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在特定T细胞亚群耗竭的小鼠中诱导自身免疫性甲状腺炎。I. 诱导甲状腺炎对Lyt-1迟钝L3T4明亮正常T细胞的需求。

Autoimmune thyroiditis induced in mice depleted of particular T cell subsets. I. Requirement of Lyt-1 dull L3T4 bright normal T cells for the induction of thyroiditis.

作者信息

Sugihara S, Izumi Y, Yoshioka T, Yagi H, Tsujimura T, Tarutani O, Kohno Y, Murakami S, Hamaoka T, Fujiwara H

机构信息

Biomedical Center, Osaka University Medical School, Japan.

出版信息

J Immunol. 1988 Jul 1;141(1):105-13.

PMID:2967864
Abstract

T cell-depleted C3H/He or (C57BL/6xC3H/He)F1 (B6C3F1) mice were prepared by adult thymectomy and injection of antithymocyte serum, followed 3 wk later by lethal x-irradiation and bone marrow reconstitution. When these T cell-depleted mice were not injected or injected i.v. with normal spleen and lymph node cells treated with either anti-Thy-1, -L3T4 or -Lyt-2 antibody plus C or C alone, none of the groups of mice developed thyroiditis. In contrast, the adoptive transfer of normal cells treated with anti-Lyt-1 plus C resulted in high incidence of the production of antithyroglobulin antibody and the induction of typical thyroiditis lesion. The thyroid was the sole organ involved, because neither typical inflammatory lesion in other organs nor autoantibody such as anti-DNA antibody was detected in mice that exhibited thyroiditis. Analyses of surface phenotypes of cells required for inducing thyroiditis by the adoptive transfer revealed that an appreciable percentage of Lyt-1 dull T cells remained after the treatment of normal lymphoid cells with anti-Lyt-1 plus C. Almost all of these Lyt-1 dull T cells expressed magnitudes of L3T4 or Lyt-2 Ag comparable to those detected on Lyt-1 bright T cells. More important, the induction of thyroiditis was almost completely prevented by either in vitro or in vivo elimination of Lyt-1 dull L3T4+(bright) but not of Lyt-1 dull Lyt-2+(bright) T cells. These results indicate that Lyt-1 dull L3T4+ T cells existing in normal healthy individuals have potential to induce typical thyroiditis which is associated with the production of antithyroglobulin autoantibody, and that the activation and/or function of this T cell subset is regulated by the Lyt-1 bright T cell population coexisting in normal lymphoid cell population.

摘要

通过成年胸腺切除术和注射抗胸腺细胞血清制备T细胞耗竭的C3H/He或(C57BL/6xC3H/He)F1(B6C3F1)小鼠,3周后进行致死性X射线照射并进行骨髓重建。当这些T细胞耗竭的小鼠不注射或静脉注射用抗Thy-1、-L3T4或-Lyt-2抗体加补体C处理的正常脾细胞和淋巴结细胞或仅注射补体C时,各组小鼠均未发生甲状腺炎。相比之下,用抗Lyt-1加补体C处理的正常细胞的过继转移导致抗甲状腺球蛋白抗体产生的高发生率和典型甲状腺炎病变的诱导。甲状腺是唯一受累的器官,因为在出现甲状腺炎的小鼠中未检测到其他器官的典型炎症病变或自身抗体如抗DNA抗体。对通过过继转移诱导甲状腺炎所需细胞的表面表型分析表明,在用抗Lyt-1加补体C处理正常淋巴细胞后,仍有相当比例的Lyt-1暗细胞T细胞留存。几乎所有这些Lyt-1暗细胞T细胞表达的L3T4或Lyt-2抗原量与在Lyt-1亮细胞T细胞上检测到的相当。更重要的是,通过体外或体内消除Lyt-1暗L3T4 +(亮)但不是Lyt-1暗Lyt-2 +(亮)T细胞,几乎完全阻止了甲状腺炎的诱导。这些结果表明,正常健康个体中存在的Lyt-1暗L3T4 + T细胞有诱导与抗甲状腺球蛋白自身抗体产生相关的典型甲状腺炎的潜力,并且该T细胞亚群的激活和/或功能受正常淋巴细胞群体中共存的Lyt-1亮细胞T细胞群体调节。

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