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Targeting endothelial metabolism for anti-angiogenesis therapy: A pharmacological perspective

机译:针对抗血管生成治疗的内皮代谢:药理学观点

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Abstract Current anti-angiogenic therapies in malignant and ocular diseases target growth factor signaling in order to attenuate excessive vascular growth. Although initial responses are promising, overall therapeutic success is limited due to insufficient efficiency, tumor refractoriness and resistance. Emerging evidence suggests that diverse growth factor signaling pathways in endothelial cells (ECs) converge onto cellular metabolism, creating an attractive target for novel alternative anti-angiogenic therapies. Recent studies show that ECs rely on glycolysis for ATP and biomass synthesis, necessary for proliferation and migration, key processes of angiogenesis. In addition, fatty acid β-oxidation (FAO) is essential for de novo nucleotide synthesis during EC proliferation. Initial proof-of-evidence has been given that administration of pharmacological inhibitors of those metabolic pathways can be used to inhibit pathological angiogenesis in vivo . Deciphering the role of other metabolic pathways and exploring the therapeutic potential of blocking these pathways await further investigation.
机译:摘要目前恶性和眼部疾病靶向生长因子信号传导的抗血管生成疗法,以衰减过度血管生长。虽然初始反应是有希望的,但由于效率不足,肿瘤耐火性和抗性,总体治疗成功受到限制。新兴的证据表明,内皮细胞(ECS)中的多种生长因子信号传导途径会聚到细胞代谢上,为新的替代抗血管生成疗法产生有吸引力的靶标。最近的研究表明,ECS依赖于ATP和生物质合成的糖酵解,增殖和迁移所必需的,血管生成的关键过程。此外,脂肪酸β-氧化(粮农组织)对于EC增殖期间的Novo核苷酸合成是必不可少的。已经初步证据证明,这些代谢途径的药理抑制剂的给药可用于抑制体内病理血管生成。解密其他代谢途径的作用,并探索阻止这些途径的治疗潜力等待进一步调查。

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