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首页> 外文期刊>Clinical and vaccine immunology: CVI >Cross-Reactivity, Epitope Spreading, and De Novo Immune Stimulation Are Possible Mechanisms of Cross-Protection of Nonvaccine Human Papillomavirus (HPV) Types in Recipients of HPV Therapeutic Vaccines
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Cross-Reactivity, Epitope Spreading, and De Novo Immune Stimulation Are Possible Mechanisms of Cross-Protection of Nonvaccine Human Papillomavirus (HPV) Types in Recipients of HPV Therapeutic Vaccines

机译:交叉反应性,表位扩散和从头免疫刺激是HPV治疗疫苗接受者中非疫苗的人乳头瘤病毒(HPV)类型的交叉保护的可能机制

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摘要

Numerous versions of human papillomavirus (HPV) therapeutic vaccines designed to treat individuals with established HPV infection, including those with cervical intraepithelial neoplasia (CIN), are in development because approved prophylactic vaccines are not effective once HPV infection is established. As human papillomavirus 16 (HPV-16) is the most commonly detected type worldwide, all versions of HPV therapeutic vaccines contain HPV-16, and some also contain HPV-18. While these two HPV types are responsible for approximately 70% of cervical cancer cases, there are other high-risk HPV types known to cause malignancy. Therefore, it would be of interest to assess whether these HPV therapeutic vaccines may confer cross-protection against other high-risk HPV types. Data available from a few clinical trials that enrolled subjects with CINs regardless of the HPV type(s) present demonstrated clinical responses, as measured by CIN regression, in subjects with both vaccine-matched and nonvaccine HPV types. The currently available evidence demonstrating cross-reactivity, epitope spreading, and de novo immune stimulation as possible mechanisms of cross-protection conferred by investigational HPV therapeutic vaccines is discussed.
机译:许多版本的人乳头瘤病毒(HPV)治疗性疫苗旨在治疗既定的HPV感染者,包括颈椎上皮内肿瘤(CIN)的人,因为一旦建立了HPV感染,就无效。由于人乳头瘤病毒16(HPV-16)是全球最常见的类型,因此所有版本的HPV治疗疫苗都包含HPV-16,有些也包含HPV-18。虽然这两种HPV类型造成约70%的宫颈癌病例,但还有其他已知引起恶性肿瘤的高危HPV类型。因此,评估这些HPV治疗疫苗是否可以允许其他高风险HPV类型的交叉保护是有意思的。从一些临床试验中获得的数据可从CIN回归中衡量的一些临床试验,这些临床试验招募了CIN的受试者,无论何种HPV类型,在疫苗匹配和非疫苗HPV类型的受试者中都显示出临床反应。目前可用的证据表明,讨论了研究性HPV治疗疫苗赋予的交叉保护的交叉反应性,表位扩散和从头刺激的可能机制。

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