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Drug resistance in pancreatic cancer: Impact of altered energy metabolism

机译:胰腺癌中的耐药性:改变能量新陈代谢的影响

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摘要

Pancreatic cancer is a highly deadly disease: almost all patients develop metastases and conventional treatments have little impact on survival. Therapeutically, this tumor is poorly responsive, largely due to drug resistance. Accumulating evidence suggest that this chemoresistance is intimately linked to specific metabolic aberrations of pancreatic cancer cells, notably an increased use of glucose and the amino acid glutamine fueling anabolic processes. Altered metabolism contributes also to modulation of apoptosis, angiogenesis and drug targets, conferring a resistant phenotype. As a modality to overcome chemoresistance, a variety of experimental compounds inhibiting key metabolic pathways emerged as a promising approach to potentiate the standard treatments for pancreatic cancer in preclinical studies. These results warrant confirmation in clinical trials. Thus, this review summarizes the impact of metabolic aberrations from the perspective of drug resistance and discusses possible novel applications of metabolic inhibition for the development of more effective drugs against pancreatic cancer. (C) 2017 Elsevier B.V. All rights reserved.
机译:胰腺癌是一种高度致命的疾病:几乎所有患者发育转移和常规治疗对存活都没有影响。治疗上,这种肿瘤的响应性差,主要是由于耐药性。累积证据表明,这种化学抑制性与胰腺癌细胞的特定代谢像差密切相关,特别是葡萄糖和氨基酸谷氨酰胺的使用增加了合成原则。改变的新陈代谢也有助于调节凋亡,血管生成和药物靶标,赋予耐药表型。作为克服化学渗透度的模态,各种实验化合物抑制关键代谢途径作为一种有希望在临床前研究中提高胰腺癌标准治疗的方法。这些结果在临床试验中保证确认。因此,本综述总结了代谢像差从耐药性的影响,并讨论了代谢抑制的新型应用对胰腺癌更有效的药物的发展。 (c)2017 Elsevier B.v.保留所有权利。

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