Frontiers in Oncology (Sep 2022)

Proteomics and liquid biopsy characterization of human EMT-related metastasis in colorectal cancer

  • Mao-Sen Huang,
  • Li-Hua Fu,
  • Hao-Chao Yan,
  • Lin-Yao Cheng,
  • Hai-Ming Ru,
  • Hai-Ming Ru,
  • Hai-Ming Ru,
  • Si Mo,
  • Chun-Yin Wei,
  • Chun-Yin Wei,
  • Chun-Yin Wei,
  • Dai-Mou Li,
  • Xian-Wei Mo,
  • Xian-Wei Mo,
  • Xian-Wei Mo,
  • Wei-Zhong Tang,
  • Wei-Zhong Tang,
  • Wei-Zhong Tang,
  • Lin-Hai Yan

DOI
https://doi.org/10.3389/fonc.2022.790096
Journal volume & issue
Vol. 12

Abstract

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Tumor cells undergo epithelial-mesenchymal transition (EMT), however, there is a room of disagreement in role of EMT heterogeneity to colorectal cancer metastasis (mCRC) evolution. To uncover new EMT-related metastasis proteins and pathways, we addressed the EMT status in colorectal cancer liver metastasis patient-derived CTCs to identify proteins that promote their distant metastasis. And then, we performed a comparative proteomic analysis in matched pairs of primary tumor tissues, adjacent mucosa tissues and liver metastatic tissues. By integrative analysis we show that, unstable Epithelial/Mesenchymal (E/M)-type CTCs had the strongest liver metastases formation ability and the proportion of E/M-type CTCs correlated with distant metastases. Using an optimized proteomic workflow including data independent acquisition (DIA) and parallel reaction monitoring (PRM), we identified novel EMT-related protein cluster (GNG2, COL6A1, COL6A2, DCN, COL6A3, LAMB2, TNXB, CAVIN1) and well-described (ERBB2) core protein level changes in EMT-related metastasis progression, and the proteomic data indicate ERBB2, COL6A1 and CAVIN1 are promising EMT-related metastatic biomarker candidates. This study contributes to our understanding of the role that EMT plays in CRC metastasis and identifies heterogeneous EMT phenotypes as a key piece for tumor progression and prognosis. We further propose that therapies targeting this aggressive subset (E/M-type) of CTCs and related protein may be worthy of exploration as potential suppressors of metastatic evolution.

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