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A highly potent long-acting small-molecule HIV-1 capsid inhibitor with efficacy in a humanized mouse model.

Nat Med. 2019; 
Yant SR, Mulato A, Hansen D, Tse WC,, Niedziela-Majka A, Zhang JR, Stepan GJ, Jin D, Wong MH, Perreira JM, Singer E, Papalia GA, Hu EY, Zheng J, Lu B, Schroeder SD, Chou K, Ahmadyar S, Liclican A, Yu H, Novikov N, Paoli E, Gonik D, Ram RR, Hung M, McDougall WM, Brass AL,,, Sundquist WI, Cihlar T, Link JO.
Products/Services Used Details Operation
Gene Synthesis A synthetic gene encoding secreted NanoLuc luciferase (secNLuc), an internal ribosomal entry-site element35 and Nef was purchased from GenScript and inserted into pNL4.... Capsid genes containing resistance-associated mutation(s) were synthesized at GenScript and inserted into pKS13ΔEnv, pNL4-3-JRFL-secNLuc and pJexpress-CA-4Mu22 plasmids via BssHII–ApaI ligation. Get A Quote

摘要

People living with HIV (PLWH) have expressed concern about the life-long burden and stigma associated with taking pills daily and can experience medication fatigue that might lead to suboptimal treatment adherence and the emergence of drug-resistant viral variants, thereby limiting future treatment options1-3. As such, there is strong interest in long-acting antiretroviral (ARV) agents that can be administered less frequently4. Herein, we report GS-CA1, a new archetypal small-molecule HIV capsid inhibitor with exceptional potency against HIV-2 and all major HIV-1 types, including viral variants resistant to the ARVs currently in clinical use. Mechanism-of-action studies indicate that GS-CA1 binds directly to th... More

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