Fostemsavir (FTR) is the first FDA-approved attachment inhibitor indicated for heavily treated adults with multidrug-resistant HIV-1 (Gulick, 2018). FTR is a prodrug of the active molecule temsavir, which inhibits the HIV-1 gp 120 conformational changes needed for CD4 attachment, preventing viral entry into susceptible cells (Cahn et al., 2018). The efficacy and safety of fostemsavir has been evaluated in a partially randomized, double-blind, placebo-controlled clinical trial (BRIGHTE), which enrolled 371 highly treatment-experienced patients who have failed their current regimen (Kozal et al., 2020; Lataillade et al., 2020). FTR showed sustained rates of virologic suppression over the 96 weeks of clinical trial: the proportion of participants who achieved undetectable HIV viral load was 53% at week 24, 54% at week 48, and 60% at week 96 and CD4⁺ T-cell recovery was recorded even in the most immunocompromised patients (participants with less than 20 cells/mm³ at baseline had a mean CD4⁺ T-cell increase of 240 cells/mm³ at week 96) (Ackerman et al., 2021).

The most commonly reported adverse effects for FTR included nausea, vomiting, diarrhea, and headache. Temsavir is partly metabolized by CYP3A4 enzyme, and it is contraindicated with any strong CYP3A4 inducers (carbamazepine, rifampin) (Hiryak and Koren, 2021).

Monoclonal antibodies are becoming attractive strategies for HIV treatment, with good resistance profile, ability to restore CD4 T-cell count and lack of toxicity.

Ibalizumab (IBA)- the first monoclonal antibody approved for the treatment of HIV-1 infection (Markham, 2018)- is a long-acting post-attachment inhibitor, which binds to the extracellular CD4 domain, leading to conformational changes of the CD4 T cell receptor–gp120 complex and blocking HIV entry (Chahine and Durham, 2021). Importantly, the binding of IBA to CD4 cell receptors does not induce an immunosuppressive response. Ibalizumab, in combination with other antiretrovirals, is indicated for the treatment of heavily treatment-experienced adults with multidrug-resistant HIV-1 infection with limited or no other treatment options (Markham, 2018) and it is designed for twice-monthly intravenous administration (Chahine and Durham, 2021).

The approval of ibalizumab was based on a phase III, single-group, open-label study (TMB-301), that enrolled 40 heavily treatment-experienced HIV patients who had failed several antiretroviral regimens, had >1,000 copies/mL HIV viral load and resistance to at least one NRTI, NNRTI, and a PI (Emu et al., 2018). The results showed that ibalizumab significantly decreased the viral load 7 days after being added to the failing antiretroviral regimen. Furthermore, ibalizumab plus an individually optimized background regimen significantly reduced the HIV-1 viral load at week 25, viral suppression being reported in 43% of the study participants and increased the CD4 T cell count with a mean of 62 cells/mm³.

Ibalizumab was well tolerated in the TMB-301 clinical trial, the most common adverse reactions included diarrhea, dizziness, nausea, and rash. There were no significant drug–drug interactions or adverse interactions between ibalizumab and other antiretroviral agents.

Leronlimab (PRO 140), a humanized IgG4 monoclonal antibody (mAb), acts as an HIV-1 CCR5 antagonist; it binds to hydrophilic extracellular domains on CCR5, inhibiting HIV-1 viral entry in a competitive manner (Thompson, 2018).

The safety and effectiveness of leronlimab is currently, evaluated in phase IIb/III clinical trials. In CD 02 trial (PRO 140_CD 02; NCT02483078), leronlimab was tested in treatment-experienced patients with multidrug resistant HIV. In the first week, participants received 350 mg of PRO 140 subcutaneously or placebo together with their regular medication and 1 week later, they received PRO 140 with an optimized regimen. The primary endpoint of the trial was achieved: patients in the PRO 140 arm showed a statistically significant reduction in HIV RNA viral load of greater than 0.5log from baseline versus patients in the placebo arm.⁴ A recent report showed that all CCR5-tropic strains were fully susceptible to PRO 140 in a group of heavily treatment-experienced HIV-1-positive patients harboring 4-class drug-resistance to NRTIs, NNRTIs, PIs, and InSTIs; current exposure to maraviroc (68% of the participants) was not associated with different PRO 140 activity (Rusconi et al., 2022).

CD03 clinical trial has evaluated weekly subcutaneous PRO 140 as monotherapy maintenance in patients with viral suppression (PRO 140_CD03; NCT02859961). The rate of virological failure was lower in the group of participants receiving 700 mg dose comparing with 525 mg and 350 mg dose groups (13.8, 33 and 65.9%, respectively); no evidence of treatment-emergent resistance to leronlimab was observed. A report published on March 31, 2022, showed that weekly injections of Leronlimab (700 mg dose) maintained viral suppression in the five HIV+ participants for over seven years (ClinicalTrials.gov NCT02175680 and NCT02355184) (Chang et al., 2022).

UB-421, a humanized IgG1 monoclonal antibody (mAb), acts as a CD4 attachment inhibitor. UB-421 targets domain 1 of CD4 receptor, blocking HIV entry into the cells via a competitive binding inhibition (Wang et al., 2019).

Several collaborative studies showed the efficacy of UB-421 against HIV strains resistant to broadly neutralizing HIV antibodies, entry inhibitors, and other ARV drugs [ClinicalTrials.gov NCT03164447]. Currently, UB-421 is in phase 2/phase 3 clinical trials for ART substitution (ClinicalTrials.gov NCT03149211), treatment of patients with multi-drug resistant HIV infection (ClinicalTrials.gov NCT04406727), as well as for HIV functional cure (ClinicalTrials.gov NCT04404049).

Islatravir (ISL, MK-8591) is an investigational drug belonging to a new class of antiretrovirals called nucleoside reverse transcriptase translocation inhibitors (NRTTIs) (Markowitz and Sarafianos, 2018). The active form of islatravir (islatravir-triphosphate) inhibits HIV reverse transcriptase (RT) by multiple mechanisms, including RT translocation inhibition and delayed chain termination through viral DNA structural changes (Salie et al., 2016). ISL showed potent activity against HIV-1, HIV-2, and HIV viral strains with multi-drug resistant mutations (Wu et al., 2017). Due to an unexpected decline in total lymphocyte and CD4+ T-cell counts, clinical studies of injectable islatravir for treatment and all formulations of islatravir for pre-exposure prophylaxis (PrEP) are on full or partial clinical holds, still, arms testing lower dosage are ongoing (ClinicalTrials.gov NCT03272347; NCT04564547; NCT05052996).

Lenacapavir, the first-in-class long-acting HIV capsid inhibitor, was approved in August, 2022 in the European Union and in December, 2022 in US, for the treatment of HIV infection, in combination with other antiretroviral(s), in patients with multi-drug resistant HIV who have very limited treatment choices.⁵ Lenacapavir is the only HIV treatment option that can be administered twice-yearly, in a long acting subcutaneous formulation (Dvory-Sobol et al., 2022). The novel long-acting agent targets multiple stages of the HIV life cycle: it binds directly to the HIV capsid protein and interferes with capsid-mediated nuclear import of HIV DNA, virion production and proper capsid core formation (Figure 1; Bester et al., 2020; Link et al., 2020). The approval of lenacapavir was supported by the results of the Phase 2/3, double-blinded, placebo-controlled global multicenter CAPELLA trial, that involved heavily treatment-experienced patients with multi-drug resistant HIV-1 (Segal-Maurer et al., 2022). Eighty three percent of the participants that received lenacapavir in combination with an optimized background regimen achieved viral suppression at week 52; a mean increase in CD4 count of 83 cells/μL was reported. Lenacapavir was well tolerated, no drug-related serious side effects being identified.

Maturation inhibitors-a new class of antiretroviral agents in clinical development-disrupt the proteases cleavage of the HIV-1 gag protein immediate precursor, leading to immature, noninfectious virus particles (Sundquist and Krausslich, 2012; Wang et al., 2015).

Bevirimat and BMS-955176 (GSK3532795), the first 2 maturation inhibitors, demonstrated antiviral activity but no efficacy against some polymorphisms in the HIV gag region (Wainberg and Albert, 2010) and had associated side effects in phase 2b clinical studies.⁶

GSK2838232 is a second-generation HIV-1 maturation inhibitor in phase IIa clinical trial evaluation; it allows for once-daily administration boosted with a pharmacoenhancer (DeJesus et al., 2020). GSK2838232 was well tolerated, and generated a significant viral load decrease in the group of participants receiving the highest dosage. GSK2838232 is active against HIV isolates resistant to bevirimat.

Others long-acting HIV maturation inhibitors (GSK3640254 and GSK3739937) are in earlier stages of development (Joshi et al., 2020; Spinner et al., 2022).

Host factors play an important role in HIV infection (Friedrich et al., 2011). The potential host targets can interfere with HIV entry, replication and spread of HIV infection, and may lead to a higher barrier to antiretroviral drug resistance.

Inhibitors targeting HIV viral entry are among the most attractive targets due to their potential to limit de novo infected cells. Several studies showed that HIV-1 entry is dependent on redox control and the compounds that inhibit thiol/disulfide exchange reactions could suppress HIV-1 viral entry (Moolla et al., 2016; Reiser et al., 2016).

Non-conventional viral inhibitors might act on multidrug resistant HIV strains.