Peptide mimetic NC114 induces growth arrest by preventing PKCδ activation and FOXM1 nuclear translocation in colorectal cancer cells

Yuki Taguchi; Takeo Nakaya; Kenichi Aizawa; Yoshiyuki Noguchi; Nobuhiko Maiya; Chisako Iwamoto; Kenichi Ohba; Minoru Sugawara; Masayuki Murata; Ryozo Nagai; Fumi Kano

doi:10.1002/2211-5463.13784

FEBS Open Bio (Apr 2024)

Peptide mimetic NC114 induces growth arrest by preventing PKCδ activation and FOXM1 nuclear translocation in colorectal cancer cells

Yuki Taguchi,
Takeo Nakaya,
Kenichi Aizawa,
Yoshiyuki Noguchi,
Nobuhiko Maiya,
Chisako Iwamoto,
Kenichi Ohba,
Minoru Sugawara,
Masayuki Murata,
Ryozo Nagai,
Fumi Kano

Affiliations

Yuki Taguchi: Cell Biology Center, Institute of Innovative Research Tokyo Institute of Technology Yokohama Kanagawa Japan
Takeo Nakaya: Department of Pathology Jichi Medical University Shimotsuke Tochigi Japan
Kenichi Aizawa: Department of Clinical Pharmacology Jichi Medical University Shimotsuke Tochigi Japan
Yoshiyuki Noguchi: Cell Biology Center, Institute of Innovative Research Tokyo Institute of Technology Yokohama Kanagawa Japan
Nobuhiko Maiya: Stem Cell Business Department, Healthcare Business Unit NIKON Corporation Yokohama Kanagawa Japan
Chisako Iwamoto: Marketing Department, Healthcare Business Unit NIKON Corporation Minato‐ku Tokyo Japan
Kenichi Ohba: Engineering Solution Business Division Nikon System Inc. Yokohama Kanagawa Japan
Minoru Sugawara: Cancer Precision Medicine Center Japanese Foundation for Cancer Research Koto‐ku Tokyo Japan
Masayuki Murata: Cell Biology Center, Institute of Innovative Research Tokyo Institute of Technology Yokohama Kanagawa Japan
Ryozo Nagai: Jichi Medical University Shimotsuke Tochigi Japan
Fumi Kano: Cell Biology Center, Institute of Innovative Research Tokyo Institute of Technology Yokohama Kanagawa Japan

DOI: https://doi.org/10.1002/2211-5463.13784
Journal volume & issue: Vol. 14, no. 4
pp. 695 – 720

Abstract

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The peptide mimetic, NC114, is a promising anticancer compound that specifically kills colorectal cancer cells without affecting normal colon epithelial cells. In our previous study, we observed that NC114 inhibited the Wnt/β‐catenin pathway, with significant downregulation of both Ser 675‐phosphorylated β‐catenin and its target genes, cyclin D1 and survivin. However, the molecular mechanism responsible for its cytotoxic effect has not yet been fully characterized. In the present study, we demonstrated that NC114 prevented cell cycle progression from S to G2/M phase by downregulating cell cycle‐related gene expression, and also induced growth arrest in SW480 and HCT‐116 colorectal cancer cells. A novel covariation network analysis combined with transcriptome analysis revealed a series of signaling cascades affected by NC114 treatment, and identified protein kinase C‐δ (PKCδ) and forkhead box protein M1 (FOXM1) as important regulatory factors for NC114‐induced growth arrest. NC114 treatment inhibits the activation of PKCδ and its kinase activity, which suppresses MEK/ERK signaling. Attenuated MEK/ERK signaling then results in a reduction in FOXM1 phosphorylation and subsequent nuclear translocation of FOXM1 and β‐catenin. Consequently, formation of a T‐cell factor‐4 (TCF4)/β‐catenin transcription complex in the nucleus is inhibited and transcription of its target genes, such as cell cycle‐related genes, is downregulated. The efficacy of NC114 on tumor growth was confirmed in a xenograft model. Collectively, elucidation of the mechanism by which NC114 induces growth arrest in colorectal cancer cells should provide a novel therapeutic strategy for colorectal cancer treatment.

Published in FEBS Open Bio

ISSN: 2211-5463 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General)
Website: https://febs.onlinelibrary.wiley.com/journal/22115463

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