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正常雄性小鼠去势后未成熟胸腺细胞增殖的诱导

Induction of immature thymocyte proliferation after castration of normal male mice.

作者信息

Olsen N J, Viselli S M, Shults K, Stelzer G, Kovacs W J

机构信息

Department of Medicine, Vanderbilt University, Nashville, Tennessee 37232.

出版信息

Endocrinology. 1994 Jan;134(1):107-13. doi: 10.1210/endo.134.1.8275924.


DOI:10.1210/endo.134.1.8275924
PMID:8275924
Abstract

The physiological basis and immunological significance of thymic enlargement in castrate male animals is not known. We used normal male C57 Bl/6 mice to examine the contribution of in situ thymocyte proliferation to castration-induced enlargement of the thymus. Animals castrated at 8-10 weeks of age were compared to normal intact males. Thymocytes were examined 4-120 days after castration using flow cytometry to determine DNA content and thus the number of cells in active phases of the cell cycle. These properties were examined in unseparated thymocytes and in phenotypic subpopulations defined by expression of CD3, CD4, and CD8. For thymocytes obtained from intact control glands, a mean of 11.0 +/- 1.0% were in active phases of the cell cycle. The percentage of cycling thymocytes was increased to a mean of 22.5 +/- 1.9% in the week after castration (P < 0.001). This change occurred in the absence of significant thymic enlargement. At 8-10 days after castration, thymic weight increased abruptly to a new steady state which was double that of intact controls (78.0 +/- 4.1 vs. 39.1 +/- 2.6 mg; P < 0.001). In these enlarged glands, only 9.9 +/- 0.8% of cells were cycling, which was not significantly different than controls (P > 0.3). Proliferating cells identified in fixed thymus tissue sections after in vivo administration of bromodeoxyuridine were located in the subcapsular cortex and medulla. Analyses of thymocyte subpopulations indicated that most cycling cells had immature phenotypes (CD4+CD8+, CD4-CD8+, and CD3lo or CD3-). Castrate glands studied in the steady state period 8-120 days after surgery contained significantly fewer CD3+ cells than intact controls (P < or = 0.045). The findings suggest an intrathymic role for androgens in affecting generation of the mature T cell repertoire.

摘要

去势雄性动物胸腺增大的生理基础和免疫学意义尚不清楚。我们使用正常雄性C57 Bl/6小鼠来研究原位胸腺细胞增殖对去势诱导的胸腺增大的作用。将8 - 10周龄去势的动物与正常未阉割的雄性动物进行比较。在去势后4 - 120天使用流式细胞术检测胸腺细胞,以确定DNA含量,从而确定细胞周期活跃期的细胞数量。在未分离的胸腺细胞以及由CD3、CD4和CD8表达所定义的表型亚群中检测这些特性。对于从未阉割的对照腺体获得的胸腺细胞,平均有11.0±1.0%处于细胞周期的活跃期。去势后一周内,处于细胞周期的胸腺细胞百分比增加到平均22.5±1.9%(P < 0.001)。这种变化发生在胸腺无明显增大的情况下。去势后8 - 10天,胸腺重量突然增加到一个新的稳定状态,是未阉割对照的两倍(78.0±4.1对39.1±2.6毫克;P < 0.001)。在这些增大的腺体中,只有9.9±0.8%的细胞处于细胞周期,与对照无显著差异(P > 0.3)。在体内给予溴脱氧尿苷后,在固定的胸腺组织切片中鉴定出的增殖细胞位于被膜下皮质和髓质。胸腺细胞亚群分析表明,大多数处于细胞周期的细胞具有未成熟表型(CD4 + CD8 +、CD4 - CD8 +以及CD3lo或CD3 -)。在手术后8 - 120天的稳定期研究的去势腺体中,CD3 +细胞明显少于未阉割对照(P≤0.045)。这些发现表明雄激素在影响成熟T细胞库的产生方面在胸腺内发挥作用。

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