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雄激素作用缺陷小鼠的免疫功能研究。区分因激素不敏感导致的免疫功能改变和因其他遗传因素导致的改变。

Studies of immunological function in mice with defective androgen action. Distinction between alterations in immune function due to hormonal insensitivity and alterations due to other genetic factors.

作者信息

Olsen N J, Watson M B, Kovacs W J

机构信息

Department of Medicine, Vanderbilt University School of Medicine, Nashville, TN 37232.

出版信息

Immunology. 1991 May;73(1):52-7.

Abstract

The presence of androgen receptors in thymocytes and the well-described effects of exogenous androgens on thymus size suggest a role for androgenic hormones in thymocyte growth and maturation. Testicular feminization (Tfm/Y) mice which bear a heritable defect in the androgen receptor protein were studied to investigate how androgens might influence immune phenotype and function. These mice were compared to two types of controls; their Tabby/Y normal male littermates and male mice of the C57 Bl/6 strain from which the Tabby and Tfm mice were derived. Thymuses and spleens from Tfm/Y mice were larger than both types of controls. Phenotypic differences in thymocyte and splenocyte subpopulations identified by the T-cell markers CD3, CD4 and CD8 suggested that T-cell maturation was altered in the androgen-resistant animal. However, both Ta/Y and Tfm/Y were found to be high producers of interleukin-4 (IL-4) by both spleen and thymus cells, while cells from the C57 mice produced predominantly IL-2. These findings suggest that some immunological features of the Tfm/Y mouse may be related to its defect in androgen action, but that high levels of IL-4 production are probably related to other genetic changes in the C57 background.

摘要

胸腺细胞中存在雄激素受体,以及外源性雄激素对胸腺大小的显著影响,提示雄激素在胸腺细胞生长和成熟过程中发挥作用。研究了雄激素受体蛋白存在遗传性缺陷的睾丸雌性化(Tfm/Y)小鼠,以探讨雄激素如何影响免疫表型和功能。将这些小鼠与两种类型的对照进行比较:它们的Tabby/Y正常雄性同窝仔鼠,以及Tabby和Tfm小鼠所源自的C57 Bl/6品系雄性小鼠。Tfm/Y小鼠的胸腺和脾脏比两种对照都大。通过T细胞标志物CD3、CD4和CD8鉴定的胸腺细胞和脾细胞亚群的表型差异表明,雄激素抵抗动物的T细胞成熟发生了改变。然而,发现Ta/Y和Tfm/Y的脾脏和胸腺细胞都是白细胞介素-4(IL-4)的高产者,而C57小鼠的细胞主要产生IL-2。这些发现表明,Tfm/Y小鼠的一些免疫特征可能与其雄激素作用缺陷有关,但高水平的IL-4产生可能与C57背景中的其他基因变化有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0bc5/1384517/7bf0c1ad9d0c/immunology00116-0057-a.jpg

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