首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >CD43-independent augmentation of mouse T-cell function by glycoprotein cleaving enzymes.
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CD43-independent augmentation of mouse T-cell function by glycoprotein cleaving enzymes.

机译:糖蛋白裂解酶使CD43依赖性的小鼠T细胞功能增强。

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Previous work has shown that the function of mouse CD4+ T cells can be augmented by an enzyme, O-sialoglycoprotein endopeptidase (OSGE), which cleaves surface CD43, suggesting the idea that the high levels of glycosylated CD43 found on T cells from aged mice may contribute to immune senescence. New results now show that OSGE improves T-cell function even in mice lacking CD43, showing that other glycoproteins must contribute to the OSGE effect on function. Evaluation of other enzymes found two whose ability to stimulate CD4 activation was higher in aged than in young T cells. One of these, PNGase F, is a glycosidase specific for N-linked glycans, and the other, ST-Siase(2,3) from Salmonella typhimurium, is specific for alpha2,3-linked terminal sialic acid residues. Parallel lectin-binding experiments showed that removal of alpha2,3-linked sialic acid residues vulnerable to PNGase F and ST-Siase(2,3) was also greater in old than in young T cells. The preferential ability of PNGase F and ST-Siase(2,3) to improve the function of T cells from aged mice may involve cleavage of glycoproteins containing alpha2,3-linked sialic acid residues on N-linked or O-linked glycans or both.
机译:先前的研究表明,可以通过裂解表面CD43的O-唾液酸糖蛋白内肽酶(OSGE)来增强小鼠CD4 + T细胞的功能,这表明,高龄小鼠T细胞上糖基化CD43含量高的想法可能促进免疫衰老。现在的新结果表明,即使在缺乏CD43的小鼠中,OSGE仍能改善T细胞功能,表明其他糖蛋白必须对OSGE的功能产生影响。对其他酶的评估发现,在老年人中,两种酶刺激CD4活化的能力高于年轻T细胞。其中一个PNGase F是对N-连接的聚糖特异的糖苷酶,另一个是鼠伤寒沙门氏菌的ST-Siase(2,3)对alpha2,3-连接的末端唾液酸残基具有特异性。平行的凝集素结合实验显示,易受PNGase F和ST-Siase(2,3)破坏的α2,3连接的唾液酸残基在老年患者中的清除率也要高于年轻T细胞。 PNGase F和ST-Siase(2,3)改善老龄小鼠T细胞功能的优先能力可能涉及在N-或O-连接的聚糖上裂解包含alpha2,3-link唾液酸残基的糖蛋白。

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