Carrimycin, a first in-class anti-cancer agent, targets selenoprotein H to induce nucleolar oxidative stress and inhibit ribosome biogenesis

LaYow C. Yu, Danielle D. Dang, Sophie Zhuang, Shuran Chen, Zhengping Zhuang, Jared S. Rosenblum
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引用次数: 1

Abstract

Carrimycin is a synthetic macrolide antibiotic that has been shown to have anti-cancer activity; however, its exact mechanism of action and molecular target were previously unknown. It was recently elucidated that Isovalerylspiramycin I (ISP I), the active component of carrimycin, targets selenoprotein H (SelH), a nucleolar reactive oxygen species-scavenging enzyme in the selenoprotein family. ISP I treatment accelerates SelH degradation, resulting in oxidative stress, disrupted ribosomal biogenesis, and apoptosis in tumor cells. Specifically, ISP I disrupts the association between RNA polymerase I and ribosomal DNA in the nucleolus. This inhibits ribosomal RNA transcription and subsequent ribosomal assembly, which prevents cancer cells from sustaining elevated rates of protein synthesis and cellular proliferation that are necessary for tumor growth and malignancy. In this review, we (1) describe the historical categorization and evolution of anti-cancer agents, including macrolide antibiotics, (2) outline the discovery of SelH as a target of ISP I, and (3) summarize the ways in which carrimycin has been used both clinically and at the bench to date and propose additional potential therapeutic uses.

Abstract Image

卡霉素是第一类抗癌剂,靶向硒蛋白H,诱导核仁氧化应激并抑制核糖体生物发生。
卡霉素是一种合成的大环内酯类抗生素,已被证明具有抗癌活性;然而,它的确切作用机制和分子靶点以前是未知的。最近有人阐明,卡霉素的活性成分异戊酰螺旋霉素I(ISP I)靶向硒蛋白H(SelH),硒蛋白H是硒蛋白家族中的一种核仁活性氧清除酶。ISP I治疗加速了SelH的降解,导致氧化应激、核糖体生物发生中断和肿瘤细胞凋亡。具体来说,ISP I破坏了RNA聚合酶I和核仁中核糖体DNA之间的联系。这抑制了核糖体RNA转录和随后的核糖体组装,从而阻止癌症细胞维持肿瘤生长和恶性肿瘤所必需的蛋白质合成和细胞增殖的提高速率。在这篇综述中,我们(1)描述了抗癌药物的历史分类和演变,包括大环内酯类抗生素,(2)概述了SelH作为ISP I靶点的发现,(3)总结了迄今为止卡霉素在临床和临床上的使用方式,并提出了其他潜在的治疗用途。
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来源期刊
Cancer pathogenesis and therapy
Cancer pathogenesis and therapy Surgery, Radiology and Imaging, Cancer Research, Oncology
CiteScore
0.80
自引率
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审稿时长
54 days
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