Mechanistic basis of post-treatment control of SIV after anti-α4β7 antibody therapy | Zendy

Chad R. Wells | Zendy; Youfang Cao | Zendy; David P. Durham | Zendy; Siddappa N. Byrareddy | Zendy; Aftab A. Ansari | Zendy; Nancy H. Ruddle | Zendy; Jeffrey P. Townsend | Zendy; Alison P. Galvani | Zendy; Alan S. Perelson | Zendy

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Mechanistic basis of post-treatment control of SIV after anti-α4β7 antibody therapy

Author(s) -

Chad R. Wells,

Youfang Cao,

David P. Durham,

Siddappa N. Byrareddy,

Aftab A. Ansari,

Nancy H. Ruddle,

Jeffrey P. Townsend,

Alison P. Galvani,

Alan S. Perelson

Publication year - 2021

Publication title -

plos computational biology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.628

H-Index - 182

eISSN - 1553-7358

pISSN - 1553-734X

DOI - 10.1371/journal.pcbi.1009031

Subject(s) - viral load , cart , viremia , antibody , virology , immune system , immunology , simian immunodeficiency virus , virus , biology , drug holiday , cd8 , human immunodeficiency virus (hiv) , mechanical engineering , engineering

Treating macaques with an anti-α4β7 antibody under the umbrella of combination antiretroviral therapy (cART) during early SIV infection can lead to viral remission, with viral loads maintained at < 50 SIV RNA copies/ml after removal of all treatment in a subset of animals. Depletion of CD8 + lymphocytes in controllers resulted in transient recrudescence of viremia, suggesting that the combination of cART and anti-α4β7 antibody treatment led to a state where ongoing immune responses kept the virus undetectable in the absence of treatment. A previous mathematical model of HIV infection and cART incorporates immune effector cell responses and exhibits the property of two different viral load set-points. While the lower set-point could correspond to the attainment of long-term viral remission, attaining the higher set-point may be the result of viral rebound. Here we expand that model to include possible mechanisms of action of an anti-α4β7 antibody operating in these treated animals. We show that the model can fit the longitudinal viral load data from both IgG control and anti-α4β7 antibody treated macaques, suggesting explanations for the viral control associated with cART and an anti-α4β7 antibody treatment. This effective perturbation to the virus-host interaction can also explain observations in other nonhuman primate experiments in which cART and immunotherapy have led to post-treatment control or resetting of the viral load set-point. Interestingly, because the viral kinetics in the various treated animals differed—some animals exhibited large fluctuations in viral load after cART cessation—the model suggests that anti-α4β7 treatment could act by different primary mechanisms in different animals and still lead to post-treatment viral control. This outcome is nonetheless in accordance with a model with two stable viral load set-points, in which therapy can perturb the system from one set-point to a lower one through different biological mechanisms.

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