Cardiac-targeted delivery of a novel Drp1 inhibitor for acute cardioprotection

Jarmon G. Lees , David W. Greening , David A. Rudd , Jonathon Cross , Ayeshah A. Rosdah , Xiangfeng Lai , Tsung Wu Lin , Ren Jie Phang , Anne M. Kong , Yali Deng , Simon Crawford , Jessica K. Holien , Derek J. Hausenloy , Hsin-Hui Shen , Shiang Y. Lim
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Abstract

Dynamin-related protein 1 (Drp1) is a mitochondrial fission protein and a viable target for cardioprotection against myocardial ischaemia-reperfusion injury. Here, we reported a novel Drp1 inhibitor (DRP1i1), delivered using a cardiac-targeted nanoparticle drug delivery system, as a more effective approach for achieving acute cardioprotection. DRP1i1 was encapsulated in cubosome nanoparticles with conjugated cardiac-homing peptides (NanoDRP1i1) and the encapsulation efficiency was 99.3 ± 0.1 %. In vivo, following acute myocardial ischaemia-reperfusion injury in mice, NanoDRP1i1 significantly reduced infarct size and serine-616 phosphorylation of Drp1, and restored cardiomyocyte mitochondrial size to that of sham group. Imaging by mass spectrometry revealed higher accumulation of DRP1i1 in the heart tissue when delivered as NanoDRP1i1. In human cardiac organoids subjected to simulated ischaemia-reperfusion injury, treatment with NanoDRP1i1 at reperfusion significantly reduced cardiac cell death, contractile dysfunction, and mitochondrial superoxide levels. Following NanoDRP1i1 treatment, cardiac organoid proteomics further confirmed reprogramming of contractile dysfunction markers and enrichment of the mitochondrial protein network, cytoskeletal and metabolic regulation networks when compared to the simulated injury group. These proteins included known cardioprotective regulators identified in human organoids and in vivo murine studies following ischaemia-reperfusion injury. DRP1i1 is a promising tool compound to study Drp1-mediated mitochondrial fission and exhibits promising therapeutic potential for acute cardioprotection, especially when delivered using the cardiac-targeted cubosome nanoparticles.

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以心脏为靶向输送新型 Drp1 抑制剂,实现急性心肌保护
Dynamin相关蛋白1(Drp1)是一种线粒体裂变蛋白,也是心肌缺血再灌注损伤心脏保护的可行靶点。在此,我们报道了一种新型 Drp1 抑制剂(DRP1i1),它采用心脏靶向纳米颗粒给药系统,是实现急性心脏保护的更有效方法。DRP1i1被封装在带有共轭心脏归位肽的立方体纳米颗粒(NanoDRP1i1)中,封装效率为99.3 ± 0.1 %。在体内,小鼠急性心肌缺血再灌注损伤后,NanoDRP1i1 可显著缩小梗死面积,降低 Drp1 的丝氨酸-616 磷酸化,并使心肌细胞线粒体大小恢复到假组的水平。质谱成像显示,以 NanoDRP1i1 形式输送时,DRP1i1 在心脏组织中的累积量更高。在模拟缺血再灌注损伤的人体心脏器官组织中,再灌注时使用 NanoDRP1i1 能显著减少心脏细胞死亡、收缩功能障碍和线粒体超氧化物水平。经 NanoDRP1i1 处理后,心脏类器官蛋白质组学进一步证实,与模拟损伤组相比,收缩功能障碍标志物重新编程,线粒体蛋白网络、细胞骨架和代谢调节网络更加丰富。这些蛋白质包括在人体器官组织和缺血再灌注损伤后的活体小鼠研究中发现的已知心脏保护调节因子。DRP1i1是研究Drp1介导的线粒体分裂的一种很有前途的工具化合物,在急性心脏保护方面具有很好的治疗潜力,尤其是在使用心脏靶向立方体纳米颗粒递送时。
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Journal of molecular and cellular cardiology plus
Journal of molecular and cellular cardiology plus Cardiology and Cardiovascular Medicine
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