| Literature DB >> 30261752 |
Constanca Figueiredo1,2,3, Marco Carvalho Oliveira1,3, Chen Chen-Wacker1,2, Katharina Jansson4,5, Klaus Höffler4, Yuliia Yuzefovych1,2, Olena Pogozhykh1,2, Zhu Jin1,2, Mark Kühnel5,6, Danny Jonigk5,6, Bettina Wiegmann4,5, Wiebke Sommer4,5, Axel Haverich2,3,4,5, Gregor Warnecke4,5, Rainer Blasczyk1,2,3.
Abstract
Disparities at the major histocompatibility complex (MHC) antigens and associated minor antigens trigger harmful immune responses, leading to graft rejection after transplantation. We showed that MHC-silenced cells and tissues are efficiently protected against rejection. In complex vascularized organs, the endothelium is the major interface between donor and recipient. This study therefore aimed to reduce the immunogenicity of the lung by silencing MHC expression on the endothelium. In porcine lungs, short-hairpin RNAs targeting beta-2-microglobulin and class II-transactivator transcripts were delivered by lentiviral vectors during normothermic ex vivo perfusion to silence swine leukocyte antigen (SLA) I and II expression permanently. The results demonstrated the feasibility of genetically engineering all lung regions, achieving a targeted silencing effect for SLA I and II of 67% and 52%, respectively, without affecting cell viability or tissue integrity. This decrease in immunogenicity carries the potential to generate immunologically invisible organs to counteract the burden of rejection and immunosuppression.Entities:
Keywords: HLA; MHC silencing; gene therapy; histocompatibility; immunogenicity; organ engineering
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Year: 2018 PMID: 30261752 DOI: 10.1089/hum.2018.117
Source DB: PubMed Journal: Hum Gene Ther ISSN: 1043-0342 Impact factor: 5.695