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通过果蝇触角足同源结构域将外源性抗原引入MHC I类加工和呈递途径可在体内引发细胞毒性T细胞。

Introduction of exogenous antigens into the MHC class I processing and presentation pathway by Drosophila antennapedia homeodomain primes cytotoxic T cells in vivo.

作者信息

Schutze-Redelmeier M P, Gournier H, Garcia-Pons F, Moussa M, Joliot A H, Volovitch M, Prochiantz A, Lemonnier F A

机构信息

AIDS-Retrovirus Department, Antiviral Cellular Immunity Unit, Pasteur Institute, Paris, France.

出版信息

J Immunol. 1996 Jul 15;157(2):650-5.

PMID:8752913
Abstract

The homeodomain of the Antennapedia molecule (AntpHD) spontaneously crosses cellular membranes and can be used to deliver up to 50 additional amino acids to the cytoplasm. We exploited this approach to deliver antigenic peptides to the MHC class I processing and presentation pathway. AntpHD-based fusion peptides expressing the 170-179 HLA-Cw3 CTL epitope (pCw3) were produced in bacteria. Incubation of these fusion peptides with H-2d target cells resulted in efficient delivery to the cytosol as indicated by protease resistance and confocal microscopy. Moreover, this introduction of an exogenous Ag resulted in sensitization of the cell to lysis by a CTL clone specific for the 170-179 HLA-Cw3-derived peptide. Sensitivity of the Ag processing to brefeldin A but not to chloroquine is consistent with the delivery of AntpHD fusion peptides to the conventional class I-associated processing pathway. Immunization of DBA/2 (H-2d) mice with AntpHD pCw3 fusion peptide in the presence of SDS primed H-2Kd-restricted HLA-Cw3-specific CTL. Similar results were obtained with AntpHD fusion peptides expressing the 147-156 influenza nucleoprotein peptide. The strategy outlined in this paper provides a new approach for introducing molecules into the MHC class I Ag-presenting pathway. This approach has clear relevance to the design of synthetic peptide-based vaccines.

摘要

触角足蛋白分子的同源结构域(AntpHD)能自发穿过细胞膜,可用于向细胞质中递送多达50个额外的氨基酸。我们利用这种方法将抗原肽递送至MHC I类加工和呈递途径。在细菌中产生了表达170 - 179 HLA - Cw3 CTL表位(pCw3)的基于AntpHD的融合肽。这些融合肽与H - 2d靶细胞孵育后,蛋白酶抗性和共聚焦显微镜结果表明其有效地递送至胞质溶胶。此外,这种外源性抗原的导入使细胞对针对170 - 179 HLA - Cw3衍生肽的CTL克隆裂解敏感。抗原加工对布雷菲德菌素A敏感而对氯喹不敏感,这与AntpHD融合肽递送至传统的I类相关加工途径一致。在SDS存在下,用AntpHD pCw3融合肽免疫DBA/2(H - 2d)小鼠,引发了H - 2Kd限制的HLA - Cw3特异性CTL。表达147 - 156流感核蛋白肽的AntpHD融合肽也得到了类似结果。本文概述的策略为将分子引入MHC I类抗原呈递途径提供了一种新方法。这种方法与基于合成肽的疫苗设计明显相关。

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