Preferential repopulation of the small intestine by gut-derived T cell precursors in the murine system.

Cytobios Pub Date : 1999-01-01
M Hamad
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Abstract

The potential of intestinal intraepithelial lymphocyte (IEL) precursors to repopulate the lymphoid components of lethally-irradiated mice was evaluated. Mice injected with total IEL, or IEL depleted of mature T cells, died within 2 weeks post-irradiation. Injection of T cell-depleted Thy-1.1 IEL and Thy-1.2 bone marrow (BM) into lethally-irradiated Thy-1.2 mice resulted in survival rates greater than 90%. The vast majority of thymocytes analysed at 2, 6, and 10 weeks post-treatment were Thy-1.2+. The Thy-1.1+ and Thy-1.2+ cells were detected in the spleen 2 and 6 weeks post-reconstitution. After 10 weeks, the majority of splenic T cells were Thy-1.2+. The majority of Thy-1+ IEL were of the Thy-1.1 subtype at 2 and 6 weeks after reconstitution. After 10 weeks, Thy-1.2+ IEL became the predominant subtype. Flow cytometry (FCM) analyses of Thy-1.1+ IEL showed that Thy-1.1 was co-expressed with CD3, CD4, CD5, CD8, TCR alpha beta and TCR gamma delta T cell markers. These findings indicate that IEL precursors home preferentially to gut epithelia and generate complex IEL phenotypic subsets.

小鼠肠道源性T细胞前体对小肠的优先再生。
评估了肠上皮内淋巴细胞(IEL)前体重新填充致死性辐照小鼠淋巴样成分的潜力。注射总IEL或缺乏成熟T细胞的IEL的小鼠在照射后2周内死亡。将T细胞耗尽的Thy-1.1 IEL和Thy-1.2骨髓(BM)注射到致命照射的Thy-1.2小鼠中,存活率大于90%。在治疗后2、6和10周,绝大多数胸腺细胞为Thy-1.2+。重建后2周和6周,在脾脏中检测到Thy-1.1+和Thy-1.2+细胞。10周后,脾T细胞以Thy-1.2+为主。在重构后2周和6周,大多数Thy-1+ IEL为Thy-1.1亚型。10周后,Thy-1.2+ IEL成为优势亚型。流式细胞术(FCM)分析显示,Thy-1.1+ IEL与CD3、CD4、CD5、CD8、TCR α β和TCR γ δ T细胞标志物共表达。这些发现表明,IEL前体优先返回肠道上皮,并产生复杂的IEL表型亚群。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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