Encapsidation of staufen-2 enhances infectivity of hiv-1

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Date
2021-12-01
Authors
Balakrishnan, Kannan
Vasudevan, Ananda Ayyappan Jaguva
Mohareer, Krishnaveni
Luedde, Tom
Münk, Carsten
Banerjee, Sharmistha
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Abstract
Staufen, the RNA-binding family of proteins, affects various steps in the Human Immuno-Deficiency Virus (HIV-1) replication cycle. While our previous study established Staufen-2–HIV-1 Rev interaction and its role in augmenting nucleocytoplasmic export of RRE-containing viral RNA, viral incorporation of Staufen-2 and its effect on viral propagation were unknown. Here, we report that Staufen-2 interacts with HIV-1 Gag and is incorporated into virions and that encapsidated Staufen-2 boosted viral infectivity. Further, Staufen-2 gets co-packaged into virions, possibly by interacting with host factors Staufen-1 or antiviral protein APOBEC3G, which resulted in different outcomes on the infectivity of Staufen-2-encapsidated virions. These observations suggest that encapsidated host factors influence viral population dynamics and infectivity. With the explicit identification of the incorporation of Staufen proteins into HIV-1 and other retroviruses, such as Simian Immunodeficiency Virus (SIV), we propose that packaging of RNA binding proteins, such as Staufen, in budding virions of retroviruses is probably a general phenomenon that can drive or impact the viral population dynamics, infectivity, and evolution.
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Keywords
HIV-1 Gag, Human Immunodeficiency Virus (HIV), Ribonucleoprotein complexes (RNPs), Staufen-2, Viral incorporation, Virus-host interaction
Citation
Viruses. v.13(12)