Epithelial WNT secretion drives niche escape of developing gastric cancer

Research output: Contribution to journalResearch articleContributedpeer-review

Contributors

  • Jaehun Lee - , Pohang University of Science and Technology (Author)
  • Soomin Kim - , Kyung Hee University (Author)
  • Youngchul Oh - , Pohang University of Science and Technology (Author)
  • Stephan R Jahn - , Department of Visceral, Thoracic and Vascular Surgery, University Hospital Carl Gustav Carus Dresden (Author)
  • Jihoon Kim - , Catholic University of Korea (Author)
  • Yeongjun Kim - , Kyung Hee University (Author)
  • Tim Schmäche - , Department of Visceral, Thoracic and Vascular Surgery, National Center for Tumor Diseases Dresden (NCT/UCC), University Hospital Carl Gustav Carus Dresden (Author)
  • Sang-Min Kim - , Yonsei University (Author)
  • Isaree Teriyapirom - , Vienna Biocenter (Author)
  • Thomas Groß - , National Center for Tumor Diseases (NCT) Dresden (Author)
  • Ohbin Kwon - , Korea Advanced Institute of Science and Technology (Author)
  • Jungmin Kim - , Yonsei University (Author)
  • Somi Kim - , Pohang University of Science and Technology (Author)
  • Anne-Marlen Ada - , Department of Visceral, Thoracic and Vascular Surgery, University Hospital Carl Gustav Carus Dresden (Author)
  • Andrea Català-Bordes - , Institute for Basic Science (Author)
  • Youngwon Cho - , Vanderbilt University Medical Center (Author)
  • Jinho Kim - , Seoul National University Bundang Hospital (Author)
  • Amanda Andersson-Rolf - , Institute of Molecular Biotechnology (IMBA) (Author)
  • Sebastian R Merker - , Department of Visceral, Thoracic and Vascular Surgery, University Hospital Carl Gustav Carus Dresden (Author)
  • Joo Yeon Lim - , Yonsei University (Author)
  • Ji-Yeon Park - , Gradiant Bioconvergence Inc. (Author)
  • Thomas M Klompstra - , Korea Advanced Institute of Science and Technology (Author)
  • Ki-Jun Yoon - , Korea Advanced Institute of Science and Technology (Author)
  • Dae-Sik Lim - , Korea Advanced Institute of Science and Technology (Author)
  • Ho-Seok Lee - , Kyung Hee University (Author)
  • Jong Kyoung Kim - , Pohang University of Science and Technology (Author)
  • Eunyoung Choi - , Vanderbilt School of Medicine (Author)
  • James R Goldenring - , Vanderbilt University Medical Center (Author)
  • Jae-Ho Cheong - , Yonsei University (Author)
  • Hyunki Kim - , Yonsei University (Author)
  • Daniel E Stange - , Department of Visceral, Thoracic and Vascular Surgery, National Center for Tumor Diseases Dresden, German Cancer Consortium (DKTK) Partner Site Dresden (Author)
  • Heetak Lee - , Institute for Basic Science (Author)
  • Bon-Kyoung Koo - , Korea Advanced Institute of Science and Technology (Author)
  • Ji-Hyun Lee - , Sungkyunkwan University (SKKU) (Author)

Abstract

BACKGROUND: WNT signaling plays a key role in maintaining the gastric epithelium and promoting tumorigenesis. However, how gastric tumors achieve WNT niche independence remains unclear, as mutations on APC or CTNNB1-common mechanisms of ligand-independent WNT activation in colorectal cancer-are infrequent in gastric cancer. Understanding how WNT self-sufficiency is acquired in the stomach is therefore critical.

METHODS: We analyzed mouse gastric organoids harboring oncogenic KRASG12D with or without RNF43/ZNRF3 (RZ) or CDH1/TP53 (CP) mutations, along with corresponding in vivo mouse models. Niche independence was assessed through growth factor withdrawal, Porcupine and pathway-specific inhibitor treatments, and WNT rescue assays. We performed single-nucleus multiome sequencing (RNA + ATAC) to investigate transcriptional and chromatin dynamics. Findings from mouse models were validated using patient-derived gastric cancer organoids, and pan-cancer cell line datasets were analyzed to evaluate clinical and cross-tissue relevance.

RESULTS: Gastric fibroblasts secreted canonical WNT2B to maintain the homeostatic gastric epithelium. Upon KRAS activation, epithelial cells were reprogrammed to secrete WNT ligands independently of additional mutations. Single-nucleus multiome analysis revealed that KRAS-driven MAPK signaling opened SMAD2/3-bound enhancers at the WNT7B locus, leading to the emergence of WNT7B-expressing subpopulations. Inhibition of SMAD2/3 phosphorylation suppressed both organoid growth and WNT7B transcription, whereas exogenous WNT restored organoid proliferation. Patient-derived organoids with HER2 amplification, KRAS amplification, or WNT2 copy-number gain exhibited Porcupine inhibitor-sensitive growth, indicating dependence on WNT secretion from the organoids. Analysis of public transcriptomic datasets further demonstrated that the KRAS-MAPK-WNT7B axis is conserved across other cancer types, including lung cancer.

CONCLUSIONS: Gastric tumors can bypass niche dependence by acquiring KRAS-MAPK-SMAD2/3-driven epithelial WNT secretion. Targeting this axis-through MAPK inhibition, SMAD2/3 blockade, or suppression of WNT secretion-may represent a therapeutic vulnerability in gastric cancer and other KRAS-high malignancies.

Details

Original languageEnglish
JournalMolecular cancer
Publication statusE-pub ahead of print - 16 Dec 2025
Peer-reviewedYes

External IDs

ORCID /0000-0003-4246-2230/work/200631125

Keywords