首页> 外文OA文献 >Major histocompatibility complex-linked immune-responsiveness is acquired by lymphocytes of low-responder mice differentiating in thymus of high-responder mice.
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Major histocompatibility complex-linked immune-responsiveness is acquired by lymphocytes of low-responder mice differentiating in thymus of high-responder mice.

机译:主要的组织相容性复合物相关的免疫反应性是由低反应性小鼠的淋巴细胞分化为高反应性小鼠的胸腺获得的。

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摘要

Female murine T cells can respond to the Y antigen of male cells by generating cytotoxic T-killer lymphocytes. Responsiveness is linked to several H-2 genes. Two types of low responders can be distinguished: the B10.A(5R) (H-2i5) strain, a low responder because it lacks Y-specific precursor T cells able to differentiate into cytotoxic T-killer cells; and the CBA/J (H-2k) strain, a low responder because it lacks Y-specific T-helper cells able to support differentiation of T-killer cell precursors. B10.A(5R) stem cells differentiating in an x-irradiated (CBA/J X C57BL/6) (H-2k X H-2b)F1 host respond to Y antigen by generating T-killer cells whereas CBA/J stem cells do not. The results are consistent with the hypothesis that diversity of T-cell receptors is generated by somatic mutation of germ-line genes encoding specificity for self-H-2. A detailed account of this hypothesis is presented.
机译:雌性鼠T细胞可通过产生细胞毒性T杀伤性淋巴细胞对雄性细胞的Y抗原作出反应。反应性与几个H-2基因有关。可以区分两种类型的低应答者:B10.A(5R)(H-2i5)菌株,一种低应答者,因为它缺乏能够分化为细胞毒性T杀伤细胞的Y特异性前体T细胞。以及CBA / J(H-2k)品系,因为它缺乏能够支持T杀伤细胞前体分化的Y特异性T辅助细胞,因此反应较慢。在X射线照射(CBA / JX C57BL / 6)(H-2k X H-2b)F1宿主中分化的B10.A(5R)干细胞通过产生T杀伤细胞来应答Y抗原,而CBA / J干细胞不。该结果与这样的假设相符,即T细胞受体的多样性是由编码对自身H-2的特异性的种系基因的体细胞突变产生的。提出了该假设的详细说明。

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