2011
DOI: 10.1016/j.str.2011.07.016
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The Phe105 Loop of Alix Bro1 Domain Plays a Key Role in HIV-1 Release

Abstract: Summary Alix and cellular paralogs HD-PTP and Brox contain N-terminal Bro1 domains that bind ESCRT-III CHMP4. In contrast to HD-PTP and Brox, expression of the Bro1 domain of Alix alleviates HIV-1 release defects due to interrupted access to ESCRT. In an attempt to elucidate this functional discrepancy, we solved the crystal structures of the Bro1 domains of HD-PTP and Brox. They revealed typical “boomerang” folds they share with the Bro1 Alix domain. However, they each contain unique structural features that … Show more

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Cited by 30 publications
(51 citation statements)
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References 85 publications
(195 reference statements)
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“…We previously presented evidence supporting a role for HIV-1 NC in the Alix-binding LYPX n L L domain budding pathway. We found that overexpression of the Alix Bro1 domain rescued virus release defects of an HIV-1 mutant lacking all L domains (26,67). Similar results were obtained with the SIVcpzGAB2 mutant lacking all L domains (data not shown).…”
Section: Nc Is Required For Ptap-mediated Budding Of Sivcpzgab2 and Ssupporting
confidence: 83%
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“…We previously presented evidence supporting a role for HIV-1 NC in the Alix-binding LYPX n L L domain budding pathway. We found that overexpression of the Alix Bro1 domain rescued virus release defects of an HIV-1 mutant lacking all L domains (26,67). Similar results were obtained with the SIVcpzGAB2 mutant lacking all L domains (data not shown).…”
Section: Nc Is Required For Ptap-mediated Budding Of Sivcpzgab2 and Ssupporting
confidence: 83%
“…Moreover, we and others have shown that NC interacts with the Bro1 domain of Alix (26,62), which mediates the recruitment of the cellular fission machinery components CHMP4 and VPS4 (26). Interestingly, this interaction is critical for the HIV-1 LYPX n L-driven budding pathway (26,62,66,67), emphasizing the role of NC in Alix-mediated HIV-1 budding. Several roles have been attributed to NC in the HIV-1 life cycle; they include reverse transcription, integration, trafficking, virus assembly, viral genome encapsidation, and cell-to-cell virus transmission (19,38,44,47,54,58,71).…”
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confidence: 72%
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