Inhibition of IRE1 RNase activity modulates tumor cell progression and enhances the response to chemotherapy in colorectal cancer

被引:1
|
作者
Abbasi, Sana [1 ]
Rivand, Helia [1 ,4 ]
Eshaghi, Fatemeh [1 ]
Moosavi, Mohammad Amin [2 ]
Amanpour, Saeid [1 ]
Mcdermott, Michael F. [3 ]
Rahmati, Marveh [1 ]
机构
[1] Univ Tehran Med Sci, Canc Inst, Canc Biol Res Ctr, Tehran, Iran
[2] Natl Inst Genet Engn & Biotechnol NIGEB, Inst Med Biotechnol IMB, Dept Mol Med, POB 14965-161, Tehran, Iran
[3] Univ Leeds, Leeds Inst Rheumat & Musculoskeletal Med LIRMM, Leeds, England
[4] Tarbiat Modares Univ, Fac Biol Sci, Dept Biochem, Tehran, Iran
关键词
4 & mu; 8C; Colorectal Cancer; IRE1 & alpha; XBP1s; UPR; ENDOPLASMIC-RETICULUM STRESS; UNFOLDED PROTEIN RESPONSE; MESSENGER-RNA; 5-FLUOROURACIL;
D O I
10.1007/s12032-023-02105-7
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
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 1a (IRE1a) arm, may be contributors to the pathogenesis of colorectal cancer (CRC). Here, we aimed to target the IRE1a/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 IRE1a inhibitor, 4 mu 8C. An MTT assay, flow cytometry and RT-PCR were performed to determine cell growth, apoptosis and IRE1a 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. 4 mu 8C was found to inhibit the growth of CRC, at a concentration of 10 mu g/ml, without detectable cytotoxic effects and also significantly enhanced the cytotoxic potential of 5-FU, in CRC cells. In vivo experiments revealed that 4 mu 8C, at a concentration of 50 mu M/kg prevented tumour growth without any cytotoxic or metastatic effects. Interestingly, the combination of 4 mu 8C 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 IRE1a/XBP1 axis of the UPR could enhance the effectiveness of chemotherapy in both in vitro and in vivo models of CRC.
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页数:11
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