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GROWTH TRANSFORMATION OF ANTIGEN-SPECIFIC T CELL LINES FROM RHESUS MONKEYS BY HERPESVIRUS SAIMIRI

机译:疱疹病毒SAIMIRI转化来自猴猴的抗原特异性T细胞系的生长转化

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摘要

This study aims in establishing the in vitro basis for a primate model to evaluate potential applications of H. saimiri-transformed T cells. T cell lines specific for myelin basic protein and streptolysin O were derived from rhesus monkeys and transformed to stable antigen-independent growth with strain G488 of H. saimiri. The transformed T cells from rhesus monkeys did not produce infectious virus and harbored the H. saimiri genome exclusively in an episomal form, whereas transformed T cells from the New World monkey Calltithrix jacchus released infectious virus. Transformed T cells from rhesus monkeys showed an unaltered surface expression of CD2 and CD3, of the activation markers CD25 and CD69, and of the costimulatory molecule CD80 (B7.1). Remarkably, both transformed and nontransformed T cell lines were largely double-positive for CD4 and CD8. In contrast to the parental cell lines, the transformed cells constitutively expressed major histocompatibility complex-DR antigens and were able to present antigen to each other. The transformed T cells from rhesus monkeys continued to express a functionally intact T cell receptor and responded to recognition of their antigen with enhanced proliferation and production of Th1-type cytokines. In conclusion, H. saimiri-transformed rhesus monkey T cells may open a way to primate models for adoptive immunotherapy and studies on the pathogenesis of autoaggressive T cells.
机译:这项研究的目的是建立灵长类动物模型的体外基础,以评估赛默氏杆菌转化的T细胞的潜在应用。特异于髓鞘碱性蛋白和链球菌溶血素O的T细胞系衍生自恒河猴,并转化为稳定的不依赖于抗原的H. saimiri菌株G488。来自恒河猴的转化的T细胞不产生传染性病毒,并且仅以附加体形式包含赛米氏嗜血杆菌基因组,而来自新大陆猴Calltithrix jacchus的转化的T细胞释放了传染性病毒。来自恒河猴的转化T细胞显示CD2和CD3,激活标记CD25和CD69以及共刺激分子CD80(B7.1)的表面表达未改变。值得注意的是,转化的和未转化的T细胞系对CD4和CD8都双重阳性。与亲代细胞系相反,转化的细胞组成型表达主要的组织相容性复合物-DR抗原,并且能够彼此呈递抗原。从恒河猴转化的T细胞继续表达功能完整的T细胞受体,并通过增强Th1型细胞因子的增殖和产生来响应对其抗原的识别。总之,H。saimiri转化的恒河猴T细胞可能为灵长类动物模型提供过继免疫治疗和研究自发性T细胞发病机制的途径。

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