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
period ending 25
July 2017
GlaxoSmithKline plc
(Name
of registrant)
980 Great West Road, Brentford, Middlesex, TW8 9GS
(Address
of principal executive offices)
Indicate
by check mark whether the registrant files or
will
file annual reports under cover Form 20-F or Form 40-F
Form
20-F x Form 40-F
--
Indicate
by check mark whether the registrant by furnishing the
information
contained in this Form is also thereby furnishing the
information
to the Commission pursuant to Rule 12g3-2(b) under the
Securities
Exchange Act of 1934.
Yes
No x
Switching to a dolutegravir regimen from a boosted protease
inhibitor regimen maintained viral suppression and improved lipid
fractions in patients with HIV and high cardiovascular
risk
Data presented at the International AIDS Society meeting in
Paris
London, UK. 25 July 2017- ViiV Healthcare and NEAT-ID
announced results from the NEAT 022 study of more than 400 patients
with HIV and high cardiovascular risk. The study was conducted by
the NEAT-ID group with support from ViiV Healthcare and St
Stephen's AIDS Trust (SSAT), and showed that switching
virologically suppressed patients at high risk of cardiovascular
disease (CVD) from a boosted protease inhibitor regimen (PI/r) to a
dolutegravir-based regimen maintained viral suppression while
decreasing blood lipids. The study results were presented at the
annual conference of the International AIDS Society (IAS) in Paris,
France.
CVD is
a leading cause of morbidity and mortality across the
world1 and
certain antiretroviral agents are associated with adverse changes
in blood lipids, an established factor contributing to risk for
CVD. The NEAT study sought to evaluate the safety and efficacy of
switching to dolutegravir in patients with HIV and high
cardiovascular risk.
Overall,
415 patients from six European countries were randomised to switch
from a boosted PI to dolutegravir or to remain on a boosted PI for
48 weeks. Of these, 89% were men, 87% were older than 50 years and
74% had a Framingham CVD risk score of greater than 10% over the
next 10 years.
The
study demonstrated that switching to a dolutegravir-based regimen
in virologically suppressed HIV-infected patients with high CVD
risk was non-inferior compared with continuing a boosted PI-based
regimen, with no emergent resistance mutations in any of the
groups. Total cholesterol and other lipid fractions (except
high-density lipoprotein cholesterol) improved significantly
(p<0.001) in the dolutegravir group. There was no significant
difference in severe, grade 3 or 4 or treatment-modifying adverse
events.
Michael
Aboud, Vice President and Global Medical Lead for dolutegravir,
said: "Simply having HIV is a risk factor for premature CVD, so it
is important for people with HIV and other CVD risk factors to have
effective treatment options that avoid adding to that risk. We were
pleased to collaborate with the NEAT-ID group on this study that
showed switching to a dolutegravir-based regimen not only
maintained viral suppression in a population with HIV and high risk
for CVD, but also improved their overall lipid
profile."
Jose M
Gatell, Senior Consultant at Hospital Clìnic/IDIBAPS,
Professor of Medicine at the University of Barcelona and chief
investigator of the NEAT 022 study, said: "This is the first
switching study targeting
a
population with high cardiovascular risk. To minimise this risk the
interventions should be in this order: maintaining the virological
suppression, switching to antiretroviral agents with a neutral
lipid profile and, if still necessary, adding lipid-lowering
agents. In the NEAT 022 study we have demonstrated that switching
from a ritonavir-boosted PI regimen to dolutegravir was able to
maintain virological suppression and significantly improved the
plasma lipid profile."
-
Ends -
Notes to editors
Tivicay is a registered trademark of the ViiV Healthcare group of
companies. For more information on the trials please visit:
www.clinicaltrials.gov
About the NEAT-ID study group
The NEAT-ID Foundation is a not for profit private foundation to
promote research and education projects in HIV, hepatitis and
global infectious diseases.
About SSAT
SSAT through its wholly owned subsidiary St Stephen's Clinical
Research sponsors, manages and conducts single and multicenter
clinical trials throughout Europe and in Africa.
About the NEAT 022 study
NEAT022-NCT02098837 is a European, open label, randomized,
non-inferiority trial. HIV-infected adults ≥ 50 years or with
a Framingham score ≥10% were eligible if HIV RNA < 50
copies/mL for at least 24 weeks while on a PI/r regimen. Patients
were randomized (1:1) to switch to DTG or to remain on PI/r.
Primary end-points were: proportion of patients with HIV RNA <
50 copies/ml at week 48 and a non-inferiority margin of -10% and
percentage change of total plasma cholesterol. Secondary end-points
included changes in other plasma lipid fractions, and adverse
events. The NEAT022/SSAT060 trial was also supported by St Stephens
AIDS Trust (SSAT) and ViiV Healthcare.
TIVICAY
(dolutegravir) tablets
Professional Indication(s) and Important Safety
Information
Indications and Usage
TIVICAY is a human immunodeficiency virus type 1 (HIV-1) integrase
strand transfer inhibitor (INSTI) indicated in combination with
other antiretroviral agents for the treatment of HIV-1 infection in
adults and paediatric patients weighing at least 30 kg
Limitations of use:
· Use
of TIVICAY in INSTI-experienced patients should be guided by the
number and type of baseline INSTI substitutions. The efficacy of
TIVICAY 50 mg twice daily is reduced in patients with an
INSTI-resistance Q148 substitution plus 2 or more additional
INSTI-resistance substitutions including T66A, L74I/M, E138A/K/T,
G140S/A/C, Y143R/C/H, E157Q, G163S/E/K/Q, or
G193E/R
Important Safety Information
Contraindications:
TIVICAY
is contraindicated in patients:
· With
previous hypersensitivity reaction to dolutegravir
· Receiving
dofetilide (antiarrhythmic)
Hypersensitivity Reactions:
·
Hypersensitivity reactions have been reported and were
characterized by rash, constitutional findings, and sometimes organ
dysfunction, including liver injury. The events were reported in
<1% of subjects receiving TIVICAY in phase III clinical
trials
· Discontinue
TIVICAY and other suspect agents immediately if signs or symptoms
of hypersensitivity reactions develop, as a delay in stopping
treatment may result in a life-threatening reaction. Monitor
clinical status, including liver aminotransferases, and initiate
appropriate therapy if hypersensitivity reaction is
suspected
Effects on Serum Liver Biochemistries in Patients with Hepatitis B
or C Co-infection:
· Patients
with underlying hepatitis B or C may be at increased risk for
worsening or development of transaminase elevations with use of
TIVICAY. In some cases the elevations in transaminases were
consistent with immune reconstitution syndrome or hepatitis B
reactivation, particularly in the setting where anti-hepatitis
therapy was withdrawn
· Appropriate
laboratory testing prior to initiating therapy and monitoring for
hepatotoxicity during therapy with TIVICAY are recommended in
patients with underlying hepatic disease such as hepatitis B or
C
Fat Redistribution or accumulation has been observed in
patients receiving antiretroviral therapy.
Immune Reconstitution Syndrome, including the occurrence of
autoimmune disorders with variable time to onset, has been
reported.
Adverse Reactions:
The
most commonly reported (≥2%) adverse reactions of moderate to
severe intensity in treatment-naïve adult subjects in any one
trial receiving TIVICAY in a combination regimen were insomnia
(3%), fatigue (2%), and headache (2%).
Drug Interactions:
·
Coadministration of TIVICAY with certain inducers of UGT1A and/or
CYP3A may reduce plasma concentrations of dolutegravir and require
dose adjustments of TIVICAY
· Administer
TIVICAY 2 hours before or 6 hours after taking polyvalent
cation-containing antacids or laxatives, sucralfate, oral
supplements containing iron or calcium, or buffered medications.
Alternatively, TIVICAY and supplements containing calcium or iron
can be taken with food
· Consult the
full Prescribing Information for TIVICAY for more information on
potentially significant drug interactions, including clinical
comments
Pregnancy: TIVICAY should be
used during pregnancy only if the potential benefit justifies the
potential risk. An Antiretroviral Pregnancy Registry has been
established.
Nursing Mothers: Breastfeeding is
not recommended due to the potential for HIV transmission and the
potential for adverse reactions in nursing infants.
About ViiV Healthcare
ViiV
Healthcare is a global specialist HIV company established in
November 2009 by GlaxoSmithKline (LSE: GSK) and Pfizer (NYSE: PFE)
dedicated to delivering advances in treatment and care for people
living with HIV and for people who are at risk of becoming infected
with HIV. Shionogi joined in October 2012. The company's aim is to
take a deeper and broader interest in HIV/AIDS than any company has
done before and take a new approach to deliver effective and
innovative medicines for HIV treatment and prevention, as well as
support communities affected by HIV. For more information on the
company, its management, portfolio, pipeline, and commitment,
please visit www.viivhealthcare.com.
About GSK
GSK -
one of the world's leading research-based pharmaceutical and
healthcare companies - is committed to improving the quality of
human life by enabling people to do more, feel better and live
longer. For further information, please visit
www.gsk.com.
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GSK
Global Media enquiries:
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Simon
Steel
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+44 (0)
20 8047 5502
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David
Daley
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+44 (0)
20 8047 5502
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ViiV
Healthcare Media enquiries:
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Sébastien
Desprez (on site at
IAS)
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+44 (0)
20 8380 6275
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Patricia
O'Connor
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+44 (0)
208 047 5982
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Marc
Meachem
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+1 919
483 8756
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GSK US
Media enquiries:
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Mary
Anne Rhyne
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+1 919
483 0492
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Sarah
Spencer
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+1 215
751 3335
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Analyst/investor
enquiries:
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Sarah
Elton-Farr
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+44 (0)
20 8047 5194
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Gary
Davies
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+44 (0)
20 8047 5503
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James
Dodwell
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+44 (0)
20 8047 2406
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Sarah
Webster
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+44 (0)
20 8047 0246
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Tom
Curry
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+1 215
751 5419
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Jeff
McLaughlin
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+1 215
751 7002
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Cautionary statement regarding forward-looking
statements
GSK
cautions investors that any forward-looking statements or
projections made by GSK, including those made in this announcement,
are subject to risks and uncertainties that may cause actual
results to differ materially from those projected. Such factors
include, but are not limited to, those described under Item 3.D
'Principal risks and uncertainties' in the company's Annual Report
on Form 20-F for 2016.
1 WHO. Cardiovascular diseases (CVDs) Fact sheet. May 2017.
Available at:
http://www.who.int/mediacentre/factsheets/fs317/en/Last accessed
July 2017
SIGNATURES
Pursuant
to the requirements of the Securities Exchange Act of 1934, the
registrant has duly caused this report to be signed on its behalf
by the undersigned, thereunto duly authorised.
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GlaxoSmithKline plc
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(Registrant)
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Date: July
25, 2017
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By: VICTORIA
WHYTE
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Victoria Whyte
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Authorised
Signatory for and on
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behalf
of GlaxoSmithKline plc
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