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一种针对皮肤型人乳头瘤病毒的广谱保护性疫苗。

A broadly protective vaccine against cutaneous human papillomaviruses.

作者信息

Mariz Filipe Colaco, Balz Kathrin, Dittrich Manuela, Zhang Yueru, Yang Fan, Zhao Xueer, Bolchi Angelo, Ottonello Simone, Müller Martin

机构信息

German Cancer Research Center, Im Neuenheimer Feld 242, 69120, Heidelberg, Germany.

Department of Chemistry, Life Sciences and Environmental Sustainability, University of Parma, 43124, Parma, Italy.

出版信息

NPJ Vaccines. 2022 Oct 10;7(1):116. doi: 10.1038/s41541-022-00539-0.

Abstract

Skin colonization by human papillomavirus (HPV) is typically related to inconspicuous cutaneous infections without major disease or complications in immunocompetent individuals. However, in immunosuppressed patients, especially organ transplanted recipients, cutaneous HPV infections may cause massive, highly spreading and recurrent skin lesions upon synergism with UV-exposure. Current HPV prophylactic vaccines are not effective against cutaneous HPV types (cHPV). By applying a modular polytope-based approach, in this work, we explored different vaccine candidates based on selected, tandemly arranged cHPV-L2 epitopes fused to thioredoxin (Trx) as a scaffold protein. Upon conversion to heptameric nanoparticles with the use of a genetically fused oligomerization domain, our candidate Trx-L2 vaccines induce broadly neutralizing immune responses against 19 cHPV in guinea pigs. Similar findings were obtained in mice, where protection against virus challenge was also achieved via passive transfer of immune sera. Remarkably, immunization with the candidate cHPV vaccines also induced immune responses against several mucosal low- and high-risk HPV types, including HPV16 and 18. Based on cumulative immunogenicity data but also on ease and yield of production, we identified a lead vaccine candidate bearing 12 different cHPV-L2 epitopes that holds great promise as a scalable and GMP production-compatible lead molecule for the prevention of post-transplantation skin lesions caused by cHPV infection.

摘要

人乳头瘤病毒(HPV)在皮肤的定植通常与免疫功能正常个体中不明显的皮肤感染有关,不会引发重大疾病或并发症。然而,在免疫抑制患者中,尤其是器官移植受者,皮肤HPV感染在与紫外线暴露协同作用时,可能会导致大量、高度扩散且反复发作的皮肤病变。目前的HPV预防性疫苗对皮肤型HPV(cHPV)无效。在这项工作中,我们采用基于模块化多聚体的方法,探索了不同的候选疫苗,这些疫苗基于选定的、串联排列的cHPV-L2表位与硫氧还蛋白(Trx)融合,Trx作为支架蛋白。通过使用基因融合的寡聚化结构域将其转化为七聚体纳米颗粒后,我们的候选Trx-L2疫苗在豚鼠中诱导了针对19种cHPV的广泛中和免疫反应。在小鼠中也获得了类似的结果,通过被动转移免疫血清也实现了对病毒攻击的保护。值得注意的是,用候选cHPV疫苗免疫还诱导了针对几种黏膜低危和高危HPV类型的免疫反应,包括HPV16和18。基于累积的免疫原性数据以及生产的简便性和产量,我们确定了一种领先的候选疫苗,它含有12种不同的cHPV-L2表位,作为一种可扩展且与GMP生产兼容的领先分子,有望预防由cHPV感染引起的移植后皮肤病变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/afa3/9550855/28351836d852/41541_2022_539_Fig1_HTML.jpg

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