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转化生长因子-β信号通路的大分子和小分子抑制剂

Large- and small-molecule inhibitors of transforming growth factor-beta signaling.

作者信息

Akhurst Rosemary J

机构信息

University of California at San Francisco, P.O. Box 0875, Cancer Research Institute, 2340 Sutter Street, San Francisco, CA 94143-0875, USA.

出版信息

Curr Opin Investig Drugs. 2006 Jun;7(6):513-21.

Abstract

A variety of drugs have been developed to inhibit transforming growth factor (TGF)beta signaling. These drugs have been designed to block TGFbeta synthesis, ligand/receptor binding or receptor kinase signaling. Preclinical studies using TGFbeta inhibitors have demonstrated efficacy in reducing metastasis and have shown improvements in cytotoxic drug delivery. Results of phase I/II clinical trials of TGFbeta inhibitors in patients with glioblastoma suggest improved survival rates compared with conventional chemotherapy. The predominant cellular target, whether cancer or stromal cell, immune cell or angiogenesis, may differ between tumor types. Different individuals may show variable responses to drug therapy dependent on both germline genetic variation and the somatic mutation profile of the tumor. A deeper understanding of these issues will assist in targeting the right patients for such therapy, and in limiting unwanted side effects.

摘要

已经研发出多种药物来抑制转化生长因子(TGF)β信号传导。这些药物旨在阻断TGFβ的合成、配体/受体结合或受体激酶信号传导。使用TGFβ抑制剂的临床前研究已证明其在减少转移方面的疗效,并显示出细胞毒性药物递送方面的改善。TGFβ抑制剂在胶质母细胞瘤患者中的I/II期临床试验结果表明,与传统化疗相比,生存率有所提高。主要的细胞靶点,无论是癌细胞还是基质细胞、免疫细胞还是血管生成,可能因肿瘤类型而异。不同个体对药物治疗的反应可能不同,这取决于种系基因变异和肿瘤的体细胞突变谱。对这些问题的更深入理解将有助于针对合适的患者进行此类治疗,并限制不必要的副作用。

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