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体内给予白细胞介素-1可诱导胸腺发育不全并提高血清皮质酮水平。

In vivo administration of IL-1 induces thymic hypoplasia and increased levels of serum corticosterone.

作者信息

Morrissey P J, Charrier K, Alpert A, Bressler L

机构信息

Immunex Corporation, Seattle, WA 98101.

出版信息

J Immunol. 1988 Sep 1;141(5):1456-63.

PMID:3261749
Abstract

Administration of IL-1 alpha or IL-1 beta to normal mice induces a decrease in thymic cellularity, the magnitude of which depends on the number of injections and dose of IL-1. Twice daily injections of 200 ng of IL-1 alpha or -beta for 4 days results in a 90% decrease in thymic cellularity, which regenerated after cessation of treatment. Study of thymocyte subpopulations revealed that the number of CD4+/CD8+ thymocytes was dramatically decreased in IL-1-treated mice. Functional assessment of the CD4-/CD8- population from treated animals showed that these cells had adequate mitogenic responses in vitro and that the proportion of these cells in cycle was not different from control CD4-/CD8- cells. IL-1 treatment also prevented the regeneration of thymic cellularity after irradiation. The use of strains of mice differing genetically at the Ly 1 locus to construct radiation bone marrow chimeras demonstrated that bone marrow-derived thymocyte precursors were able to seed the thymus in the IL-1-treated animals. Again, however, the CD4+/CD8+ thymocyte population was significantly decreased. Thymic repopulation occurred upon cessation of IL-1 therapy. Finally, we determined that a single i.p. injection of IL-1 caused a three-fold increase in serum corticosterone levels, which peaked approximately 3 h after IL-1 administration. Thus, an IL-1-dependent increase in serum corticosterone levels may be responsible for the observed thymic hypoplasia.

摘要

给正常小鼠注射白细胞介素-1α(IL-1α)或白细胞介素-1β(IL-1β)会导致胸腺细胞数量减少,减少的程度取决于注射次数和IL-1的剂量。每天两次注射200 ng的IL-1α或IL-1β,持续4天,会导致胸腺细胞数量减少90%,在停止治疗后胸腺细胞数量会再生。对胸腺细胞亚群的研究表明,在接受IL-1治疗的小鼠中,CD4⁺/CD8⁺胸腺细胞的数量显著减少。对接受治疗动物的CD4⁻/CD8⁻细胞群体进行功能评估显示,这些细胞在体外具有足够的促有丝分裂反应,并且这些细胞处于细胞周期中的比例与对照CD4⁻/CD8⁻细胞没有差异。IL-1治疗还会抑制照射后胸腺细胞数量的再生。利用在Ly 1位点基因不同的小鼠品系构建辐射骨髓嵌合体,结果表明骨髓来源的胸腺细胞前体能够在接受IL-1治疗的动物体内定植到胸腺中。然而,CD4⁺/CD8⁺胸腺细胞群体再次显著减少。在停止IL-1治疗后胸腺会重新填充。最后,我们确定单次腹腔注射IL-1会使血清皮质酮水平增加三倍,在注射IL-1后约3小时达到峰值。因此,血清皮质酮水平的IL-1依赖性升高可能是观察到的胸腺发育不全的原因。

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