- Largest head-to-head randomised clinical trial between
DTG/3TC and BIC/FTC/TAF, conducted by SEIMC-GeSIDA Foundation (FSG)
showed DTG/3TC demonstrated non-inferior efficacy compared to
BIC/FTC/TAF as a switch regimen for virologically-suppressed adults
living with HIV over 48 weeks of therapy
- DTG/3TC-treated individuals had significantly less weight
gain compared to those randomised to BIC/FTC/TAF
ViiV Healthcare, the global specialist HIV company majority
owned by GSK, with Pfizer and Shionogi as shareholders, announces
48-week findings from PASO DOBLE (GeSIDA 11720 study), the largest
head-to-head, phase IV randomised clinical trial (RCT)
investigating the 2-drug regimen Dovato (dolutegravir/lamivudine
[DTG/3TC]) compared to the 3-drug regimen Biktarvy
(bictegravir/emtricitabine/tenofovir alafenamide fumarate
[BIC/FTC/TAF]) for the treatment of HIV-1 in people who are
virologically suppressed and who could benefit from treatment
optimisation.1
Findings showed that switching to DTG/3TC in virologically
suppressed adults living with HIV demonstrated non-inferior
efficacy in maintaining viral suppression compared with switching
to BIC/FTC/TAF.1 These data will be presented at the 25th
International AIDS Conference (AIDS 2024), held in Munich, Germany
(22-26 July).
Harmony P. Garges, M.D., MPH, Chief Medical Officer at ViiV
Healthcare, said: “The results from PASO DOBLE show that Dovato
demonstrated non-inferior efficacy compared to Biktarvy, and that
the average weight gain for trial participants taking DTG/3TC was
significantly lower than those taking BIC/FTC/FTC over the course
of the year. This is a meaningful outcome, as treatment-related
weight gain is an important topic for many people living with HIV.
At ViiV Healthcare we're dedicated to bringing innovative HIV
treatments to people living with HIV that are not only safe and
effective, but also address their specific needs beyond viral
suppression.”
In the PASO DOBLE clinical trial, 553 people living with HIV and
virally suppressed switched treatment to either DTG/3TC (n=277) or
BIC/FTC/TAF (n=276).1 The study population included individuals who
were on therapy that could be optimised, such as multiple tablet
regimens, or those containing pharmacokinetic boosting agents or
drugs with cumulative toxicity, such as efavirenz or tenofovir
disoproxil fumarate (TDF).2 The study met its primary endpoint when
DTG/3TC demonstrated non-inferior efficacy versus BIC/FTC/TAF based
on the proportion of participants with viral RNA ≥50 copies/mL at
48 weeks using the FDA snapshot and a 4% non-inferiority margin in
the exposed intention-to-treat population.1
At 48 weeks, DTG/3TC was non-inferior to BIC/FTC/TAF (risk
difference between DTG/3TC [2.2%] minus BIC/FTC/TAF [0.7%] of 1.4%,
95% CI -0.5 to 3.4). One participant in the BIC/FTC/TAF arm and
zero in the DTG/3TC arm had protocol-defined confirmed virological
failure through week 48 (HIV-1 RNA ≥50 c/mL followed by a second
consecutive HIV-1 RNA assessment ≥200 c/mL).1
The study found in a key secondary endpoint that weight
increased significantly more in participants who switched to
BIC/FTC/TAF (adjusted mean change 1.81kg, 95% CI 1.28-2.34) than in
those who switched to DTG/3TC (adjusted mean change 0.89kg, 95% CI
0.37-1.41) [difference 0.92kg, 95% CI 0.17-1.66] through week 48.
Equally, the proportion of participants with weight gain greater
than 5% at week 48 was significantly higher at 29.9% for
BIC/FTC/TAF compared to 20% for DTG/3TC (adjusted OR 1.81, 95% CI
1.19-2.76).1
Weight change with DTG/3TC did not differ between men and women
or based on the previous regimen of participants, whereas the
proportion of trial participants experiencing greater than 5%
weight gain with BIC/FTC/TAF was approximately 45% higher than
those taking DTG/3TC when switching from a regimen with abacavir
(30.6% BIC/FTC/TAF vs 21.1% DTG/3TC), and about 2-fold higher when
switching from a regimen with TDF (40.7% BIC/FTC/TAF vs 19.5%
DTG/3TC). Safety was comparable through week 48 and consistent with
known safety profiles. There were few discontinuations due to
adverse events in both study arms (DTG/3TC = 1, 0.4%; BIC/FTC/TAF =
2, 0.7%), with no differences between arms.1
Esteban Martínez, MD, PhD, Chief Executive Investigator of
the PASO DOBLE study and Senior Consultant in Infectious Diseases
at Hospital Clínic of Barcelona, Spain said: “The HIV treatment
regimens that are commonly prescribed today are all highly
effective, which makes it critical that we study the impact of
these therapies beyond just viral suppression. The results from
PASO DOBLE show Dovato, a 2-drug regimen, not just demonstrated the
same efficacy as a 3-drug regimen, but also showed less weight gain
compared to BIC/FTC/TAF through 48 weeks.”
About PASO DOBLE1,2
The PASO DOBLE (NCT04884139) randomised clinical trial is a
phase IV, open-label, randomised multicentre clinical trial
evaluating the efficacy of DTG/3TC versus BIC/FTC/TAF for the
maintenance of virologic suppression in people living with HIV-1,
conducted in 30 sites across Spain. Virologically suppressed people
living with HIV on regimens containing ≥1 pill/day, boosters, or
drugs with cumulative toxicity such as efavirenz or TDF were
eligible and were randomised (1:1) to switch to either DTG/3TC or
BIC/FTC/TAF. The primary endpoint was the proportion of people
living with HIV with RNA ≥50 copies/mL at 48 weeks (FDA snapshot,
4% non-inferiority margin) in the intention-to-treat exposed
population. Secondary outcomes measured included, among others,
absolute weight gain, BMI change, and the proportion of
participants with weight change greater than 5%.
About Dovato
Dovato is indicated as a complete regimen to treat HIV-1
infection in adults with no antiretroviral (ARV) treatment history
or to replace the current ARV regimen in those who are
virologically suppressed (HIV-1 RNA <50 copies/mL) on a stable
ARV regimen with no history of treatment failure and no known
resistance to any component of Dovato.
Dovato is approved in the US, Europe, Japan, Australia, and
other countries worldwide.
Please consult the full Summary of Product Characteristics for
all the safety information: Dovato 50 mg/300 mg film-coated
tablets.
Trademarks are owned by or licensed to the ViiV Healthcare group
of companies.
About SEIMC-GeSIDA Foundation (FSG)
The SEIMC-GeSIDA Foundation (FSG) was created to encourage,
promote, and support scientific and technical research and
development, training, and publication of findings in the field of
clinical microbiology and infectious diseases and associated
conditions. FSG was founded by investigators from the Spanish
Society of Clinical Microbiology and Infectious Diseases as a tool
to promote high-quality investigation in the field of HIV infection
and other infectious diseases. The Foundation also aims to respond
to the scientific concerns of the group’s members. FSG is composed
of qualified professionals with experience in the field of clinical
trials and multicentre studies. Its streamlined infrastructure
facilitates performance of clinical studies and responds to the
needs of investigators in terms of methodology/statistical analysis
and of logistics and management of trials and other multicentre
studies. We also provide staff to run events such as scientific
meetings and conferences (national and international) and to
organise courses, lectures, talks, seminars, round-table talks, and
specialised workshops.
For more information on the FSG, please visit
https://fundacionseimcgesida.org/en/quienes-somos/
About ViiV Healthcare
ViiV Healthcare is a global specialist HIV company established
in November 2009 by GSK (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 acquiring HIV. Shionogi
became a ViiV shareholder in October 2012. The company’s aims are
to take a deeper and broader interest in HIV and 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 viivhealthcare.com.
About GSK
GSK is a global biopharma company with a purpose to unite
science, technology, and talent to get ahead of disease together.
Find out more at gsk.com.
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
“Risk factors” in GSK’s Annual Report on Form 20-F for 2023, and
GSK’s Q1 Results for 2024.
Registered in England & Wales:
GSK plc
No. 3888792
ViiV Healthcare Limited No. 06876960
Registered Office: GSK plc
980 Great West Road
Brentford, Middlesex
United Kingdom
TW8 9GS
ViiV Healthcare Limited GSK Medicines
Research Centre Gunnels Wood Road, Stevenage United Kingdom SG1
2NY
References
1 P. Ryan, et al. Non-inferior efficacy and less weight gain
when switching to DTG/3TC than when switching to BIC/FTC/TAF in
virologically suppressed people with HIV (PWH): the PASODOBLE
(GeSIDA 11720) randomised clinical trial. Presented at the 25th
International AIDS Conference. July 2024 2 Clinical Trials.gov -
DTG/3TC vs. BIC/FTC/TAF Maintenance Therapy in People Living
With HIV: (PASO-DOBLE). Available at
https://clinicaltrials.gov/ct2/show/NCT04884139. Last accessed July
2024
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