2010
DOI: 10.1128/jvi.00342-09
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The Potent Anti-HIV Activity of CXCL12γ Correlates with Efficient CXCR4 Binding and Internalization

Abstract: We previously demonstrated that the naturally occurring splice variant stromal cell-derived factor 1␥/ CXCL12␥ is the most potent CXCL12 isoform in blocking X4 HIV-1, with weak chemotactic activity. A conserved BBXB domain (B for basic and X for any residue) located in the N terminus ( 24 KHLK 27 ) is found in all six isoforms of CXCL12. To determine whether the potent antiviral activity of CXCL12␥ is due to the presence of the extra C-terminal BBXB domains, we mutated each domain individually as well as in co… Show more

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Cited by 18 publications
(35 citation statements)
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“…These results differ notably from transwell assays in which CXCR4+ cells show higher sensitivity migration toward cell-secreted or recombinant CXCL12-α (Fig. S2G) 10, 21 . Rueda and colleagues previously showed a ten-fold higher concentration of CXCL12-γ was required to drive chemotaxis of CXCR4 cells to the same extent as CXCL12-α in transwells.…”
Section: Resultscontrasting
confidence: 90%
“…These results differ notably from transwell assays in which CXCR4+ cells show higher sensitivity migration toward cell-secreted or recombinant CXCL12-α (Fig. S2G) 10, 21 . Rueda and colleagues previously showed a ten-fold higher concentration of CXCL12-γ was required to drive chemotaxis of CXCR4 cells to the same extent as CXCL12-α in transwells.…”
Section: Resultscontrasting
confidence: 90%
“…2D) also had predicted binding sites on all 3 CXCL12 isoforms (miR-101 on CXCL12␣, -␤, and -⌬; miR130a on CXCL12␣ and -⌬; miR-29b on CXCL12␤) (see Table S7 in the supplemental material). More interestingly, none of the seven THC-induced miRNAs have been predicted to directly target CXCL12␥ (gamma), the specific isoform that has been previously reported to exhibit anti-HIV effects by preventing HIV entry via competitive CXCR4 binding and internalization (59). Consistent with these predictions, cannabinoid agonists (2-AG and JWH-133) have been shown to inhibit CXCL12-mediated chemotaxis of activated T lymphocytes (60).…”
Section: Discussionsupporting
confidence: 54%
“…However, although CD4-gp120 interaction has been demonstrated to be essential for cell-to-cell viral transfer, the contributions of coreceptor interaction and fusion appear different among reports (Blanco et al, 2004;Chen et al, 2007;Emerson et al, 2010;Groot et al, 2008;Martin et al, 2010;Massanella et al, 2009), and hence are still under investigation. It has been proposed that internalization of CXCR4 triggered by binding its endogenous ligand SDF-1/ CXCL12 is an additional anti-HIV mechanism (Altenburg et al, 2010;Amara et al, 1997). We also reported the down-regulation of CXCR4 expression induced by CXCR4 antagonists and HIV-1 gp120 through macropinocytosis Tanaka et al, 2012), proposing an additional HIV-1 entry pathway using the cellular machinery.…”
Section: Discussionmentioning
confidence: 65%