Identifying the Mutational Profile of ABCB5 Upregulation in Colorectal Cancer: A Comprehensive Database Analysis

R. Sexton, K. Danasekaran, H. Khan, H. Uddin, M. N. Al-Hallak, Y. Landesman, T. Kashyap, Yiwei Li, A. Aboukameel, A. Azmi
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Abstract

Colorectal cancer (CRC) is a leading cause of cancer related deaths worldwide and the third leading cause of cancer related deaths in the United States with a 5-year survival rate of 63%. Depending on the stage of disease, there are differing rates of overall survival: Stage I (90%) vs. Stage IV (14%). There is a clear discrepancy between early and late stage disease due to a variety of factors including acquired genetic and tumor mutations and lack of initial symptoms leading to late stage detection. It is clear that further understanding into the mechanisms of CRC need to be explored in depth to improve overall survival rates. ATP binding cassette subfamily B member 5 (ABCB5) has been found to be pathogenic in a variety of diseases including melanoma and colorectal cancer but there has been few studies looking at the cellular consequences of ABCB5 upregulation in CRC cells. Using publicly accessible databases, we explored ABCB5 positivity in CRC cells and found novel interactions with 64 differentially expressed genes involved in cellular processes like modulation of inflammation, (XCL1, TNFSF4), enhanced cell signaling via interaction with serine protease inhibitors (SERPINB4, WFDC6) and downregulation of anti-apoptotic proteins (SPIN2A). Although ABCB5 upregulation is not currently targetable with pre-clinical compounds, our analysis revealed the genetic effects induced by ABCB5 upregulation are targetable, including evidence of sensitivity to the XPO1 inhibitor XPOVIO (selinexor). It is clear further pre-clinical investigation is needed to validate these findings.
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确定结直肠癌中ABCB5上调的突变谱:一个全面的数据库分析
结直肠癌(CRC)是全球癌症相关死亡的主要原因,也是美国癌症相关死亡的第三大原因,5年生存率为63%。根据疾病的分期,有不同的总生存率:I期(90%)和IV期(14%)。由于各种因素,包括获得性遗传和肿瘤突变,以及缺乏初始症状导致晚期发现,早期和晚期疾病之间存在明显差异。显然,进一步了解结直肠癌的机制需要深入探索,以提高总体生存率。ATP结合盒亚家族B成员5 (ABCB5)已被发现在包括黑色素瘤和结直肠癌在内的多种疾病中具有致病性,但很少有研究关注ABCB5上调在结直肠癌细胞中的细胞后果。利用可公开访问的数据库,我们探索了CRC细胞中的ABCB5阳性,并发现了与64种差异表达基因的新相互作用,这些基因参与细胞过程,如炎症调节(XCL1, TNFSF4),通过与丝氨酸蛋白酶抑制剂(SERPINB4, WFDC6)的相互作用增强细胞信号传导,以及抗凋亡蛋白(SPIN2A)的下调。虽然ABCB5上调目前还不能被临床前化合物靶向,但我们的分析显示,ABCB5上调诱导的遗传效应是可靶向的,包括对XPO1抑制剂XPOVIO (selinexor)的敏感性证据。显然,需要进一步的临床前研究来验证这些发现。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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