The Interferon-Induced Protein BST-2 Restricts HIV-1 Release and Is Downregulated from the Cell Surface by the Viral Vpu Protein

Damme, Nanette Van; Goff, Daniel; Katsura, Chris; Jorgenson, Rebecca L.; Mitchell, Richard S.; Johnson, Marc C.; Stephens, Edward B.; Guatelli, John

doi:10.1016/j.chom.2008.03.001

Cited by 930 publications

(1,513 citation statements)

References 34 publications

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“…In 2008, two independent laboratories showed that cell type‐specific expression of BST‐2 correlates with Vpu‐dependent release of HIV‐1. Suppression of endogenous BST‐2 expression resulted in Vpu‐independent virus release whereas rescue of expression with exogenous BST‐2 in cells that otherwise do not have high BST‐2 renders these cells Vpu‐dependent for virus release 6, 7. These findings revealed that BST‐2 is an inhibitor of virus release and a target of Vpu 6, 7.…”

Section: Viral Antagonists Of Bst‐2 and Neutralization Of Bst‐2 Antivmentioning

confidence: 93%

“…In 2008, BST‐2 was rediscovered as the host factor responsible for preventing the release of HIV‐1 with mutated Vpu (HIV‐1 ΔVpu) from host cells 6, 7. Following these discoveries, BST‐2 was renamed tetherin 7.…”

Section: Bst‐2/tetherin: Roles In Viral Pathogenesismentioning

confidence: 99%

“…Following virus tethering, BST‐2 facilitates virus internalization to early endosomes and subsequent lysosomal degradation. The resulting viral products serve as PAMPs that activate TLRs 6, 48, 49 (Fig. 2 #3).…”

Section: Bst‐2/tetherin: Roles In Viral Pathogenesismentioning

confidence: 99%

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The role of BST‐2/Tetherin in host protection and disease manifestation

Mahauad‐Fernandez

Okeoma

2015

Immunity, Inflammation and Disease

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Host cells respond to viral infections by activating immune response genes that are not only involved in inflammation, but may also predispose cells to cancerous transformation. One such gene is BST‐2, a type II transmembrane protein with a unique topology that endows it tethering and signaling potential. Through this ability to tether and signal, BST‐2 regulates host response to viral infection either by inhibiting release of nascent viral particles or in some models inhibiting viral dissemination. However, despite its antiviral functions, BST‐2 is involved in disease manifestation, a function linked to the ability of BST‐2 to promote cell‐to‐cell interaction. Therefore, modulating BST‐2 expression and/or activity has the potential to influence course of disease.

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Section: Viral Antagonists Of Bst‐2 and Neutralization Of Bst‐2 Antivmentioning

confidence: 93%

Section: Bst‐2/tetherin: Roles In Viral Pathogenesismentioning

confidence: 99%

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The role of BST‐2/Tetherin in host protection and disease manifestation

Mahauad‐Fernandez

Okeoma

2015

Immunity, Inflammation and Disease

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“…Recent experiments indicate that Vpu facilitates viral budding through interactions with host cell proteins that otherwise inhibit viral budding, 35 in particular an integral membrane protein dubbed tetherin, CD317, or BST-2. 36,37 Tetherin tethers budding virions to host cells by linking the viral and host cell membranes. 38 Vpu interferes with tetherin by targeting tetherin for degradation, in a manner similar to that by which Vpu downregulates CD4.…”

Section: Introductionmentioning

confidence: 99%

Oligomerization state and supramolecular structure of the HIV‐1 Vpu protein transmembrane segment in phospholipid bilayers

et al. 2010

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HIV-1 Vpu is an 81-residue protein with a single N-terminal transmembrane (TM) helical segment that is involved in the release of new virions from host cell membranes. Vpu and its TM segment form ion channels in phospholipid bilayers, presumably by oligomerization of TM helices into a pore-like structure. We describe measurements that provide new constraints on the oligomerization state and supramolecular structure of residues 1-40 of Vpu (Vpu 1-40 ), including analytical ultracentrifugation measurements to investigate oligomerization in detergent micelles, photo-induced crosslinking experiments to investigate oligomerization in bilayers, and solid-state nuclear magnetic resonance measurements to obtain constraints on intermolecular contacts between and orientations of TM helices in bilayers. From these data, we develop molecular models for Vpu TM oligomers. The data indicate that a variety of oligomers coexist in phospholipid bilayers, so that a unique supramolecular structure can not be defined. Nonetheless, since oligomers of various sizes have similar intermolecular contacts and orientations, molecular models developed from our data are most likely representative of Vpu TM oligomers that exist in host cell membranes.

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“…Vpu was classified as a class IA viroporin (Fischer et al, 2012;Luis Nieva et al, 2012). Recently it was found that Vpu antagonizes tetherin, a cellular antiviral defense factor that cross-links budding virions to the host cell membrane and thus inhibits virus release (Neil et al, 2008;Van Damme et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

Full-length Vpu and human CD4(372–433) in phospholipid bilayers as seen by magic angle spinning NMR

Quynh¹,

Wittlich²,

Glück³

et al. 2013

Biological Chemistry

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HIV-1 Vpu and CD4(372-433), a peptide comprising the transmembrane and cytoplasmic domain of human CD4, were recombinantly expressed in Escherichia coli, uniformly labeled with 13 C and 15 N isotopes, and separately reconstituted into phospholipid bilayers. Highly resolved dipolar cross-polarization (CP)-based solid-state NMR spectra of the two transmembrane proteins were recorded under magic angle sample spinning. Partial assignment of 13 C resonances was achieved. Site-specific assignments were obtained for 13 amino acid residues of CD4(372-433) and two Vpu residues. Additional amino acid type-specific assignments were achieved for 10 amino acid spin systems for both CD4(372-433) and Vpu. Further, structural flexibility was probed with different dipolar recoupling techniques, and the correct insertion of the transmembrane domains into the lipid bilayers was confirmed by proton spin diffusion experiments.

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The Interferon-Induced Protein BST-2 Restricts HIV-1 Release and Is Downregulated from the Cell Surface by the Viral Vpu Protein

Cited by 930 publications

References 34 publications

The role of BST‐2/Tetherin in host protection and disease manifestation

The role of BST‐2/Tetherin in host protection and disease manifestation

Oligomerization state and supramolecular structure of the HIV‐1 Vpu protein transmembrane segment in phospholipid bilayers

Full-length Vpu and human CD4(372–433) in phospholipid bilayers as seen by magic angle spinning NMR

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