Resistance of human T cell leukemia virus type 1 to APOBEC3G restriction is mediated by elements in nucleocapsid

Derse, David; Hill, S. A.; Princler, Gerald L.; Lloyd, Patricia A.; Heidecker, Gisela

doi:10.1073/pnas.0609444104

Cited by 113 publications

(121 citation statements)

References 36 publications

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“…Some retroviruses, such as HIV, simian immunodeficiency virus (SIV), and feline immunodeficiency virus (FIV), encode Vif proteins that bind APOBEC3 proteins and target them for degradation in virus-producing cells. Additionally, the Bet protein of feline foamy viruses inhibits APOBEC3 by as yet undetermined means (16) and human T-cell leukemia virus I prevents packaging of APOBEC3G, although not APOBEC3A, 3B, or 3H (47,48). However, APOBEC3 inhibits infection by a number of viruses that encode no apparent vif-or bet-like genes, and how these viruses overcome restriction is not known.…”

Section: Discussionmentioning

confidence: 99%

Murine leukemia virus glycosylated Gag blocks apolipoprotein B editing complex 3 and cytosolic sensor access to the reverse transcription complex

Stavrou

Nitta

Kotla

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

194

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Pathogenic retroviruses have evolved multiple means for evading host restriction factors such as apolipoprotein B editing complex (APOBEC3) proteins. Here, we show that murine leukemia virus (MLV) has a unique means of counteracting APOBEC3 and other cytosolic sensors of viral nucleic acid. Using virus isolated from infected WT and APOBEC3 KO mice, we demonstrate that the MLV glycosylated Gag protein (glyco-Gag) enhances viral core stability. Moreover, in vitro endogenous reverse transcription reactions of the glyco-Gag mutant virus were substantially inhibited compared with WT virus, but only in the presence of APOBEC3. Thus, glyco-Gag rendered the reverse transcription complex in the viral core resistant to APOBEC3. Glyco-Gag in the virion also rendered MLV resistant to other cytosolic sensors of viral reverse transcription products in newly infected cells. Strikingly, glycoGag mutant virus reverted to glyco-Gag-containing virus only in WT and not APOBEC3 KO mice, indicating that counteracting APOBEC3 is the major function of glyco-Gag. Thus, in contrast to the HIV viral infectivity factor protein, which prevents APOBEC3 packaging in the virion, the MLV glyco-Gag protein uses a unique mechanism to counteract the antiviral action of APOBEC3 in vivonamely, protecting the reverse transcription complex in viral cores from APOBEC3. These data suggest that capsid integrity may play a critical role in virus resistance to intrinsic cellular antiviral resistance factors that act at the early stages of infection.intrinsic immunity | trex1 | virus restriction factors

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Section: Discussionmentioning

confidence: 99%

Murine leukemia virus glycosylated Gag blocks apolipoprotein B editing complex 3 and cytosolic sensor access to the reverse transcription complex

Stavrou

Nitta

Kotla

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

194

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“…However, restriction factors for HTLV-1 have not been studied extensively. It has been reported that APO-BEC3G suppresses replication of HTLV-1 whereas Gag protein inhibits incorporation of APOBEC3G into the virion (32). Recently, SAMHD1 has been reported to suppress replication of HTLV-1 in monocytes (33).…”

Section: Discussionmentioning

confidence: 99%

TCF1 and LEF1 act as T-cell intrinsic HTLV-1 antagonists by targeting Tax

Ma¹,

Yasunaga²,

Akari³

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

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“…More straightforward alternatives might be to avert APOBEC proteins by not encapsidating them into virions (e.g. human T-cell leukaemia virus type-I, HTLV-I, and Mason-Pfizer monkey virus, M-PMV ) (Doehle et al 2006;Derse et al 2007) or, perhaps, by simply replicating in nonexpressing cells (Delebecque et al 2006).…”

Section: Anti-hiv-1 Phenotypes Of Diverse Human Apobec Proteinsmentioning

confidence: 99%

APOBEC proteins and intrinsic resistance to HIV-1 infection

Malim

2008

Phil. Trans. R. Soc. B

243

268

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Members of the APOBEC family of cellular polynucleotide cytidine deaminases, most notably APOBEC3G and APOBEC3F, are potent inhibitors of HIV-1 infection. Wild type HIV-1 infections are largely spared from APOBEC3G/F function through the action of the essential viral protein, Vif. In the absence of Vif, APOBEC3G/F are encapsidated by budding virus particles leading to excessive cytidine (C) to uridine (U) editing of negative sense reverse transcripts in newly infected cells. This registers as guanosine (G) to adenosine (A) hypermutations in plus-stranded cDNA. In addition to this profoundly debilitating effect on genetic integrity, APOBEC3G/F also appear to inhibit viral DNA synthesis by impeding the translocation of reverse transcriptase along template RNA. Because the functions of Vif and APOBEC3G/F proteins oppose each other, it is likely that fluctuations in the Vif–APOBEC balance may influence the natural history of HIV-1 infection, as well as viral sequence diversification and evolution. Given Vif's critical role in suppressing APOBEC3G/F function, it can be argued that pharmacologic strategies aimed at restoring the activity of these intrinsic anti-viral factors in the context of infected cells in vivo have clear therapeutic merit, and therefore deserve aggressive pursuit.

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Resistance of human T cell leukemia virus type 1 to APOBEC3G restriction is mediated by elements in nucleocapsid

Cited by 113 publications

References 36 publications

Murine leukemia virus glycosylated Gag blocks apolipoprotein B editing complex 3 and cytosolic sensor access to the reverse transcription complex

Murine leukemia virus glycosylated Gag blocks apolipoprotein B editing complex 3 and cytosolic sensor access to the reverse transcription complex

TCF1 and LEF1 act as T-cell intrinsic HTLV-1 antagonists by targeting Tax

APOBEC proteins and intrinsic resistance to HIV-1 infection

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