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首页> 外文期刊>Developmental Immunology: Journal of Immunology Research >Temporary, but Essential Requirement of CD8+T Cells Early in the Pathogenesis of Diabetes in BB Rats as Revealed by Thymectomy and CD8 Depletion
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Temporary, but Essential Requirement of CD8+T Cells Early in the Pathogenesis of Diabetes in BB Rats as Revealed by Thymectomy and CD8 Depletion

机译:胸腺切除术和CD8耗竭揭示了BB大鼠糖尿病发病早期CD8 + T细胞的临时但基本的需求

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摘要

Autoimmunity-prone BB rats demonstrate a T lymphocytopenia and abnormal T cell subset distribution. To test whether the life span of all T cells or only of certain subsets is reduced in BB rats, we thymectomised 8-week-old BB and PVG rats and subsequently assessed size and composition of the T cell population over a 6-week-period. In both strains, thymectomy (Tx) was followed by a decrease in peripheral T cell numbers, which was proportionally larger in BB rats. The decline of the Thy-1+recent thymic migrant (RTM) T cell phenotype was similar in both strains. BB rats showed a rapid preferential loss of CD8+and CD45RC+T cells, whereas the relative loss of RT6+T cells was proportional to that of all T cells and not significantly different from that in PVG rats. Tx at 8-week did not prevent diabetes. Tx of 4-week-old BB rats revealed essentially the same changes in peripheral T cell subset distribution as in 8-week-old animals. However, Tx at week 4 did prevent diabetes. Since this raised the possibility of a temporary requirement of CD8+T cells for the development of diabetes, we performed CD8 depletions during different pre-diabetic intervals. We found that CD8 depletion from 4 to 8 and 4 to 14 weeks, but not from 8 to 14 weeks of age prevented diabetes. We conclude that the protective effect of early adult Tx is, at least in part, due to the rapid loss of CD8+T cells, and that these cells are only required between 4 and 8 weeks of age for diabetes to develop in BB rats.
机译:自身免疫倾向的BB大鼠表现出T淋巴细胞减少和异常的T细胞亚群分布。为了测试BB大鼠的所有T细胞或仅某些亚群的寿命是否减少,我们对8周龄的BB和PVG大鼠进行了胸腺切除术,随后评估了6周内T细胞群体的大小和组成。在这两种品系中,胸腺切除术(Tx)继之以外周T细胞数量的减少,这在BB大鼠中成比例地更大。在两个菌株中,Thy-1 +最近胸腺移民(RTM)T细胞表型的下降是相似的。 BB大鼠表现出CD8 +和CD45RC + T细胞的快速优先损失,而RT6 + T细胞的相对损失与所有T细胞的损失成正比,与PVG大鼠没有明显差异。在第8周进行Tx不能预防糖尿病。 4周大的BB大鼠的Tx揭示了外周T细胞亚群分布与8周大的动物基本相同。但是,第4周的Tx确实可以预防糖尿病。由于这增加了暂时将CD8 + T细胞用于糖尿病发展的可能性,因此我们在不同的糖尿病前期进行了CD8耗竭。我们发现CD8耗竭4到8周和4到14周,但没有从8到14周龄可以预防糖尿病。我们得出的结论是,成年早期Tx的保护作用至少部分是由于CD8 + T细胞的迅速丧失,并且这些细胞仅在BB大鼠中需要4至8周龄才能发展为糖尿病。

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