Antibody-mediated depletion of viral reservoirs is limited in SIV-infected macaques treated early with antiretroviral therapy

在接受早期抗逆转录病毒治疗的SIV感染猕猴中,抗体介导的病毒库清除作用有限。

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作者:Adrienne E Swanstrom ,Taina T Immonen ,Kelli Oswald ,Cathi Pyle ,James A Thomas ,William J Bosche ,Lorna Silipino ,Michael Hull ,Laura Newman ,Vicky Coalter ,Adam Wiles ,Rodney Wiles ,Jacob Kiser ,David R Morcock ,Rebecca Shoemaker ,Randy Fast ,Matthew W Breed ,Joshua Kramer ,Duncan Donohue ,Tyler Malys ,Christine M Fennessey ,Charles M Trubey ,Claire Deleage ,Jacob D Estes ,Jeffrey D Lifson ,Brandon F Keele ,Gregory Q Del Prete

Abstract

The effectiveness of virus-specific strategies, including administered HIV-specific mAbs, to target cells that persistently harbor latent, rebound-competent HIV genomes during combination antiretroviral therapy (cART) has been limited by inefficient induction of viral protein expression. To examine antibody-mediated viral reservoir targeting without a need for viral induction, we used an anti-CD4 mAb to deplete both infected and uninfected CD4+ T cells. Ten rhesus macaques infected with barcoded SIVmac239M received cART for 93 weeks starting 4 days after infection. During cART, 5 animals received 5 to 6 anti-CD4 antibody administrations and CD4+ T cell populations were then allowed 1 year on cART to recover. Despite profound CD4+ T cell depletion in blood and lymph nodes, time to viral rebound following cART cessation was not significantly delayed in anti-CD4-treated animals compared with controls. Viral reactivation rates, determined based on rebounding SIVmac239M clonotype proportions, also were not significantly different in CD4-depleted animals. Notably, antibody-mediated depletion was limited in rectal tissue and negligible in lymphoid follicles. These results suggest that, even if robust viral reactivation can be achieved, antibody-mediated viral reservoir depletion may be limited in key tissue sites.

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