靶向Hedgehog通路治疗胰腺癌的药物。

Savita Bisht, Peter Brossart, Anirban Maitra, Georg Feldmann
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引用次数: 0

摘要

最近的证据表明,刺猬信号通路的异常再激活有助于各种人类恶性肿瘤的发生和进展,包括胰腺癌;因此,刺猬通路已成为一个有希望的新治疗靶点。利用小分子抑制剂环巴胺(cycloparamine)对Hedgehog通路Smoothened (SMO)组分进行的初步转化研究表明,药物阻断异常Hedgehog信号传导具有抑制肿瘤发生、进展和转移扩散的潜力。在各种胰腺癌和其他恶性肿瘤的临床前模型中使用不同的化合物证实了这一概念;其中一些研究表明,Hedgehog抑制剂可能与已建立的抗肿瘤药物具有治疗协同作用。这篇综述提供了一个简明的翻译研究的概述,评估使用Hedgehog抑制剂作为癌症,特别是胰腺癌的新治疗策略。
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Agents targeting the Hedgehog pathway for pancreatic cancer treatment.

Recent evidence has demonstrated that aberrant reactivation of the Hedgehog signaling pathway contributes to tumor initiation and progression in various human malignancies, including pancreatic cancer; therefore, the Hedgehog pathway has emerged as a promising novel therapeutic target. Initial translational studies conducted using cyclopamine, a small-molecule inhibitor of the Smoothened (SMO) component of the Hedgehog pathway, demonstrated that pharmacological blockade of aberrant Hedgehog signaling has the potential to inhibit tumor initiation, progression and metastatic spread. This concept has been corroborated using different compounds in various preclinical models of pancreatic cancer and other malignancies; several of these studies suggest possible therapeutic synergisms of Hedgehog inhibitors with established antineoplastic agents. This review provides a concise overview of translational studies assessing the use of Hedgehog inhibitors as novel therapeutic strategy for cancer, particularly pancreatic cancer.

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