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Review
. 2025 Oct;12(10):e732-e736.
doi: 10.1016/S2352-3018(25)00128-6. Epub 2025 Jun 18.

Lenacapavir-associated drug resistance: implications for scaling up long-acting HIV pre-exposure prophylaxis

Gert van Zyl  1 Mateo Prochazka  2 Heather-Marie Ann Schmidt  2 Catherine Orrell  3 Jonathan M Schapiro  4 Suzanne M McCluskey  5 Marco Vitoria  2 Rami Kantor  6 Urvi M Parikh  7 Michelle Rodolph  2 Michael R Jordan  8 Robert W Shafer  9
Affiliations
Review

Lenacapavir-associated drug resistance: implications for scaling up long-acting HIV pre-exposure prophylaxis

Gert van Zyl et al. Lancet HIV. 2025 Oct.

Abstract

Although drug resistance could emerge if lenacapavir is initiated during undiagnosed acute infection or if infection occurs during the drug's pharmacokinetic tail, these cases will not compromise the effectiveness of WHO-recommended therapies, as there is no cross-resistance between lenacapavir and other licensed antiretroviral drugs. Lenacapavir pre-exposure prophylaxis (PrEP) is also unlikely to drive population-level lenacapavir resistance given the rarity of breakthrough infections and the reduced replication capacity of most lenacapavir-resistant variants, which most likely reduces their transmission potential. Conversely, the risk of acquiring lenacapavir-resistant HIV-1 while receiving lenacapavir PrEP is likely to remain extremely low, as lenacapavir-associated drug-resistance mutations are rare among individuals without previous lenacapavir exposure, and widespread use of lenacapavir-based regimens remains years away. Nonetheless, as the number of lenacapavir PrEP programmes increase, surveillance for emerging lenacapavir resistance should also be implemented.

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Conflict of interest statement

Declaration of interests RWS received honoraria for lectures from Gilead Sciences and ViiV Healthcare in 2022. GvZ received honoraria for a lecture from ThermoFisher. JMS received honoraria for participating in advisory boards for Merck, Gilead Sciences, GlaxoSmithKline, ViiV Healthcare, Moderna, and Pfizer; speaker fees from Merck, Gilead Sciences, GlaxoSmithKline, and ViiV Healthcare; and consulting fees from Teva, GlaxoSmithKline, and ViiV Healthcare. RK received honoraria for a lecture from ThermoFisher. UMP received consulting fees from Merck and honoraria for a lecture from ThermoFisher. SMM received grant funding from Merck and ViiV Healthcare paid to her institution. All other authors declare no competing interests.

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