JAK/STAT3 represents a therapeutic target for colorectal cancer patients with stromal-rich tumors

Kathryn A.F. Pennel; Phimmada Hatthakarnkul; Colin S. Wood; Guang‐Yu Lian; Sara Samir Foad Al-Badran; Jean A. Quinn; Assya Legrini; Jitwadee Inthagard; Peter Alexander; Hester van Wyk; Ahmad Kurniawan; Umar Hashmi; Michael A. Gillespie; Megan L. Mills; Aula Ammar; Jennifer Hay; Ditte K. Andersen; Colin Nixon; Selma Rebus; David K. Chang; Caroline Kelly; Andrea Harkin; Janet Graham; David N. Church; Ian D. Tomlinson; Mark Saunders; Timothy Iveson; Tamsin R.M. Lannagan; René Jackstadt; Noori Maka; Paul G. Horgan; Campbell S.D. Roxburgh; Owen J. Sansom; Donald C. McMillan; Colin W. Steele; Nigel B. Jamieson; James H. Park; Antonia K. Roseweir; Joanne Edwards

doi:10.1186/s13046-024-02958-4

JAK/STAT3 represents a therapeutic target for colorectal cancer patients with stromal-rich tumors

Kathryn A.F. Pennel(University of Glasgow), Phimmada Hatthakarnkul(University of Glasgow), Colin S. Wood(Glasgow Royal Infirmary), Guang‐Yu Lian(University of Glasgow), Sara Samir Foad Al-Badran(University of Glasgow), Jean A. Quinn(University of Glasgow), Assya Legrini(University of Glasgow), Jitwadee Inthagard(University of Glasgow), Peter Alexander(Glasgow Royal Infirmary), Hester van Wyk(Glasgow Royal Infirmary), Ahmad Kurniawan(University of Glasgow), Umar Hashmi(University of Glasgow), Michael A. Gillespie(Cancer Research UK Scotland Institute), Megan L. Mills(Cancer Research UK Scotland Institute), Aula Ammar(University of Glasgow), Jennifer Hay(Queen Elizabeth University Hospital), Ditte K. Andersen(Queen Elizabeth University Hospital), Colin Nixon(Cancer Research UK Scotland Institute), Selma Rebus(University of Glasgow), David K. Chang(Glasgow Royal Infirmary), Caroline Kelly(Beatson West of Scotland Cancer Centre), Andrea Harkin(Beatson West of Scotland Cancer Centre), Janet Graham(Beatson West of Scotland Cancer Centre), David N. Church(Centre for Human Genetics), Ian D. Tomlinson(Edinburgh Cancer Research), Mark Saunders(The Christie NHS Foundation Trust), Timothy Iveson(University Hospital Southampton NHS Foundation Trust), Tamsin R.M. Lannagan(Cancer Research UK Scotland Institute), René Jackstadt(Cancer Research UK Scotland Institute), Noori Maka(Queen Elizabeth University Hospital), Paul G. Horgan(Glasgow Royal Infirmary), Campbell S.D. Roxburgh(Glasgow Royal Infirmary), Owen J. Sansom(Cancer Research UK Scotland Institute), Donald C. McMillan(Glasgow Royal Infirmary), Colin W. Steele(Glasgow Royal Infirmary), Nigel B. Jamieson(University of Glasgow), James H. Park(Queen Elizabeth University Hospital), Antonia K. Roseweir(University of Glasgow), Joanne Edwards(University of Glasgow)

Journal of Experimental & Clinical Cancer Research

March 1, 2024

10.1186/s13046-024-02958-4

Cited by 45Open Access

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Abstract

Abstract Colorectal cancer (CRC) is a heterogenous malignancy underpinned by dysregulation of cellular signaling pathways. Previous literature has implicated aberrant JAK/STAT3 signal transduction in the development and progression of solid tumors. In this study we investigate the effectiveness of inhibiting JAK/STAT3 in diverse CRC models, establish in which contexts high pathway expression is prognostic and perform in depth analysis underlying phenotypes. In this study we investigated the use of JAK inhibitors for anti-cancer activity in CRC cell lines, mouse model organoids and patient-derived organoids. Immunohistochemical staining of the TransSCOT clinical trial cohort, and 2 independent large retrospective CRC patient cohorts was performed to assess the prognostic value of JAK/STAT3 expression. We performed mutational profiling, bulk RNASeq and NanoString GeoMx® spatial transcriptomics to unravel the underlying biology of aberrant signaling. Inhibition of signal transduction with JAK1/2 but not JAK2/3 inhibitors reduced cell viability in CRC cell lines, mouse, and patient derived organoids (PDOs). In PDOs, reduced Ki67 expression was observed post-treatment. A highly significant association between high JAK/STAT3 expression within tumor cells and reduced cancer-specific survival in patients with high stromal invasion (TSP high ) was identified across 3 independent CRC patient cohorts, including the TrasnSCOT clinical trial cohort. Patients with high phosphorylated STAT3 (pSTAT3) within the TSP high group had higher influx of CD66b + cells and higher tumoral expression of PDL1. Bulk RNAseq of full section tumors showed enrichment of NFκB signaling and hypoxia in these cases. Spatial deconvolution through GeoMx® demonstrated higher expression of checkpoint and hypoxia-associated genes in the tumor (pan-cytokeratin positive) regions, and reduced lymphocyte receptor signaling in the TME (pan-cytokeratin- and αSMA-) and αSMA (pan-cytokeratin- and αSMA +) areas. Non-classical fibroblast signatures were detected across αSMA + regions in cases with high pSTAT3. Therefore, in this study we have shown that inhibition of JAK/STAT3 represents a promising therapeutic strategy for patients with stromal-rich CRC tumors. High expression of JAK/STAT3 proteins within both tumor and stromal cells predicts poor outcomes in CRC, and aberrant signaling is associated with distinct spatially-dependant differential gene expression.

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