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Lyt-2阳性T细胞的扩增与新西兰黑鼠的功能损伤及自身免疫性溶血性贫血相关。

Enlargement of Lyt-2-positive T cells is associated with functional impairment and autoimmune hemolytic anemia in New Zealand Black mice.

作者信息

McCoy K L, Baker P J, Malek T R, Chused T M

出版信息

J Immunol. 1985 Oct;135(4):2432-7.

PMID:3928748
Abstract

We investigated the relationship between the increased cell diameter of Lyt-2+ T cells and the development of autoimmune disease in aging NZB and NZB X NZW F1 hybrid (BW) mice. Individual animals were analyzed for Lyt-2+ T cell size (by narrow-angle forward light scatter), anti-erythrocyte autoantibodies, anemia, proteinuria, and splenomegaly. The peak light scatter of the Lyt-2+ T cells correlated with the level of anti-erythrocyte autoantibodies and severity of hemolytic anemia, but not with proteinuria or splenomegaly. The cell size of this T cell subset did not increase in old BW or in NZB mice homozygous for the xid gene (NZB.xid). The in vivo administration of bacterial lipopolysaccharide to young NZB mice did not stimulate the enlargement of Lyt-2+ T cells. Ly-2+ T cells from old NZB mice could be stimulated by concanavalin A (Con A) to express interleukin 2 (IL 2) receptors and to synthesize DNA in vitro. However, in vivo administration of Con A to old NZB mice did not induce the expression of IL 2 receptors on Lyt-2+ T cells. Further, in vivo T suppressor function was impaired in old NZB mice with enlarged Lyt-2+ T cells. Thus, the enlargement of Lyt-2+ T cells in old NZB mice appears related to impaired T cell function in vivo and is associated with the development of anti-erythrocyte autoantibodies and autoimmune hemolytic anemia.

摘要

我们研究了Lyt-2⁺ T细胞直径增加与衰老的新西兰黑鼠(NZB)和新西兰黑鼠与新西兰白杂交F1代(BW)小鼠自身免疫性疾病发展之间的关系。对每只动物分析Lyt-2⁺ T细胞大小(通过窄角前向光散射)、抗红细胞自身抗体、贫血、蛋白尿和脾肿大情况。Lyt-2⁺ T细胞的光散射峰值与抗红细胞自身抗体水平及溶血性贫血严重程度相关,但与蛋白尿或脾肿大无关。在年老的BW小鼠或xid基因纯合的NZB小鼠(NZB.xid)中,这个T细胞亚群的细胞大小没有增加。给年轻的NZB小鼠体内注射细菌脂多糖不会刺激Lyt-2⁺ T细胞增大。来自年老NZB小鼠的Ly-2⁺ T细胞可被刀豆蛋白A(Con A)刺激,在体外表达白细胞介素2(IL-2)受体并合成DNA。然而,给年老NZB小鼠体内注射Con A不会诱导Lyt-2⁺ T细胞表达IL-2受体。此外,Lyt-2⁺ T细胞增大的年老NZB小鼠体内T抑制功能受损。因此,年老NZB小鼠中Lyt-2⁺ T细胞的增大似乎与体内T细胞功能受损有关,且与抗红细胞自身抗体的产生及自身免疫性溶血性贫血的发展相关。

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