Distinct viral determinants for the packaging of human cytidine deaminases APOBEC3G and APOBEC3C

Tao Wang; Wenyan Zhang; Chunjuan Tian; Bindong Liu; Yunkai Yu; Lingmei Ding; Paul Spearman; Xiao Fang Yu

doi:10.1016/j.virol.2008.04.012

Distinct viral determinants for the packaging of human cytidine deaminases APOBEC3G and APOBEC3C

Tao Wang, Wenyan Zhang, Chunjuan Tian, Bindong Liu, Yunkai Yu, Lingmei Ding, Paul Spearman, Xiao Fang Yu

Research output: Contribution to journal › Article › peer-review

37 Scopus citations

Abstract

Human APOBEC3G and other APOBEC3 cytidine deaminases inhibit a variety of retroviruses, including Vif-deficient HIV-1. These host proteins are packaged into viral particles and inhibit the replication of virus in new target cells. A3G and A3F are known to be efficiently packaged into HIV-1 virions by binding to 7SL RNA through the Gag NC domain; however, the packaging mechanisms of other APOBEC3 proteins are poorly defined. We have now demonstrated that APOBEC3C (A3C) can be efficiently packaged into HIV-1 virions that are deficient for viral genomic RNA. Inhibition of the encapsidation of 7SL RNA into HIV-1 virions blocked the packaging of A3G, but not A3C. While the NC domain is required for efficient packaging of A3G, deletion of this domain had little effect on A3C packaging into HIV-1 Gag particles. A3C interacted with HIV-1 Gag which was MA domain-dependent and RNA-dependent. Deletion of the MA domain of HIV-1 Gag inhibited A3C but not A3G packaging into HIV-1 Gag particles. Thus, A3G and A3C have evolved to use distinct mechanisms for targeting retroviruses.

Original language	English (US)
Pages (from-to)	71-79
Number of pages	9
Journal	Virology
Volume	377
Issue number	1
DOIs	https://doi.org/10.1016/j.virol.2008.04.012
State	Published - Jul 20 2008
Externally published	Yes

Keywords

APOBEC3C
APOBEC3G
Cytidine deaminase
HIV-1
Vif

ASJC Scopus subject areas

Virology

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10.1016/j.virol.2008.04.012

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@article{d1668cdf04dd40ae8a204b9e2cd7962d,

title = "Distinct viral determinants for the packaging of human cytidine deaminases APOBEC3G and APOBEC3C",

abstract = "Human APOBEC3G and other APOBEC3 cytidine deaminases inhibit a variety of retroviruses, including Vif-deficient HIV-1. These host proteins are packaged into viral particles and inhibit the replication of virus in new target cells. A3G and A3F are known to be efficiently packaged into HIV-1 virions by binding to 7SL RNA through the Gag NC domain; however, the packaging mechanisms of other APOBEC3 proteins are poorly defined. We have now demonstrated that APOBEC3C (A3C) can be efficiently packaged into HIV-1 virions that are deficient for viral genomic RNA. Inhibition of the encapsidation of 7SL RNA into HIV-1 virions blocked the packaging of A3G, but not A3C. While the NC domain is required for efficient packaging of A3G, deletion of this domain had little effect on A3C packaging into HIV-1 Gag particles. A3C interacted with HIV-1 Gag which was MA domain-dependent and RNA-dependent. Deletion of the MA domain of HIV-1 Gag inhibited A3C but not A3G packaging into HIV-1 Gag particles. Thus, A3G and A3C have evolved to use distinct mechanisms for targeting retroviruses.",

keywords = "APOBEC3C, APOBEC3G, Cytidine deaminase, HIV-1, Vif",

author = "Tao Wang and Wenyan Zhang and Chunjuan Tian and Bindong Liu and Yunkai Yu and Lingmei Ding and Paul Spearman and Yu, {Xiao Fang}",

note = "Funding Information: We thank Dr. Michael Malim for A3C-HA vector, Anjie Zhen and Lindi Tan for technical assistance and thoughtful discussions, and Dr. Deborah McClellan for editorial assistance. This work was supported by grants from the NIH (AI062644 and AI071769), a grant from the Johns Hopkins Center for AIDS Research (CFAR), and funding from the National Science Foundation of China (NSFC-30425012) and Cheung Kong Scholars Program Foundation of the Chinese Ministry of Education to X-F.Yu.",

year = "2008",

month = jul,

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doi = "10.1016/j.virol.2008.04.012",

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volume = "377",

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T1 - Distinct viral determinants for the packaging of human cytidine deaminases APOBEC3G and APOBEC3C

AU - Wang, Tao

AU - Zhang, Wenyan

AU - Tian, Chunjuan

AU - Liu, Bindong

AU - Yu, Yunkai

AU - Ding, Lingmei

AU - Spearman, Paul

AU - Yu, Xiao Fang

N1 - Funding Information: We thank Dr. Michael Malim for A3C-HA vector, Anjie Zhen and Lindi Tan for technical assistance and thoughtful discussions, and Dr. Deborah McClellan for editorial assistance. This work was supported by grants from the NIH (AI062644 and AI071769), a grant from the Johns Hopkins Center for AIDS Research (CFAR), and funding from the National Science Foundation of China (NSFC-30425012) and Cheung Kong Scholars Program Foundation of the Chinese Ministry of Education to X-F.Yu.

PY - 2008/7/20

Y1 - 2008/7/20

N2 - Human APOBEC3G and other APOBEC3 cytidine deaminases inhibit a variety of retroviruses, including Vif-deficient HIV-1. These host proteins are packaged into viral particles and inhibit the replication of virus in new target cells. A3G and A3F are known to be efficiently packaged into HIV-1 virions by binding to 7SL RNA through the Gag NC domain; however, the packaging mechanisms of other APOBEC3 proteins are poorly defined. We have now demonstrated that APOBEC3C (A3C) can be efficiently packaged into HIV-1 virions that are deficient for viral genomic RNA. Inhibition of the encapsidation of 7SL RNA into HIV-1 virions blocked the packaging of A3G, but not A3C. While the NC domain is required for efficient packaging of A3G, deletion of this domain had little effect on A3C packaging into HIV-1 Gag particles. A3C interacted with HIV-1 Gag which was MA domain-dependent and RNA-dependent. Deletion of the MA domain of HIV-1 Gag inhibited A3C but not A3G packaging into HIV-1 Gag particles. Thus, A3G and A3C have evolved to use distinct mechanisms for targeting retroviruses.

AB - Human APOBEC3G and other APOBEC3 cytidine deaminases inhibit a variety of retroviruses, including Vif-deficient HIV-1. These host proteins are packaged into viral particles and inhibit the replication of virus in new target cells. A3G and A3F are known to be efficiently packaged into HIV-1 virions by binding to 7SL RNA through the Gag NC domain; however, the packaging mechanisms of other APOBEC3 proteins are poorly defined. We have now demonstrated that APOBEC3C (A3C) can be efficiently packaged into HIV-1 virions that are deficient for viral genomic RNA. Inhibition of the encapsidation of 7SL RNA into HIV-1 virions blocked the packaging of A3G, but not A3C. While the NC domain is required for efficient packaging of A3G, deletion of this domain had little effect on A3C packaging into HIV-1 Gag particles. A3C interacted with HIV-1 Gag which was MA domain-dependent and RNA-dependent. Deletion of the MA domain of HIV-1 Gag inhibited A3C but not A3G packaging into HIV-1 Gag particles. Thus, A3G and A3C have evolved to use distinct mechanisms for targeting retroviruses.

KW - APOBEC3C

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KW - HIV-1

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ER -

Distinct viral determinants for the packaging of human cytidine deaminases APOBEC3G and APOBEC3C

Abstract

Keywords

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