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Investigation of the Role of B-Cells in Type 1 Diabetes in the NOD Mouse.

机译:在NOD小鼠中B细胞在1型糖尿病中的作用研究。

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B-cells are important in the development of type 1 diabetes, but their role is not completely defined. Although B-cells produce autoantibodies, these are not thought to be pathogenic; however, their antigen-presenting function is postulated to be critical. To examine the relative importance of these functions of B-cells, we have generated nonobese diabetic (NOD) B-cell-deficient mice that express a transgene encoding a mutant heavy chain immunoglobulin transgene on the cell surface but cannot secrete immunoglobulins (mIgs). This allowed us to dissect the importance of the relative roles of antigen presentation, dissociated from antibody production. We found that the expression of the mIg transgene increased insulitis and the incidence of diabetes compared with transgene-negative NOD B-cell-deficient mice, indicating that the ability to produce antibodies is not necessary for B-cells to have some effect on the development of diabetes. However, diabetes was not restored to the level seen in normal NOD mice. This may relate to reduced ability to activate an islet-specific T-cell repertoire, presumably due to the reduced islet-specific B-cell repertoire. Our results implicate a specific antigen-presenting function for B-cells.
机译:B细胞在1型糖尿病的发展中很重要,但其作用尚未完全确定。尽管B细胞会产生自身抗体,但它们并不被认为具有致病性。然而,假定它们的抗原呈递功能是至关重要的。为了检查B细胞这些功能的相对重要性,我们产生了非肥胖糖尿病(NOD)B细胞缺陷小鼠,该小鼠在细胞表面表达编码突变型重链免疫球蛋白转基因的转基因,但不能分泌免疫球蛋白(mIgs)。这使我们能够剖析与抗体生产无关的抗原提呈相对作用的重要性。我们发现,与转基因阴性的NOD B细胞缺陷小鼠相比,mIg转基因的表达增加了胰岛素炎和糖尿病的发病率,这表明产生抗体的能力对于B细胞对发育有一定影响不是必需的糖尿病但是,糖尿病并未恢复到正常NOD小鼠所见的水平。这可能与激活胰岛特异性T细胞库的能力降低有关,大概是由于胰岛特异性B细胞库的减少。我们的结果暗示了B细胞的特定抗原呈递功能。

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