Dennis C. George , Fred E. Bertrand , George Sigounas
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引用次数: 0
摘要
结肠癌是导致癌症死亡的第二大原因。据预测,结肠癌新增病例超过 15.3 万例,是第三大最常诊断出的癌症。早期发现可导致治愈性手术干预,但复发和晚期转移性疾病通常采用基于 DNA 损伤诱导的化疗方案。了解结肠肿瘤细胞内 DNA 损伤修复的调控机制对于制定有效的治疗策略至关重要。众所周知,Notch 信号通路参与结肠的正常发育,我们最近描述了一种通路,通过这种通路,Notch-1、Notch-3 和 Smad 可调控结肠肿瘤细胞的 EMT 和干样特性,从而促进肿瘤发生。人们对 Notch 如何调控耐药性知之甚少。在这项研究中,我们使用 shRNA 生成了 Notch-3 表达缺失的结肠肿瘤细胞。这些细胞表现出碱基切除修复蛋白 PARP1 和 APE1 的表达减少,同时对 ara-c 和顺铂的敏感性增加。这些数据表明,Notch-3 信号通路可以调节结肠肿瘤细胞内的 DNA 修复,并表明以 Notch-3 为靶点可能是使结肠肿瘤对化疗药物敏感的有效方法。
Notch-3 affects chemoresistance in colorectal cancer via DNA base excision repair enzymes
Colon cancer is the second leading cause of cancer death. With over 153,000 new CRC cases predicted, it is the third most commonly diagnosed cancer. Early detection can lead to curative surgical intervention, but recurrent and late metastatic disease is frequently treated with chemotherapeutic options based on induction of DNA damage. Understanding mechanism(s) that regulate DNA damage repair within colon tumor cells is essential to developing effective therapeutic strategies. The Notch signaling pathway is known to participate in normal colon development and we have recently described a pathway by which Notch-1, Notch-3 and Smad may regulated EMT and stem-like properties in colon tumor cells, promoting tumorigenesis. Little is known about how Notch may regulate drug resistance. In this study, we used shRNA to generate colon tumor cells with loss of Notch-3 expression. These cells exhibited reduced expression of the base-excision repair proteins PARP1 and APE1, along with increased sensitivity to ara-c and cisplatin. These data point to a pathway in which Notch-3 signaling can regulate DNA repair within colon tumor cells and suggests that targeting Notch-3 may be an effective approach to rendering colon tumors sensitive to chemotherapeutic drugs.