LIN28B-mediated PI3K/AKT pathway activation promotes metastasis in colorectal cancer models
Alice E. Shin, … , Peter A. Sims, Anil K. Rustgi
Alice E. Shin, … , Peter A. Sims, Anil K. Rustgi
Published January 14, 2025
Citation Information: J Clin Invest. 2025;135(8):e186035. https://doi.org/10.1172/JCI186035.
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Research Article Gastroenterology Oncology

LIN28B-mediated PI3K/AKT pathway activation promotes metastasis in colorectal cancer models

Abstract

Colorectal cancer (CRC) remains a leading cause of cancer death because of metastatic spread. LIN28B is overexpressed in 30% of CRCs and promotes metastasis, yet its mechanisms remain unclear. In this study, we genetically modified CRC cell lines to overexpress LIN28B, resulting in enhanced PI3K/AKT pathway activation and liver metastasis in mice. We developed genetically modified mouse models with constitutively active Pik3ca that form intestinal tumors progressing to liver metastases with an intact immune system, addressing the limitations of previous Pik3ca-mutant models, including long tumor latency, mixed histology, and lack of distant metastases. The PI3Kα-specific inhibitor alpelisib reduced migration and invasion in vitro and metastasis in vivo. We present a comprehensive analysis of vertical inhibition of the PI3K/AKT pathway in CRC using the FDA-approved drugs alpelisib and capivasertib (an AKT inhibitor) in combination with LY2584702 (a ribosomal protein S6 kinase inhibitor) in CRC cell lines and mouse- and patient-derived organoids. Tissue microarrays from patients with CRC verified that LIN28B and PI3K/AKT pathway activation correlate with CRC progression. These findings highlight the critical role of the LIN28B-mediated PI3K/AKT pathway in CRC metastasis, the therapeutic potential of targeted inhibition, and the promise of patient-derived organoids in precision medicine in metastatic CRC.

Authors

Alice E. Shin, Kensuke Sugiura, Secunda W. Kariuki, David A. Cohen, Samuel P. Flashner, Andres J. Klein-Szanto, Noriyuki Nishiwaki, Dechokyab De, Neil Vasan, Joel T. Gabre, Christopher J. Lengner, Peter A. Sims, Anil K. Rustgi

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Figure 6

Pharmacologic inhibition of the S6K/RPS6 axis suppresses LIN28B-driven cell migration and invasion in CRC cells.

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Pharmacologic inhibition of the S6K/RPS6 axis suppresses LIN28B-driven c...
(A) GSEA from RNA-Seq showing hallmark pathways enriched in LIN28Bhi cells compared with LIN28Bhi cells treated with 5 μM alpelisib. (B) GSEA from RNA-Seq showing hallmark pathways enriched in liver metastasis compared with matched primary tumors in patients with CRC (GSE50760). (C) Quantification of phosphorylated protein targets involved in the PI3K/AKT pathway in EV, LIN28Bhi, and LIN28Bhi cells treated with 5 μM alpelisib (1-way ANOVA for each protein target, mean ± SEM). (D) Western blot analysis of LIN28B, p-AKT (Ser473), p-S6K (Thr389/412), total S6K, p-RPS6 (Ser235/236), t-RPS6, and GAPDH in CRC cells treated with 5 μM alpelisib (alp, alpelisib; 1-way ANOVA, mean ± SEM). (E) Representative IHC images of p-S6K (Thr389/412) and p-RPS6 (Ser235/236) in colonic tissues from VilCre mice. Scale bars: 100 μm. (F) Western blot analysis of p-RPS6, t-RPS6, and GAPDH in CRC cells treated with varying concentrations of LY2584702 (S6K inhibitor) (1-way ANOVA, mean ± SEM). (G) Wound healing assay showing cell migration of LIN28Bhi CRC cells (n = 3; 2-way ANOVA, mean ± SEM). Scale bars: 500 μm. (H) Transwell ECM invasion assay of LIN28Bhi CRC cells (1-way ANOVA, mean ± SEM). Scale bars: 1 mm. *P < 0.05, **P < 0.01, ****P < 0.0001.