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Discovery of Selective Inhibitors for In Vitro and In Vivo Interrogation of Skeletal Myosin II

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Figshare2021-09-24 更新2026-04-28 收录
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https://figshare.com/articles/dataset/Discovery_of_Selective_Inhibitors_for_i_In_Vitro_i_and_i_In_Vivo_i_Interrogation_of_Skeletal_Myosin_II/16677432
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Myosin IIs, actin-based motors that utilize the chemical energy of adenosine 5′-triphosphate (ATP) to generate force, have potential as therapeutic targets. Their heavy chains differentiate the family into muscle (skeletal [SkMII], cardiac, smooth) and nonmuscle myosin IIs. Despite the therapeutic potential for muscle disorders, SkMII-specific inhibitors have not been reported and characterized. Here, we present the discovery, synthesis, and characterization of “skeletostatins,” novel derivatives of the pan-myosin II inhibitor blebbistatin, with selectivity 40- to 170-fold for SkMII over all other myosin II family members. In addition, the skeletostatins bear improved potency, solubility, and photostability, without cytotoxicity. Based on its optimal in vitro profile, MT-134’s in vivo tolerability, efficacy, and pharmacokinetics were determined. MT-134 was well-tolerated in mice, impaired motor performance, and had excellent exposure in muscles. Skeletostatins are useful probes for basic research and a strong starting point for drug development.
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2021-09-24
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