The Caenorhabditis elegans protein SOC-3 permits an alternative mode of signal transduction by the EGL-15 FGF receptor

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS

ACS Applied Bio Materials Pub Date : 2024-08-21 DOI:10.1016/j.ydbio.2024.08.014

Claudia S. Rodriguez Torres , Nicole B. Wicker , Victória Puccini de Castro , Mariya Stefinko , Daniel C. Bennett , Brooke Bernhardt , Melissa Garcia Montes de Oca , Sainabou Jallow , Katelyn Flitcroft , Jessica-Jae S. Palalay , Omar A. Payán Parra , Yaakov E. Stern , Michael R. Koelle , Cindy Voisine , Ian G. Woods , Te-Wen Lo , Michael J. Stern , Claire C. de la Cova

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Abstract

Fibroblast Growth Factors and their receptors (FGFRs) comprise a cell signaling module that can stimulate signaling by Ras and the kinases Raf, MEK, and ERK to regulate animal development and homeostatic functions. In Caenorhabditis elegans, the sole FGFR ortholog EGL-15 acts with the GRB2 ortholog SEM-5 to promote chemoattraction and migration by the sex myoblasts (SMs) and fluid homeostasis by the hypodermis (Hyp7). Cell-specific differences in EGL-15 signaling were suggested by the phenotypes caused by egl-15(n1457), an allele that removes a region of its C-terminal domain (CTD) known to bind SEM-5. To determine how mutations altered EGL-15 activity in the SMs and Hyp7, we used the kinase reporter ERK-KTR to measure activation of the ERK ortholog MPK-1. Consequences of egl-15(n1457) were cell-specific, resulting in loss of MPK-1 activity in the SMs and elevated activity in Hyp7. Previous studies of Hyp7 showed that loss of the CLR-1 phosphatase causes a fluid homeostasis defect termed “Clear” that is suppressed by reduction of EGL-15 signaling, a phenotype termed “Suppressor of Clear” (Soc). To identify mechanisms that permit EGL-15 signaling in Hyp7, we conducted a genetic screen for Soc mutants in the clr-1; egl-15(n1457) genotype. We report the identification of SOC-3, a protein with putative SEM-5-binding motifs and PH and PTB domains similar to DOK and IRS proteins. In combination with the egl-15(n1457) mutation, loss of either soc-3, the GAB1 ortholog soc-1, or the SHP2 ortholog ptp-2, reduced MPK-1 activation. We generated alleles of soc-3 to test the requirement for the SEM-5-binding motifs, finding that residue Tyr³⁵⁶ is required for function. We propose that EGL-15-mediated SM chemoattraction relies solely on the direct interaction between SEM-5 and the EGL-15 CTD. In Hyp7, EGL-15 signaling uses two mechanisms: the direct SEM-5 binding mechanism; and an alternative, CTD-independent mechanism involving SOC-3, SOC-1, and PTP-2. This work demonstrates that FGF signaling uses distinct, tissue-specific mechanisms in development, and identifies SOC-3 as a potential adaptor that facilitates Ras pathway activation by FGFR.

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草履虫蛋白 SOC-3 允许 EGL-15 FGF 受体以另一种模式进行信号转导。

成纤维细胞生长因子及其受体（FGFR）构成了一个细胞信号模块，可刺激 Ras 和激酶 Raf、MEK 和 ERK 发出信号，从而调节动物的发育和平衡功能。在秀丽隐杆线虫中，唯一的表皮生长因子受体直向同源物 EGL-15 与 GRB2 直向同源物 SEM-5 共同作用，促进性肌母细胞（SMs）的趋化和迁移，以及皮下组织（Hyp7）的体液平衡。egl-15(n1457)等位基因去除了已知能与SEM-5结合的C-端结构域（CTD）区域，其导致的表型表明EGL-15信号传导存在细胞特异性差异。为了确定突变如何改变 EGL-15 在 SMs 和 Hyp7 中的活性，我们使用激酶报告因子 ERK-KTR 来测量 ERK 同源物 MPK-1 的活化情况。egl-15(n1457)对细胞的影响是特异性的，它导致MPK-1在SMs中失去活性，而在Hyp7中活性升高。以前对 Hyp7 的研究表明，CLR-1 磷酸酶的缺失会导致一种被称为 "Clear "的液体平衡缺陷，这种缺陷会因 EGL-15 信号的减少而被抑制，这种表型被称为 "Clear 的抑制因子"（Soc）。为了确定在 Hyp7 中允许 EGL-15 信号传导的机制，我们对 clr-1; egl-15(n1457) 基因型的 Soc 突变体进行了遗传筛选。我们报告了 SOC-3 的鉴定结果，它是一种具有假定 SEM-5 结合基序以及与 DOK 和 IRS 蛋白类似的 PH 和 PTB 结构域的蛋白质。结合egl-15（n1457）突变，缺失soc-3、GAB1直向同源物soc-1或SHP2直向同源物ptp-2都会降低MPK-1的激活。我们生成了 soc-3 的等位基因，以测试对 SEM-5 结合基序的要求，发现残基 Tyr356 是功能所必需的。我们认为，EGL-15 介导的 SM 趋化吸引完全依赖于 SEM-5 与 EGL-15 CTD 之间的直接相互作用。在 Hyp7 中，EGL-15 信号转导使用两种机制：SEM-5 直接结合机制；另一种不依赖 CTD 的机制，涉及 SOC-3、SOC-1 和 PTP-2。这项工作证明了生长因子受体信号在发育过程中使用了不同的组织特异性机制，并确定了 SOC-3 是促进生长因子受体激活 Ras 通路的潜在适配体。

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来源期刊

ACS Applied Bio Materials Chemistry-Chemistry (all)

CiteScore

9.40

自引率

2.10%

发文量

464