What Is Biktarvy Used For? FDA Indications, How It Works, and 5-Year Clinical Data – Sunny Pharma® | Patient Access Partner for Medication Information

Name: What Is Biktarvy Used For? FDA Indications, Mechanism & 5-Year Clinical Data (2026)
Creator: Ray Ashton
Published: 2026-03-07

Medically reviewed by Dr. Ranjit Mohan, MD

—

Written by Ray Ashton

— Updated March 20, 2026

Disclosure: This page is for education only and does not sell medication. No content here directs you toward any pharmacy or commercial service. All recommendations point to clinician-led decisions, manufacturer programs, and government resources. Read our editorial standards →

Biktarvy is the most widely prescribed HIV medication in the United States. But the question patients most often arrive with isn’t whether it works — it’s a more fundamental one: what is it actually for, and will it work for me?

This page answers that completely. It covers every FDA-approved indication including the July 2025 expansion, exactly how the drug works inside the body, who qualifies and who should not take it, and what five years of clinical data actually shows — including the resistance finding that no earlier HIV regimen has matched.

Quick Answer

Biktarvy is FDA-approved to treat HIV-1 infection in adults and children weighing at least 14 kg. It is a once-daily, single-tablet complete regimen delivering 98.6% viral suppression at 5 years with zero treatment-emergent resistance. It is not approved for HIV-2, PrEP, or PEP. It is not a cure — it suppresses the virus to undetectable levels when taken consistently every day.

What Is Biktarvy Used For — At a Glance 2026

FDA Approval Date

Feb 2018

Approved For

HIV-1

5-Year Viral Suppression

98.6%

Treatment-Emergent Resistance

Zero

Dosing

1 pill/day

US Generic Available?

No (~2036)

Clinical data: Studies 1489 and 1490, eClinicalMedicine / The Lancet, 2023. Indication data: FDA prescribing information, updated through July 2025.

Key Takeaways

Approved for HIV-1 only — not HIV-2, not PrEP, not PEP.
98.6% viral suppression at 5 years with zero treatment-emergent resistance in clinical trials.
July 2025 expansion added treatment-experienced adults restarting ART — broadest indication set of any single-tablet regimen.
One pill, once daily — no food requirement, no booster, complete regimen.
Absolute contraindication: dofetilide (Tikosyn) — life-threatening cardiac arrhythmia risk.
Undetectable ≠ cured — treatment must continue indefinitely; stopping causes viral rebound.

In This Guide

What Is Biktarvy?
FDA-Approved Indications (All, Including July 2025)
How Biktarvy Works Inside the Body
Who Can Take Biktarvy — and Who Should Not
5-Year Clinical Data
What Biktarvy Does Not Do
Dosing & Key Drug Interactions
Frequently Asked Questions

What Is Biktarvy?

Biktarvy (bictegravir/emtricitabine/tenofovir alafenamide) is a once-daily, single-tablet, complete HIV-1 treatment regimen developed by Gilead Sciences and first approved by the US FDA on February 7, 2018. It is a complete regimen in a single pill — one tablet, once daily, with or without food, is the entire treatment.

Component	Dose	Drug Class	Abbreviation
Bictegravir	50 mg	Integrase Strand Transfer Inhibitor (INSTI)	BIC / B
Emtricitabine	200 mg	Nucleoside Reverse Transcriptase Inhibitor (NRTI)	FTC / F
Tenofovir Alafenamide	25 mg	Nucleotide Reverse Transcriptase Inhibitor (NtRTI)	TAF

The combination is referred to as B/F/TAF or BIC/FTC/TAF in clinical literature. A lower-dose pediatric tablet (BIC 30 mg / FTC 120 mg / TAF 15 mg) is approved for children weighing 14–25 kg.

Important: Biktarvy is not a cure for HIV or AIDS. When taken consistently, it suppresses the virus to undetectable levels, keeping the immune system healthy, preventing AIDS-related illness, and stopping HIV transmission to others (U=U: Undetectable = Untransmittable). If treatment is stopped, the virus rebounds — typically within two to eight weeks.

FDA-Approved Indications (All, Including July 2025)

Biktarvy’s FDA label has been expanded five times since its 2018 approval. As of 2026, it covers six distinct patient populations — more than any other single-tablet HIV regimen currently available.

Patient Population	Key Criteria	Approval
Treatment-naïve adults	No prior antiretroviral treatment history	Feb 2018
Virologically suppressed adults & adolescents (≥25 kg)	HIV-1 RNA <50 copies/mL on stable regimen ≥3 months; no known resistance to BIC/FTC/TAF	Feb 2018
Children weighing ≥25 kg	Treatment-naïve or virologically suppressed	Jun 2019
Children weighing ≥14 kg	Virologically suppressed or treatment-naïve; uses 30/120/15 mg low-dose tablet	Oct 2021
Suppressed adults with M184V/I resistance	Pre-existing NRTI resistance including M184V/I; virally suppressed; no resistance to BIC or tenofovir	2024
Treatment-experienced adults restarting ART	Not currently virologically suppressed; restarting treatment; no known INSTI, FTC, or TFV resistance	Jul 2025 — New

What the July 2025 expansion means: Previously, treatment-experienced patients with a detectable viral load who were restarting ART had limited single-tablet options. Biktarvy is now the first INSTI-based single-tablet regimen FDA-approved and DHHS guideline-recommended for this population — provided they have no known resistance to the INSTI class, emtricitabine, or tenofovir.

Switching from another regimen

Adults already on a stable HIV regimen can switch to Biktarvy without a washout period, provided their viral load has been below 50 copies/mL for at least three months, they have no known resistance to any of Biktarvy’s components, and they are not taking contraindicated medications. Switch studies (GS-US-380-1878 and GS-US-380-1844) demonstrated virologic suppression was maintained in over 97% of patients following the switch.

How Biktarvy Works Inside the Body

HIV replicates through a defined sequence of steps. Biktarvy’s three components block that sequence at two separate checkpoints — which is why resistance to all three simultaneously is so clinically rare.

HIV enters the CD4 cell

The virus binds to CD4 and co-receptors on the T cell surface, fuses with the cell membrane, and injects its RNA genome and replication enzymes into the host cytoplasm. Biktarvy does not act at this step.

Reverse transcription — blocked by FTC + TAF

HIV’s reverse transcriptase converts viral RNA into DNA using natural nucleoside building blocks. FTC and TAF mimic those building blocks and get incorporated into the growing chain — but they lack the chemical group needed to continue extension, so the chain terminates and DNA synthesis stops before it can complete.

Integration — blocked by BIC

Any viral DNA that escapes the reverse transcription blockade must be inserted into the host chromosome by the viral integrase enzyme. BIC chelates the magnesium ions in the integrase active site, blocking strand transfer entirely. Without successful integration, HIV cannot produce new proteins, assemble new virions, or infect additional cells.

Viral load falls toward undetectable

With both checkpoints blocked, active HIV replication ceases. Plasma viral load typically falls below 50 copies/mL within 24–48 weeks in treatment-naïve patients. The immune system stabilizes and CD4 count recovers.

Why TAF instead of TDF?

Tenofovir alafenamide (TAF) is a prodrug that activates inside cells rather than in the bloodstream, reaching effective intracellular concentrations at a much lower oral dose than tenofovir disoproxil fumarate (TDF). The result is significantly lower plasma tenofovir exposure — and the reason Biktarvy shows better kidney and bone safety markers than TDF-containing regimens in five-year trials.

Why is resistance so rare?

HIV mutates rapidly. Using three agents from two drug classes means the virus would need to simultaneously develop mutations defeating all three mechanisms. Bictegravir also has a higher genetic barrier to resistance than first-generation integrase inhibitors like raltegravir, meaning partial mutations are insufficient to compromise it. In five years of clinical trials across hundreds of patients, this combination produced zero cases of treatment-emergent resistance.

The latent reservoir: Biktarvy suppresses active viral replication but does not eliminate HIV DNA from cells infected before treatment began. This latent reservoir is why therapy must continue indefinitely — stopping Biktarvy allows reservoir cells to reactivate and viral load to rebound, typically within two to eight weeks.

Who Can Take Biktarvy — and Who Should Not

✓ Appropriate Candidates

Treatment-naïve adults with HIV-1
Virologically suppressed adults switching regimens (RNA <50 c/mL for ≥3 months)
Children and adolescents weighing ≥14 kg
Adults with M184V/I resistance who are virologically suppressed
Treatment-experienced adults restarting ART (July 2025 expansion)
Patients with mild–moderate hepatic impairment (Child-Pugh A or B)
Patients on hemodialysis (virologically suppressed)

✗ Not Appropriate / Contraindicated

HIV-2 infection (not studied or approved)
PrEP or PEP (not approved for prevention)
Children weighing <14 kg
Currently taking dofetilide (Tikosyn) — absolute contraindication
Currently taking rifampin
Known resistance to BIC, FTC, or TAF
Severe hepatic impairment (Child-Pugh C)
eGFR <30 mL/min (non-dialysis, non-suppressed patients)

5-Year Clinical Data — What the Trials Show

Studies 1489 and 1490 were Phase 3 randomized trials comparing Biktarvy to dolutegravir-based regimens in treatment-naïve adults. Results at Week 240 were published in eClinicalMedicine (The Lancet journal family) in 2023 — the most complete long-term efficacy dataset for any single-tablet HIV regimen currently available.

98.6%

Viral suppression at Week 240 among patients with available data

Zero

Cases of treatment-emergent resistance through 240 weeks

<1%

Discontinued due to drug-related adverse events over 5 years

67.2%

Intent-to-treat suppression (missing = failure)

Understanding the two suppression figures

The 98.6% is an observed analysis — the proportion of patients still in the trial at Week 240 who had undetectable viral loads. The 67.2% uses intent-to-treat methodology, counting every patient who enrolled — including those lost to follow-up, who withdrew for non-drug reasons, or who died of unrelated causes — as treatment failures. The 98.6% answers does it work in patients who take it? The 67.2% answers of everyone who enrolled, how many were still suppressed five years later?

Outcome	Result	Notes
Viral suppression — observed analysis	98.6%	426 of 432 patients with available data at Week 240
Viral suppression — intent-to-treat	67.2%	Missing = failure; 426 of 634 enrolled
Treatment-emergent resistance	Zero	To BIC, FTC, or TAF through 240 weeks
Discontinuation due to drug AEs	<1%	Cumulative over 5 years
Diarrhea (most common side effect)	6%	Treatment-emergent, any grade
Nausea	6%	Treatment-emergent, any grade
Headache	5%	Treatment-emergent, any grade

On the resistance finding: Zero treatment-emergent resistance through 240 weeks is the most clinically distinctive finding in the Biktarvy dataset. In earlier integrase inhibitor trials, resistance emergence at five years — while low — was non-zero. This is the primary reason current DHHS guidelines recommend Biktarvy as a preferred regimen for most treatment-naïve patients.

For the complete side effects profile including kidney, bone, and metabolic monitoring: Biktarvy Side Effects: Complete Guide →

What Biktarvy Does Not Do

Biktarvy does not cure HIV

No approved antiretroviral eliminates the latent HIV reservoir. Biktarvy suppresses viral replication to undetectable levels, but HIV DNA persists in long-lived CD4 cells. If Biktarvy is stopped, viral rebound typically occurs within two to eight weeks in most patients.

Biktarvy is not a preventive medication (PrEP or PEP)

Biktarvy is a treatment for people already living with HIV-1. HIV-negative individuals seeking prevention should discuss FDA-approved PrEP options with a provider — options include Truvada (FTC/TDF) and Descovy (FTC/TAF). Biktarvy has not been studied for and is not approved for pre- or post-exposure prophylaxis.

Undetectable does not mean HIV is gone

“Undetectable” means HIV RNA is below the assay threshold (typically 20–50 copies/mL). The U=U framework (Undetectable = Untransmittable) is based on evidence that undetectable viral load during consistent treatment eliminates sexual transmission risk — not on the premise that the virus has been eliminated.

Biktarvy does not treat HIV-2

HIV-2 is a distinct viral species with different virological characteristics. Clinical data for Biktarvy in HIV-2 is absent. Patients with HIV-2 require a separately tailored regimen under expert guidance.

Dosing & Key Drug Interactions

Biktarvy is taken as one tablet orally once daily, with or without food. Consistency matters more than the specific hour — the long half-life of bictegravir (approximately 17–19 hours) provides a pharmacokinetic buffer against minor timing variations. Consecutive missed days, however, risk viral rebound.

Absolute contraindication — dofetilide (Tikosyn): Bictegravir inhibits the renal transporter that eliminates dofetilide, causing dangerous accumulation and risk of life-threatening cardiac arrhythmias. Do not take Biktarvy if you are on dofetilide under any circumstances.

Drug / Supplement	Interaction	Management
Dofetilide (Tikosyn)	Contraindicated	Do not combine under any circumstances
Rifampin	Contraindicated	Reduces bictegravir by ~75%; rifabutin with specialist guidance may be an option
St. John’s Wort	Avoid	CYP3A inducer; significantly lowers bictegravir and TAF levels
Carbamazepine, phenobarbital, phenytoin	Avoid	P-gp inducers that reduce TAF absorption
Antacids (Mg, Al, Ca)	Timing	Take Biktarvy 2 hrs before, or together with food
Iron / zinc / multivitamins	Timing	Take Biktarvy 2 hrs before, or together with food
Metformin	Monitor	BIC inhibits renal tubular transporters; may increase metformin exposure
Other HIV antiretrovirals	Do not add	Biktarvy is a complete regimen; do not combine without specialist guidance

For the full interactions guide: Biktarvy Drug Interactions: Complete Guide → and What Can You Not Take With Biktarvy? →

Frequently Asked Questions

What is Biktarvy used for? ▼

Biktarvy is FDA-approved to treat HIV-1 infection in adults and children weighing at least 14 kg. It covers treatment-naïve patients, virologically stable adults and children switching from another regimen, adults with pre-existing M184V/I resistance who are suppressed, and (as of July 2025) treatment-experienced adults restarting ART who are not virologically suppressed, provided they have no known INSTI, FTC, or tenofovir resistance. It is not a cure — it suppresses HIV to undetectable levels when taken daily.

Can Biktarvy be used to prevent HIV (PrEP)? ▼

No. Biktarvy is not approved for pre-exposure prophylaxis (PrEP) or post-exposure prophylaxis (PEP). It is a treatment for people already living with HIV-1. For PrEP, FDA-approved options include Truvada (FTC/TDF) and Descovy (FTC/TAF). Discuss PrEP options with an HIV specialist or sexual health provider.

What does Biktarvy actually do inside the body? ▼

Biktarvy blocks HIV replication at two separate stages. Emtricitabine (FTC) and tenofovir alafenamide (TAF) block the reverse transcriptase enzyme from converting HIV RNA into DNA. Bictegravir (BIC) blocks the viral integrase enzyme from inserting HIV DNA into the host cell’s chromosome. Together, these two blockades make it extremely difficult for the virus to replicate or develop resistance to all three components simultaneously.

How long has Biktarvy been shown to work? ▼

Studies 1489 and 1490 (published in eClinicalMedicine / The Lancet, 2023) followed patients for 240 weeks — approximately five years. Among the 432 patients with available data at Week 240, 98.6% maintained HIV-1 RNA below 50 copies/mL. Zero cases of treatment-emergent resistance were detected through the entire period. Fewer than 1% of patients stopped Biktarvy due to drug-related adverse events over 5 years.

What is Biktarvy’s drug class? ▼

Biktarvy is a complete fixed-dose combination combining three drug classes: bictegravir is a second-generation integrase strand transfer inhibitor (INSTI); emtricitabine is a nucleoside reverse transcriptase inhibitor (NRTI); tenofovir alafenamide is a nucleotide reverse transcriptase inhibitor (NtRTI). The INSTI + dual NRTI combination is the backbone of current HIV treatment guidelines.

Who should not take Biktarvy? ▼

Biktarvy must not be taken with dofetilide (Tikosyn) — an absolute contraindication due to potentially fatal cardiac arrhythmia risk — or with rifampin. It is also not appropriate for patients with known resistance to BIC, FTC, or TAF; children under 14 kg; severe renal impairment (CrCl below 30 mL/min) in non-dialysis, non-suppressed patients; severe hepatic impairment (Child-Pugh C); or HIV-2, for which it is not approved.

Does Biktarvy work for HIV-2? ▼

No. Biktarvy is approved for HIV-1 only. HIV-2 is a distinct viral species with different virological characteristics, and clinical data for Biktarvy in HIV-2 is absent. People with HIV-2 require a separately tailored regimen developed in consultation with an HIV specialist experienced in HIV-2 management.

Can Biktarvy be taken once a day? ▼

Yes. Biktarvy is a once-daily, single-tablet regimen — one pill, once per day, with or without food. No food requirement, no pharmacokinetic booster, no additional HIV drugs needed. The long half-life of bictegravir (approximately 17–19 hours) supports once-daily dosing without compromising efficacy.

When will a generic Biktarvy be available in the US? ▼

Based on current patent analysis, the earliest estimated date for generic Biktarvy entry in the United States is November 8, 2036. Biktarvy is protected by 9–13 US patents and regulatory exclusivity expiring in 2031. No US generic is approved or imminent as of 2026. Patients facing cost barriers should contact Gilead’s PAP line at 1-800-226-2056, or find a Ryan White clinic at findhivcare.hrsa.gov.