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白细胞介素1调节人胸腺上皮细胞锌胸腺素的分泌及其对T淋巴细胞增殖和核蛋白激酶C的作用。

Interleukin 1 regulates secretion of zinc-thymulin by human thymic epithelial cells and its action on T-lymphocyte proliferation and nuclear protein kinase C.

作者信息

Coto J A, Hadden E M, Sauro M, Zorn N, Hadden J W

机构信息

University of South Florida Medical College, Department of Internal Medicine, Tampa, FL 33612.

出版信息

Proc Natl Acad Sci U S A. 1992 Aug 15;89(16):7752-6. doi: 10.1073/pnas.89.16.7752.

Abstract

Thymic epithelial cells (TEC) are known to secrete thymic hormones that influence maturation of T lymphocytes. One of these peptides, thymulin, requires zinc in an equimolar ratio for biological activity. A previous study [Cousins, R. J. & Leinart, A. S. (1988) FASEB J. 2, 2884-2890] showed that interleukin 1 (IL-1) in vivo stimulates zinc uptake by the thymus. Both the alpha and beta forms of IL-1, which stimulate proliferation of human TEC, also stimulate their uptake of zinc in vitro, and this latter stimulation is both dependent and independent of proliferation. Zinc induces zinc accumulation without proliferation. Two other stimulants of proliferation, bovine pituitary extract and epidermal growth factor, stimulate zinc uptake by TEC, but only in a manner dependent on proliferation. Utilizing in situ hybridization, we show that the IL-1 alpha and beta forms and zinc induce metallothionein mRNA expression TEC. Metallothionein is thought to be involved in the transfer of zinc to thymulin. IL-1 was shown to stimulate the secretion of thymulin as measured both by its ability to stimulate induction of IL-2 receptor-positive lymphocytes from human peripheral blood lymphocytes and by the azathioprine-sensitive rosette assay. In addition, the zinc-thymulin complex in the presence, but not absence, of IL-1 stimulates nuclear protein kinase C in isolated lymphocyte nuclei. IL-1 apparently regulates the synthesis or secretion and delivery of zinc-thymulin complex to the T-lymphocyte system.

摘要

胸腺上皮细胞(TEC)已知可分泌影响T淋巴细胞成熟的胸腺激素。这些肽之一的胸腺素,其生物活性需要等摩尔比的锌。先前的一项研究[考辛斯,R. J. & 莱纳特,A. S.(1988年)《美国实验生物学会联合会杂志》2,2884 - 2890]表明,体内白细胞介素1(IL - 1)刺激胸腺对锌的摄取。刺激人TEC增殖的IL - 1的α和β两种形式,在体外也刺激它们对锌的摄取,而且后一种刺激既依赖于增殖又独立于增殖。锌可在无增殖的情况下诱导锌积累。另外两种增殖刺激物,牛垂体提取物和表皮生长因子,刺激TEC对锌的摄取,但仅以依赖增殖的方式。利用原位杂交技术,我们发现IL - 1的α和β两种形式以及锌可诱导TEC中金属硫蛋白mRNA的表达。金属硫蛋白被认为参与锌向胸腺素的转移。通过其刺激从人外周血淋巴细胞诱导出IL - 2受体阳性淋巴细胞的能力以及硫唑嘌呤敏感的玫瑰花结试验测定,发现IL - 1可刺激胸腺素的分泌。此外,在有IL - 1存在但无IL - 1不存在的情况下,锌 - 胸腺素复合物可刺激分离的淋巴细胞核中的蛋白激酶C。IL - 1显然调节锌 - 胸腺素复合物向T淋巴细胞系统的合成、分泌和传递。

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