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生长激素在调节老年、裸鼠及转基因啮齿动物中依赖T细胞的免疫事件中的作用。

Role of growth hormone in regulating T-dependent immune events in aged, nude, and transgenic rodents.

作者信息

Davila D R, Brief S, Simon J, Hammer R E, Brinster R L, Kelley K W

机构信息

Department of Animal Sciences, University of Illinois, Urbana 61801.

出版信息

J Neurosci Res. 1987;18(1):108-16. doi: 10.1002/jnr.490180118.

Abstract

Growth hormone (GH) appears to play a major role in a reciprocal axis that has been postulated between the thymus and pituitary glands. Our previous studies showed that thymic structure, as well as T-cell proliferation and IL-2 synthesis, could be restored in aged female Wistar-Furth rats by the implantation of GH3 pituitary adenoma cells. These cells secrete GH and some prolactin. We have now used three different approaches to determine whether GH affects a variety of immune events in vivo in both old and young rodents, and whether GH3 cells can directly affect progenitor T-cells in nude rats that congenitally lack a thymus gland. To test the effects of GH in aged rats, 750 micrograms of pituitary-derived ovine GH was injected 2 x daily into 26-month-old Fischer 344 rats for 5 weeks. This approach demonstrated that GH augments splenocyte proliferation to T-cell lectins as well as natural killer (NK) activity at low effector:target ratios even though morphologic characteristics of the thymus were not altered. To assess the effect of GH in young rodents, mice were studied that were transgenic for the rat metallothionein-GH gene. Histologic evaluation of thymus glands revealed that the amount of adipose tissue and the number of epithelial cells and Hassall's corpuscles are augmented in transgenic mice. Splenocyte proliferation at suboptimal mitogen doses is greater in transgenic than in control littermate mice, but neither IL-2 synthesis nor antibody synthesis to sheep erythrocytes is affected. The role of pituitary hormones on progenitor T-cells was then explored by implanting GH3 cells into Rowett nude rats.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

生长激素(GH)似乎在胸腺与垂体之间假定的相互轴中发挥主要作用。我们之前的研究表明,通过植入GH3垂体腺瘤细胞,老年雌性Wistar-Furth大鼠的胸腺结构以及T细胞增殖和白细胞介素-2合成可以得到恢复。这些细胞分泌生长激素和一些催乳素。我们现在使用了三种不同的方法来确定生长激素是否会影响老年和幼年啮齿动物体内的各种免疫事件,以及GH3细胞是否能直接影响先天性无胸腺的裸鼠中的祖T细胞。为了测试生长激素对老年大鼠的影响,每天给26个月大的Fischer 344大鼠注射750微克垂体来源的羊生长激素,共注射5周,每天注射2次。这种方法表明,尽管胸腺的形态特征没有改变,但生长激素在低效应细胞:靶细胞比例下能增强脾细胞对T细胞凝集素的增殖以及自然杀伤(NK)活性。为了评估生长激素对幼年啮齿动物的影响,研究了转大鼠金属硫蛋白-生长激素基因的小鼠。胸腺组织学评估显示,转基因小鼠的脂肪组织量、上皮细胞数量和哈氏小体数量增加。在亚最佳促有丝分裂原剂量下,转基因小鼠的脾细胞增殖比同窝对照小鼠更大,但白细胞介素-2合成和对绵羊红细胞的抗体合成均未受影响。然后通过将GH3细胞植入罗威特裸鼠来探索垂体激素对祖T细胞的作用。(摘要截短至250字)

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