Inhibition of Ire1 Rnase Activity Modulates Tumor Cell Progression and Enhances the Response to Chemotherapy in Colorectal Cancer

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Inhibition of Ire1 Rnase Activity Modulates Tumor Cell Progression and Enhances the Response to Chemotherapy in Colorectal Cancer Publisher Pubmed

Abbasi S¹ ; Rivand H^{1, 4} ; Eshaghi F¹ ; Moosavi MA² ; Amanpour S¹ ; Mcdermott MF³ ; Rahmati M¹

Source: Medical Oncology Published:2023

Abstract

Drug resistance is one of the clinical challenges that limits the effectiveness of chemotherapy. Recent reports suggest that the unfolded protein response (UPR) and endoplasmic reticulum stress-adaptation signalling pathway, along with increased activation of its inositol-requiring enzyme 1α (IRE1α) arm, may be contributors to the pathogenesis of colorectal cancer (CRC). Here, we aimed to target the IRE1α/XBP1 pathway in order to sensitise CRC cells to the effects of chemotherapy. The CT26 colorectal cell line was treated with tunicamycin, and then was exposed to different concentrations of 5-fluorouracil (5-FU), either alone and/or in combination with the IRE1α inhibitor, 4µ8C. An MTT assay, flow cytometry and RT-PCR were performed to determine cell growth, apoptosis and IRE1α activity, respectively. In vivo BALB/c syngeneic colorectal mice received chemotherapeutic drugs. Treatment responses, tumour sizes and cytotoxicity were assessed via a range of pathological tests. 4µ8C was found to inhibit the growth of CRC, at a concentration of 10 µg/ml, without detectable cytotoxic effects and also significantly enhanced the cytotoxic potential of 5-FU, in CRC cells. In vivo experiments revealed that 4µ8C, at a concentration of 50 µM/kg prevented tumour growth without any cytotoxic or metastatic effects. Interestingly, the combination of 4µ8C with 5-FU remarkably enhanced drug responses, up to 40–60% and also lead to significantly greater inhibition of tumour growth, in comparison to monotherapy, in CRC mice. Targeting the IRE1α/XBP1 axis of the UPR could enhance the effectiveness of chemotherapy in both in vitro and in vivo models of CRC. © 2023, The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.

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Style	Citing Format
MLA	Abbasi S, et al.. "Inhibition of Ire1 Rnase Activity Modulates Tumor Cell Progression and Enhances the Response to Chemotherapy in Colorectal Cancer." Medical Oncology, vol. 40, no. 9, 2023, pp. -.
APA	Abbasi S, Rivand H, Eshaghi F, Moosavi MA, Amanpour S, Mcdermott MF, Rahmati M (2023). Inhibition of Ire1 Rnase Activity Modulates Tumor Cell Progression and Enhances the Response to Chemotherapy in Colorectal Cancer. Medical Oncology, 40(9), -.
Chicago	Abbasi S, Rivand H, Eshaghi F, Moosavi MA, Amanpour S, Mcdermott MF, Rahmati M. "Inhibition of Ire1 Rnase Activity Modulates Tumor Cell Progression and Enhances the Response to Chemotherapy in Colorectal Cancer." Medical Oncology 40, no. 9 (2023): -.
Harvard	Abbasi S et al. (2023) 'Inhibition of Ire1 Rnase Activity Modulates Tumor Cell Progression and Enhances the Response to Chemotherapy in Colorectal Cancer', Medical Oncology, 40(9), pp. -.
Vancouver	Abbasi S, Rivand H, Eshaghi F, Moosavi MA, Amanpour S, Mcdermott MF, et al.. Inhibition of Ire1 Rnase Activity Modulates Tumor Cell Progression and Enhances the Response to Chemotherapy in Colorectal Cancer. Medical Oncology. 2023;40(9):-.
BibTex	@article{ author = {Abbasi S and Rivand H and Eshaghi F and Moosavi MA and Amanpour S and Mcdermott MF and Rahmati M}, title = {Inhibition of Ire1 Rnase Activity Modulates Tumor Cell Progression and Enhances the Response to Chemotherapy in Colorectal Cancer}, journal = {Medical Oncology}, volume = {40}, number = {9}, pages = {-}, year = {2023} }
RIS	TY - JOUR AU - Abbasi S AU - Rivand H AU - Eshaghi F AU - Moosavi MA AU - Amanpour S AU - Mcdermott MF AU - Rahmati M TI - Inhibition of Ire1 Rnase Activity Modulates Tumor Cell Progression and Enhances the Response to Chemotherapy in Colorectal Cancer JO - Medical Oncology VL - 40 IS - 9 SP - EP - PY - 2023 ER -

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