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Targeting MIF in Cancer: Therapeutic Strategies, Current Developments, and Future Opportunities

机译:针对癌症中的MIF:治疗策略,当前进展和未来机会

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摘要

Strong evidence has been presented linking chronic inflammation to the onset and pathogenesis of cancer. The multifunctional pro-inflammatory protein macrophage migration inhibitory factor (MIF) occupies a central role in the inflammatory pathway and has been implicated in the tumorigenesis, angiogenesis, and metastasis of many cancer phenotypes. This review highlights the current state of the art, which presents MIF, and the second member of the MIF structural superfamily, d-DT (MIF2), as significant mediators in the inflammatory-cancer axis. Although the mechanism by which MIF asserts its biological activity has yet to be fully understood, it has become clear in recent years that for certain phenotypes of cancer, MIF represents a valid therapeutic target. Current research efforts have focused on small molecule approaches that target MIF's unique tautomerase active site and neutralization of MIF with anti-MIF antibodies. These approaches have yielded promising results in a number of preclinical murine cancer models and have helped to increase our understanding of MIF biological activity. More recently, MIF's involvement in a number of key protein-protein interactions, such as with CD74 and HSP90, has been highlighted and provides a novel platform for the development of anti-MIF chemotherapeutic strategies in the future.
机译:已经提出了强有力的证据,将慢性炎症与癌症的发作和发病机理联系起来。多功能促炎蛋白巨噬细胞迁移抑制因子(MIF)在炎症途径中起着核心作用,并与许多癌症表型的肿瘤发生,血管生成和转移有关。这篇综述重点介绍了MIF和MIF结构超家族d-DT(MIF2)的第二个成员,它们是炎性肿瘤轴上的重要介体。尽管MIF声称其生物学活性的机制尚未完全了解,但近年来已变得明确,对于某些癌症表型,MIF代表有效的治疗靶点。当前的研究工作集中在针对MIF独特互变异构酶活性位点和用抗MIF抗体中和MIF的小分子方法上。这些方法已在许多临床前鼠癌模型中产生了令人鼓舞的结果,并有助于增进我们对MIF生物活性的了解。最近,MIF参与了许多关键的蛋白质-蛋白质相互作用,例如与CD74和HSP90的相互作用,这一点已得到强调,并为将来开发抗MIF化疗策略提供了一个新颖的平台。

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