小檗碱(一种用于治疗癌症和减轻体重的药物)对心脏和骨骼肌的脱靶效应分析

Jushuo Wang, Yingli Fan, Syamalima Dube, Patricia Benz, Dipak Dube, Jean M Sanger, Joseph W Sanger
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摘要

我们实验室以前的报告描述了在培养的胚胎心肌细胞和骨骼肌细胞中肌原纤维的形成过程,报告提出肌原纤维的形成过程分为三个步骤,蛋白质组织不断增加:首先是前肌原纤维,然后是新生肌原纤维,最后是成熟肌原纤维。泛素蛋白酶体系统(UPS)抑制剂可阻止培养的心肌细胞和骨骼肌细胞中的新生肌原纤维直接发展为成熟肌原纤维,从而支持三步组装模型,即新生肌原纤维中的部分蛋白质被蛋白水解,从而组装成成熟肌原纤维。在培养的肌肉细胞中应用 UPS 抑制剂可以解释用于癌症患者的 UPS 药物对心脏和骨骼肌产生的脱靶不良反应。小檗碱是一种植物衍生物,已被用于治疗多种癌症,包括多发性骨髓瘤。与使用 UPS 药物不同的是,有报告称小檗碱在多发性骨髓瘤患者身上取得了成功,而且对他们的心脏没有产生脱靶效应。小檗碱是 UHRF1(具有 PHD 和 RING 手指结构域的类泛素)的连接酶抑制剂。小檗碱抑制了胚胎骨骼肌细胞新生肌原纤维阶段的肌原纤维组装,但对胚胎心脏细胞成熟肌原纤维的组装没有影响。RT-PCR 实验表明,小檗碱能抑制骨骼肌细胞中肌肉肌球蛋白 II 重链的 mRNA,但不能抑制肌肉肌动蛋白 mRNA。小檗碱还被用作一种流行的减肥复方制剂,因为它比含塞马鲁肽的减肥药(Wegovy 和 Ozempic)便宜得多,而且无需处方即可买到。与小檗碱相反,在心肌细胞和骨骼肌细胞的培养试验中,塞马鲁肽对肌原纤维的组装没有影响。我们推测,对培养的胚胎心肌细胞和骨骼肌细胞进行分析将为新型抗癌药物的临床前试验提供一种方法,从而改善患者的治疗效果,这是癌症治疗的一个重要目标。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Analyses of Off-Target Effects on Cardiac and Skeletal Muscles by Berberine, a Drug Used to Treat Cancers and Induce Weight Loss.

Previous reports from our laboratory describing the formation of myofibrils in cultured embryonic cardiac and skeletal muscle cells have proposed that myofibrillogenesis occurs in three steps of increasing protein organization: beginning with premyofibrils, followed by nascent myofibrils, and ending in mature myofibrils. Inhibitors of the ubiquitin proteasome system (UPS) prevented nascent myofibrils from progressing directly to mature myofibrils in cultured cardiac and skeletal muscle cells, supporting a three-step model of assembly in which some of the proteins in nascent myofibrils are proteolyzed to allow the assembly of mature myofibrils. Application of UPS inhibitors on cultured muscle cells suggests possible explanations for the off-target cardiac and skeletal muscle adverse effects of UPS drugs, which are used on cancer patients. Berberine, a plant derivative, has been used to treat various cancers, including multiple myelomas. In contrast to the use of UPS drugs, success was reported with Berberine in multiple myeloma patients with no off-target effects on their hearts. We have exposed cultured cardiac and skeletal muscle cells to Berberine, a ligase inhibitor of UHRF1 (ubiquitin-like with PHD and RING finger domains). Berberine inhibited myofibril assembly at the nascent myofibril stage in embryonic skeletal muscle cells but had no effect in the assembly of mature myofibrils in embryonic heart cells. RT-PCR experiments demonstrated Berberine inhibition of mRNA for muscle myosin II heavy chains but not for muscle actin mRNA in skeletal muscle cells. Berberine is also being used as a popular weight losing compound, because it is much cheaper and available without a prescription than the semaglutide containing weight losing drugs (Wegovy and Ozempic). In contrast to Berberine, semaglutide had no effects on myofibril assembly in culture assays for both cardiac and skeletal muscle cells. We postulate that analyses of cultured embryonic cardiac and skeletal muscle cells will provide a preclinical assay for the testing of novel cancer drugs with improved outcomes for patients, an important goal for cancer therapeutics.

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