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异种移植中病毒颗粒上的α-半乳糖表位对人畜共患病的天然保护作用。

Natural protection from zoonosis by alpha-gal epitopes on virus particles in xenotransmission.

作者信息

Kim Na Young, Jung Woon-Won, Oh Yu-Kyung, Chun Taehoon, Park Hong-Yang, Lee Hoon-Taek, Han In-Kwon, Yang Jai Myung, Kim Young Bong

机构信息

Department of Animal Biotechnology, Konkuk University, Seoul, Korea.

出版信息

Xenotransplantation. 2007 Mar;14(2):104-11. doi: 10.1111/j.1399-3089.2007.00377.x.

Abstract

Clinical transplantation has become one of the preferred treatments for end-stage organ failure, and one of the novel approaches being pursued to overcome the limited supply of human organs involves the use of organs from other species. The pig appears to be a near ideal animal due to proximity to humans, domestication, and ability to procreate. The presence of Gal-alpha1,3-Gal residues on the surfaces of pig cells is a major immunological obstacle to xenotransplantation. Alpha1,3galactosyltransferase (alpha1,3GT) catalyzes the synthesis of Gal alpha 1-3Gal beta 1-4GlcNAc-R (alpha-gal epitope) on the glycoproteins and glycolipids of non-primate mammals, but this does not occur in humans. Moreover, the alpha-gal epitope causes hyperacute rejection of pig organs in humans, and thus, the elimination of this antigen from pig tissues is highly desirable. Recently, concerns have been raised that the risk of virus transmission from such pigs may be increased due to the absence of alpha-gal on their viral particles. In this study, transgenic cells expressing alpha1,3GT were selected using 1.25 mg/ml neomycin. The development of HeLa cells expressing alpha1,3GT now allows accurate studies to be conducted on the function of the alpha-gal epitope in xenotransmission. The expressions of alpha-gal epitopes on HeLa/alpha-gal cells were demonstrated by flow cytometry and confocal microscopy using cells stained with IB4-fluorescein isothiocyanate lectin. Vaccinia viruses propagated in HeLa/alpha-gal cells also expressed alpha-gal on their viral envelopes and were more sensitive to inactivation by human sera than vaccinia virus propagated in HeLa cells. Moreover, neutralization of vaccinia virus was inhibited in human serum by 10 mm ethylene glycol bis(beta-aminoethylether)tetraacetic acid (EDTA) treatment. Our data indicated that alpha-gal epitopes are one of the major barriers to zoonosis via xenotransmission.

摘要

临床移植已成为终末期器官衰竭的首选治疗方法之一,而克服人体器官供应有限所采用的新方法之一是使用其他物种的器官。由于猪与人类亲缘关系近、已被驯化且具有繁殖能力,它似乎是近乎理想的动物。猪细胞表面存在的α1,3 - 半乳糖残基是异种移植的主要免疫障碍。α1,3 - 半乳糖基转移酶(α1,3GT)催化在非灵长类哺乳动物的糖蛋白和糖脂上合成Galα1 - 3Galβ1 - 4GlcNAc - R(α - 半乳糖表位),但在人类中不会发生这种情况。此外,α - 半乳糖表位会导致人类对猪器官产生超急性排斥反应,因此,从猪组织中消除这种抗原是非常必要的。最近,有人担心由于这种猪的病毒颗粒上不存在α - 半乳糖,可能会增加病毒传播的风险。在本研究中,使用1.25mg/ml新霉素筛选表达α1,3GT的转基因细胞。表达α1,3GT的HeLa细胞的培育现在使得能够对α - 半乳糖表位在异种传播中的功能进行准确研究。通过使用异硫氰酸荧光素标记的IB4凝集素染色的细胞,通过流式细胞术和共聚焦显微镜证实了HeLa/α - 半乳糖细胞上α - 半乳糖表位的表达。在HeLa/α - 半乳糖细胞中繁殖的痘苗病毒在其病毒包膜上也表达α - 半乳糖,并且比在HeLa细胞中繁殖的痘苗病毒对人血清灭活更敏感。此外,通过10mM乙二醇双(β - 氨基乙基醚)四乙酸(EDTA)处理,人血清中痘苗病毒的中和作用受到抑制。我们的数据表明,α - 半乳糖表位是通过异种传播导致人畜共患病的主要障碍之一。

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