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新生期胸腺切除小鼠中与自身免疫性卵巢炎和卵巢肿瘤发生相关的细胞事件。

Cellular events associated with autoimmune oophoritis and ovarian tumorigenesis in neonatally thymectomized mice.

作者信息

De Angelo L, Michael S D

机构信息

Department of Biological Sciences, State University of New York, Binghamton 13901.

出版信息

J Reprod Immunol. 1987 Sep;12(1):63-78. doi: 10.1016/0165-0378(87)90081-7.

Abstract

Thymectomy at 3 days of age (Tx-3) in (C3H/HeMs x 129/J)F1 (C31) female mice results in post-pubertal ovarian dysgenesis associated with high levels of circulating auto-oocyte antibodies (AOA) prior to ovarian tumor formation. Evidence suggests that the etiology for the ovarian dysgenesis resulting from Tx-3 is autoimmune and involves helper T cell abnormalities. The present study characterized circulating leukocytes and mitogenic activity using concanavalin A (ConA) with serologically selected spleen T cells. We observed no sustained abnormalities in either number of circulating leukocytes or percentages of granulocytes or lymphocytes. Circulating mononuclear cells with positive immunofluorescence for Thy 1.2 and Lyt 1.1+Lyt 1.2 cell markers were similar in all mice. However, the spleen cells from Tx-3 mice with ovarian dysgenesis remaining after adsorption with antisera to the Lyt 2.1+Lyt 2.2 antigens (helper T cells remaining) showed increased incorporation of [3H]thymidine compared to the intact mice. This stimulated activity occurred during the periods of early ovarian dysgenesis and active tumor growth. Apparently, the autoimmune oophoritis results from an imbalance within the Lyt 1 cells which may represent a primary insult to the ovary that results in later ovarian tumor development.

摘要

在(C3H/HeMs×129/J)F1(C31)雌性小鼠3日龄时进行胸腺切除术(Tx-3),会导致青春期后卵巢发育不全,且在卵巢肿瘤形成之前循环中存在高水平的自身卵母细胞抗体(AOA)。有证据表明,Tx-3导致卵巢发育不全的病因是自身免疫性的,且涉及辅助性T细胞异常。本研究使用伴刀豆球蛋白A(ConA)对经血清学选择的脾脏T细胞进行了循环白细胞和促有丝分裂活性的特征分析。我们观察到循环白细胞数量、粒细胞或淋巴细胞百分比均无持续异常。所有小鼠中,对Thy 1.2和Lyt 1.1+Lyt 1.2细胞标志物呈阳性免疫荧光的循环单核细胞相似。然而,用抗Lyt 2.1+Lyt 2.2抗原血清吸附后剩余的患有卵巢发育不全的Tx-3小鼠的脾细胞(剩余辅助性T细胞),与完整小鼠相比,显示出[3H]胸腺嘧啶核苷掺入增加。这种刺激活性发生在早期卵巢发育不全和肿瘤活跃生长期间。显然,自身免疫性卵巢炎是由Lyt 1细胞内的失衡引起的,这可能是对卵巢的原发性损伤,导致后期卵巢肿瘤的发展。

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