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首页> 外文期刊>Bulletin of experimental biology and medicine >Cross Reactivity of T Cell Receptor on Memory CD8+ Cells Isolated after Immunization with Allogeneic Tumor Cells.
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Cross Reactivity of T Cell Receptor on Memory CD8+ Cells Isolated after Immunization with Allogeneic Tumor Cells.

机译:同种异体肿瘤细胞免疫接种后,T细胞受体对内存CD8 +细胞的交叉反应性。

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Experiments on mice deficient in expression of class I major histocompatibility complex molecules showed that memory CD8+ cells recognizing the alloantigen by the direct allogeneic recognition mechanism selectively proliferated in response to heated allogeneic cells. Adoptive transfer of memory cells from mice expressing green fluorescent protein transgene to wild-type animals showed for the first time that long-living memory cells suppress the response of naive T cells and abolish their involvement in the pool of memory cells. The pool of long-living memory T cells was obtained in vitro with heated allogeneic stimulators. Apart from immunizing alloantigen, this clone recognized foreign molecules of the major histocompatibility complex. Cloning and sequencing of rearranged regions in memory T cells showed that two alpha-chains and one functional beta-chain are rearranged in cells of this pool. Only one alpha-chain was capable of forming protein product, which determines expression of only one form of Tcell receptor. Experimental data directly confirm the hypothesis about degeneracy of recognition of allelic products of major histocompatibility complex molecules by T cell receptors. Suppression of the response of naive cells by memory cells probably underlies a previously unknown type of polarization of the immune response and determines clonal dominance and peripheral selection of T lymphocytes.
机译:I类主要组织相容性复合物分子表达缺乏的小鼠实验表明,通过直接同种异体识别机制识别出血液鉴定的记忆CD8 +细胞响应于加热的同种异体细胞选择性增殖。从表达绿色荧光蛋白转基因的小鼠对野生型动物的小鼠的记忆细胞的养存细胞显示在野生型动物的第一次显示中,第一次抑制幼稚T细胞的响应并取消他们参与存储器电池池。在体外用加热的同种异体刺激器获得长生存记忆T细胞库。除了免疫含有血管蛋白外,该克隆公认的主要组织相容性复合物的外部分子。内存T细胞中重排区域的克隆和测序显示,在该池的细胞中重新排列了两个α-链和一个功能性β-链。只有一个α链能够形成蛋白质产物,这决定了一种形式的Tcell受体的表达。实验数据直接确认了T细胞受体识别主要组织相容性复合物分子的等位基因产物的退化性的假设。通过记忆细胞抑制幼稚细胞的响应可能是先前未知的免疫应答的偏振类型,并确定克隆优势和外周选择T淋巴细胞。

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