MPI8 通过双重和选择性抑制 SARS-CoV-2 主要蛋白酶和宿主组织蛋白酶 L 对 SARS-CoV-2 有效。
MPI8 is Potent against SARS-CoV-2 by Inhibiting Dually and Selectively the SARS-CoV-2 Main Protease and the Host Cathepsin L.
机构信息
Texas A&M Drug Discovery Laboratory, Department of Chemistry, Texas A&M University, College Station, TX 77843, USA.
Institute of Biosciences and Technology and Department of Translational Medical Sciences, College of Medicine, Texas A&M University, Houston, TX 77030, USA.
出版信息
ChemMedChem. 2022 Jan 5;17(1):e202100456. doi: 10.1002/cmdc.202100456. Epub 2021 Jul 29.
A number of inhibitors have been developed for the SARS-CoV-2 main protease (M ) as potential COVID-19 medications but little is known about their selectivity. Using enzymatic assays, we characterized inhibition of TMPRSS2, furin, and cathepsins B/K/L by more than a dozen of previously developed M inhibitors including MPI1-9, GC376, 11a, 10-1, 10-2, and 10-3. MPI1-9, GC376 and 11a all contain an aldehyde for the formation of a reversible covalent hemiacetal adduct with the M active site cysteine and 10-1, 10-2 and 10-3 contain a labile ester to exchange with the M active site cysteine for the formation of a thioester. Our data revealed that all these inhibitors are inert toward TMPRSS2 and furin. Diaryl esters also showed low inhibition of cathepsins. However, all aldehyde inhibitors displayed high potency in inhibiting three cathepsins. Their determined IC values vary from 4.1 to 380 nM for cathepsin B, 0.079 to 2.3 nM for cathepsin L, and 0.35 to 180 nM for cathepsin K. All aldehyde inhibitors showed similar inhibition levels toward cathepsin L. A cellular analysis indicated high potency of MPI5 and MPI8 in inhibiting lysosomal activity, which is probably attributed to their inhibition of cathepsins. Among all aldehyde inhibitors, MPI8 shows the best selectivity toward cathepsin L. With respect to cathepsins B and K, the selective indices are 192 and 150, respectively. MPI8 is the most potent compound among all aldehyde inhibitors in cellular M inhibition potency and anti-SARS-CoV-2 activity in Vero E6 cells. Cathepsin L has been demonstrated to play a critical role in the SARS-CoV-2 cell entry. By selectively inhibiting both SARS-CoV-2 M and the host cathepsin L, MPI8 potentiates dual inhibition effects to synergize its overall antiviral potency and efficacy. Due to its high selectivity toward cathepsin L that reduces potential toxicity toward host cells and high cellular and antiviral potency, we urge serious consideration of MPI8 for preclinical and clinical investigations for treating COVID-19.
已经开发出许多针对 SARS-CoV-2 主要蛋白酶(M)的抑制剂作为潜在的 COVID-19 药物,但它们对其选择性知之甚少。我们使用酶促测定法,对 TMPRSS2、furin 和组织蛋白酶 B/K/L 的抑制作用进行了表征,这些抑制剂包括之前开发的十几个 M 抑制剂,包括 MPI1-9、GC376、11a、10-1、10-2 和 10-3。MPI1-9、GC376 和 11a 都含有醛基,可与 M 活性位点半胱氨酸形成可逆的半缩醛加合物,而 10-1、10-2 和 10-3 则含有不稳定的酯基,可与 M 活性位点半胱氨酸交换形成硫酯。我们的数据表明,所有这些抑制剂对 TMPRSS2 和 furin 均无活性。二芳基酯对组织蛋白酶也表现出低抑制作用。然而,所有醛基抑制剂对三种组织蛋白酶均显示出高抑制活性。它们的测定 IC 值分别为:对组织蛋白酶 B 为 4.1-380 nM,对组织蛋白酶 L 为 0.079-2.3 nM,对组织蛋白酶 K 为 0.35-180 nM。所有醛基抑制剂对组织蛋白酶 L 的抑制水平相似。细胞分析表明 MPI5 和 MPI8 具有抑制溶酶体活性的高活性,这可能归因于它们对组织蛋白酶的抑制作用。在所有醛基抑制剂中,MPI8 对组织蛋白酶 L 的选择性最好。对于组织蛋白酶 B 和 K,选择性指数分别为 192 和 150。在细胞 M 抑制活性和 Vero E6 细胞中抗 SARS-CoV-2 活性方面,MPI8 是所有醛基抑制剂中最有效的化合物。已经证明组织蛋白酶 L 在 SARS-CoV-2 细胞进入中起关键作用。通过选择性抑制 SARS-CoV-2 M 和宿主组织蛋白酶 L,MPI8 增强了双重抑制作用,从而协同提高其整体抗病毒效力和功效。由于其对组织蛋白酶 L 的高选择性,减少了对宿主细胞的潜在毒性,以及高细胞和抗病毒效力,我们强烈敦促考虑将 MPI8 用于 COVID-19 的临床前和临床研究。
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