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Calreticulin Is a Negative Regulator of Bronchial Smooth Muscle Cell Proliferation

机译:钙网蛋白是支气管平滑肌细胞增殖的负调节剂。

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Background. Calreticulin controls the C/EBPαp42/p30 at the translational level trough a cis-regulatory CNG rich loop in the CEBPA mRNA. We determined the effects of steroids and long-acting beta-agonists on the p42/p30 ratio and on calreticulin expression in primary human bronchial smooth muscle (BSM) cells. Methods. The effects of budesonide (10?8?M) and formoterol (10?8?M) were studied in BSM cells pre-treated with siRNA targeting calreticulin. The expression of C/EBPα and calreticulin was determined by immuno-blotting. Automated cell counts were performed to measure proliferation. Results. All tested BSM cell lines (n=5) expressed C/EBPα and calreticulin. In the presence of 5% FBS, the p42/p30 ratio significantly decreased (n=3, P0.05) and coincided with BSM cell proliferation. High levels of calreticulin were associated with a decreased p42/p30 isoform ratio. FBS induced the expression of calreticulin (n=3, P0.05), which was further increased by formoterol. siRNA targeting calreticulin increased the p42/p30 ratio in non-stimulated BSM cells and significantly inhibited the proliferation of PDGF-BB-stimulated BSM cells (n=5, P0.05). Neither budesonide nor formoterol restored the p42 isoform expression. Conclusions. Our data show calreticulin is a negative regulator of C/EBPα protein expression in BSM cells. Modulation of calreticulin levels may provide a novel target to reduce BSM remodeling.
机译:背景。钙网蛋白通过CEBPA mRNA中一个顺式调控的富含CNG的环在翻译水平上控制C /EBPαp42/ p30。我们确定了类固醇和长效β受体激动剂对人原发性支气管平滑肌(BSM)细胞中p42 / p30比率和钙网蛋白表达的影响。方法。在用靶向钙网蛋白的siRNA预处理的BSM细胞中研究了布地奈德(10?8?M)和福莫特罗(10?8?M)的作用。通过免疫印迹测定C /EBPα和钙网蛋白的表达。进行自动细胞计数以测量增殖。结果。所有测试的BSM细胞系(n = 5)表达C /EBPα和钙网蛋白。在5%FBS存在下,p42 / p30比值显着降低(n = 3,P <0.05),并且与BSM细胞增殖相符。高水平的钙网蛋白与p42 / p30亚型比率降低有关。 FBS诱导钙网蛋白的表达(n = 3,P <0.05),福莫特罗使之进一步增加。靶向钙网蛋白的siRNA增加了未刺激的BSM细胞中的p42 / p30比,并显着抑制了PDGF-BB刺激的BSM细胞的增殖(n = 5,P <0.05)。布地奈德和福莫特罗均未恢复p42亚型的表达。结论。我们的数据显示钙网蛋白是BSM细胞中C /EBPα蛋白表达的负调节剂。钙网蛋白水平的调节可提供减少BSM重塑的新目标。

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