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FLR-4 a Novel Serine/Threonine Protein Kinase Regulates Defecation Rhythm in Caenorhabditis elegans

机译:FLR-4一种新型的丝氨酸/苏氨酸蛋白激酶可调节秀丽隐杆线虫的排便节律

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摘要

The defecation behavior of the nematode Caenorhabditis elegans is controlled by a 45-s ultradian rhythm. An essential component of the clock that regulates the rhythm is the inositol trisphosphate receptor in the intestine, but other components remain to be discovered. Here, we show that the flr-4 gene, whose mutants exhibit very short defecation cycle periods, encodes a novel serine/threonine protein kinase with a carboxyl terminal hydrophobic region. The expression of functional flr-4::GFP was detected in the intestine, part of pharyngeal muscles and a pair of neurons, but expression of flr-4 in the intestine was sufficient for the wild-type phenotype. Furthermore, laser killing of the flr-4–expressing neurons did not change the defecation phenotypes of wild-type and flr-4 mutant animals. Temperature-shift experiments with a temperature-sensitive flr-4 mutant suggested that FLR-4 acts in a cell-functional rather than developmental aspect in the regulation of defecation rhythms. The function of FLR-4 was impaired by missense mutations in the kinase domain and near the hydrophobic region, where the latter allele seemed to be a weak antimorph. Thus, a novel protein kinase with a unique structural feature acts in the intestine to increase the length of defecation cycle periods.
机译:线虫秀丽隐杆线虫的排便行为受45秒的超节律控制。调节节律的时钟的重要组成部分是肠中的肌醇三磷酸受体,但仍有待发现其他组成部分。在这里,我们表明,其flr-4基因,其突变体表现出非常短的排便周期周期,编码具有羧基末端疏水区的新型丝氨酸/苏氨酸蛋白激酶。在肠,咽部肌肉的一部分和一对神经元中检测到功能性flr-4 :: GFP的表达,但是在肠道中flr-4的表达足以用于野生型表型。此外,用激光杀死表达flr-4的神经元并没有改变野生型和flr-4突变动物的排便表型。对温度敏感的flr-4突变体进行的温度漂移实验表明,FLR-4在排便节律的调节中起着细胞功能而非发育方面的作用。 FLR-4的功能因激酶结构域和疏水区域附近的错义突变而受损,后者的等位基因似乎是弱的抗变体。因此,具有独特结构特征的新型蛋白激酶在肠中起作用以增加排便周期的长度。

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