The Role of endoplasmic reticulum metallo protease 1 on Autophagy Pathway in HCT-116 Colorectal Cancer Cell Line

Mozhdeh Zamani, S. Dastghaib, Mehran Erfani, S. Hosseini, P. Mokarram
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Abstract

BackgroundAutophagy and unfolded protein response (UPR) are mechanisms with dual roles in both maintaining the cellular homeostasis and progression of various diseases such as cancer. Therefore, identification of different molecules and proteins involved in the regulation of these pathways may contribute to find new therapeutic targets. A member of the M28 family of the metallopeptidases, Endoplasmic Reticulum Metallo Protease 1 (ERMP1), is overexpressed in cancers such as colorectal cancer. The role of this protein in the UPR activation was previously reported in breast cancer. We aimed to evaluate the role of ERMP1 in the activation of autophagy and apoptosis in colorectal cancer.MethodsERMP1 Gene silencing was performed using specific small hairpin RNA (shRNA) in HCT-116 colorectal cancer cell line. Then, autophagy associated protein markers including Beclin 1, p62 and LC3II were evaluated using western blot. The effect of ERMP1 knockdown on cellular apoptosis was also assessed by propidium iodide staining flow cytometry analysis. Statistical analysis was performed using SPSS software version 20.ResultsAll three autophagy markers were increased significantly in the ERMP1-silenced HCT116 cell lines compared with negative control cells (P 0.05).ConclusionThe oncogenic protein, ERMP1, activates autophagy in colorectal cancer cell line. Targeting of ERMP1 may be considered as a proper approach in colorectal cancer therapy. Further investigations are required to confirm these results.
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内质网金属蛋白酶1在HCT-116结直肠癌细胞自噬途径中的作用
自噬和未折叠蛋白反应(UPR)在维持细胞稳态和癌症等多种疾病的进展中具有双重作用。因此,鉴定参与这些途径调控的不同分子和蛋白质可能有助于发现新的治疗靶点。作为金属肽酶M28家族的一员,内质网金属蛋白酶1 (ERMP1)在结直肠癌等癌症中过度表达。该蛋白在UPR激活中的作用先前在乳腺癌中有报道。我们的目的是评估ERMP1在大肠癌自噬和凋亡激活中的作用。方法采用特异性小发夹RNA (shRNA)对HCT-116结直肠癌细胞株进行sermp1基因沉默。然后用western blot检测自噬相关蛋白标志物Beclin 1、p62和LC3II。用碘化丙啶染色流式细胞术分析ERMP1敲低对细胞凋亡的影响。采用SPSS软件20进行统计分析。结果ermp1沉默的HCT116细胞3种自噬标志物均较阴性对照显著升高(P < 0.05)。结论致癌蛋白ERMP1激活结直肠癌细胞自噬。以ERMP1为靶点治疗结直肠癌可能是一种合适的方法。需要进一步调查以证实这些结果。
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