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θ防御素通过抑制病毒黏附和进入来保护细胞免受单纯疱疹病毒感染。

Theta defensins protect cells from infection by herpes simplex virus by inhibiting viral adhesion and entry.

作者信息

Yasin Bushra, Wang Wei, Pang Mabel, Cheshenko Natalia, Hong Teresa, Waring Alan J, Herold Betsy C, Wagar Elizabeth A, Lehrer Robert I

机构信息

Department of Pathology and Laboratory Medicine, David Geffen School of Medicine at UCLA, Los Angeles, CA 90095-1731, USA.

出版信息

J Virol. 2004 May;78(10):5147-56. doi: 10.1128/jvi.78.10.5147-5156.2004.

Abstract

We tested the ability of 20 synthetic theta defensins to protect cells from infection by type 1 and type 2 herpes simplex viruses (HSV-1 and -2, respectively). The peptides included rhesus theta defensins (RTDs) 1 to 3, originally isolated from rhesus macaque leukocytes, and three peptides (retrocyclins 1 to 3) whose sequences were inferred from human theta-defensin (DEFT) pseudogenes. We also tested 14 retrocyclin analogues, including the retro, enantio, and retroenantio forms of retrocyclin 1. Retrocyclins 1 and 2 and RTD 3 protected cervical epithelial cells from infection by both HSV serotypes, but only retrocyclin 2 did so without causing cytotoxicity or requiring preincubation with the virus. Surface plasmon resonance studies revealed that retrocyclin 2 bound to immobilized HSV-2 glycoprotein B (gB2) with high affinity (K(d), 13.3 nM) and that it did not bind to enzymatically deglycosylated gB2. Temperature shift experiments indicated that retrocyclin 2 and human alpha defensins human neutrophil peptide 1 (HNP 1) to HNP 3 protected human cells from HSV-2 by different mechanisms. Retrocyclin 2 blocked viral attachment, and its addition during the binding or penetration phases of HSV-2 infection markedly diminished nuclear translocation of VP16 and expression of ICP4. In contrast, HNPs 1 to 3 had little effect on binding but reduced both VP16 transport and ICP4 expression if added during the postbinding (penetration) period. We recently reported that theta defensins are miniature lectins that bind gp120 of human immunodeficiency virus type 1 (HIV-1) with high affinity and inhibit the entry of R5 and X4 isolates of HIV-1. Given its small size (18 residues), minimal cytotoxicity, lack of activity against vaginal lactobacilli, and effectiveness against both HSV-2 and HIV-1, retrocyclin 2 provides an intriguing prototype for future topical microbicide development.

摘要

我们测试了20种合成θ防御素保护细胞免受1型和2型单纯疱疹病毒(分别为HSV-1和HSV-2)感染的能力。这些肽包括最初从恒河猴白细胞中分离出的恒河猴θ防御素(RTDs)1至3,以及三种从人θ防御素(DEFT)假基因推断出序列的肽(反向环素1至3)。我们还测试了14种反向环素类似物,包括反向环素1的反向、对映体和反向对映体形式。反向环素1和2以及RTD 3可保护宫颈上皮细胞免受两种HSV血清型的感染,但只有反向环素2能做到这一点,且不会引起细胞毒性,也无需与病毒进行预孵育。表面等离子体共振研究表明,反向环素2以高亲和力(K(d),13.3 nM)结合固定化的HSV-2糖蛋白B(gB2),且不与酶促去糖基化的gB2结合。温度变化实验表明,反向环素2和人α防御素人中性粒细胞肽1(HNP 1)至HNP 3通过不同机制保护人细胞免受HSV-2感染。反向环素2阻断病毒附着,在HSV-2感染的结合或穿透阶段添加该肽可显著减少VP16的核转位和ICP4的表达。相比之下,HNP 1至3对结合影响不大,但如果在结合后(穿透)阶段添加,则会降低VP16的转运和ICP4的表达。我们最近报道,θ防御素是微型凝集素,能以高亲和力结合1型人类免疫缺陷病毒(HIV-1)的gp120,并抑制HIV-1的R5和X4分离株的进入。鉴于其体积小(18个残基)、细胞毒性极小、对阴道乳酸杆菌无活性以及对HSV-2和HIV-1均有效,反向环素2为未来局部杀菌剂的开发提供了一个引人关注的原型。

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