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体内长期β-肾上腺素能受体阻断诱导的胸腺细胞表型改变及其对胸腺细胞增殖和凋亡的影响

Characterization of thymocyte phenotypic alterations induced by long-lasting beta-adrenoceptor blockade in vivo and its effects on thymocyte proliferation and apoptosis.

作者信息

Leposavić G, Arsenović-Ranin N, Radojević K, Kosec D, Pesić V, Vidić-Danković B, Plećas-Solarović B, Pilipović I

机构信息

Immunology Research Center "Branislav Janković", Institute of Immunology and Virology "Torlak", Belgrade, Serbia and Montenegro.

出版信息

Mol Cell Biochem. 2006 Apr;285(1-2):87-99. doi: 10.1007/s11010-005-9059-5. Epub 2006 Feb 14.

DOI:10.1007/s11010-005-9059-5
PMID:16477376
Abstract

Adult male Wistar rats were subjected to propranolol (P, 0.40 mg/100 g/day) or saline (S) administration (controls) over 14 days. The expression of major differentiation molecules on thymocytes and Thy-1 (CD90) molecules, which are shown to adjust thymocyte sensitivity to TCRalphabeta signaling, was studied. In addition, the sensitivity of thymocytes to induction of apoptosis and concanavalin A (Con A) signaling was estimated. The thymocytes from P-treated (PT) rats exhibited an increased sensitivity to induction of apoptosis, as well as to Con A stimulation. Furthermore, P treatment produced changes in the distribution of thymocyte subsets suggesting that more cells passed positive selection and further differentiated into mature CD4+ or CD8+ single positive (SP) TCRalphabeta(high) cells. These changes may, at least partly, be related to the markedly increased density of Thy-1 surface expression on TCRalphabeta(low) thymocytes from these rats. The increased frequency of cells expressing the CD4+25+ phenotype, which has been shown to be characteristic for regulatory cells in the thymus, may also indicate alterations in thymocyte selection following P treatment. Inasmuch as positive and negative selections play an important role in continuously reshaping the T-cell repertoire and maintaining tolerance, the hereby presented study suggests that pharmacological manipulations with beta-AR signaling, or chemically evoked alterations in catecholamine release, may interfere with the regulation of thymocyte selection, and consequently with the immune response.

摘要

成年雄性Wistar大鼠连续14天接受普萘洛尔(P,0.40mg/100g/天)或生理盐水(S)给药(对照组)。研究了胸腺细胞上主要分化分子以及Thy-1(CD90)分子的表达,这些分子可调节胸腺细胞对TCRαβ信号的敏感性。此外,还评估了胸腺细胞对凋亡诱导和刀豆蛋白A(Con A)信号的敏感性。来自P处理(PT)大鼠的胸腺细胞对凋亡诱导以及Con A刺激表现出更高的敏感性。此外,P处理导致胸腺细胞亚群分布发生变化,表明更多细胞通过阳性选择并进一步分化为成熟的CD4+或CD8+单阳性(SP)TCRαβ(高)细胞。这些变化可能至少部分与这些大鼠TCRαβ(低)胸腺细胞上Thy-1表面表达密度的显著增加有关。表达CD4+25+表型的细胞频率增加,这已被证明是胸腺中调节性细胞的特征,也可能表明P处理后胸腺细胞选择发生了改变。鉴于阳性和阴性选择在不断重塑T细胞库和维持耐受性方面起着重要作用,本研究表明,对β-AR信号进行药理学操作或化学诱导的儿茶酚胺释放变化可能会干扰胸腺细胞选择的调节,进而干扰免疫反应。

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Con A activates an Akt/PKB dependent survival mechanism to modulate TCR induced cell death in double positive thymocytes.刀豆球蛋白A激活一种依赖Akt/蛋白激酶B的存活机制,以调节双阳性胸腺细胞中T细胞受体诱导的细胞死亡。
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