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小鼠细胞毒性T淋巴细胞库的外周(体细胞)扩展。I. 对成年或老年DBA/2J小鼠胸腺和脾脏来源的同种反应性T细胞识别库多样性的分析。

Peripheral (somatic) expansion of the murine cytotoxic T lymphocyte repertoire. I. Analysis of diversity in recognition repertoire of alloreactive T cells derived from the thymus and spleen of adult or aged DBA/2J mice.

作者信息

Chang M P, Gorczynski R M

出版信息

J Immunol. 1984 Nov;133(5):2375-80.

PMID:6332848
Abstract

Cytotoxic T lymphocyte precursors (CTLp) in the spleen or thymus of individual adult (8 to 10 wk) or aged (greater than 20 mo) DBA/2J mice have been activated by irradiated H-2Kb antigens under limiting dilution conditions such that cytotoxic cells in responder wells result from stimulation of a single CTLp. After division into several equal samples and expansion in the presence of IL 2 and more irradiated H-2Kb stimulators, the contents of replicate individual wells were tested for their ability to lyse a panel of selected H-2Kb mutant targets. The heterogeneity within a given age group, and the similarity of CTLp repertoires between different age groups were then compared for splenic and thymic CTLp repertoires. Our data indicate a far greater mouse-to-mouse variation for the splenic CTLp repertoire of aged mice compared with young mice, despite the greater heterogeneity of the repertoire in the latter case. Less difference was seen for the thymic CTLp repertoire. When we studied the correlation between the repertoires present in the thymus and spleen within a given age group, it seemed that the most striking difference in aged mice was a loss of systematic expansion of the early appearing thymic CTLp repertoire. These findings are discussed in terms of a two-stage model of T cell differentiation.

摘要

在有限稀释条件下,用经照射的H-2Kb抗原激活了成年(8至10周)或老龄(大于20个月)DBA/2J小鼠脾脏或胸腺中的细胞毒性T淋巴细胞前体(CTLp),使得应答孔中的细胞毒性细胞来自单个CTLp的刺激。将细胞分成几个相等的样本,并在白细胞介素2和更多经照射的H-2Kb刺激物存在下进行扩增,然后测试重复的单个孔的内容物裂解一组选定的H-2Kb突变靶标的能力。然后比较了给定年龄组内的异质性以及不同年龄组之间脾脏和胸腺CTLp库的相似性。我们的数据表明,与年轻小鼠相比,老龄小鼠脾脏CTLp库在小鼠之间的差异要大得多,尽管年轻小鼠的库异质性更大。胸腺CTLp库的差异较小。当我们研究给定年龄组内胸腺和脾脏中存在的库之间的相关性时,似乎老龄小鼠最显著的差异是早期出现的胸腺CTLp库的系统性扩增丧失。根据T细胞分化的两阶段模型对这些发现进行了讨论。

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