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Therapeutic Potential of Autophagy Modulation in Cholangiocarcinoma

机译:自噬调节在胆管癌中的治疗潜力。

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摘要

Autophagy is a multistep catabolic process through which misfolded, aggregated or mutated proteins and damaged organelles are internalized in membrane vesicles called autophagosomes and ultimately fused to lysosomes for degradation of sequestered components. The multistep nature of the process offers multiple regulation points prone to be deregulated and cause different human diseases but also offers multiple targetable points for designing therapeutic strategies. Cancer cells have evolved to use autophagy as an adaptive mechanism to survive under extremely stressful conditions within the tumor microenvironment, but also to increase invasiveness and resistance to anticancer drugs such as chemotherapy. This review collects clinical evidence of autophagy deregulation during cholangiocarcinogenesis together with preclinical reports evaluating compounds that modulate autophagy to induce cholangiocarcinoma (CCA) cell death. Altogether, experimental data suggest an impairment of autophagy during initial steps of CCA development and increased expression of autophagy markers on established tumors and in invasive phenotypes. Preclinical efficacy of autophagy modulators promoting CCA cell death, reducing invasiveness capacity and resensitizing CCA cells to chemotherapy open novel therapeutic avenues to design more specific and efficient strategies to treat this aggressive cancer.
机译:自噬是一个多步骤的分解代谢过程,通过该过程,错误折叠,聚集或突变的蛋白质和受损的细胞器被内化在称为自噬小体的膜囊泡中,并最终融合到溶酶体中以降解被隔离的成分。该过程的多步骤性质提供了易于被放松调节并引起不同人类疾病的多个调节点,但也为设计治疗策略提供了多个目标点。癌细胞已经进化为使用自噬作为一种适应性机制,可以在肿瘤微环境中的极度压力条件下生存,而且还可以提高其侵袭性和对诸如化疗等抗癌药物的抵抗力。这篇综述收集了胆管癌发生过程中自噬失调的临床证据,以及评估可调节自噬诱导胆管癌(CCA)细胞死亡的化合物的临床前报道。总之,实验数据表明,在CCA发育的初始阶段,自噬会受到损害,在已建立的肿瘤和侵袭性表型中,自噬标记物的表达会增加。自噬调节剂促进CCA细胞死亡,降低侵袭能力并使CCA细胞对化学疗法再敏感的临床前功效开辟了新的治疗途径,以设计更特异性和有效的策略来治疗这种侵袭性癌症。

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