Safety, pharmacokinetics, and biological activity of CD4-mimetic BNM-III-170 in SHIV-infected rhesus macaques.

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Tác giả: James Auger, Catherine Bourassa, Saverio Capuano, Nicolas Chomont, Natasha M Clark, Shilei Ding, David T Evans, Andrés Finzi, Romain Gasser, Fleur Gaudette, Christina Gavegnano, Andres G Grandea, Iman Hammad, Justin Harper, Selwyn J Hurwitz, Deanna A Kulpa, Priti Kumar, Lorie Marchitto, Malcolm A Martin, Halima Medjahed, Kevin Nguyen, Amélie Pagliuzza, Mirko Paiardini, Jun Park, Marzena Pazgier, Jérémie Prévost, Jonathan Richard, Raymond F Schinazi, Guido Silvestri, Amos B Smith, Joseph Sodroski, Cesar Ariel Trifone, Elise G Viox

Ngôn ngữ: eng

Ký hiệu phân loại: 069.50289 Collections and exhibits of museum objects

Thông tin xuất bản: United States : Journal of virology , 2025

Mô tả vật lý:

Bộ sưu tập: NCBI

ID: 743243

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Anti-HIV-1 antibodies capable of mediating ADCC are elicited by the majority of people with HIV-1 and preferentially target the "open," CD4-bound conformation of HIV-1 envelope glycoproteins (Env). However, due to the "closed" conformation sampled by unliganded HIV-1-Envs, these antibodies are ineffective at eliminating infected cells. BNM-III-170 is a small-molecule CD4-mimetic compound that binds the Phe43 cavity of the gp120 subunit of Env, forcing Env to "open up," thus exposing epitopes targeted by CD4-induced (CD4i), ADCC-mediating antibodies. Here, we assessed the safety, pharmacokinetics, and biological activity of BNM-III-170 in uninfected and SHIV-AD8-EO-infected rhesus macaques (RMs). In uninfected RMs, single subcutaneous administrations of 3-36 mg/kg BNM-III-170 were well-tolerated, with serum half-lives ranging from 3 to 6 h. In SHIV-infected RMs, four different regimens were evaluated: 2 × 36 mg/kg daily, 1 × 24 mg/kg, 3 × 36 mg/kg every 7 days, and 3 × 36 mg/kg every 3 days. While toxicity was observed with daily doses, all other regimens demonstrated reasonable safety profiles. No changes in plasma viral loads were observed in SHIV-infected RMs following any of the evaluated BNM-III-170 dosing regimens. However, plasma collected following BNM-III-170 administration was shown to have increased binding to infected cells and to sensitize SHIV AD8-EO virions to neutralization by otherwise non-neutralizing antibodies. In addition, the plasma of treated animals mediated ADCC in the presence of BNM-III-170. These results establish a well-tolerated BNM-III-170 dosing regimen in SHIV-infected RMs and serve as proof of concept for its biological activity in promoting the targeting of infected cells by CD4i ADCC-mediating antibodies. Thus, they inform future studies evaluating CD4mc treatment in ART-treated animals.IMPORTANCEA therapeutic regimen able to eradicate or functionally cure HIV-1 remains elusive and may require a "shock-and-kill" approach to reactivate and then purge the latent HIV-1 reservoir. The small-molecule CD4-mimetic compound BNM-III-170 has previously been shown to (i) sensitize HIV-1-infected cells to ADCC mediated by plasma from people with HIV-1 (PWH)

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