2009
DOI: 10.1182/blood-2008-04-150342
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HTLV-1 uses HSPG and neuropilin-1 for entry by molecular mimicry of VEGF165

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Cited by 139 publications
(142 citation statements)
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“…8 pDCs participate in innate and adaptive immunity, 9,10 are located in blood and lymphoid organs, 10,11 and produce up to 1000-fold more interferon-␣ (IFN-␣) than other cell types in response to virus exposure. 12 Three molecules have been characterized for HTLV-1 entry into cells, heparan sulfate proteoglycans 13 and BDCA-4 (also called neuropilin-1) 14 for the initial virus binding to target cells 15 and glucose transporter 1 for the postattachment and the viral fusion. 16,17 Interestingly, BDCA-4 is expressed by mDC and T cells 18,19 but cells expressing the greatest level of BDCA-4 in blood are pDCs, 20 strongly suggesting that HTLV-1 could interact with pDCs.…”
Section: Introductionmentioning
confidence: 99%
“…8 pDCs participate in innate and adaptive immunity, 9,10 are located in blood and lymphoid organs, 10,11 and produce up to 1000-fold more interferon-␣ (IFN-␣) than other cell types in response to virus exposure. 12 Three molecules have been characterized for HTLV-1 entry into cells, heparan sulfate proteoglycans 13 and BDCA-4 (also called neuropilin-1) 14 for the initial virus binding to target cells 15 and glucose transporter 1 for the postattachment and the viral fusion. 16,17 Interestingly, BDCA-4 is expressed by mDC and T cells 18,19 but cells expressing the greatest level of BDCA-4 in blood are pDCs, 20 strongly suggesting that HTLV-1 could interact with pDCs.…”
Section: Introductionmentioning
confidence: 99%
“…Initially, it was described as a regulator of axon collapse and enhancer of angiogenesis. Subsequently, new functions of NRP-1 were characterized and the expanded contemporary view of NRP-1 includes among its functions antigen recognition (3), adhesion via interaction with ␤ integrins (4,5), activation of latent forms of cytokines (6), control of stem cell differentiation (7)(8)(9), and viral infection (10).…”
mentioning
confidence: 99%
“…HSPG had been showed to bind the HIV-1 protein gp120, therefore facilitating HIV-1 infection. Studies demonstrated that inhibition of HSPG dramatically reduced syncitium formation and infection in CD4+ T cells (Lambert, Bouttier et al, 2009). Furthermore, inhibition of HSPG also reduced infection of dendritic cells.…”
Section: Htlv-1 Receptor Complexmentioning
confidence: 99%