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羧酸封端的 Ru265 类似物是 MCU 抑制剂前药。

Carboxylate-Capped Analogues of Ru265 Are MCU Inhibitor Prodrugs.

机构信息

Department of Chemistry and Chemical Biology, Cornell University, Ithaca, New York 14853, United States.

Robert F. Smith School of Engineering, Cornell University, Ithaca, New York 14853, United States.

出版信息

Inorg Chem. 2022 Oct 31;61(43):17299-17312. doi: 10.1021/acs.inorgchem.2c02930. Epub 2022 Oct 19.

Abstract

The mitochondrial calcium uniporter (MCU) is a transmembrane protein that resides on the inner membrane of the mitochondria and mediates calcium uptake into this organelle. Given the critical role of mitochondrial calcium trafficking in cellular function, inhibitors of this channel have arisen as tools for studying the biological relevance of this process and as potential therapeutic agents. In this study, four new analogues of the previously reported Ru-based MCU inhibitor [ClRu(NH)(μ-N)Ru(NH)Cl]Cl (Ru265) are reported. These compounds, which bear axial carboxylate ligands, are of the general formula [(RCO)Ru(NH)(μ-N)Ru(NH)(OCR)]X, where X = NO or CFSO and R = H (), CH (), CHCH (), and (CH)CH (). These complexes were fully characterized by IR spectroscopy, NMR spectroscopy, and elemental analysis. X-ray crystal structures of and were obtained, revealing the expected presence of both the linear Ru(μ-N)Ru core and axial formate and propionate ligands. The axial carboxylate ligands of complexes - are displaced by water in buffered aqueous solution to give the aquated compound Ru265'. The kinetics of these processes were measured by H NMR spectroscopy, revealing half-lives that span 5.9-9.9 h at 37 °C. Complex with axial formate ligands underwent aquation approximately twice as fast as the other compounds. In vitro cytotoxicity and mitochondrial membrane potential measurements carried out in HeLa and HEK293T cells demonstrated that none of these four complexes negatively affects cell viability or mitochondrial function. The abilities of - to inhibit mitochondrial calcium uptake in permeabilized HEK293T cells were assessed and compared to that of Ru265. Fresh solutions of - are approximately 2-fold less potent than Ru265 with IC values in the range of 14.7-19.1 nM. Preincubating - in aqueous buffers for longer time periods to allow for the aquation reactions to proceed increases their potency of mitochondrial uptake inhibition to match that of Ru265. This result indicates that - are aquation-activated prodrugs of Ru265'. Finally, - were shown to inhibit mitochondrial calcium uptake in intact, nonpermeabilized cells, revealing their value as tools and potential therapeutic agents for mitochondrial calcium-related disorders.

摘要

线粒体钙单向转运蛋白(MCU)是一种跨膜蛋白,位于线粒体的内膜上,介导钙离子进入细胞器。鉴于线粒体钙转运在细胞功能中的关键作用,该通道的抑制剂已成为研究这一过程生物学相关性的工具,并可能成为潜在的治疗药物。在这项研究中,报道了先前报道的基于 Ru 的 MCU 抑制剂 [ClRu(NH)(μ-N)Ru(NH)Cl]Cl(Ru265)的四个新类似物。这些化合物带有轴向羧酸配体,通式为 [(RCO)Ru(NH)(μ-N)Ru(NH)(OCR)]X,其中 X = NO 或 CFSO 和 R = H (), CH (), CHCH (), 和 (CH)CH (). 通过红外光谱、NMR 光谱和元素分析对这些化合物进行了全面表征。获得了 和 的 X 射线晶体结构,揭示了预期的线性 Ru(μ-N)Ru 核和轴向甲酸盐和丙酸盐配体的存在。在缓冲水溶液中,- 的轴向羧酸配体被水取代,得到水合化合物 Ru265'。通过 1H NMR 光谱测量这些过程的动力学,发现在 37°C 时半衰期为 5.9-9.9 h。带有轴向甲酸盐配体的复合物 水合速度大约是其他化合物的两倍。在 HeLa 和 HEK293T 细胞中进行的体外细胞毒性和线粒体膜电位测量表明,这四种化合物均不会对细胞活力或线粒体功能产生负面影响。评估了 - 抑制透化 HEK293T 细胞中线粒体钙离子摄取的能力,并与 Ru265 进行了比较。- 的新鲜溶液的 IC 值在 14.7-19.1 nM 范围内,其抑制线粒体钙离子摄取的效力约为 Ru265 的 2 倍。将 - 在水性缓冲液中预孵育更长时间以允许进行水合反应,可提高其对线粒体摄取抑制的效力,使其与 Ru265 相匹配。这一结果表明,- 是 Ru265'的水合激活前药。最后,- 被证明可以抑制完整的、未透化的细胞中线粒体钙离子摄取,揭示了它们作为线粒体钙相关疾病的工具和潜在治疗药物的价值。

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