Structural basis for viral late-domain binding to Alix

Sangho Lee; Anjali Joshi; Kunio Nagashima; Eric O. Freed; James H. Hurley

doi:10.1038/nsmb1203

Structural basis for viral late-domain binding to Alix

Sangho Lee, Anjali Joshi, Kunio Nagashima, Eric O. Freed, James H. Hurley

National Institutes of Health

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

138 Scopus citations

Abstract

The modular protein Alix is a central node in endosomal-lysosomal trafficking and the budding of human immunodeficiency virus (HIV)-1. The Gag p6 protein of HIV-1 contains a LYPx_nLxxL motif that is required for Alix-mediated budding and binds a region of Alix spanning residues 360-702. The structure of this fragment of Alix has the shape of the letter 'V' and is termed the V domain. The V domain has a topologically complex arrangement of 11 α-helices, with connecting loops that cross three times between the two arms of the V. The conserved residue Phe676 is at the center of a large hydrophobic pocket and is crucial for binding to a peptide model of HIV-1 p6. Overexpression of the V domain inhibits HIV-1 release from cells. This inhibition of release is reversed by mutations that block binding of the Alix V domain to p6.

Original language	English
Pages (from-to)	194-199
Number of pages	6
Journal	Nature Structural and Molecular Biology
Volume	14
Issue number	3
DOIs	https://doi.org/10.1038/nsmb1203
State	Published - Mar 2007
Externally published	Yes

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title = "Structural basis for viral late-domain binding to Alix",

abstract = "The modular protein Alix is a central node in endosomal-lysosomal trafficking and the budding of human immunodeficiency virus (HIV)-1. The Gag p6 protein of HIV-1 contains a LYPxnLxxL motif that is required for Alix-mediated budding and binds a region of Alix spanning residues 360-702. The structure of this fragment of Alix has the shape of the letter 'V' and is termed the V domain. The V domain has a topologically complex arrangement of 11 α-helices, with connecting loops that cross three times between the two arms of the V. The conserved residue Phe676 is at the center of a large hydrophobic pocket and is crucial for binding to a peptide model of HIV-1 p6. Overexpression of the V domain inhibits HIV-1 release from cells. This inhibition of release is reversed by mutations that block binding of the Alix V domain to p6.",

author = "Sangho Lee and Anjali Joshi and Kunio Nagashima and Freed, \{Eric O.\} and Hurley, \{James H.\}",

year = "2007",

month = mar,

doi = "10.1038/nsmb1203",

language = "English",

volume = "14",

pages = "194--199",

journal = "Nature Structural and Molecular Biology",

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T1 - Structural basis for viral late-domain binding to Alix

AU - Lee, Sangho

AU - Joshi, Anjali

AU - Nagashima, Kunio

AU - Freed, Eric O.

AU - Hurley, James H.

PY - 2007/3

Y1 - 2007/3

N2 - The modular protein Alix is a central node in endosomal-lysosomal trafficking and the budding of human immunodeficiency virus (HIV)-1. The Gag p6 protein of HIV-1 contains a LYPxnLxxL motif that is required for Alix-mediated budding and binds a region of Alix spanning residues 360-702. The structure of this fragment of Alix has the shape of the letter 'V' and is termed the V domain. The V domain has a topologically complex arrangement of 11 α-helices, with connecting loops that cross three times between the two arms of the V. The conserved residue Phe676 is at the center of a large hydrophobic pocket and is crucial for binding to a peptide model of HIV-1 p6. Overexpression of the V domain inhibits HIV-1 release from cells. This inhibition of release is reversed by mutations that block binding of the Alix V domain to p6.

AB - The modular protein Alix is a central node in endosomal-lysosomal trafficking and the budding of human immunodeficiency virus (HIV)-1. The Gag p6 protein of HIV-1 contains a LYPxnLxxL motif that is required for Alix-mediated budding and binds a region of Alix spanning residues 360-702. The structure of this fragment of Alix has the shape of the letter 'V' and is termed the V domain. The V domain has a topologically complex arrangement of 11 α-helices, with connecting loops that cross three times between the two arms of the V. The conserved residue Phe676 is at the center of a large hydrophobic pocket and is crucial for binding to a peptide model of HIV-1 p6. Overexpression of the V domain inhibits HIV-1 release from cells. This inhibition of release is reversed by mutations that block binding of the Alix V domain to p6.

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DO - 10.1038/nsmb1203

M3 - Article

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SN - 1545-9993

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SP - 194

EP - 199

JO - Nature Structural and Molecular Biology

JF - Nature Structural and Molecular Biology

IS - 3

ER -

Structural basis for viral late-domain binding to Alix

Abstract

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