop
and commercialise roxadustat in the US, China and all major markets
excluding Japan, Europe, the Commonwealth of Independent States,
the Middle East and South Africa, which are covered by an existing
agreement between Fibrogen and Astellas Pharma Inc.
In February 2018, the first patient was dosed in
the roxadustat 082 MDS trial; the purpose of the trial
is to determine whether roxadustat is safe and effective in the
treatment of anaemia in patients with lower-risk
myelodysplastic syndrome and low red blood-cell transfusion burden.
This is the first trial in the lifecycle management programme for
roxadustat.
Table 20: Major Ongoing Cardiovascular Outcomes Trials
Major
ongoing outcomes trials for patients in CVRM are highlighted in the
following table:
Medicine
|
Trial
|
Mechanism
|
Population
|
Primary Endpoint
|
Timeline
|
Farxiga
|
DECLARE
|
SGLT2
inhibitor
|
c.17,00032
patients with type-2 diabetes
|
Time to
first occurrence of CV death, non-fatal MI or non-fatal
stroke
|
Data
anticipated H2 2018 (final analysis)
|
Farxiga
|
DAPA-HF
|
SGLT2
inhibitor
|
c.4,500
patients with HF33
|
Time to
first occurrence of CV death or hHF or an urgent HF
visit
|
FPCD
Q1
2017Data anticipated 2019
|
Farxiga
|
DAPA-CKD
|
SGLT2
inhibitor
|
c.4,000
patients with CKD34
|
Time to
first occurrence of ≥50% sustained decline in
eGFR35 or reaching ESRD36 or CV death or renal death
|
FPCD
Q1
2017Data anticipated 2020
|
Brilinta
|
THEMIS
|
P2Y12
receptor antagonist
|
c.19,000
patients with type-2 diabetes
and
CAD
without
a history of
MI or
stroke
|
Composite
of
CV
death, non-fatal MI
and
non-fatal stroke
|
Data
anticipated 2019
|
Brilinta
|
THALES
|
P2Y12
receptor antagonist
|
c.13,000
patients with acute ischaemic stroke or transient ischaemic
attack
|
Prevention
of the composite of subsequent stroke and death at 30
days
|
Data
anticipated 2020
|
Epanova
|
STRENGTH
|
Omega-3
carboxylic acids
|
c.13,000
patients with mixed dyslipidaemia
|
Time to
first occurrence of CV death, non-fatal MI or non-fatal
stroke
|
Data
anticipated 2019
|
RESPIRATORY
AstraZeneca’s
Respiratory focus is aimed at transforming the treatment of asthma
and COPD through combined inhaled therapies, biologics for the
unmet medical needs of specific patient populations and an early
pipeline focused on disease modification.
The
growing range of medicines includes up to four anticipated launches
between 2017 and 2020; of these, Bevespi and Fasenra are already benefitting
patients. The capability in inhalation technology spans both
pressurised, metered-dose inhalers and dry-powder inhalers to serve
patient needs, as well as the innovative Aerosphere Delivery Technology, a focus
of AstraZeneca’s future-platform development for
respiratory-disease combination therapies.
a) Symbicort
(asthma)
On 17 May 2018, positive results from the Phase III SYGMA trials
of Symbicort Turbuhaler
were published in the
New England
Journal of Medicine; they will
be presented on 20 May 2018 at the American Thoracic Society
International Congress. The trials were designed to evaluate
efficacy of Symbicort
Turbuhaler, taken only as
needed, as an anti-inflammatory reliever vs. SoC medicines for mild
asthma. In November 2017, the Company announced that both trials
had met their individual primary efficacy
outcomes.
In March 2018, the China FDA approved Symbicort Turbuhaler as a maintenance and reliever therapy, designed
for the treatment of asthma in adolescent patients (12-17 years) in
China.
b) Daxas
(COPD)
In
April 2018, the EMA announced approval of a 250mcg tablet for
Daxas to be used as a
starting-dose treatment for the first four weeks, followed by an
increase to the maintenance dosage of 500mcg. Daxas is indicated for maintenance
treatment of severe COPD associated with chronic bronchitis in
adult patients with a history of frequent exacerbations, as add-on
to bronchodilator treatment.
c) Bevespi
(COPD)
In
March 2018, Health Canada granted approval for Bevespi Aerosphere as a long-term
treatment for adults with COPD. Canada was the second market, after
the US, to approve Bevespi
Aerosphere.
d) Fasenra
(severe, uncontrolled
asthma and COPD)
On 11 May 2018, AstraZeneca announced that the GALATHEA Phase III
trial did not met its primary endpoint of a
statistically-significant reduction of exacerbations in patients
with COPD. The trial assessed the safety and efficacy of
Fasenra, as an add-on treatment to dual or triple inhaled
therapy compared to placebo for patients with moderate to very
severe COPD with a history of exacerbations across a range of
baseline blood eosinophils. The safety and tolerability findings in
GALATHEA were consistent with those previously observed in trials
with Fasenra and the results do not impact the approved
indication in severe eosinophilic asthma. The second Phase III trial, TERRANOVA, is ongoing
and the Company anticipates results in Q2 2018. Following the
top-line results of TERRANOVA, AstraZeneca will conduct a full
evaluation of both trials to determine the next steps for
Fasenra
in COPD.
In November 2017, Fasenra was approved in the US as a new medicine for
patients aged 12 years and older with severe, uncontrolled asthma
and with an eosinophilic phenotype. In January 2018, the EMA
approved Fasenra as an add-on maintenance treatment in adult
patients with severe, inadequately-controlled eosinophilic asthma,
despite their treatment with high-dose inhaled corticosteroids plus
LABA. In Japan, Fasenra was approved as an add-on treatment for bronchial
asthma in patients who continue to experience asthma exacerbations,
despite treatment with high-dose inhaled corticosteroid and other
asthma controller(s).
During the period, the Company also commenced a Phase III trial
of Fasenra for the treatment of nasal
polyposis.
e) PT010 (and PT009) (COPD)
During the period, the Phase III SOPHOS trial read out, which
compared PT009 (budesonide/formoterol fumarate) to PT005
(formoterol fumarate) and assessed lung function in patients with
moderate to very-severe COPD. The trial, which was designed to
qualify PT009 as an active comparator in the PT010 clinical-trial
programme, met its primary endpoint, with PT009 delivering
superior efficacy to PT005 at morning pre-dose trough
FEV137 at Week 24. A full evaluation of the SOPHOS trial data is
ongoing and the Company intends to present the data at a
forthcoming medical meeting.
For
more details on the development pipeline, please refer to the
latest Clinical Trials
Appendix.
Development Pipeline 31 March 2018
AstraZeneca-sponsored or -directed trials
Phase III / Pivotal Phase II / Registration
New Molecular Entities (NMEs) and significant additional
indications
Regulatory
submission dates shown for potential new medicines in Phase III and
beyond. As disclosure of compound information is balanced by the
business need to maintain confidentiality, information in relation
to some compounds listed here has not been disclosed at this
time.
Compound
|
Mechanism
|
Area Under Investigation
|
Date Commenced Phase
|
Estimated Regulatory Acceptance Date /Submission
Status
|
US
|
EU
|
Japan
|
China
|
Oncology
|
|
|
|
|
|
|
|
|
BTK
inhibitor
|
B-cell
malignancy
|
Q1
2015
|
Launched
|
|
|
|
SAVOIR
|
MET
inhibitor
|
papillary
renal cell carcinoma
|
Q3
2017
|
2020
|
2020
|
|
|
selumetinib
ASTRA
|
MEK
inhibitor
|
differentiated
thyroid cancer
|
Q3
2013
|
H2
2018
(Orphan
Drug Designation)
|
H2
2018
|
|
|
PLAIT
|
anti-CD22
recombinant immunotoxin
|
3rd-line hairy cell
leukaemia
|
Q2
2013
|
Accepted
(Orphan
Drug Designation, Priority Review)
|
|
|
|
MYSTIC
|
PD-L1 mAb + CTLA-4
mAb
|
1st-line
NSCLC
|
Q3
2015
|
H2
2018
|
H2
2018
|
H2
2018
|
|
NEPTUNE
|
PD-L1 mAb + CTLA-4
mAb
|
1st-line
NSCLC
|
Q4
2015
|
2019
|
2019
|
2019
|
2020
|
Imfinzi38 + tremelimumab
+ chemotherapy
POSEIDON
|
PD-L1 mAb + CTLA-4
mAb
|
1st-line
NSCLC
|
Q2
2017
|
2019
|
2019
|
2019
|
2020
|
Imfinzi38 + tremelimumab
+ SoC
CASPIAN
|
PD-L1 mAb + CTLA-4
mAb + SoC
|
1st-line
SCLC
|
Q1
2017
|
2019
|
2019
|
2019
|
|
Imfinzi38 +
tremelimumabKESTREL
|
PD-L1 mAb + CTLA-4
mAb
|
1st-line
HNSCC
|
Q4
2015
|
2019
|
2019
|
2019
|
|
Imfinzi38 +
tremelimumabEAGLE
|
PD-L1 mAb + CTLA-4
mAb
|
2nd-line
HNSCC
|
Q4
2015
|
H2
2018
|
H2
2018
|
H2
2018
|
|
DANUBE
|
PD-L1 mAb + CTLA-4
mAb
|
1st-line bladder
cancer
|
Q4
2015
|
2019
|
2019
|
2019
|
|
Imfinzi38 + tremelimumab
HIMALAYA
|
PD-L1 mAb + CTLA-4
mAb
|
1st-line
hepatocellular carcinoma
|
Q4
2017
|
2021
|
2021
|
2021
|
2021
|
CONCERTO
|
PARP inhibitor +
VEGF inhibitor
|
recurrent
platinum-resistant ovarian cancer
|
Q1
2017
|
2019
|
|
|
|
CVRM
|
|
|
|
|
|
Epanova
|
omega-3
carboxylic acids
|
severe
hypertriglycerid-aemia
|
|
Approved
|
|
2020
|
|
Lokelma (ZS-9) (sodium zirconium
cyclosilicate)
|
potassium
binder
|
hyperkalaemia
|
|
Accepted
|
Approved
|
2019
|
|
OLYMPUS
(US) ROCKIES (US)
|
hypoxia-inducible
factor prolyl hydroxylase inhibitor
|
anaemia
in CKD / end-stage renal disease
|
Q3
2014
|
2019
|
|
|
|
|
hypoxia-inducible
factor prolyl hydroxylase inhibitor
|
anaemia
in myelodysplastic syndrome
|
Q1
2018
|
2021
|
|
|
2020
|
Respiratory
|
Bevespi
(PT003)
|
LABA/LAMA
|
COPD
|
|
Launched
|
Accepted
|
H2
2018
|
H2
2018
|
(benralizumab)
CALIMA
SIROCCO ZONDA
BISE
BORA
GREGALE
|
IL-5R
mAb
|
severe,
uncontrolled asthma
|
|
Launched
|
Launched
|
Launched
|
2021
|
PT010
|
LABA/LAMA/
ICS
|
COPD
|
Q3
2015
|
2019
|
2019
|
H2
2018
|
H2
2018
|
tezepelumab
NAVIGATOR
SOURCE
|
TSLP
mAb
|
severe,
uncontrolled asthma
|
Q1
2018
|
2021
|
2021
|
2021
|
|
Other
|
|
|
|
|
|
|
|
|
Type
I IFN receptor mAb
|
systemic
lupus erythematosus
|
Q3
2015
|
2019
(Fast
Track)
|
2019
|
2019
|
|
AMARANTH
+ extension, DAYBREAK-ALZ
|
beta-secretase
inhibitor
|
Alzheimer’s
disease
|
Q2
2016
|
2020
(Fast
Track)
|
2020
|
2020
|
|
Phases I and II
NMEs and significant additional indications
Compound
|
Mechanism
|
Area Under Investigation
|
Phase
|
Date Commenced Phase
|
|
Oncology
|
|
|
|
|
Imfinzi
|
PD-L1
mAb
|
solid
tumours
|
II
|
Q3
2014
|
|
PD-L1 mAb + CTLA-4
mAb
|
gastric
cancer
|
II
|
Q2
2015
|
|
PD-L1 mAb + CTLA-4
mAb
|
biliary tract,
osophageal
|
II
|
Q4
2013
|
Imfinzi38 + tremelimumab
+ chemo
|
PD-L1 mAb + CTLA-4
mAb
|
1st-line
pancreatic ductal
adenocarcinoma, osophageal and SCLC
|
I
|
Q2
2016
|
|
PD-L1
mAb + CXCR2 antagonist
|
pancreatic
ductal adenocarcinoma
|
II
|
Q2
2017
|
Imfinzi38 + AZD5069 or Imfinzi38 +
danvatirsen38 (AZD9150)
|
PD-L1
mAb + CXCR2 antagonist or PD-L1 mAb + STAT3 inhibitor
|
HNSCC
|
II
|
Q3
2015
|
Imfinzi38 + dabrafenib + trametinib
|
PD-L1
mAb + BRAF inhibitor + MEK inhibitor
|
melanoma
|
I
|
Q1
2014
|
Imfinzi38 +
adavosertib38 (AZD1775)
|
PD-L1
mAb + Wee1 inhibitor
|
solid
tumours
|
I
|
Q4
2015
|
|
PD-L1
mAb + PD-1 mAb
|
solid
tumours
|
II
|
Q3
2016
|
Imfinzi38 or Imfinzi38 + (tremelimumab or danvatirsen38 (AZD9150))
|
PD-L1
mAb or PD-L1 mAb + (CTLA-4 mAb or STAT3 inhibitor)
|
diffuse
large B-cell lymphoma
|
I
|
Q3
2016
|
Imfinzi38 + danvatirsen (AZD9150) +
chemotherapy
|
PD-L1
mAB + STAT3 inhibitor + chemotherapy
|
solid
tumours
|
I
|
Q1
2018
|
|
PD-L1
mAb + EGFR inhibitor
|
NSCLC
|
I
|
Q2
2014
|
|
PD-L1
mAb + humanised OX40 agonist
|
solid
tumours
|
I
|
Q2
2016
|
|
PD-L1
mAb + TLR 7/8 agonist
|
solid
tumours
|
I
|
Q2
2017
|
|
PD-L1
mAb + CD73 mAb
|
solid
tumours
|
I
|
Q1
2016
|
|
PD-L1
mAb + NKG2a mAb
|
solid
tumours
|
I
|
Q1
2016
|
|
PD-L1
mAb + MEK inhibitor
|
solid
tumours
|
I
|
Q4
2015
|
|
PD-L1
mAb + CTLA-4 mAb
|
solid
tumours
|
I
|
Q4
2013
|
tremelimumab + MEDI056238
|
CTLA-4
mAb + humanised OX40 agonist
|
solid
tumours
|
I
|
Q2
2016
|
|
PD-L1
mAb + azacitidine
|
myelodysplastic
syndrome
|
I
|
Q2
2016
|
|
PD-L1
mAb + DNA HPV vaccine
|
HNSCC
|
II
|
Q4
2017
|
Imfinzi38 + RT (platform)
CLOVER
|
PD-L1
mAb + RT
|
locally-advanced
HNSCC, NSCLC, SCLC
|
I
|
Q1
2018
|
BAYOU
|
PDL-1
mAb + PARP inhibitor
|
1st-line
unresectable stage IV bladder cancer
|
II
|
Q1
2018
|
|
PARP
inhibitor + ATR inhibitor
|
gastric
cancer
|
II
|
Q3
2016
|
Lynparza38 + adavosertib38 (AZD1775#)
|
PARP
inhibitor + Wee1 inhibitor
|
solid
tumours
|
I
|
Q3
2015
|
MEDIOLA
|
PARP
inhibitor + PD-L1 mAb
|
solid
tumours
|
II
|
Q2
2016
|
Tagrisso + (selumetinib38 or savolitinib38)
TATTON
|
EGFR
inhibitor + (MEK inhibitor or MET inhibitor)
|
advanced
EGFRm NSCLC
|
II
|
Q2
2016
|
Tagrisso BLOOM
|
EGFR
inhibitor
|
CNS
metastases in advanced EGFRm NSCLC
|
II
|
Q4
2015
|
adavosertib38 (AZD177538) +
chemotherapy
|
Wee1
inhibitor + chemotherapy
|
ovarian
cancer
|
II
|
Q1
2015
|
adavosertib38 (AZD177538)
|
Wee1
inhibitor
|
solid
tumours
|
I
|
Q3
2015
|
vistusertib
|
mTOR
inhibitor
|
solid
tumours
|
II
|
Q1
2013
|
capivasertib38 (AZD536338)
|
AKT
inhibitor
|
breast
cancer
|
II
|
Q1
2014
|
AZD4547
|
FGFR
inhibitor
|
solid
tumours
|
II
|
Q4
2011
|
AZD0156
|
ATM
inhibitor
|
solid
tumours
|
I
|
Q4
2015
|
AZD1390
|
ATM
inhibitor
|
healthy
volunteer trial
|
I
|
Q4
2017
|
|
Aurora
B inhibitor
|
solid
tumours
|
I
|
Q4
2015
|
AZD4573
|
CDK9
inhibitor
|
haematological
malignancies
|
I
|
Q4
2017
|
AZD4635
|
A2aR
inhibitor
|
solid
tumours
|
I
|
Q2
2016
|
AZD4785
|
KRAS
inhibitor
|
solid
tumours
|
I
|
Q2
2017
|
AZD5153
|
BRD4
inhibitor
|
solid
tumours
|
I
|
Q3
2017
|
AZD5991
|
MCL1
inhibitor
|
haematological
malignancies
|
I
|
Q3
2017
|
Calquence +
vistusertib
|
BTK
inhibitor + mTor inhibitor
|
haematological
malignancies
|
I
|
Q3
2017
|
Calquence + AZD6738
|
BTK
inhibitor + ATR inhibitor
|
haematological
malignancies
|
I
|
Q1
2018
|
AZD6738
|
ATR
inhibitor
|
solid
tumours
|
I
|
Q4
2013
|
AZD8186
|
PI3k
inhibitor
|
solid
tumours
|
I
|
Q2
2013
|
AZD9496
|
selective
oestrogen receptor degrader
|
oestrogen
receptor +ve breast cancer
|
I
|
Q4
2014
|
|
humanised
OX40 agonist
|
solid
tumours
|
I
|
Q1
2015
|
MEDI1873
|
GITR
agonist fusion protein
|
solid
tumours
|
I
|
Q4
2015
|
|
PSMA
antibody drug conjugate
|
prostate
cancer
|
I
|
Q1
2017
|
MEDI4276
|
HER2
bi-specific antibody drug conjugate
|
solid
tumours
|
I
|
Q4
2015
|
MEDI5083
|
CD40
ligand fusion protein
|
solid
tumours
|
I
|
Q1
2017
|
MEDI7247
|
antibody
drug conjugate
|
haematological
malignancies
|
I
|
Q2
2017
|
|
TLR
7/8 agonist
|
solid
tumours
|
I
|
Q4
2015
|
oleclumab
|
CD73
mAb
|
solid
tumours
|
I
|
Q3
2015
|
CVRM
|
|
|
|
verinurad
|
URAT1
inhibitor
|
CKD
|
II
|
Q2
2017
|
MEDI0382
|
GLP-1
/
glucagon
dual agonist
|
type-2
diabetes / obesity
|
II
|
Q3
2016
|
MEDI6012
|
LCAT
|
CV
disease
|
II
|
Q4
2015
|
AZD4831
|
myeloperoxidase
|
HF
with a preserved ejection fraction
|
I
|
Q3
2016
|
AZD5718
|
FLAP
|
coronary
artery disease
|
II
|
Q4
2017
|
|
VEGF-A
|
CV
disease
|
II
|
Q1
2018
|
AZD9977
|
MCR
|
CV
disease
|
I
|
Q1
2018
|
|
cholesterol
modulation
|
CV
disease
|
II
|
Q4
2017
|
MEDI7219
|
anti-diabetic
|
type-2
diabetes
|
I
|
Q1
2018
|
Respiratory
|
|
|
|
|
|
LABA
|
asthma
/ COPD
|
II
|
Q4
2007
|
|
TSLP
mAb
|
atopic
dermatitis
|
II
|
Q2
2015
|
|
inhaled
TLR9 agonist
|
asthma
|
II
|
Q4
2016
|
AZD7594
|
inhaled
SGRM
|
asthma
/ COPD
|
II
|
Q3
2015
|
|
MABA
|
COPD
|
II
|
Q1
2017
|
PT010
|
LABA/LAMA/ICS
|
asthma
|
II
|
Q2
2014
|
AZD5634
|
inhaled
ENaC
|
cystic
fibrosis
|
I
|
Q1
2016
|
|
inhaled
SGRM + LABA
|
asthma
/ COPD
|
I
|
Q4
2016
|
|
DPP1
|
COPD
|
II
|
Q4
2017
|
AZD9567
|
oral
SGRM
|
rheumatoid
arthritis / respiratory
|
II
|
Q1
2018
|
|
Inhaled
IL-4Ra
|
asthma
|
I
|
Q4
2017
|
MEDI3506
|
IL-33
mAb
|
COPD
|
I
|
Q2
2017
|
Other
|
|
|
|
|
|
Type
1 IFN receptor mAb
|
lupus
nephritis
|
II
|
Q4
2015
|
|
Type
1 IFN receptor mAb
|
systemic
lupus erythematosus (subcutaneous)
|
II
|
Q1
2017
|
MEDI3902
|
Psl/PcrV
bispecific mAb
|
prevention of nosocomial Pseudomonas aeruginosa
pneumonia
|
II
(Fast
Track, US)
|
Q2
2016
|
suvratoxumab
|
mAb binding to S. aureus toxin
|
prevention of nosocomial Staphylococcus
aureus pneumonia
|
II
(Fast
Track, US)
|
Q4
2014
|
|
B7RP1
mAb
|
primary
Sjögren’s
syndrome
|
II
|
Q3
2015
|
MEDI8852
|
influenza
A mAb
|
influenza
A treatment
|
II
(Fast Track,
US)
|
Q4
2015
|
|
RSV
mAb-YTE
|
passive
RSV prophylaxis
|
II
(Fast
Track, US)
|
Q1
2015
|
AZD0284
|
RORg
|
psoriasis
/ respiratory
|
I
|
Q4
2016
|
|
BAFF/B7RP1
bispecific mAb
|
systemic
lupus erythematosus
|
I
|
Q1
2016
|
|
amyloid
beta mAb
|
Alzheimer’s
disease
|
I
|
Q2
2014
|
MEDI7352
|
NGF/TNF
bi-specific mAb
|
osteoarthritis
pain
|
I
|
Q1
2016
|
MEDI1341
|
alpha
synuclein mAb
|
Parkinson’s
disease
|
I
|
Q4
2017
|
Significant Lifecycle Management
Compound
|
Mechanism
|
Area Under Investigation
|
Date
Commenced Phase
|
Estimated
Regulatory Acceptance Date / Submission Status
|
US
|
EU
|
Japan
|
China
|
Oncology
|
|
|
|
|
|
|
|
|
BTK
inhibitor
|
1st-line chronic
lymphocytic leukaemia
|
Q3
2015
|
2020
(Orphan
Drug Designation)
|
2020
(Orphan
designation)
|
|
|
|
BTK
inhibitor
|
relapsed/refractory
chronic lymphocytic leukaemia, high risk
|
Q4
2015
|
2019
(Orphan
Drug Designation)
|
2019
(Orphan
designation)
|
|
|
|
BTK
inhibitor
|
1st-line
mantle cell lymphoma
|
Q1
2017
|
2023
|
|
|
|
|
PD-L1
mAb
|
locally-advanced
(Stage III), NSCLC
|
Q2
2014
|
Approved
(Breakthrough
Therapy Designation & Priority Review)
|
Accepted
|
Accepted
|
|
PEARL
(China)
|
PD-L1
mAb
|
1st-line
NSCLC
|
Q1
2017
|
|
|
|
2020
|
|
PARP
inhibitor
|
gBRCA metastatic breast cancer
|
Q2
2014
|
Approved
(Priority
Review)
|
Accepted
|
Accepted
(Orphan drug
designation, Priority Review)
|
H2
2018
|
|
PARP
inhibitor
|
2nd-line
or greater BRCAm PSR ovarian cancer, maintenance
monotherapy
|
Q3
2013
|
Approved
(Priority
Review)
|
Approved
|
Approved
(Orphan drug
designation)
|
Accepted
|
|
PARP
inhibitor
|
1st-line BRCAm ovarian cancer
|
Q3
2013
|
H2
2018
|
H2
2018
|
H2
2018
|
2019
|
|
PARP
inhibitor
|
gBRCA PSR ovarian cancer
|
Q1
2015
|
H2
2018
|
|
|
|
|
PARP
inhibitor
|
pancreatic
cancer
|
Q1
2015
|
2019
|
2019
|
|
|
PROfound
|
PARP
inhibitor
|
prostate
cancer
|
Q1
2017
|
2020
(Breakthrough
Therapy Designation)
|
2020
|
2020
|
2020
|
OlympiA
|
PARP
inhibitor
|
gBRCA adjuvant breast cancer
|
Q2
2014
|
2021
|
2021
|
2021
|
|
Tagrisso
FLAURA
|
EGFR
inhibitor
|
1st-line
advanced EGFRm NSCLC
|
Q1
2015
|
Approved
(Breakthrough
Therapy designation)
|
Accepted
(CHMP positive
opinion)
|
Accepted
|
H2
2018
|
Tagrisso
ADAURA
|
EGFR
inhibitor
|
adjuvant
EGFRm NSCLC
|
Q4
2015
|
2022
|
2022
|
2022
|
2022
|
CVRM
|
|
|
|
|
|
THALES
|
P2Y12
receptor antagonist
|
acute
ischaemic stroke or transient ischaemic attack
|
Q1
2018
|
2020
|
2020
|
|
2020
|
THEMIS
|
P2Y12
receptor antagonist
|
CV outcomes trial in patients with type-2 diabetes
and coronary artery disease without a previous history
of MI or stroke
|
Q1
2014
|
2019
|
2019
|
2019
|
2020
|
HESTIA
|
P2Y12
receptor antagonist
|
prevention
of vaso-occlusive crises in paediatric patients with sickle cell
disease
|
Q1
2014
|
2021
|
2021
|
|
|
|
SGLT2
inhibitor
|
CV
outcomes trial in patients with type-2 diabetes
|
Q2
2013
|
2019
|
2019
|
|
|
|
SGLT2
inhibitor
|
type-1
diabetes
|
Q4
2014
|
H2
2018
|
Accepted
|
H2
2018
|
|
|
SGLT2
inhibitor
|
worsening
HF or CV death in patients with chronic HF
|
Q1
2017
|
2020
|
2020
|
2020
|
2020
|
|
SGLT2
inhibitor
|
renal outcomes and CV mortality in patients with CKD
|
Q1
2017
|
2021
|
2021
|
2021
|
2021
|
Xigduo XR/
|
SGLT2
inhibitor/ metformin FDC
|
type-2
diabetes
|
|
Launched
|
Launched
|
|
2020
|
Qtern
|
DPP-4
inhibitor / SGLT2 inhibitor FDC
|
type-2
diabetes
|
|
Launched
|
Launched
|
|
|
BydureonBCise
/ Bydureon autoinjector44
|
GLP-1
receptor agonist
|
type-2
diabetes
|
Q1
2013
|
Launched
|
Accepted
|
|
|
Bydureon EXSCEL
|
GLP-1
receptor agonist
|
type-2
diabetes outcomes trial
|
Q2
2010
|
Q2
2018
|
Accepted
|
|
H2
2018
|
saxagliptin/
dapagliflozin/
metformin
|
DPP-4
inhibitor / SGLT2 inhibitor
|
type-2
diabetes
|
Q2
2017
|
Q2
2018
|
Q2
2018
|
|
|
Epanova
STRENGTH
|
omega-3
carboxylic acids
|
CV
outcomes trial in statin-treated patients at high CV risk, with
persistent hypertriglyceridae-mia plus low
HDL-cholesterol
|
Q4
2014
|
2020
|
2020
|
2020
|
2020
|
Respiratory
|
|
|
|
|
|
|
|
TERRANOVA
GALATHEA
|
IL-5R
mAb
|
COPD
|
Q3
2014
|
H2
2018
|
H2
2018
|
2019
|
|
OSTRO
|
IL-5R
mAb
|
nasal
polyposis
|
Q1
2018
|
2020
|
2020
|
|
|
Symbicort
SYGMA
|
ICS/LABA
|
as-needed
use in mild asthma
|
Q4
2014
|
|
H2
2018
|
|
2019
|
|
LAMA/LABA
|
COPD
|
|
Q2
2018
|
Launched
|
|
2019
|
Other
|
|
|
|
|
|
|
|
Nexium
|
proton-pump
inhibitor
|
stress
ulcer prophylaxis
|
|
|
|
|
Accepted
|
Nexium
|
proton-pump
inhibitor
|
paediatrics
|
|
Launched
|
Launched
|
Launched
|
|
|
GC-C
receptor peptide agonist
|
irritable
bowel syndrome with constipation (IBS-C)
|
|
|
|
|
Accepted
|
Terminations (discontinued projects: 1 January to 31 March
2018)
NME / Line Extension
|
Compound
|
Reason for Discontinuation
|
Area Under Investigation
|
NME
|
|
safety / efficacy
|
solid tumours
|
NME
|
MEDI9314
|
strategic
|
atopic dermatitis
|
Completed Projects/Divestitures (1 January to 31 March
2018)
Compound
|
Mechanism
|
Area Under Investigation
|
Completed/
Divested
|
|
Faslodex
(FALCON)
|
oestrogen
receptor antagonist
|
1st-line
hormone receptor +ve advanced breast cancer
|
Completed
|
|
GM-CSFR
mAb
|
rheumatoid
arthritis
|
divested
|
|
CD19
mAb
|
neuromyelitis
optica
|
divested
|
MEDI4920
|
anti-CD40L-Tn3
fusion protein
|
primary
Sjögren’s syndrome
|
divested
|
MEDI7734
|
ILT7
mAb
|
myositis
|
divested
|
Condensed Consolidated Statement Of Comprehensive
Income
For the
quarter ended 31
March
|
|
2018
$m
|
|
2017
$m
|
Product
Sales
|
|
4,985
|
|
4,843
|
Externalisation
Revenue
|
|
193
|
|
562
|
Total Revenue
|
|
5,178
|
|
5,405
|
Cost of
sales
|
|
(1,134)
|
|
(894)
|
Gross profit
|
|
4,044
|
|
4,511
|
Distribution
costs
|
|
(81)
|
|
(77)
|
Research
and development expense
|
|
(1,279)
|
|
(1,453)
|
Selling,
general and administrative costs
|
|
(2,457)
|
|
(2,300)
|
Other
operating income & expense
|
|
469
|
|
236
|
Operating profit
|
|
696
|
|
917
|
Finance
income
|
|
35
|
|
18
|
Finance
expense
|
|
(343)
|
|
(340)
|
Share
of after tax losses in associates and joint ventures
|
|
(14)
|
|
(13)
|
Profit before tax
|
|
374
|
|
582
|
Taxation
|
|
(58)
|
|
(70)
|
Profit for the period
|
|
316
|
|
512
|
|
|
|
|
|
Other comprehensive income
|
|
|
|
|
Items that will not be reclassified to profit or loss
|
|
|
|
|
Remeasurement
of the defined benefit pension liability
|
|
27
|
|
1
|
Fair
value movements on equity investments
|
|
118
|
|
-
|
Fair
value movements related to own credit risk on bonds designated as
fair value through profit or loss
|
|
(1)
|
|
-
|
Tax on
items that will not be reclassified to profit or loss
|
|
(27)
|
|
(1)
|
|
|
117
|
|
-
|
Items that may be reclassified subsequently to profit or
loss
|
|
|
|
|
Foreign
exchange arising on consolidation
|
|
167
|
|
154
|
Foreign
exchange arising on designating borrowings in net investment
hedges
|
|
(99)
|
|
100
|
Fair
value movements on cash flow hedges
|
|
101
|
|
7
|
Fair
value movements on cash flow hedges transferred to profit or
loss
|
|
(80)
|
|
(39)
|
Fair
value movements on derivatives designated in net investment
hedges
|
|
(46)
|
|
(30)
|
Fair
value movements on equity investments
|
|
-
|
|
(150)
|
Tax on
items that may be reclassified subsequently to profit or
loss
|
|
20
|
|
24
|
|
|
63
|
|
66
|
Other comprehensive income for the period, net of tax
|
|
180
|
|
66
|
Total comprehensive income for the period
|
|
496
|
|
578
|
|
|
|
|
|
Profit attributable to:
|
|
|
|
|
Owners
of the Parent
|
|
340
|
|
537
|
Non-controlling
interests
|
|
(24)
|
|
(25)
|
|
|
316
|
|
512
|
|
|
|
|
|
Total comprehensive income attributable to:
|
|
|
|
|
Owners
of the Parent
|
|
520
|
|
603
|
Non-controlling
interests
|
|
(24)
|
|
(25)
|
|
|
496
|
|
578
|
|
|
|
|
|
Basic
earnings per $0.25 Ordinary Share
|
|
|