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抗肝素硫酸盐肽可阻断体内单纯疱疹病毒感染。

Anti-heparan sulfate peptides that block herpes simplex virus infection in vivo.

机构信息

Departments of Ophthalmology and Visual Sciences, University of Illinois, Chicago, Illinois 60612, USA.

出版信息

J Biol Chem. 2011 Jul 15;286(28):25406-15. doi: 10.1074/jbc.M110.201103. Epub 2011 May 19.

Abstract

Heparan sulfate (HS) and its highly modified form, 3-O-sulfated heparan sulfate (3-OS HS), contribute strongly to herpes simplex virus type-1 (HSV-1) infection in vitro. Here we report results from a random M13-phage display library screening to isolate 12-mer peptides that bind specifically to HS, 3-OS HS, and block HSV-1 entry. The screening identified representative candidates from two-different groups of anti-HS peptides with high positive charge densities. Group 1, represented by G1 peptide (LRSRTKIIRIRH), belongs to a class with alternating charges (XRXRXKXXRXRX), and group 2, represented by G2 peptide (MPRRRRIRRRQK), shows repetitive charges (XXRRRRXRRRXK). Viral entry and glycoprotein D binding assays together with fluorescent microscopy data indicated that both G1 and G2 were potent in blocking HSV-1 entry into primary cultures of human corneal fibroblasts and CHO-K1 cells transiently expressing different glycoprotein D receptors. Interestingly, G2 peptide isolated against 3-OS HS displayed wider ability to inhibit entry of clinically relevant strains of HSV-1 and some divergent members of herpesvirus family including cytomegalovirus and human herpesvirus-8. To identify functional residues within G1 and G2, we performed point mutations and alanine-scanning mutagenesis. Several arginine and a lysine residues were needed for anti-HSV-1 activity, suggesting the importance of the positively charged residues in virus-cell binding and virus-induced membrane fusion. In vivo administration of G1 or G2 peptide as a prophylactic eye drop completely blocked HSV-1 spread in the mouse cornea as evident by immunohistochemistry. This result also highlights an in vivo significance of HS and 3-OS HS during ocular herpes infection.

摘要

硫酸乙酰肝素 (HS) 及其高度修饰形式 3-O-硫酸乙酰肝素 (3-OS HS),强烈促进单纯疱疹病毒 1 型 (HSV-1) 在体外感染。在这里,我们报告了从随机 M13 噬菌体展示文库筛选中分离出的 12 肽的结果,这些肽特异性结合 HS、3-OS HS,并阻断 HSV-1 进入。筛选鉴定了来自两个具有高正电荷密度的抗 HS 肽不同组的代表性候选物。第 1 组,由 G1 肽 (LRSRTKIIRIRH) 代表,属于交替电荷 (XRXRXKXXRXRX) 类,第 2 组,由 G2 肽 (MPRRRRIRRRQK) 代表,显示重复电荷 (XXRRRRXRRRXK)。病毒进入和糖蛋白 D 结合实验以及荧光显微镜数据表明,G1 和 G2 都能有效阻断 HSV-1 进入原代人角膜成纤维细胞和瞬时表达不同糖蛋白 D 受体的 CHO-K1 细胞。有趣的是,针对 3-OS HS 分离的 G2 肽显示出更广泛的抑制能力,可抑制临床相关 HSV-1 株和疱疹病毒科的一些分化成员,包括巨细胞病毒和人疱疹病毒 8 的进入。为了鉴定 G1 和 G2 中的功能残基,我们进行了点突变和丙氨酸扫描诱变。抗 HSV-1 活性需要几个精氨酸和赖氨酸残基,表明正电荷残基在病毒-细胞结合和病毒诱导的膜融合中很重要。作为预防性滴眼剂,体内给予 G1 或 G2 肽完全阻止了 HSV-1 在小鼠角膜中的传播,这一点通过免疫组织化学得到了证明。这一结果也突出了 HS 和 3-OS HS 在眼部疱疹感染过程中的体内意义。

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