首页> 美国卫生研究院文献>Clinical and Experimental Immunology >L3T4 and Lyt-2 T cells are both involved in the generation of low-dose streptozotocin-induced diabetes in mice.
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L3T4 and Lyt-2 T cells are both involved in the generation of low-dose streptozotocin-induced diabetes in mice.

机译:L3T4和Lyt-2 T细胞均参与小鼠低剂量链脲佐菌素诱导的糖尿病的产生。

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摘要

In order to determine the role of different T lymphocyte subsets in the pathogenesis of low-dose streptozotocin (LD-Sz) induced diabetes, we treated mice with Sz together with repeated injections of rat monoclonal antibodies (MoAb) with specificity towards the mouse T cell differentiation markers L3T4 ('helper/inducer' T cells and some macrophages), Lyt-2 ('cytotoxic/suppressor' T cells and NK cells) and Thy-1 (pan T lymphocytes). Treatment depleted target cells in peripheral blood and spleen; decreased the ability of spleen cells to respond to mitogens; and, in the case of depletion of the L3T4 T cell subset, prevented a humoral immune response to SRBC. Treatment with MoAb against either of the two T cell subtypes could protect from hyperglycaemia and loss of body weight, suggesting that both T cell subsets were implicated in the development of LD-Sz induced diabetes. Immunocytochemical analysis of pancreatic sections showed that both L3T4+ and Lyt-2+ cells participated in islet infiltration together with macrophages. Treatment with MoAb markedly reduced islet infiltration by both L3T4+ and Lyt-2+ cells but not by macrophages. The suppressive effect of MoAb against either L3T4 or Lyt-2 on diabetes development suggests that the pathomechanism involved is different from that in experimental autoimmune neuritis and adjuvant arthritis where Lyt-2 cells are not involved.
机译:为了确定不同的T淋巴细胞亚群在低剂量链脲佐菌素(LD-Sz)诱导的糖尿病发病中的作用,我们用Sz处理小鼠,并反复注射对小鼠T细胞具有特异性的大鼠单克隆抗体(MoAb)分化标记L3T4(“辅助/诱导” T细胞和一些巨噬细胞),Lyt-2(“细胞毒性/抑制” T细胞和NK细胞)和Thy-1(泛T淋巴细胞)。治疗消耗掉外周血和脾脏中的靶细胞;降低脾细胞对有丝分裂原的反应能力;并且,在耗尽L3T4 T细胞亚群的情况下,可以防止对SRBC的体液免疫反应。用MoAb对抗这两种T细胞亚型中的任何一种均可预防高血糖症和减轻体重,这表明这两种T细胞亚型均与LD-Sz诱导的糖尿病的发生有关。胰腺切片的免疫细胞化学分析表明,L3T4 +和Lyt-2 +细胞均与巨噬细胞一起参与了胰岛浸润。用MoAb处理可显着减少L3T4 +和Lyt-2 +细胞的胰岛浸润,但巨噬细胞则不会。 MoAb对L3T4或Lyt-2的抑制作用对糖尿病的发展提示所涉及的发病机制与不涉及Lyt-2细胞的实验性自身免疫性神经炎和佐剂性关节炎不同。

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