Army Liposome Formulation Containing QS-21 Render Human Monocyte-derived Macrophages Less Permissive to HIV-1 Infection by Upregulating ABOBEC3A

Overview

Journal Sci Rep

Specialty Science

Date 2022 May 9

PMID 35534646

Authors

Ousman Jobe

Jiae Kim

Daniel O Pinto

Zuzana Villar

Tiffany Hewitt

Elizabeth H Duncan

Alexander Anderson

Neelakshi Gohain

Hua Gong

Courtney Tucker

Carl R Alving

Gary R Matyas

Elke Bergmann-Leitner

Mangala Rao

Affiliations

Soon will be listed here.

Abstract

Monocyte-derived macrophages (MDM) are highly permissive to HIV-1 infection potentially due to the downregulation of innate factors during the differentiation process. The environmental milieu and innate anti-viral factors which are modulated during macrophage differentiation, have been associated with their increased permissiveness to HIV-1 infection. Here, we demonstrate that the Army Liposome Formulation containing MPLA, and QS-21 (ALFQ) activated MDM that are normally permissive to HIV-1 infection to generate a proinflammatory environment and upregulated anti-viral factors notably APOBEC3A. Induction of APOBEC3A by ALFQ decreased permissiveness to HIV-1 infection, while knockdown of APOBEC3A with APOBEC3AsiRNA resulted in a significant loss in the restriction of HIV-1 infectivity. The liposome formulation ALF55, with identical lipid composition but lacking QS-21 had no effect. Furthermore, the capacity of ALFQ to modulate MDM permissiveness to HIV-1 infection was predominantly mediated by large ALFQ liposomes. Our findings highlight a relationship between innate immune activation, proinflammatory milieu, and upregulation of anti-HIV proteins. Induction of these responses can switch the HIV-1 permissive MDM into a more refractory phenotype.

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