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具有抗体聚集病毒抗原的H-2抗原的选择性和单向膜再分布:与细胞毒性T细胞相互作用机制的关系。

Selective and unidirectional membrane redistribution of an H-2 antigen with an antibody-clustered viral antigen: relationship to mechanisms of cytotoxic T-cell interactions.

作者信息

Geiger B, Rosenthal K L, Klein J, Zinkernagel R M, Singer S J

出版信息

Proc Natl Acad Sci U S A. 1979 Sep;76(9):4603-7. doi: 10.1073/pnas.76.9.4603.

Abstract

We have studied the co-redistribution of vesicular stomatitis virus (VSV) antigen and of individual H-2 antigens on the surfaces of mouse cells, and in parallel we have also used these VSV-infected cells as targets in cytotoxic T-cell killing experiments. Antibody-induced patching and capping of the VSV antigen caused an extensive co-patching and co-capping of the H-2Kb antigen but not of the H-2Db antigen. In reciprocal experiments, the antibody-induced patching of the H-2Kb or H-2Db antigen did not result in a co-patching of the VSV antigen. Radioimmunoassays showed that the relative numbers of H-2Kb, H-2Db, and VSV antigens on the surfaces of the cells exhibiting such nonreciprocal co-redistributions were closely similar. Furthermore, the H-2 restricted cytotoxic T-cell lysis of these target cells showed a marked preference for H-2Kb compared to H-2Db compatibility. We propose that the VSV and H-2 antigens are molecularly independent entities in the unpreturbed target cell membrane but that the antibody-induced clustering of the VSV antigen causes a selective and unidirectional co-redistribution (which we designate as syn-capping) of H-2Kb with the VSV antigen clusters. It is suggested that such a T-cell-induced syn-capping process involving an antigen and an H-2 molecule on the target cell may play a critical role in the mechanism of cytotoxic T-cell killing.

摘要

我们研究了水疱性口炎病毒(VSV)抗原与单个H-2抗原在小鼠细胞表面的共同再分布情况,同时,我们还将这些感染VSV的细胞用作细胞毒性T细胞杀伤实验的靶标。抗体诱导的VSV抗原的斑块形成和帽化导致H-2Kb抗原广泛的共同斑块形成和共同帽化,但H-2Db抗原没有。在反向实验中,抗体诱导的H-2Kb或H-2Db抗原的斑块形成并未导致VSV抗原的共同斑块形成。放射免疫分析表明,表现出这种非相互性共同再分布的细胞表面上H-2Kb、H-2Db和VSV抗原的相对数量非常相似。此外,与H-2Db相容性相比,这些靶细胞的H-2限制性细胞毒性T细胞裂解对H-2Kb表现出明显的偏好。我们提出,在未受干扰的靶细胞膜中,VSV和H-2抗原是分子独立的实体,但抗体诱导的VSV抗原聚集导致H-2Kb与VSV抗原簇发生选择性和单向的共同再分布(我们将其称为同步帽化)。有人认为,这种涉及靶细胞上抗原和H-2分子的T细胞诱导的同步帽化过程可能在细胞毒性T细胞杀伤机制中起关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8ea3/411627/139eae4c517d/pnas00009-0453-a.jpg

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