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

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作者
G. Leposavić
N. Arsenović-Ranin
K. Radojević
D. Kosec
V. Pešić
B. Vidić-Danković
B. Plećaš-Solarović
I. Pilipović
机构
[1] Department of Immunology and Microbiology,Immunology Research Center “Branislav Janković”
[2] Institute of Immunology and Virology “Torlak”,undefined
[3] Department of Physiology,undefined
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β-adrenoceptor blockade; CD90 expression; Con A; T-cell differentiation; thymocyte apoptosis; thymocyte proliferation;
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摘要
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 TCRαβ 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) TCRαβhigh cells. These changes may, at least partly, be related to the markedly increased density of Thy-1 surface expression on TCRαβlow 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 β-AR signaling, or chemically evoked alterations in catecholamine release, may interfere with the regulation of thymocyte selection, and consequently with the immune response. (Mol Cell Biochem xxx: 1–13, 2005)
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页码:87 / 99
页数:12
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