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首页> 外文OA文献 >An AGEF-1/Arf GTPase/AP-1 ensemble antagonizes LET-23 EGFR basolateral localization and signaling during C. elegans vulva induction
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An AGEF-1/Arf GTPase/AP-1 ensemble antagonizes LET-23 EGFR basolateral localization and signaling during C. elegans vulva induction

机译:AGEF-1 / Arf GTPase / AP-1集合体在线虫外阴诱导过程中拮抗LET-23 EGFR基底外侧的定位和信号传导

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LET-23 Epidermal Growth Factor Receptor (EGFR) signaling specifies the vulval cell fates during C. elegans larval development. LET-23 EGFR localization on the basolateral membrane of the vulval precursor cells (VPCs) is required to engage the LIN-3 EGF-like inductive signal. The LIN-2 Cask/LIN-7 Veli/LIN-10 Mint (LIN-2/7/10) complex binds LET-23 EGFR, is required for its basolateral membrane localization, and therefore, vulva induction. Besides the LIN-2/7/10 complex, the trafficking pathways that regulate LET-23 EGFR localization have not been defined. Here we identify vh4, a hypomorphic allele of agef-1, as a strong suppressor of the lin-2 mutant Vulvaless (Vul) phenotype. AGEF-1 is homologous to the mammalian BIG1 and BIG2 Arf GTPase guanine nucleotide exchange factors (GEFs), which regulate secretory traffic between the Trans-Golgi network, endosomes and the plasma membrane via activation of Arf GTPases and recruitment of the AP-1 clathrin adaptor complex. Consistent with a role in trafficking we show that AGEF-1 is required for protein secretion and that AGEF-1 and the AP-1 complex regulate endosome size in coelomocytes. The AP-1 complex has previously been implicated in negative regulation of LET-23 EGFR, however the mechanism was not known. Our genetic data indicate that AGEF-1 is a strong negative regulator of LET-23 EGFR signaling that functions in the VPCs at the level of the receptor. In line with AGEF-1 being an Arf GEF, we identify the ARF-1.2 and ARF-3 GTPases as also negatively regulating signaling. We find that the agef-1(vh4) mutation results in increased LET-23 EGFR on the basolateral membrane in both wild-type and lin-2 mutant animals. Furthermore, unc-101(RNAi), a component of the AP-1 complex, increased LET-23 EGFR on the basolateral membrane in lin-2 and agef-1(vh4); lin-2 mutant animals. Thus, an AGEF-1/Arf GTPase/AP-1 ensemble functions opposite the LIN-2/7/10 complex to antagonize LET-23 EGFR basolateral membrane localization and signaling.
机译:LET-23表皮生长因子受体(EGFR)信号转导线虫幼虫发育过程中的外阴细胞命运。需要LET-23 EGFR在外阴前体细胞(VPC)的基底外侧膜上定位,以接合LIN-3 EGF样诱导信号。 LIN-2木桶/ LIN-7 Veli / LIN-10薄荷(LIN-2 / 7/10)复合物结合LET-23 EGFR,是其基底外侧膜定位所必需的,因此需要诱导外阴。除了LIN-2 / 7/10复合物外,尚未定义调节LET-23 EGFR定位的运输途径。在这里我们确定vh4,agef-1的一个亚等位基因,是lin-2突变体Vulvaless(Vul)表型的强抑制剂。 AGEF-1与哺乳动物BIG1和BIG2 Arf GTPase鸟嘌呤核苷酸交换因子(GEF)同源,后者通过激活Arf GTPases和募集AP-1网格蛋白来调节Trans-Golgi网络,内体和质膜之间的分泌运输。适配器复合体。与在贩运中的作用一致,我们显示了AGEF-1是蛋白质分泌所必需的,并且AGEF-1和AP-1复合物可调节血管内皮细胞的内体大小。 AP-1复合物以前曾牵涉到LET-23 EGFR的负调控,但是其机制尚不清楚。我们的遗传数据表明,AGEF-1是LET-23 EGFR信号转导的强负调节剂,在受体水平上在VPC中起作用。与作为Arf GEF的AGEF-1一致,我们将ARF-1.2和ARF-3 GTPases识别为也负调控信号。我们发现agef-1(vh4)突变导致野生型和lin-2突变动物的基底外侧膜上的LET-23 EGFR升高。此外,unc-101(RNAi)是AP-1复合物的组成部分,在lin-2和agef-1(vh4)的基底外侧膜上增加了LET-23 EGFR。 lin-2突变动物。因此,AGEF-1 / Arf GTPase / AP-1集合的功能与LIN-2 / 7/10复合物相反,可拮抗LET-23 EGFR基底外侧膜的定位和信号传导。

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