PeptidesCategoriesResearch

Enfuvirtide

Enfuvirtide (T-20, Fuzeon) is a 36-amino acid synthetic peptide derived from the HR2 region of HIV-1 gp41. It is the first FDA-approved HIV fusion inhibitor (2003), blocking viral entry by preventing six-helix bundle formation required for membrane fusion.

Enfuvirtide (T-20, marketed as Fuzeon) is a 36-amino acid synthetic peptide that mimics the heptad repeat 2 (HR2) region of the HIV-1 transmembrane glycoprotein gp41. By binding to the HR1 region of gp41 during the conformational change triggered by CD4/co-receptor engagement, enfuvirtide prevents formation of the six-helix bundle structure required for viral-host membrane fusion, thereby blocking HIV-1 entry into target cells.

Overview

Enfuvirtide emerged from pioneering work by Carl Wild and Tom Matthews at Duke University in the early 1990s, who identified that synthetic peptides corresponding to the C-terminal heptad repeat (HR2) of HIV-1 gp41 could potently inhibit HIV-1 infection in vitro (Wild et al., 1994). The peptide exploits a critical vulnerability in the HIV entry mechanism: after the viral envelope glycoprotein gp120 binds CD4 and a co-receptor (CCR5 or CXCR4), gp41 undergoes a dramatic conformational rearrangement exposing its HR1 coiled-coil trimer. Enfuvirtide binds this transient HR1 intermediate, competitively blocking the interaction between HR1 and HR2 that would normally drive six-helix bundle formation and membrane fusion.

The development of enfuvirtide by Trimeris (later acquired by Roche) represented a proof-of-concept that viral entry could be therapeutically targeted with peptide drugs. Its clinical utility, however, has been constrained by the requirement for twice-daily subcutaneous injections, significant injection site reactions, high manufacturing cost, and the emergence of resistance mutations in the gp41 HR1 domain. Enfuvirtide is therefore reserved primarily for heavily treatment-experienced patients in salvage regimens where other active agents are limited.

Mechanism of Action

Enfuvirtide's mechanism targets the HIV-1 entry process at the membrane fusion step:

  • HR1 binding: After gp120 engages CD4 and a co-receptor, gp41 extends its N-terminal fusion peptide toward the host cell membrane and exposes the HR1 coiled-coil trimer. Enfuvirtide binds this HR1 trimer in a dominant-negative fashion, mimicking the endogenous HR2 domain and preventing the native HR1-HR2 interaction (Chan et al., 1997).
  • Six-helix bundle inhibition: The formation of the thermostable six-helix bundle (6-HB), in which three HR2 helices pack into the grooves of the HR1 trimer, is the energy source driving membrane fusion. By occupying the HR2-binding groove on HR1, enfuvirtide arrests this process at a pre-fusion intermediate state (Weissenhorn et al., 1997).
  • Entry-stage specificity: Unlike reverse transcriptase or protease inhibitors, enfuvirtide acts extracellularly at the viral entry step, before the viral genome enters the host cell. This provides a mechanistically distinct target for combination therapy (Kilby et al., 1998).
  • Strain specificity: Enfuvirtide is primarily active against HIV-1; it has limited activity against HIV-2 due to sequence divergence in the gp41 HR1 domain.

Reconstitution Calculator

Reconstitution Calculator

Calculate your peptide dosing

Draw Volume
0.100mL
Syringe Units
10units
Concentration
2,500mcg/mL
Doses / Vial
20doses
Vial Total
5mg
Waste / Vial
0mcg
Syringe Cap.
100units · 1mL
How to reconstitute
Gather & prepare
1/6Gather & prepare

Set up a clean workspace with all supplies ready.

1.Wash hands thoroughly, put on disposable gloves
2.Your 5mg peptide vial (lyophilized powder)
3.Bacteriostatic water (you'll need 2mL)
4.A 3–5mL syringe with 21–25 gauge needle for reconstitution
5.Alcohol swabs (70% isopropyl)
Use bacteriostatic water (0.9% benzyl alcohol) for multi-dose vials. Sterile water is only safe for single-use.
Supply Planner

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2vials
28 doses20 days/vial12 leftover
Cost Breakdown
Vial price
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$0.00 /week$0 /month
Store 2-8°C30 day shelf lifeSwirl gentlyFor research purposes only

Research

Pivotal Clinical Trials (TORO-1 and TORO-2)

The FDA approval of enfuvirtide was based on two large, randomized, open-label Phase III trials — TORO-1 (North America/Brazil) and TORO-2 (Europe/Australia) — conducted in treatment-experienced patients with triple-class antiretroviral resistance. Lalezari et al. (2003) reported TORO-1 results: enfuvirtide plus optimized background regimen (OBR) achieved a mean viral load reduction of 1.696 log₁₀ copies/mL at 24 weeks, compared to 0.764 log₁₀ with OBR alone. Lazzarin et al. (2003) reported concordant TORO-2 results with similar virological and immunological benefits. Combined 48-week data showed durable viral suppression in a significant proportion of patients with otherwise limited treatment options (Nelson et al., 2005).

Resistance

Resistance to enfuvirtide develops through mutations in the HR1 domain of gp41, primarily at positions 36-45 (HXB2 numbering). Wei et al. (2002) characterized the key resistance mutations, with G36D/S, V38A/M/E, Q40H, N42T, and N43D being most commonly observed. These mutations alter the HR1 groove geometry, reducing enfuvirtide binding affinity. Notably, some resistance mutations impose a fitness cost on the virus, as they can impair the efficiency of six-helix bundle formation (Lu et al., 2006).

Salvage Therapy

Enfuvirtide's value in salvage therapy has been demonstrated in patients with extensive resistance to nucleoside/nucleotide reverse transcriptase inhibitors, non-nucleoside reverse transcriptase inhibitors, and protease inhibitors. When combined with newer agents such as darunavir, tipranavir, raltegravir, or maraviroc, enfuvirtide contributes to achieving viral suppression in highly treatment-experienced populations (Hicks et al., 2006).

Safety Profile

Enfuvirtide's safety profile is well characterized from clinical trials and extensive post-marketing experience:

  • Injection site reactions (ISRs): Occur in ~98% of patients; pain, induration, erythema, nodules, and pruritus at injection sites. ISRs are the most common reason for discontinuation. Rotating injection sites and proper technique reduce severity (Ball et al., 2003).
  • Hypersensitivity: Rare (<1%) systemic hypersensitivity reactions including rash, fever, nausea, rigors, and hypotension; enfuvirtide should be discontinued and not rechallenge.
  • Bacterial pneumonia: A higher rate of bacterial pneumonia was observed in enfuvirtide arms of TORO trials (4.68 vs 0.61 events per 100 patient-years); causal relationship uncertain.
  • Eosinophilia: Observed in some patients; generally asymptomatic.
  • Immune reconstitution: As with all effective antiretrovirals, immune reconstitution inflammatory syndrome (IRIS) may occur in patients with profound immunosuppression.

Pharmacokinetic Profile

Enfuvirtide — Pharmacokinetic Curve

90 mg subcutaneous injection twice daily
0%25%50%75%100%0m3.8h7.6h11.4h15.2h19hTimeConcentration (% peak)T_max 1.5hT_1/2 3.8h
Half-life: 3.8hT_max: 1.5hDuration shown: 19h

Quick Start

Route
90 mg subcutaneous injection twice daily

Molecular Structure

2D Structure
Enfuvirtide molecular structure
Molecular Properties
Formula
C204H301N51O64
Weight
4492 Da
PubChem CID
16130199
Exact Mass
4491.1934 Da
LogP
-14.7
TPSA
1900 Ų
H-Bond Donors
63
H-Bond Acceptors
67
Rotatable Bonds
151
Complexity
11200
Identifiers (SMILES, InChI)
InChI
InChI=1S/C204H301N51O64/c1-20-102(15)166(253-195(310)137(75-100(11)12)239-200(315)150(93-258)251-190(305)143(82-112-90-215-95-219-112)248-203(318)167(103(16)21-2)254-196(311)138(76-101(13)14)240-201(316)151(94-259)252-204(319)168(105(18)260)255-197(312)139(221-106(19)261)78-108-45-47-113(262)48-46-108)202(317)233-131(58-68-164(280)281)178(293)228-130(57-67-163(278)279)182(297)250-149(92-257)198(313)232-125(52-62-155(210)266)179(294)245-145(84-157(212)268)191(306)229-124(51-61-154(209)265)175(290)224-122(49-59-152(207)263)173(288)226-126(53-63-159(270)271)176(291)222-120(43-31-33-69-205)172(287)244-144(83-156(211)267)192(307)231-127(54-64-160(272)273)177(292)225-123(50-60-153(208)264)174(289)227-128(55-65-161(274)275)180(295)235-134(72-97(5)6)185(300)237-133(71-96(3)4)184(299)230-129(56-66-162(276)277)181(296)236-135(73-98(7)8)187(302)247-147(86-165(282)283)194(309)223-121(44-32-34-70-206)171(286)241-140(79-109-87-216-117-40-28-25-37-114(109)117)183(298)220-104(17)170(285)249-148(91-256)199(314)238-136(74-99(9)10)186(301)242-142(81-111-89-218-119-42-30-27-39-116(111)119)189(304)246-146(85-158(213)269)193(308)243-141(80-110-88-217-118-41-29-26-38-115(110)118)188(303)234-132(169(214)284)77-107-35-23-22-24-36-107/h22-30,35-42,45-48,87-90,95-105,120-151,166-168,216-218,256-260,262H,20-21,31-34,43-44,49-86,91-94,205-206H2,1-19H3,(H2,207,263)(H2,208,264)(H2,209,265)(H2,210,266)(H2,211,267)(H2,212,268)(H2,213,269)(H2,214,284)(H,215,219)(H,220,298)(H,221,261)(H,222,291)(H,223,309)(H,224,290)(H,225,292)(H,226,288)(H,227,289)(H,228,293)(H,229,306)(H,230,299)(H,231,307)(H,232,313)(H,233,317)(H,234,303)(H,235,295)(H,236,296)(H,237,300)(H,238,314)(H,239,315)(H,240,316)(H,241,286)(H,242,301)(H,243,308)(H,244,287)(H,245,294)(H,246,304)(H,247,302)(H,248,318)(H,249,285)(H,250,297)(H,251,305)(H,252,319)(H,253,310)(H,254,311)(H,255,312)(H,270,271)(H,272,273)(H,274,275)(H,276,277)(H,278,279)(H,280,281)(H,282,283)/t102-,103-,104-,105+,120-,121-,122-,123-,124-,125-,126-,127-,128-,129-,130-,131-,132-,133-,134-,135-,136-,137-,138-,139-,140-,141-,142-,143-,144-,145-,146-,147-,148-,149-,150-,151-,166-,167-,168-/m0/s1
InChIKeyPEASPLKKXBYDKL-FXEVSJAOSA-N

Research Protocols

subcutaneous Injection

Its clinical utility, however, has been constrained by the requirement for twice-daily subcutaneous injections, significant injection site reactions, high manufacturing cost, and the emergence of resistance mutations in the gp41 HR1 domain.

GoalDoseFrequency
Adults90 mgTwice daily
Pediatrics (6-16 years)2 mg, 90 mgTwice daily
Reconstitution108 mgPer protocol

What to Expect

What to Expect

Onset

Effects begin within hours of administration based on half-life of 3.8 hours

Month 9-12

Combined 48-week data showed durable viral suppression in a significant proportion of patients with otherwise limited treatment options .

Daily Use

Due to short half-life (3.8 hours), effects are expected per-dose; consistent daily administration maintains therapeutic levels

Ongoing

Regular administration schedule required; effects are dose-dependent and do not persist between doses

Quality Indicators

What to look for

  • Phase 3 clinical trial data available
  • Extensive peer-reviewed research base

Caution

  • Injection site reactions reported

Frequently Asked Questions

References (13)

  1. [1]
    Wild CT, Shugars DC, Greenwell TK, et al Peptides corresponding to a predictive alpha-helical domain of human immunodeficiency virus type 1 gp41 are potent inhibitors of virus infection Proc Natl Acad Sci USA (1994)
  2. [2]
    Chan DC, Fass D, Berger JM, Kim PS Core structure of gp41 from the HIV envelope glycoprotein Cell (1997)
  3. [3]
    Weissenhorn W, Dessen A, Harrison SC, Skehel JJ Atomic structure of the ectodomain from HIV-1 gp41 Nature (1997)
  4. [4]
    Kilby JM, Hopkins S, Venetta TM, et al Potent suppression of HIV-1 replication in humans by T-20, a peptide inhibitor of gp41-mediated virus entry Nat Med (1998)
  5. [5]
    Lalezari JP, Henry K, O'Hearn M, et al Enfuvirtide, an HIV-1 fusion inhibitor, for drug-resistant HIV infection in North and South America N Engl J Med (2003)
  6. [6]
    Lazzarin A, Clotet B, Cooper D, et al Efficacy of enfuvirtide in patients infected with drug-resistant HIV-1 in Europe and Australia N Engl J Med (2003)
  7. [7]
    Wei X, Decker JM, Liu H, et al Emergence of resistant human immunodeficiency virus type 1 in patients receiving fusion inhibitor (T-20) monotherapy Antimicrob Agents Chemother (2002)
  8. [8]
    Nelson M, Arasteh K, Clotet B, et al Durable efficacy of enfuvirtide over 48 weeks in heavily treatment-experienced HIV-1-infected patients in the T-20 versus optimized background regimen only 1 and 2 clinical trials J Acquir Immune Defic Syndr (2005)
  9. [9]
    Lu J, Deeks SG, Hoh R, et al Rapid emergence of enfuvirtide resistance in HIV-1-infected patients J Acquir Immune Defic Syndr (2006)
  10. [10]
    Hicks CB, Cahn P, Cooper DA, et al Durable efficacy of tipranavir-ritonavir in combination with an optimised background regimen of antiretroviral drugs AIDS (2006)
  11. [11]
    Patel et al — Long-acting HIV fusion inhibitors: next-generation peptide and lipopeptide derivatives of enfuvirtide (2023)
  12. [12]
    Chong et al — Development of HIV-1/2 broadly cross-reactive fusion inhibitors with enhanced potency and resistance profile (2022)
  13. [13]
    Dwyer et al — Enfuvirtide in clinical practice: sustained efficacy and evolving role in the era of integrase inhibitors (2022)
Updated 2026-03-0810 citationsSources: peptide-wiki-mdx, pubchem, peptide-wiki-mdx-v2

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On this page

Overview
Reconstitution Calculator
Mechanism of Action
Research
Pivotal Clinical Trials (TORO-1 and TORO-2)
Resistance
Salvage Therapy
Safety Profile
Pharmacokinetic Profile
Quick Start
Molecular Structure
Research Protocols
What to Expect
Quality Indicators
FAQ
References
Related Peptides