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秀丽隐杆线虫中运动神经元MC引起咽部兴奋所需的相互作用基因。

Interacting genes required for pharyngeal excitation by motor neuron MC in Caenorhabditis elegans.

作者信息

Raizen D M, Lee R Y, Avery L

机构信息

Department of Biochemistry, University of Texas Southwestern Medical Center, Dallas 75235-9038, USA.

出版信息

Genetics. 1995 Dec;141(4):1365-82. doi: 10.1093/genetics/141.4.1365.

Abstract

We studied the control of pharyngeal excitation in Caenorhabditis elegans. By laser ablating subsets of the pharyngeal nervous system, we found that the MC neuron type is necessary and probably sufficient for rapid pharyngeal pumping. Electropharyngeograms showed that MC transmits excitatory postsynaptic potentials, suggesting that MC acts as a neurogenic pacemaker for pharyngeal pumping. Mutations in genes required for acetylcholine (ACh) release and an antagonist of the nicotinic ACh receptor (nAChR) reduced pumping rates, suggesting that a nAChR is required for MC transmission. To identify genes required for MC neurotransmission, we screened for mutations that cause slow pumping but no other defects. Mutations in two genes, eat-2 and eat-18, eliminated MC neurotransmission. A gain-of-function eat-18 mutation, ad820sd, and a putative loss-of-function eat-18 mutation, ad1110, both reduced the excitation of pharyngeal muscle in response to the nAChR agonists nicotine and carbachol, suggesting that eat-18 is required for the function of a pharyngeal nAChR. Fourteen recessive mutations in eat-2 fell into five complementation classes. We found allele-specific genetic interactions between eat-2 and eat-18 that correlated with complementation classes of eat-2. We propose that eat-18 and eat-2 function in a multisubunit protein complex involved in the function of a pharyngeal nAChR.

摘要

我们研究了秀丽隐杆线虫中咽部兴奋的控制机制。通过激光消融咽部神经系统的不同亚群,我们发现MC神经元类型对于快速咽部蠕动是必需的,并且可能是充分的。咽电图显示MC传递兴奋性突触后电位,这表明MC作为咽部蠕动的神经源性起搏器发挥作用。乙酰胆碱(ACh)释放所需基因的突变以及烟碱型ACh受体(nAChR)的拮抗剂降低了蠕动速率,这表明nAChR对于MC的传递是必需的。为了鉴定MC神经传递所需的基因,我们筛选了导致蠕动缓慢但无其他缺陷的突变。两个基因eat-2和eat-18的突变消除了MC神经传递。功能获得性eat-18突变体ad820sd和假定的功能丧失性eat-18突变体ad1110,均降低了咽部肌肉对nAChR激动剂尼古丁和卡巴胆碱的反应性兴奋,这表明eat-18是咽部nAChR功能所必需的。eat-2中的14个隐性突变分为五个互补类。我们发现eat-2和eat-18之间存在等位基因特异性遗传相互作用,这与eat-2的互补类相关。我们提出,eat-18和eat-2在参与咽部nAChR功能的多亚基蛋白复合物中发挥作用。

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