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一种合理设计的双金属铂(II)-二茂铁抗肿瘤剂诱导非凋亡性细胞死亡并发挥体内疗效。

A Rationally Designed Bimetallic Platinum (II)-Ferrocene Antitumor Agent Induces Non-Apoptotic Cell Death and Exerts in Vivo Efficacy.

机构信息

Medicinal Chemistry and Cell Biology Laboratory, Department of Chemical Sciences, Tata Institute of Fundamental Research, Homi Bhabha Road, Mumbai, Maharashtra, 400005, India.

Molecular Physiology Laboratory, Department of Biological Sciences, Tata Institute of Fundamental Research, Homi Bhabha Road, Mumbai, Maharashtra, 400005, India.

出版信息

Chemistry. 2022 Aug 16;28(46):e202201259. doi: 10.1002/chem.202201259. Epub 2022 Jun 30.

Abstract

Despite phenomenal clinical success, the efficacy of platinum anticancer drugs is often compromised due to inherent and acquired drug resistant phenotypes in cancers. To circumvent this issue, we designed two heterobimetallic platinum (II)-ferrocene hybrids that display multi-pronged anticancer action. In cancer cells, our best compound, 2, platinates DNA, produces reactive oxygen species, and has nucleus, mitochondria, and endoplasmic reticulum as potential targets. The multi-modal mechanism of action of these hybrid agents lead to non-apoptotic cell death induction which enables circumventing apoptosis resistance and significant improvement in platinum cross resistance profile. Finally, in addition to describing detail mechanistic insights, we also assessed its stability in plasma and demonstrate anticancer efficacy in an in vivo A2780 xenograft model. Strikingly, compared to oxaliplatin, our compound displays better tolerability, safety profile and efficacy in vivo.

摘要

尽管临床效果显著,但由于癌症中固有的和获得性的耐药表型,铂类抗癌药物的疗效往往受到影响。为了解决这个问题,我们设计了两种异双金属铂(II)-二茂铁配合物,它们具有多方面的抗癌作用。在癌细胞中,我们最好的化合物 2 可以使 DNA铂化,产生活性氧,并将细胞核、线粒体和内质网作为潜在的靶标。这些混合药物的多模式作用机制导致非凋亡性细胞死亡的诱导,从而能够规避凋亡抵抗,并显著改善铂类交叉耐药谱。最后,除了描述详细的机制见解外,我们还评估了其在血浆中的稳定性,并在体内 A2780 异种移植模型中证明了其抗癌功效。值得注意的是,与奥沙利铂相比,我们的化合物在体内显示出更好的耐受性、安全性和疗效。

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