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引用次数: 5
摘要
实验研究了2,3,7,8-四氯二苯并-对二恶英(TCDD)对血管平滑肌细胞(SMCs)生长相关信号的影响。只有在细胞周期的G0/G1过渡期间加入TCDD时,SMCs中DNA合成峰降低了40%。在此期间,几种内源性蛋白的磷酸化增强与TCDD刺激后15分钟酪氨酸激酶活性增加相一致。在G1/S期或S期,TCDD处理的细胞的蛋白磷酸化状态未发生变化。静止SMCs与10 nM TCDD和血清共处理3小时,血清诱导的与12- o -十四烷醇- 13-醋酸酯反应元件(TRE)的结合活性降低了约40%。在TCDD处理的静止SMCs中,长达5小时未观察到组成性TRE结合的改变。这些数据表明,在G0/G1过渡期间,TCDD选择性地调节了血管SMCs中有丝分裂原相关的信号传导,这些效应影响了这些细胞的生长行为。
Growth-related signaling in vascular smooth muscle cells is deregulated by TCDD during the G0/G1 transition.
Experiments have been conducted to examine the impact of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) on growth-related signaling in vascular smooth muscle cells (SMCs). A 40% reduction of peak DNA synthesis was observed in SMCs only when TCDD was added during the G0/G1 transition of the cell cycle. Enhanced phosphorylation of several endogenous proteins during this period was coincident with increased tyrosine kinase activity as early as 15 min following TCDD challenge. No changes in protein phosphorylation status occurred in cells treated with TCDD during the G1/S transition or during S phase. Cotreatment of quiescent SMCs with 10 nM TCDD and serum for 3 h reduced serum-inducible binding activity to a 12-O-tetradecanoyl phorbol 13-acetate responsive element (TRE) by approximately 40%. No alterations of constitutive TRE binding were observed in quiescent SMCs treated with TCDD for up to 5 h. These data show that mitogen-related signaling in vascular SMCs is modulated by TCDD selectively during the G0/G1 transition, and these effects influence the growth behavior of these cells.
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