Mithramycin and its analogs: Molecular features and antitumor action

IF 12 1区 医学 Q1 PHARMACOLOGY & PHARMACY
José Portugal
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引用次数: 0

Abstract

The antitumor antibiotic mithramycin A (MTA) binds to G/C-rich DNA sequences in the presence of dications. MTA inhibits transcription regulated by the Sp1 transcription factor, often enhanced during tumor development. It shows antitumor activity, but its clinical use was discontinued due to toxic side effects. However, recent observations have led to its use being reconsidered. The MTA biosynthetic pathways have been modified to produce mithramycin analogs (mithralogs) that encompass lower toxicity and improved pharmacological activity. Some mithralogs reduce gene expression in human ovarian and prostate tumors, among other types of cancer. They down-regulate gene expression in various cellular processes, including Sp1-responsive genes that control tumor development. Moreover, MTA and several mithralogs, such as EC-8042 (DIG-MSK) and EC-8105, effectively treat Ewing sarcoma by inhibiting transcription controlled by the oncogenic EWS-FLI1 transcription factor.

米曲霉毒素及其类似物:分子特征和抗肿瘤作用
抗肿瘤抗生素米曲霉素 A(MTA)能在双阳离子存在的情况下与富含 G/C 的 DNA 序列结合。MTA 可抑制受 Sp1 转录因子调控的转录,而 Sp1 转录因子在肿瘤发展过程中往往会增强。它具有抗肿瘤活性,但由于其毒副作用而停止了临床应用。不过,最近的观察结果促使人们重新考虑其使用。人们对 MTA 的生物合成途径进行了改造,生产出了毒性更低、药理活性更强的米曲霉素类似物(mithralogs)。一些米曲霉素类似物可降低人类卵巢和前列腺肿瘤以及其他类型癌症的基因表达。它们能下调各种细胞过程中的基因表达,包括控制肿瘤发生的 Sp1 反应基因。此外,MTA 和几种 mithralogs,如 EC-8042 (DIG-MSK) 和 EC-8105,通过抑制由致癌 EWS-FLI1 转录因子控制的转录,有效治疗尤文肉瘤。
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来源期刊
CiteScore
23.00
自引率
0.70%
发文量
222
审稿时长
90 days
期刊介绍: Pharmacology & Therapeutics, in its 20th year, delivers lucid, critical, and authoritative reviews on current pharmacological topics.Articles, commissioned by the editor, follow specific author instructions.This journal maintains its scientific excellence and ranks among the top 10 most cited journals in pharmacology.
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