Dolutegravir plus lamivudine as simplification dual therapy in virologically suppressed HIV-1 infected subjects

Laura Comi1*, Elisa Di Filippo1, Franco Maggiolo1

1Division of Infectious Diseases, ASST Papa Giovanni XXIII, Bergamo, Italy


Introduction: The use of combination antiretroviral therapy (cART) containing three active drugs from at least two different classes is the standard of care for HIV treatment worldwide. The availability of newer drugs with improved potency and tolerability and higher barrier to the development of resistance allows exploring the feasibility of ARV-sparing strategies, namely dual therapies. A dual therapy based on dolutegravir plus lamivudine could be an intriguing simplification strategy for individuals with stable HIV suppression on cART.

Results: Seven studies of dual therapy regimens based on dolutegravir plus lamivudine were critiqued. All of them report a low rate of therapeutic failure due to any cause and a small number of virologic failures. More important virologic failures were not associated with loss of future option as no resistance inducing mutation to ongoing drugs emerged. On the safety side, after the switch, very few short-term adverse events leading to treatment discontinuation were observed and surrogate markers of long term toxicities such as changes in lipid profile and renal function were minimally influenced or improved.

Discussion: Dolutegravir plus lamivudine as a switch option in patients with sustained viral control is still to be considered an experimental approach. Although small in number and heterogeneous in nature the studies that evaluated the effectiveness of dolutegravir plus lamivudine dual therapy have documented substantial virologic efficacy and tolerability of the regimen without exposing patients to the risk of selecting for INSTI-inducing resistance mutations.


Introduction

The use of combination antiretroviral therapy (cART) containing three active drugs from at least two different classes began in the mid-1990s, and since then has been the standard of care for HIV treatment worldwide. Current HIV treatment guidelines recommend first line anti-retroviral (ARV) regimens consisting of two nucleoside reverse transcriptase inhibitors as a backbone combined with a third agent from either the non-nucleoside reverse transcriptase inhibitor, or the boosted protease inhibitor (PI), or the integrase strand transfer inhibitor (INSTI) classes1-2. Advances in the virologic and safety profiles of antiretroviral drugs have created opportunities to investigate alternative approaches. The availability of newer drugs with improved potency and tolerability and higher barrier to the development of resistance allows exploring the feasibility of ARV-sparing strategies, namely dual therapies. Potential advantages of two-drug regimens include reduced long-term toxicity, complexity, and costs3. This approach may result particularly suited for maintenance therapy in patients with steadily controlled viral replication, who wish or need to simplify cART.

In these settings, several experiences of 2-drugs regimens based on a boosted PI plus lamivudine (3TC) have demonstrated favorable results in terms of efficacy, but are somehow penalized by metabolic side effects and risk for drug-drug interactions4-5.

Dolutegravir (DTG) is a potent INSTI, exhibiting a rapid reduction in viral load (VL) and a high barrier to resistance. DTG is a once daily drug, well tolerated, that can be taken with or without food, with a low potential for drug-drug interactions and a high genetic barrier. Maintenance therapy with DTG plus rilpivirine was comparable to standard triple cART in largely randomized trials6. A possible alternative and intriguing simplification strategy for individuals with stable HIV suppression on cART is the use of a dual therapy based on dolutegravir plus lamivudine, a potent cytidine nucleoside analogue without major side effects, and that has a well-proven safety profile7.

In this paper, we review all available data of the DTG+3TC combination in pre-treated HIV positive patients in order to offer a comprehensive evaluation of this option that is already used in clinical practice although it should still be considered as experimental.

We searched Medline, Embase, Cochrane central and web of science, as well as abstract of major HIV conferences for studies which included HIV-infected individuals with undetectable viral load on triple antiretroviral therapy who switched to DGT+3TC dual therapy.

DTG+3TC is an investigational 2-drug regimen potential for co-formulation into a once daily single tablet regimen with lower cART cost8. In the proof-of-concept PADDLE study9, 18/20 naïve patients, with baseline HIV-RNA < 100,000 copies/ml and CD4 count > 200 cells/mcL, had a viral load < 50 copies/ml 96 weeks after starting DTG+3TC dual therapy. In the ACTG 5353 pilot study 120 naïve subjects received DTG+3TC and were virologically evaluated by FDA snapshot analysis after 24 weeks10. Virologic efficacy was demonstrated in 108/120 patients. Three patients experienced virologic failure and one of them selected for the M184V reverse transcriptase and the R263K integrase mutations.

Overall DTG+3TC in switch studies demonstrated a low rate of therapeutic failure for any cause and a very low rate of virologic failures (table 1).

Table 1: Summary of studies on DTG+3TC in experienced patients
Study Type Country Patients on DTG+3TC Number (median)/
Time (years) on previous ARV
Presence of mutations prior to switch Virological failure Discontinuation due to adverse events/ any
DOLAM [11] Open-label randomized trial Spain 29 /
>1 years
NO 1
No resistance
0
Taiwo[12] Randomized clinical trial USA 44 /
5.7 years
NO 1 1/2
LAMIDOL [13] Single arm trial France 104 /
4 years
NO 1
No resistence
1/3
DOLULAM [14] Prospective cohort France 27 /
17 years
YES 0 (2 blips) 0/3
Maggiolo [16] Prospective, cohort Italy 203 3/
10.3 years
NO 0 5/12
Borghetti [17] Retrospective, cohort Italy 183 /
9 years
YES 3
No resistence
11/21
Hidalgo- Tenorio [18] Retrospective cohort Spain 105 3/
13 years
Not reported 0 (2 blips) 0
Yagci Caglayik [19] Retrospective cohort Turkey 32 3/
13 years
Not reported 0 0

So far only two randomized studies on DTG+3TC simplification have been published. Blanco and Colleagues, enrolled in an open label, non inferiority, randomized controlled trial (DOLAM study)11 91 HIV infected adults on stable triple ART. All of them had a viral load of less than 50 copies/ml in the last year, no prior viral failure or resistance mutations to 3TC/FTC or INSTI, and a negative HBsAg. They were randomized 1:1:1 to continue triple cART (control), or switch to either DTG+3TC or DTG monotherapy. After 24 weeks of follow-up, 3 patients prematurely discontinued due to low-level viral failure: 1 patient in the dual group, without the emergence of resistance conferring mutations, and 2 patients in the dolutegravir monotherapy arm, with evidence of resistance mutations. As a consequence, the Data Safety Monitoring Board recommended stopping DTG monotherapy and allowed the DTG+3TC arm to be continued.

The second study, recently published by Taiwo. et al12, is a pilot randomized clinical trial in which 90 HIV infected adults, virologically suppressed on stable triple ARV, without history of virologic failure and negative hepatitis B surface antigen were randomized to continue triple ART (45 pts) or switch to DTG+3TC (44 pts).After 48 weeks of follow-up, only 1 patient in the DTG + 3TC arm showed an HIVRNA > 50 cp/ml, without the emergence of viral mutations.

The LAMIDOL trial13 is an open label, single arm trial, in which 110 virologically suppressed patients, on a first line cART based on a classic triple drug combination were enrolled in 19 Clinics in France. They were first switched to dolutegravir as a substitute for the third agent and then, after 8 weeks, received DTG+3TC. One hundred and four patients started DTG+3TC: of those 86% were males, 70% MSM with a median age of 45 years and a median time since HIV diagnosis of 6.3 years (2.3-24.5). At week 48 of follow-up 3 therapeutic failures, only one due to virological failure, were observed.

Most patients enrolled in all the above-mentioned studies were on their first or second-line therapies. However, most of the data on the DTG+3TC strategy have been generated by clinical cohorts, which comprehended heavily pre-treated patients on ART for a longer time, in some cases longer than 10-15 years and with a median of 3 different antiretroviral regimens prior to the switch.

A small prospective cohort (DOLULAM)14 enrolled 27 patients that had been taking cART for a median of 215 months (IQR 22-239) and the last therapy for a median of 51 (IQR 13-108) months. All patients received dolutegravir plus lamivudine, even if ten of them had evidence of M184V mutation in a previous genotypic test prior switch with the evidence of M184V mutation. No virological failure was reported after a median follow-up time of 96 weeks.

An Italian prospective, multi-center, cohort study, enrolled 203 patients that were on stable cART, with a confirmed viremia <50 copies/ml in the last six months, in the absence of M184V mutation or HBsAg positivity15-16. All needed to switch therapy due to clinically relevant reasons such as concomitant diseases, altered laboratory tests, drug adverse events or risk of drug-to-drug interactions.

Patients enrolled were mostly men (75.4%) with a median age of 52 years (IQR 47-58). At switch patients were on ARV drugs for a median of 10.3 years (IQR 5.5-17-6), virologically suppressed for a median of 72 months (IQR 33-121) and experienced a median of three therapeutic lines.

All subjects were prospectively followed up to week 48, and all remained on the dual therapy during the whole period. Neither virological failure nor viral blip was detected15. According to a more recent report with extended follow-up, 12 patients stopped therapy after week 4816.

Another Italian cohort study retrospectively evaluated 494 cART-experienced and virologically suppressed HIV positive patients, according to different simplification strategies (lamivudine+boosted PIs versus DTG+3TC). One-hundred eighty-three subjects received dolutegravir, 170 switched to darunavir and 141 to atazanavir. Groups differed for age, HIV risk-factor, time since HIV diagnosis, time on antiretroviral therapy, previous cART regimen and reasons for switching17.

Time to treatment discontinuation, due to any reason, and virological failure were the endpoints compared by Kaplan-Meier estimator. Probabilities of remaining on the considered treatment at week 48 and 96 were respectively: 79.8% and 48.3% for darunavir, 87% and 70.9% for atazanavir, 88.2% and 82.6% for dolutegravir. Moreover, among patients who discontinued, virological failure was the cause in 3/21 cases in the dolutegravir group, 6/123 in the darunavir group and 4/97 in the atazanavir group17.

Furthermore, a recent Spanish cohort18 reported 105 patients treated for a median of 13 years with a median of 3 different cART combinations. Baseline HIV-RNA was < 50 copies/ml in 96.2% of cases, and they had a median CD4 count of 732 cells/mcL. The most frequent reasons for the switch were simplification (39%) and toxicity (44.8%). Eighty-four of them performed at least an HIV-RNA test after the therapeutic switch to DTG+3TC and over a median follow-up of 23 weeks. Viral load was < 50 copies/ml in 97.2 subjects, showing the last 2 individuals viral blips of 55 and 239 copies/ml, respectively.

Finally, in a small Turkish cohort study19, 32 patients were included from 6 centers. Twenty-nine patients were virologically suppressed before switch, three patients had HIV-RNA levels 21503, 656 and 59 copies/mL. No patient experienced virologic failure with prior regimens. CD4 T cell counts were > 200 cells/mm3 in all patients, except one (90 cells/mm³) before switch. No patient experienced serious adverse events, AIDS-related events, or died during the follow-up period. Authors defined DTG+3TC combination as efficient and well tolerated, and did not report any virologic failure.

The main rationale for dual therapy is to optimize health status and quality of life without compromising control of HIV infection. Very few short-term adverse events leading to treatment discontinuation were observed in DTG+3TC studies. No patient stopped therapy because of an adverse event in the Spanish cohort18, in the DOLAM study11, or in a Turkish cohort19 in which 32 patients were switched to DTG-3TC because of documented renal toxicity or renal impairment, hyperlipidemia, adverse events with current cART, prevention of potential toxicities and regimen simplification. In a recent update of a previously described cohort16, 5/203 patients discontinued treatment for intolerance, being muscle aches the most common cause. In the same cohort 3 patients died, but because of underlying diseases unrelated to HIV or therapy16. In the LAMIDOL trial,13 8/110 patients stopped therapy because of an adverse event and 4 of them were possibly related to DTG use. As a whole, studies on DTG+3TC did not report a relevant occurrence of CNS related adverse events.

There are a few data about long-term adverse effects of DTG + 3TC and most of them are based on surrogate markers such as changes in lipid profile and renal function. Both the Italian cohorts investigated the metabolic assets of patients after the switch with substantially similar results15,17. The authors registered a decrease in median triglycerides and total cholesterol, an increment of HDL-cholesterol and a reduction of median LDL-cholesterol. Changes were, however, limited: total cholesterol -7 mg/dL (p=0.047); LDL-cholesterol -7 mg/dL (p=0.335), HDL-cholesterol + 4 mg/dL (p= 0.047) and triglycerides -31 mg/dL (p= 0.012) in the first cohort16 and total cholesterol -24 mg/dL (p< 0.01); LDL-cholesterol – 15 mg/dL (p=0.009) and triglycerides – 66 mg/dL (p< 0.001) in the second cohort14. The clinical implications of these results are still to be elucidated.

Kidney function was evaluated in both Italian cohort15-17 and in the DOLULAM study14 and the dual combination was not associated with a decline in renal function. However, it must be noted that a relevant proportion of subjects included in these studies were previously exposed to tenofovir whose withdrawal could partially influence the outcome.

Dual antiretroviral therapy seeks to reduce toxicities and improve quality of life by reducing the drug burden. Toxicities associated with antiretroviral agents are often drug class specific. Nucleoside analogs use has been commonly associated with mitochondrial toxicity (lipoathrophy, functional kidney dysfunction, cardiovascular accidents, and osteoporosis)20,21.

So far, however, the need of maintaining the efficacy and convenience of robust cART limited clinicians’ options.

Dolutegravir, similarly to boosted-darunavir, is characterized by a high affinity to its target, resulting in strong and sustained binding22. As a consequence, in vitro selection of mutants resistant to dolutegravir is very difficult. To date, no emergent dolutegravir-resistant virus has ever been reported in a patient in whom dolutegravir was prescribed as a first INI23.

Dolutegravir plus lamivudine as a switch option in patients with sustained viral control is still to be considered an experimental approach, that finds a contraindication in chronic hepatitis B co-infected patients. So far, 7 DTG+3TC switch studies evaluated the effectiveness of this dual therapy regimen.

Although small in numbers and heterogeneous in nature these experiences have documented a substantial virologic efficacy and tolerability of the dual regimen without exposing patients to the risk of selecting for INSTI-inducing resistance mutations.

Two randomized study (DOLAM study and ASPIRE study)11,12 provide a preliminary comparative evidence that virologic suppression is similar to that obtained with standard cART. In these studies, only 2 patient (one in each study) discontinued due to low-level viral failure and without losing future options as, at failure, there was no evidence of induced resistance mutations. The other studies support this result.

The dual therapy is substantially well tolerated without specific signature adverse events and with evidence of a neutral effect on lipid parameters and on kidney function.

Altogether, these data suggest that a dual therapy with DTG+3TC in treatment experienced and virologically suppressed patients contributes to set up the new paradigm of induction-maintenance in the management of HIV treatment24. Up to date, however, the scattered nature of data, the type of studies, mostly observational, and the limited experience both in terms of number of treated subjects and on time on active follow-up do not allow to make a definitive point about how much the dual therapeutic option would be advantageous for chronically infective patients. This is a limit of the present review, too.

Finally, dual therapy with dolutegravir plus lamivudine could also be an option to contain therapeutic costs, which is an aspect of increasing relevance worldwide. Using a mathematical simulation, a group of American researchers projected the clinical and economic outcomes of 4 different therapeutic strategies over a period of five years. They demonstrated that DTG + 3TC could result in cost-effective allowing for a global reduction of more than 500 million dollars in cART costs in the United States over the considered time period8.

Despite the fact that the newest dual regimens such as DTG+3TC could save money, reduce toxicity and spare drug options for the future, the observational and non-randomized nature of most studies, the limited number of subjects treated and the limited follow-up should induce caution when this approach is used in clinical practice. A large, worldwide, randomized, clinical study involving 550 experienced patients has recently started recruitment and will hopefully reframe the picture in the near future25.

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Article Info

Article Notes

  • Published on: February 24, 2018

Keywords

  • Dolutegravir

  • Lamivudine
  • Dual therapy
  • INSTI
  • Virological failure
  • Maintenance therapy

*Correspondence:

Dr. Laura Comi
Division of Infectious Diseases
ASST Papa Giovanni XXIII, Bergamo, Italy
Email: lalla.comi@gmail.com