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硫酸乙酰肝素蛋白聚糖介导1型人类T细胞白血病病毒颗粒附着并进入CD4+ T细胞。

Heparan sulfate proteoglycans mediate attachment and entry of human T-cell leukemia virus type 1 virions into CD4+ T cells.

作者信息

Jones Kathryn S, Petrow-Sadowski Cari, Bertolette Daniel C, Huang Ying, Ruscetti Francis W

机构信息

Basic Research Program, SAIC-Frederick, National Cancer Institute-Frederick, MD 21702-1201, USA.

出版信息

J Virol. 2005 Oct;79(20):12692-702. doi: 10.1128/JVI.79.20.12692-12702.2005.

Abstract

Heparan sulfate proteoglycans (HSPGs) are used by a number of viruses to facilitate entry into host cells. For the retrovirus human T-cell leukemia virus type 1 (HTLV-1), it has recently been reported that HSPGs are critical for efficient binding of soluble HTLV-1 SU and the entry of HTLV pseudotyped viruses into non-T cells. However, the primary in vivo targets of HTLV-1, CD4(+) T cells, have been reported to express low or undetectable levels of HSPGs. For this study, we reexamined the expression of HSPGs in CD4(+) T cells and examined their role in HTLV-1 attachment and entry. We observed that while quiescent primary CD4(+) T cells do not express detectable levels of HSPGs, HSPGs are expressed on primary CD4(+) T cells following immune activation. Enzymatic modification of HSPGs on the surfaces of either established CD4(+) T-cell lines or primary CD4(+) T cells dramatically reduced the binding of both soluble HTLV-1 SU and HTLV-1 virions. HSPGs also affected the efficiency of HTLV-1 entry, since blocking the interaction with HSPGs markedly reduced both the internalization of HTLV-1 virions and the titer of HTLV-1 pseudotyped viral infection in CD4(+) T cells. Thus, HSPGs play a critical role in the binding and entry of HTLV-1 into CD4(+) T cells.

摘要

硫酸乙酰肝素蛋白聚糖(HSPGs)被多种病毒用于促进进入宿主细胞。对于逆转录病毒人类T细胞白血病病毒1型(HTLV-1),最近有报道称,HSPGs对于可溶性HTLV-1 SU的有效结合以及HTLV假型病毒进入非T细胞至关重要。然而,据报道,HTLV-1的主要体内靶标CD4(+) T细胞表达低水平或无法检测到的HSPGs。在本研究中,我们重新检查了CD4(+) T细胞中HSPGs的表达,并研究了它们在HTLV-1附着和进入中的作用。我们观察到,虽然静止的原代CD4(+) T细胞不表达可检测水平的HSPGs,但免疫激活后的原代CD4(+) T细胞会表达HSPGs。对已建立的CD4(+) T细胞系或原代CD4(+) T细胞表面的HSPGs进行酶促修饰,可显著降低可溶性HTLV-1 SU和HTLV-1病毒粒子的结合。HSPGs也影响HTLV-1进入的效率,因为阻断与HSPGs的相互作用会显著降低HTLV-1病毒粒子在CD4(+) T细胞中的内化以及HTLV-1假型病毒感染的滴度。因此,HSPGs在HTLV-1进入CD4(+) T细胞的过程中起着关键作用。

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