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监测异种移植后的 PERV。

Monitoring for PERV Following Xenotransplantation.

机构信息

Institute of Virology, Free University Berlin, Berlin, Germany.

出版信息

Transpl Int. 2024 Oct 7;37:13491. doi: 10.3389/ti.2024.13491. eCollection 2024.

Abstract

Porcine endogenous retroviruses (PERVs) are integrated in the genome of all pigs. PERV-A, PERV-B and PERV-C can be released as infectious virus particles and PERV-A and PERV-B can infect human cells in culture. PERV-C does not infect human cells, but high-titer recombinant PERV-A/C can infect them. Retroviruses are able to induce immunosuppression and/or tumors in the infected host. Numerous methods have been developed to study PERV in donor pigs. No PERV infections were observed in infection experiments as well as in preclinical and clinical xenotransplantation trials. Despite this, several strategies have been developed to prevent PERV infection of the recipient. PCR-based and immunological methods are required to screen xenotransplant recipients. Since the proviruses are integrated into the pig genome, PERV infection has to be distinguished from microchimerism, e.g., the presence of pig cells in the recipient, which is common in xenotransplantation. Sensitive PCR methods using pig short interspersed nuclear elements (SINE) sequences allow to detect pig cells easily. Virus infection can also be detected by an increase of viral genomic or mRNA in human cells. The method of choice, however, is to screen for specific antibodies against PERV using different recombinant PERV proteins, purified viruses or peptides.

摘要

猪内源性逆转录病毒(PERVs)整合在所有猪的基因组中。PERV-A、PERV-B 和 PERV-C 可以作为感染性病毒颗粒释放,并且 PERV-A 和 PERV-B 可以感染培养中的人类细胞。PERV-C 不能感染人类细胞,但高滴度重组 PERV-A/C 可以感染它们。逆转录病毒能够在感染的宿主中诱导免疫抑制和/或肿瘤。已经开发了许多方法来研究供体猪中的 PERV。在感染实验以及临床前和临床异种移植试验中均未观察到 PERV 感染。尽管如此,已经开发了几种策略来防止 PERV 感染受体。需要基于 PCR 的和免疫学方法来筛选异种移植受体。由于前病毒整合到猪的基因组中,因此必须将 PERV 感染与微嵌合体区分开来,例如,受体中存在猪细胞,这在异种移植中很常见。使用猪短散布核元件(SINE)序列的敏感 PCR 方法可以轻松检测猪细胞。通过人细胞中病毒基因组或 mRNA 的增加也可以检测到病毒感染。然而,选择的方法是使用不同的重组 PERV 蛋白、纯化的病毒或肽来筛选针对 PERV 的特异性抗体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f54d/11491343/17951ea7ca30/ti-37-13491-g001.jpg

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