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沙利度胺类似物的生物学:癌症治疗中的免疫、分子和表观遗传靶点。

Thalidomide-analogue biology: immunological, molecular and epigenetic targets in cancer therapy.

机构信息

Gene Regulation Laboratory, Cancer Therapeutics Program, Peter MacCallum Cancer Centre, Locked Bag 1, A'Beckett St, Melbourne, Victoria, Australia.

出版信息

Oncogene. 2013 Sep 5;32(36):4191-202. doi: 10.1038/onc.2012.599. Epub 2013 Jan 14.

DOI:10.1038/onc.2012.599
PMID:23318436
Abstract

Thalidomide and its analogues (lenalidomide and pomalidomide) are small molecule glutamic acid derivatives of the immunomodulatory drug (IMiD) class. In addition to the immuno-adjuvant and anti-inflammatory properties that define an IMiD, the thalidomide analogues demonstrate an overlapping and diverse range of biological activities, including anti-angiogenic, teratogenic and epigenetic effects. Importantly, the IMiDs possess anti-cancer activity with selectivity for molecularly defined subgroups of hematological malignancies, specifically mature B-cell neoplasms and myelodysplasia with deletion of chromosome 5q. Emerging insight into the pathophysiological drivers of these IMiD-responsive disease states can now be synthesized using previously disclosed IMiD activities and recently discovered thalidomide targets to build unifying models of IMiD mechanism of action. Attention to mechanisms of IMiD-induced clinical toxicities, in particular the recently identified association of lenalidomide with second primary malignancies, provides an additional tool for determination of drug mechanism. This review seeks to define the molecular IMiD targets and biological outputs that underpin their anti-neoplastic activity. It is anticipated that elucidation of important IMiD targets will allow the rational development of new-generation therapeutics with the potential to separate thalidomide-analogue efficacy from clinical toxicity.

摘要

沙利度胺及其类似物(来那度胺和泊马度胺)是免疫调节药物(IMiD)类别的小分子谷氨酸衍生物。除了定义 IMiD 的免疫佐剂和抗炎特性外,沙利度胺类似物还表现出重叠且多样化的生物活性,包括抗血管生成、致畸和表观遗传效应。重要的是,IMiD 具有抗癌活性,对特定的血液恶性肿瘤分子定义亚群具有选择性,特别是成熟 B 细胞肿瘤和 5q 染色体缺失的骨髓增生异常。现在可以使用先前公开的 IMiD 活性和最近发现的沙利度胺靶标来综合这些对 IMiD 有反应的疾病状态的病理生理驱动因素的新知识,以构建统一的 IMiD 作用机制模型。对 IMiD 诱导的临床毒性机制的关注,特别是最近发现的来那度胺与第二原发恶性肿瘤的关联,为确定药物机制提供了另一种工具。本综述旨在确定支持其抗肿瘤活性的分子 IMiD 靶标和生物学产物。阐明重要的 IMiD 靶标有望促进新一代治疗药物的合理开发,从而有可能将沙利度胺类似物的疗效与临床毒性分开。

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