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Targeting hypoxia and angiogenesis through HIF-1alpha inhibition.

机译:通过抑制HIF-1alpha来靶向缺氧和血管生成。

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摘要

Hypoxia is an important phenomenon in the tumor microenvironment. Hypoxic tumors are more aggressive and resistant to anti-neoplastic treatments. HIF-1alpha plays a major role in the response of tumors to hypoxia, and it is mainly responsible for the "angiogenic switch". HIF-1alpha contributes to tumor aggressiveness, invasiveness, and resistance to radiotherapy and chemotherapy. Targeting HIF-1alpha is an attractive strategy, with the potential for disrupting multiple pathways crucial for tumor growth. We review recent findings on the potential efficacy of small molecules to downregulate HIF-1alpha. These promising drugs inhibit HIF-1alpha synthesis or transcriptional activity by blocking a variety of steps in several different signaling pathways. Blocking HIF-1alpha activity should not only downregulate tumor angiogenesis, but also interfere with glycolytic metabolism and tumor cell growth. This strategy could also improve the efficiency of established tumor therapies.
机译:缺氧是肿瘤微环境中的重要现象。缺氧肿瘤更具侵略性,并且对抗肿瘤治疗具有抵抗力。 HIF-1α在肿瘤对缺氧的反应中起主要作用,并且其主要负责“血管生成转换”。 HIF-1alpha有助于肿瘤的侵袭性,侵袭性以及对放射疗法和化学疗法的抵抗力。靶向HIF-1alpha是一种有吸引力的策略,具有破坏对肿瘤生长至关重要的多种途径的潜力。我们回顾了有关小分子下调HIF-1alpha的潜在功效的最新发现。这些有前途的药物通过阻断几种不同信号途径中的多个步骤来抑制HIF-1alpha合成或转录活性。阻断HIF-1alpha活性不仅应下调肿瘤血管生成,还应干扰糖酵解代谢和肿瘤细胞的生长。该策略还可以提高已建立的肿瘤治疗的效率。

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