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Hedgehog Inhibition as an Anti-Cancer Strategy

机译:抑制刺猬作为一种抗癌策略

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Dysregulated Hedgehog (Hh) signaling has been implicated in a growing number of human cancers. Although first identified as an important developmental signaling pathway crucial for cellular proliferation, differentiation, and migration during organogenesis in invertebrates, these fundamental processes have been co-opted in human cancers. Initial evidence for the Hh pathway in tumor biology comes from mutations of signaling pathway components in a hereditary cancer syndrome that typically results in basal-cell carcinoma and medulloblastoma. Subsequent analysis revealed that Hh pathway mutations are found in sporadic tumors as well as activated Hh signaling in several epithelial cancers independent of Hh pathway mutation status. Further, recent evidence has demonstrated paracrine Hh signaling within stromal cells of the tumor microenvironment with implications for drug delivery. Several Hh antagonists targeting the Hh receptor, Smoothened (SMO), have been developed and show efficacy in preclinical studies and early-stage clinical trials in humans. However, major issues with these small molecule compounds include rapid acquired resistance, potential developmental toxicities secondary to use in children, and limited efficacy in cancers driven by Hh signaling downstream of the SMO receptor.
机译:刺猬(Hh)信号转导失调已涉及越来越多的人类癌症。尽管最初被确定为重要的发育信号通路,对无脊椎动物的器官发生过程中的细胞增殖,分化和迁移至关重要,但这些基本过程已在人类癌症中被采用。肿瘤生物学中Hh通路的初步证据来自遗传性癌症综合征中信号通路成分的突变,这种突变通常导致基底细胞癌和髓母细胞瘤。随后的分析表明,在散发性肿瘤中发现了Hh通路突变,并且在几种上皮癌中也发现了活化的Hh信号传导,这些信号与Hh通路的突变状态无关。此外,最近的证据表明,肿瘤微环境基质细胞内的旁分泌Hh信号与药物传递有关。已经开发了几种靶向Hh受体的平滑肌(SMO)Hh拮抗剂,它们在人类的临床前研究和早期临床试验中显示出功效。但是,这些小分子化合物的主要问题包括快速获得的抗药性,继发于儿童的潜在发育毒性以及在SMO受体下游Hh信号驱动的癌症中疗效有限。

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