Cell Death Discovery (Jan 2022)

NLK is required for Ras/ERK/SRF/ELK signaling to tune skeletal muscle development by phosphorylating SRF and antagonizing the SRF/MKL pathway

  • Shang-Ze Li,
  • Ze-Yan Zhang,
  • Jie Chen,
  • Ming-You Dong,
  • Xue-Hua Du,
  • Jie Gao,
  • Qi-Peng Shu,
  • Chao Li,
  • Xin-Yi Liang,
  • Zhi-Hao Ding,
  • Run-Lei Du,
  • Junli Wang,
  • Xiao-Dong Zhang

DOI
https://doi.org/10.1038/s41420-021-00774-9
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 12

Abstract

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Abstract Serum response factor (SRF) regulates differentiation and proliferation by binding to RhoA-actin-activated MKL or Ras-MAPK-activated ELK transcriptional coactivators, but the molecular mechanisms responsible for SRF regulation remain unclear. Here, we show that Nemo-like kinase (NLK) is required for the promotion of SRF/ELK signaling in human and mouse cells. NLK was found to interact with and phosphorylate SRF at serine residues 101/103, which in turn enhanced the association between SRF and ELK. The enhanced affinity of SRF/ELK antagonized the SRF/MKL pathway and inhibited mouse myoblast differentiation in vitro. In a skeletal muscle-specific Nlk conditional knockout mouse model, forming muscle myofibers underwent hypertrophic growth, resulting in an increased muscle and body mass phenotype. We propose that both phosphorylation of SRF by NLK and phosphorylation of ELKs by MAPK are required for RAS/ELK signaling, confirming the importance of this ancient pathway and identifying an important role for NLK in modulating muscle development in vivo.