Nature Communications (Nov 2024)

A Huluwa phosphorylation switch regulates embryonic axis induction

  • Yao Li,
  • Yun Yan,
  • Bo Gong,
  • Qianwen Zheng,
  • Haiyan Zhou,
  • Jiarui Sun,
  • Mingpeng Li,
  • Zhao Wang,
  • Yaohui Li,
  • Yunjing Wan,
  • Weixi Chen,
  • Shiqian Qi,
  • Xianming Mo,
  • Anming Meng,
  • Bo Xiang,
  • Jing Chen

DOI
https://doi.org/10.1038/s41467-024-54450-4
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 15

Abstract

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Abstract Embryonic axis formation is essential for patterning and morphogenesis in vertebrates and is tightly regulated by the dorsal organizer. Previously, we demonstrated that maternally derived Huluwa (Hwa) acts as a dorsal determinant, dictating axis formation by activating β-catenin signaling in zebrafish and Xenopus. However, the mechanism of activation and fine regulation of the Hwa protein remains unclear. Through candidate screening we identified a mutation at Ser168 in the PPNSP motif of Hwa that dramatically abolishes its axis-inducing activity. Mechanistically, mutating the Ser168 residue reduced its binding affinity to Tankyrase 1/2 and the degradation of the Axin protein, weakening β-catenin signaling activation. We confirmed that Ser168 is phosphorylated and that phosphorylation increases Hwa activity in β-catenin signaling and axis induction. Several kinases including Cdk16, Cdk2, and GSK3β, were found to enhance Ser168 phosphorylation in vitro and in vivo. Both dominant-negative Cdk16 expression and pHwa (Ser168) antibody treatment reduce Hwa function. Lastly, a knock-in allele mutating Ser168 to alanine resulted in embryos lacking body axes, demonstrating that Ser168 is essential to axis formation. In summary, Ser168 acts as a phosphorylation switch in Hwa/β-catenin signaling for embryonic axis induction, regulated by multiple kinases.