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首页> 外文期刊>Vaccine >A trivalent gC2/gD2/gE2 vaccine for herpes simplex virus generates antibody responses that block immune evasion domains on gC2 better than natural infection
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A trivalent gC2/gD2/gE2 vaccine for herpes simplex virus generates antibody responses that block immune evasion domains on gC2 better than natural infection

机译:用于疱疹病毒的三价GC2 / GD2 / GE2疫苗产生抗体反应,其比自然感染更好地嵌入GC2上的免疫湿度域

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摘要

Vaccines for prevention and treatment of genital herpes are high public health priorities. Our approach towards vaccine development is to focus on blocking virus entry mediated by herpes simplex virus type 2 (HSV-2) glycoprotein D (gD2) and to prevent the virus from evading complement and antibody attack by blocking the immune evasion domains on HSV-2 glycoproteins C (gC2) and E (gE2), respectively. HSV-2 gC2 and gE2 are expressed on the virion envelope and infected cell surface where they are potential targets of antibodies that bind and block their immune evasion activities. We demonstrate that antibodies produced during natural infection in humans or intravaginal inoculation in guinea pigs bind to gC2 but generally fail to block the immune evasion domains on this glycoprotein. In contrast, immunization of naive or previously HSV-2-infected guinea pigs with gC2 subunit antigen administered with CpG and alum as adjuvants produces antibodies that block domains involved in immune evasion. These results indicate that immune evasion domains on gC2 are weak antigens during infection, yet when used as vaccine immunogens with adjuvants the antigens produce antibodies that block immune evasion domains. (C) 2018 Elsevier Ltd. All rights reserved.
机译:用于预防和治疗生殖器疱疹的疫苗是高公共卫生优先事项。我们对疫苗开发的方法是专注于阻断单纯疱疹病毒型2(HSV-2)糖蛋白D(GD2)介导的病毒进入,并通过阻断HSV-2上的免疫湿度域来防止病毒逃避补体和抗体攻击糖蛋白C(GC2)和E(GE2)分别。 HSV-2 GC2和GE2在病毒群封套和受感染的细胞表面上表达,其中它们是抗体的潜在靶标,其结合并阻止其免疫逃逸活性。我们证明,在人类或豚鼠中静脉内接种期间产生的抗体与GC2结合,但通常不能阻断这种糖蛋白的免疫湿度域。相反,幼稚或先前HSV-2感染的豚鼠免疫与CpG和Alum施用的GC2亚基抗原作为佐剂产生抗体,其抑制涉及免疫逃逸的域。这些结果表明,在感染期间GC2上的免疫逃逸结构域是弱抗原,但用作辅助疫苗免疫原的抗原产生阻断免疫避免结构域的抗体。 (c)2018年elestvier有限公司保留所有权利。

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