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一种新型PDZ蛋白调节鸟苷酸环化酶C(热稳定肠毒素受体)的活性。

A novel PDZ protein regulates the activity of guanylyl cyclase C, the heat-stable enterotoxin receptor.

作者信息

Scott Robert O, Thelin William R, Milgram Sharon L

机构信息

Department of Cell and Developmental Biology, University of North Carolina, Chapel Hill, North Carolina 27599, USA.

出版信息

J Biol Chem. 2002 Jun 21;277(25):22934-41. doi: 10.1074/jbc.M202434200. Epub 2002 Apr 11.

Abstract

Secretory diarrhea is the leading cause of infectious diarrhea in humans. Secretory diarrhea may be caused by binding of heat-stable enterotoxins to the intestinal receptor guanylyl cyclase C (GCC). Activation of GCC catalyzes the formation of cGMP, initiating a signaling cascade that opens the cystic fibrosis transmembrane conductance regulator chloride channel at the apical cell surface. To identify proteins that regulate the trafficking or function of GCC, we used the unique COOH terminus of GCC as the "bait" to screen a human intestinal yeast two-hybrid library. We identified a novel protein, IKEPP (intestinal and kidney-enriched PDZ protein) that associates with the COOH terminus of GCC in biochemical assays and by co-immunoprecipitation. IKEPP is expressed in the intestinal epithelium, where it is preferentially accumulated at the apical surface. The GCC-IKEPP interaction is not required for the efficient targeting of GCC to the apical cell surface. Rather, the association with IKEPP significantly inhibits heat-stable enterotoxin-mediated activation of GCC. Our findings are the first to identify a regulatory protein that associates with GCC to modulate the catalytic activity of the enzyme and provides new insights in mechanisms that regulate GCC activity in response to bacterial toxin.

摘要

分泌性腹泻是人类感染性腹泻的主要原因。分泌性腹泻可能由热稳定肠毒素与肠道受体鸟苷酸环化酶C(GCC)结合引起。GCC的激活催化cGMP的形成,启动信号级联反应,打开顶端细胞表面的囊性纤维化跨膜传导调节因子氯通道。为了鉴定调节GCC转运或功能的蛋白质,我们使用GCC独特的COOH末端作为“诱饵”来筛选人肠道酵母双杂交文库。我们鉴定出一种新型蛋白质IKEPP(肠道和肾脏富集的PDZ蛋白),在生化分析和共免疫沉淀中,它与GCC的COOH末端相关联。IKEPP在肠道上皮中表达,优先在顶端表面积累。GCC靶向顶端细胞表面不需要GCC-IKEPP相互作用。相反,与IKEPP的结合显著抑制热稳定肠毒素介导的GCC激活。我们的发现首次鉴定出一种与GCC相关联以调节该酶催化活性的调节蛋白,并为响应细菌毒素调节GCC活性的机制提供了新见解。

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