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P-Type ATPase TAT-2 Negatively Regulates Monomethyl Branched-Chain Fatty Acid Mediated Function in Post-Embryonic Growth and Development in C. elegans

机译:P型ATPase TAT 2负调节线虫后胚生长和发育中的单甲基支链脂肪酸介导的功能。

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摘要

Monomethyl branched-chain fatty acids (mmBCFAs) are essential for Caenorhabditis elegans growth and development. To identify factors acting downstream of mmBCFAs for their function in growth regulation, we conducted a genetic screen for suppressors of the L1 arrest that occurs in animals depleted of the 17-carbon mmBCFA C17ISO. Three of the suppressor mutations defined an unexpected player, the P-type ATPase TAT-2, which belongs to the flippase family of proteins that are implicated in mediating phospholipid bilayer asymmetry. We provide evidence that TAT-2, but not other TAT genes, has a specific role in antagonizing the regulatory activity of mmBCFAs in intestinal cells. Interestingly, we found that mutations in tat-2 also suppress the lethality caused by inhibition of the first step in sphingolipid biosynthesis. We further showed that the fatty acid side-chains of glycosylceramides contain 20%–30% mmBCFAs and that this fraction is greatly diminished in the absence of mmBCFA biosynthesis. These results suggest a model in which a C17ISO-containing sphingolipid may mediate the regulatory functions of mmBCFAs and is negatively regulated by TAT-2 in intestinal cells. This work indicates a novel connection between a P-type ATPase and the critical regulatory function of a specific fatty acid.
机译:单甲基支链脂肪酸(mmBCFAs)对于秀丽隐杆线虫的生长和发育至关重要。为了确定在mmBCFAs下游起作用的因子,以了解其在生长调节中的功能,我们进行了遗传筛选,以检测L17阻滞剂的发生情况,该抑制因子发生在消耗17碳mmBCFA C17ISO的动物体内。三个抑制突变定义了一个意外的参与者,即P型ATPase TAT-2,该酶属于翻转蛋白家族的蛋白质,与介导磷脂双层不对称有关。我们提供的证据表明,TAT-2(而不是其他TAT基因)在拮抗mmBCFA在肠细胞中的调节活性方面具有特定作用。有趣的是,我们发现tat-2中的突变还抑制了鞘脂生物合成第一步的抑制作用所致的杀伤力。我们进一步表明,糖基神经酰胺的脂肪酸侧链包含20%–30%的mmBCFA,在没有mmBCFA生物合成的情况下,该比例大大降低。这些结果提示了一种模型,其中含C17ISO的鞘脂可能介导mmBCFA的调节功能,并在肠细胞中被TAT-2负调节。这项工作表明P型ATP酶和特定脂肪酸的关键调节功能之间的新型联系。

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