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首页> 美国卫生研究院文献>other >Apoptosis Signal Regulating Kinase-1 and NADPH Oxidase Mediate Human Amylin Evoked Redox Stress and Apoptosis in Pancreatic Beta-Cells
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Apoptosis Signal Regulating Kinase-1 and NADPH Oxidase Mediate Human Amylin Evoked Redox Stress and Apoptosis in Pancreatic Beta-Cells

机译:凋亡信号调节激酶1和NADPH氧化酶介导人类胰岛淀粉样蛋白诱发的氧化还原应激和胰腺β细胞凋亡。

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Misfolded toxic human islet amyloid polypeptide or amylin (hA) and plasma membrane-associated redox complex, NADPH oxidase (NOX), have been implicated in the islet β-cell demise associated with type-2 diabetes mellitus (T2DM). Studies show that hA accumulation is stressful to β-cells and that misfolding of human amylin evokes redox stress and activates mitogen activated protein (MAP) kinases, p38 MAPK and c-Jun N-terminal (JNK) kinase. However, the molecular link and causality between hA-evoked redox stress, NOX activity and MAP kinases signaling in pancreatic β-cells is incompletely understood. Here, we show that in the process of activating JNK, aggregation prone hA also activates an upstream apoptosis signal regulating kinase-1 (ASK1) with concomitant decrease in intracellular levels of reduced glutathione. Inhibition of ASK1 kinase activity, either by specific ASK1 inhibitor, NQDI1 or by thiol antioxidants reduces human amylin-evoked ASK1 and JNK activation and consequently human amylin toxicity in rat insulinoma Rin-m5F cells and human islets. β-cell specific overexpression of human amylin in mouse islets elicited ASK1 phosphorylation and activation in β-cells but not in other rodent’s islet or exocrine cells. This ASK1 activation strongly correlated with islet amyloidosis and diabetes progression. Cytotoxic human amylin additionally stimulated pro-oxidative activity and expressions of plasma membrane bound NADPH oxidase (NOX) and its regulatory subunits. siRNA mediated NOX1 knockdown and selective NOX inhibitors, ML171 and apocynin, significantly reduced hA-induced mitochondrial stress in insulinoma beta-cells. However, NOX inhibitors were largely ineffective against hA-evoked redox stress and activation of cytotoxic ASK1/JNK signaling complex. Thus, our studies suggest that NOX1 and ASK1 autonomously mediate human amylin-evoked redox and mitochondrial stress in pancreatic β-cells.
机译:错误折叠的有毒人类胰岛淀粉样多肽或胰岛淀粉样多肽(hA)以及与质膜相关的氧化还原复合物NADPH氧化酶(NOX)与2型糖尿病(T2DM)相关的胰岛β细胞死亡有关。研究表明,hA积累对β细胞产生压力,人胰岛淀粉样多肽的错误折叠会引起氧化还原应激并激活促分裂原活化蛋白(MAP)激酶,p38 MAPK和c-Jun N端(JNK)激酶。然而,胰腺β细胞中hA引起的氧化还原应激,NOX活性和MAP激酶信号传导之间的分子联系和因果关系尚不完全清楚。在这里,我们表明,在激活JNK的过程中,易于凝集的hA还激活了上游凋亡信号调节激酶1(ASK1),同时减少了还原型谷胱甘肽的细胞内水平。通过特定的ASK1抑制剂,NQDI1或巯基抗氧化剂抑制ASK1激酶活性,可降低人胰岛淀粉样蛋白诱发的ASK1和JNK活化,从而降低人胰岛淀粉样多肽对大鼠胰岛素瘤Rin-m5F细胞和人胰岛的毒性。人胰岛淀粉样多肽在小鼠胰岛中的β细胞特异性过度表达引起β细胞中ASK1的磷酸化和激活,而在其他啮齿动物的胰岛或外分泌细胞中则没有。这种ASK1激活与胰岛淀粉样变性和糖尿病进展密切相关。细胞毒性人胰岛淀粉样多肽还刺激前氧化活性以及质膜结合的NADPH氧化酶(NOX)及其调节亚基的表达。 siRNA介导的NOX1敲低和选择性NOX抑制剂ML171和载脂蛋白在胰岛素瘤β细胞中显着降低了hA诱导的线粒体应激。但是,NOX抑制剂对hA诱发的氧化还原应激和激活细胞毒性ASK1 / JNK信号复合物的作用很大。因此,我们的研究表明,NOX1和ASK1自主介导胰岛β细胞中人胰岛淀粉样蛋白诱发的氧化还原和线粒体应激。

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