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Autophagy in pancreatic cancer pathogenesis and treatment

机译:自噬在胰腺癌的发病机理和治疗中的作用

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Pancreatic cancer is the fourth most common cancer to cause death due to advanced stage at diagnosis and poor response to current treatment. Autophagy is the lysosome-mediated degradation pathway which plays a critical role in cellular defense, quality control, and energy metabolism. Targeting autophagy is now an exciting field for translational cancer research, as autophagy dysfunction is among the hallmarks of cancer. Pancreatic tumors have elevated autophagy under basal conditions when compared with other epithelial cancers. This review describes our current understanding of the interaction between autophagy and pancreatic cancer development, including risk factors (e.g., pancreatitis, smoking, and alcohol use), tumor microenvironment (e.g., hypoxia and stromal cells), and molecular biology (e.g., K-Ras and p53) of pancreatic cancer. The importance of the HMGB1-RAGE pathway in regulation of autophagy and pancreatic cancer is also presented. Finally, we describe current studies involving autophagy inhibition using either pharmacological inhibitors (e.g., chloroquine) or RNA interference of essential autophagy genes that regulate chemotherapy sensitivity in pancreatic cancer. Summarily, autophagy plays multiple roles in the regulation of pancreatic cancer pathogenesis and treatment, although the exact mechanisms remain unknown.
机译:胰腺癌是第四种最常见的导致死亡的癌症,这是由于诊断晚期和对当前治疗的不良反应所致。自噬是溶酶体介导的降解途径,在细胞防御,质量控制和能量代谢中起关键作用。自噬功能障碍是癌症的特征之一,靶向自噬现在是转化癌症研究的一个令人兴奋的领域。与其他上皮癌相比,胰腺肿瘤在基础条件下具有较高的自噬能力。这篇综述描述了我们目前对自噬与胰腺癌发展之间相互作用的理解,包括危险因素(例如胰腺炎,吸烟和饮酒),肿瘤微环境(例如缺氧和基质细胞)和分子生物学(例如K- Ras和p53)胰腺癌。还介绍了HMGB1-RAGE通路在调节自噬和胰腺癌中的重要性。最后,我们描述了当前涉及使用药理抑制剂(例如氯喹)或调节胰腺癌化学疗法敏感性的自噬基因的RNA干扰进行自噬抑制的研究。综上所述,自噬在胰腺癌的发病机制和治疗中起着多种作用,尽管确切的机制尚不清楚。

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