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糖尿病自身抗原ICA69及其秀丽隐杆线虫同源物ric-19是神经内分泌分泌的保守调节因子。

The diabetes autoantigen ICA69 and its Caenorhabditis elegans homologue, ric-19, are conserved regulators of neuroendocrine secretion.

作者信息

Pilon M, Peng X R, Spence A M, Plasterk R H, Dosch H M

机构信息

Department of Pediatrics, University of Toronto, The Hospital for Sick Children, Research Institute, Toronto, Ontario, Canada M5G 1X8.

出版信息

Mol Biol Cell. 2000 Oct;11(10):3277-88. doi: 10.1091/mbc.11.10.3277.

Abstract

ICA69 is a diabetes autoantigen with no homologue of known function. Given that most diabetes autoantigens are associated with neuroendocrine secretory vesicles, we sought to determine if this is also the case for ICA69 and whether this protein participates in the process of neuroendocrine secretion. Western blot analysis of ICA69 tissue distribution in the mouse revealed a correlation between expression levels and secretory activity, with the highest expression levels in brain, pancreas, and stomach mucosa. Subcellular fractionation of mouse brain revealed that although most of the ICA69 pool is cytosolic and soluble, a subpopulation is membrane-bound and coenriched with synaptic vesicles. We used immunostaining in the HIT insulin-secreting beta-cell line to show that ICA69 localizes in a punctate manner distinct from the insulin granules, suggesting an association with the synaptic-like microvesicles found in these cells. To pursue functional studies on ICA69, we chose to use the model organism Caenorhabditis elegans, for which a homologue of ICA69 exists. We show that the promoter of the C. elegans ICA69 homologue is specifically expressed in all neurons and specialized secretory cells. A deletion mutant was isolated and found to exhibit resistance to the drug aldicarb (an inhibitor of acetylcholinesterase), suggesting defective neurotransmitter secretion in the mutant. On the basis of the aldicarb resistance phenotype, we named the gene ric-19 (resistance to inhibitors of cholinesterase-19). The resistance to aldicarb was rescued by introducing a ric-19 transgene into the ric-19 mutant background. This is the first study aimed at dissecting ICA69 function, and our results are consistent with the interpretation that ICA69/RIC-19 is an evolutionarily conserved cytosolic protein participating in the process of neuroendocrine secretion via association with certain secretory vesicles.

摘要

ICA69是一种糖尿病自身抗原,没有已知功能的同源物。鉴于大多数糖尿病自身抗原都与神经内分泌分泌囊泡相关,我们试图确定ICA69是否也是如此,以及这种蛋白质是否参与神经内分泌分泌过程。对小鼠ICA69组织分布的蛋白质印迹分析显示,表达水平与分泌活性之间存在相关性,在脑、胰腺和胃黏膜中的表达水平最高。对小鼠脑进行亚细胞分级分离显示,虽然大多数ICA69存在于胞质溶胶中且可溶,但有一部分是膜结合的,并与突触囊泡共同富集。我们在HIT胰岛素分泌β细胞系中使用免疫染色表明,ICA69以与胰岛素颗粒不同的点状方式定位,表明它与这些细胞中发现的突触样微囊泡有关。为了对ICA69进行功能研究,我们选择使用模式生物秀丽隐杆线虫,它存在ICA69的同源物。我们表明,秀丽隐杆线虫ICA69同源物的启动子在所有神经元和特化分泌细胞中特异性表达。分离出一个缺失突变体,发现它对药物涕灭威(一种乙酰胆碱酯酶抑制剂)具有抗性,这表明该突变体中神经递质分泌存在缺陷。基于涕灭威抗性表型,我们将该基因命名为ric-19(对胆碱酯酶-19抑制剂的抗性)。通过将ric-19转基因引入ric-19突变体背景中,挽救了对涕灭威的抗性。这是第一项旨在剖析ICA69功能的研究,我们的结果与以下解释一致,即ICA69/RIC-19是一种进化保守的胞质蛋白,通过与某些分泌囊泡结合参与神经内分泌分泌过程。

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