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磷酸脂酸与 patched 的结合有助于抑制 Smoothened 和 Hedgehog 信号通路在 wing 发育中的作用。

Phosphatidic acid binding to Patched contributes to the inhibition of Smoothened and Hedgehog signaling in wing development.

机构信息

Markey Cancer Center, University of Kentucky College of Medicine, Lexington, KY 40536, USA.

Department of Molecular and Cellular Biochemistry, University of Kentucky College of Medicine, Lexington, KY 40536, USA.

出版信息

Sci Signal. 2023 Oct 17;16(807):eadd6834. doi: 10.1126/scisignal.add6834.

Abstract

Hedgehog (Hh) signaling controls growth and patterning during embryonic development and homeostasis in adult tissues. Hh binding to the receptor Patched (Ptc) elicits intracellular signaling by relieving Ptc-mediated inhibition of the transmembrane protein Smoothened (Smo). We uncovered a role for the lipid phosphatidic acid (PA) in the regulation of the Hh pathway in . Deleting the Ptc C-terminal tail or mutating the predicted PA-binding sites within it prevented Ptc from inhibiting Smo in wing discs and in cultured cells. The C-terminal tail of Ptc directly interacted with PA in vitro, an association that was reduced by Hh, and increased the amount of PA at the plasma membrane in cultured cells. Smo also interacted with PA in vitro through a binding pocket located in the transmembrane region, and mutating residues in this pocket reduced Smo activity in vivo and in cells. By genetically manipulating PA amounts in vivo or treating cultured cells with PA, we demonstrated that PA promoted Smo activation. Our findings suggest that Ptc may sequester PA in the absence of Hh and release it in the presence of Hh, thereby increasing the amount of PA that is locally available to promote Smo activation.

摘要

Hedgehog (Hh) 信号通路在胚胎发育过程中控制生长和模式形成,并在成年组织中维持内稳态。Hh 与受体 Patched (Ptc) 结合,通过解除 Ptc 对跨膜蛋白 Smoothened (Smo) 的抑制作用,引发细胞内信号转导。我们在 中发现了脂质磷脂酸 (PA) 在 Hh 通路调控中的作用。删除 Ptc 的 C 端尾巴或突变其中预测的 PA 结合位点,可阻止 Ptc 在翅盘和培养细胞中抑制 Smo。Ptc 的 C 端尾巴在体外与 PA 直接相互作用,这种结合在 Hh 存在下减少,并增加培养细胞中质膜上的 PA 含量。Smo 也通过位于跨膜区的结合口袋与 PA 在体外相互作用,并且该口袋中的突变残基降低了 Smo 的体内和细胞活性。通过在体内遗传操纵 PA 含量或用 PA 处理培养细胞,我们证明了 PA 促进了 Smo 的激活。我们的研究结果表明,在没有 Hh 的情况下,Ptc 可能会将 PA 隔离起来,而在有 Hh 的情况下,Ptc 会释放 PA,从而增加局部可用的 PA 量,以促进 Smo 的激活。

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