Induction of resistance to oxaliplatin in cancer by a microRNA/Fem1B/Gli1 pathway

Yi-Chen Su; Landon Tyler Metzen; Leandro Martín Vélez; Elodie Bournique; Marcus Seldin; Rémi Buisson; Wei-Wen Kuo; Chih-Yang Huang; Peter Kaiser

Induction of resistance to oxaliplatin in cancer by a microRNA/Fem1B/Gli1 pathway

Am J Cancer Res. 2023 Dec 15;13(12):6011-6025. eCollection 2023.

Authors

Yi-Chen Su^{1

2

3}, Landon Tyler Metzen¹, Leandro Martín Vélez¹, Elodie Bournique¹, Marcus Seldin¹, Rémi Buisson¹, Wei-Wen Kuo⁴, Chih-Yang Huang^{2

5

6

7

8

3}, Peter Kaiser¹

Affiliations

¹ Department of Biological Chemistry, University of California Irvine, California 92697, USA.
² Graduate Institute of Basic Medical Science, China Medical University Taichung 404, Taiwan.
³ Graduate Institute of Biomedical Sciences, China Medical University Taichung 404, Taiwan.
⁴ Department of Biological Science and Technology, China Medical University Taichung 404, Taiwan.
⁵ Cardiovascular and Mitochondrial Related Disease Research Center, Hualien Tzu Chi Hospital, Buddhist Tzu Chi Medical Foundation Hualien 970, Taiwan.
⁶ Center of General Education, Buddhist Tzu Chi Medical Foundation, Tzu Chi University of Science and Technology Hualien 970, Taiwan.
⁷ Department of Medical Research, China Medical University Hospital, China Medical University Taichung 404, Taiwan.
⁸ Department of Medical Laboratory Science and Biotechnology, Asia University Taichung 413, Taiwan.

PMID: 38187042
PMCID: PMC10767360

Abstract

Colorectal cancer is among the most common cancers worldwide and a frequent cause of cancer related deaths. Oxaliplatin is the first line chemotherapeutics for treatment, but the development of resistance leads to recurrence of oxaliplatin insensitive tumors. To understand possible mechanisms of drug tolerance we developed oxaliplatin resistant derivatives (OR-LoVo) of the established LoVo cell line originally isolated from a metastatic colon adenocarcinoma. We compared the microRNA (miRNA) expression profile of the cell pair and found expression of miR-29a-3p significantly increased in OR-LoVo cells compared to parent cells. In addition, miR-29a-3p was significantly elevated in tumor tissue when compared to matched surrounding tissue in human, suggesting potential clinical importance. Ectopic miR-29-a-3p expression induced chemoresistance in a number of different cancer cell lines as well as colorectal tumors in mice. We further demonstrated that miR-29-a-3p downregulates expression of the ubiquitin ligase component FEM1B and that reduction of Fem1b levels is sufficient to confer oxaliplatin resistance. FEM1B targets the glioma associated oncogene Gli1 for degradation, suggesting that increased Gli1 levels could contribute to oxaliplatin tolerance. Accordingly, knockdown of GLI1 reverted chemoresistance of OR-LoVo cells. Mechanistically, resistant cells experienced significantly lower DNA damage upon oxaliplatin treatment, which can be partially explained by reduced oxaliplatin uptake and enhanced repair. These results suggest that miR-29-a-3p overexpression induces oxaliplatin resistance through misregulation of Fem1B and Gli1 levels. TCGA analyses provides strong evidence that the reported findings regarding induced drug tolerance by the miR-29a/Fem1B axis is clinically relevant. The reported findings can help to predict oxaliplatin sensitivity and resistance of colorectal tumors.

Keywords: DNA damage; Drug-resistance mechanism; fem-1 homolog B (Fem1B); glioma-associated oncogene homolog 1 (Gli1); microRNAs; oxaliplatin.

Grants and funding

R35 GM148350/GM/NIGMS NIH HHS/United States