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基于腺病毒的 HPV L2 疫苗可诱导广泛的交叉反应性体液免疫应答。

Adenovirus based HPV L2 vaccine induces broad cross-reactive humoral immune responses.

机构信息

Janssen Vaccines and Prevention, Pharmaceutical Companies of Johnson and Johnson, Leiden, The Netherlands.

Janssen Vaccines and Prevention, Pharmaceutical Companies of Johnson and Johnson, Leiden, The Netherlands.

出版信息

Vaccine. 2018 Jul 16;36(30):4462-4470. doi: 10.1016/j.vaccine.2018.06.024. Epub 2018 Jun 18.

DOI:10.1016/j.vaccine.2018.06.024
PMID:29914845
Abstract

Oncogenic high-risk human papillomavirus (HPV) infections cause a substantial number of genital and non-genital cancers worldwide. Approximately 70% of all cervical cancers are caused by the high-risk HPV16 and 18 types. The remaining 30% can be attributed to twelve other high-risk HPV-types. Highly efficacious 2-valent, 4-valent and 9-valent L1 protein based prophylactic HPV vaccines are available however with limited cross-protection. To further increase the coverage, development of a multivalent cross-protective HPV vaccine is currently focused on the conserved N-terminus of HPV's L2 protein. We have developed a vaccine candidate based on the rare human adenovirus type 35 (HAdV35) vector that displays a concatemer of L2 protein epitopes from four different HPV-types via protein IX (pIX). A mix of two heterologous HAdV35 pIX-L2 display vectors present highly conserved linear epitopes of nine HPV-types. Each HAdV35 pIX-L2 display vector exhibits a good manufacturability profile. HAdV35 pIX-L2 display vaccine vectors were immunogenic and induced neutralizing antibodies against HPV-types included in the vaccine and cross-neutralizing antibodies against distant a HPV-type not included in the vaccine in mice. The HAdV35 pIX-L2 display vectors offer an opportunity for a multivalent HAdV-based prophylactic HPV vaccine.

摘要

致癌性高危型人乳头瘤病毒(HPV)感染在全球范围内导致了大量的生殖器和非生殖器癌症。大约 70%的宫颈癌由高危型 HPV16 和 18 型引起。其余 30%可归因于另外 12 种高危型 HPV。目前已有高效的二价、四价和九价基于 L1 蛋白的预防性 HPV 疫苗,但交叉保护作用有限。为了进一步提高覆盖面,目前正在开发一种多价交叉保护 HPV 疫苗,重点是 HPV 的 L2 蛋白保守的 N 端。我们已经开发了一种基于罕见的人腺病毒 35 型(HAdV35)载体的疫苗候选物,该载体通过蛋白 IX(pIX)展示来自四种不同 HPV 型的 L2 蛋白表位的串联体。两种异源 HAdV35 pIX-L2 展示载体的混合物呈现出九种 HPV 型的高度保守线性表位。每种 HAdV35 pIX-L2 展示载体都具有良好的可制造性特征。HAdV35 pIX-L2 展示疫苗载体具有免疫原性,并在小鼠中诱导了针对疫苗中包含的 HPV 型的中和抗体以及针对疫苗中未包含的遥远 HPV 型的交叉中和抗体。HAdV35 pIX-L2 展示载体为基于 HAdV 的多价预防性 HPV 疫苗提供了机会。

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