Retrovirus budding.

Retrovirus budding. Research Abstract Details 

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Retrovirus budding. Abstract Text:

Eiji Morita,Wesley I Sundquist,

Human immunodeficiency virus (HIV) and other retroviruses acquire their envelopes and spread infection by budding through the limiting membranes of producer cells. To facilitate budding, retroviruses usurp a cellular pathway that is normally used to create vesicles that bud into late endosomal compartments called multivesicular bodies (MVB). Research on yeast and human MVB biogenesis has led to the identification of 25 human proteins that are required for vesicle formation and for HIV-1 budding, and has produced a working model for sequential recruitment of these proteins during MVB vesicle formation. Retroviruses can redirect this machinery to the plasma membrane and leave the cell in a single step or, alternatively, can bud directly into MVB compartments and then exit cells via the exosome pathway. Remarkably, virus release from both the plasma membrane and MVB compartments can occur directionally into specialized sites of cell-to-cell contact called virological synapses. Thus retroviruses have evolved elaborate mechanisms for escaping the cell and maximizing their chances of infecting a new host.

Retrovirus budding. Publishing Authors By Initials

E Morita,WI Sundquist,

For similar proteins: viral proteins research abstracts see: proteins: viral proteins research

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Retrovirus budding. Journal Published:

PUBLICATION TYPE: Review

Journal: Annual review of cell and developmental biology

VOLUME: 20

Page Numbers: 395-425

Journal Abbreviation: Annu. Rev. Cell Dev. Biol.

ISSN: 1081-0706

DAY: 14

MONTH: 12

YEAR: 2004

Retrovirus budding. Information

Number of References: 162

LANGUAGE: eng

NlmUniqueID: 9600627

Retrovirus budding. Keywords Mesh Terms:

KEYWORDS: Viral Proteins

MESH TERMS: metabolism

Chemical & Substance for Abstract: Retrovirus budding. Information

Substance Name: Viral Proteins

Registry Number: 0

Grant and Affiliation Information for Retrovirus budding.

AFFILIATION: Department of Biochemistry, University of Utah, Salt Lake City, UT 84132, USA. moritae@biochem.utah.edu

Country: United States

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MEDLINETA: Annu Rev Cell Dev Biol

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