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Tat介导的蛋白质递送可促进抗原的MHC I类呈递。

Tat-mediated protein delivery can facilitate MHC class I presentation of antigens.

作者信息

Moy P, Daikh Y, Pepinsky B, Thomas D, Fawell S, Barsoum J

机构信息

Biogen Inc., Cambridge, MA 02142, USA.

出版信息

Mol Biotechnol. 1996 Oct;6(2):105-13. doi: 10.1007/BF02740767.

Abstract

We have previously shown that the tat protein of HIV-1 can be used as a carrier to promote the intracellular delivery of heterologous proteins. Here we have tested if the tat-delivery technology can be used to direct MHC class I presentation of native protein, using ovalbumin (OVA) as a model system. We show that a tat-ovalbumin conjugate (tatOVA) can be delivered into cells and that subsequent processing and presentation occurs, resulting in effective and specific killing of these target cells by an OVA specific cytotoxic T-lymphocyte (CTL) line. Comparison with the E.G7 line that expresses the OVA gene indicates that tat-mediated delivery is as efficient as endogenous expression in this system. Tat-mediated antigenic protein delivery may be useful both as a research technique and, potentially, as a therapeutic or prophylactic vaccine.

摘要

我们之前已经表明,HIV-1的tat蛋白可作为载体促进异源蛋白的细胞内递送。在此,我们以卵清蛋白(OVA)作为模型系统,测试了tat递送技术是否可用于指导天然蛋白的MHC I类呈递。我们发现,tat-卵清蛋白偶联物(tatOVA)能够递送至细胞内,随后发生加工和呈递,导致OVA特异性细胞毒性T淋巴细胞(CTL)系对这些靶细胞进行有效且特异性的杀伤。与表达OVA基因的E.G7细胞系比较表明,在该系统中tat介导的递送与内源性表达一样高效。tat介导的抗原性蛋白递送作为一种研究技术,以及潜在地作为一种治疗性或预防性疫苗可能都是有用的。

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