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Self-Masked Aldehyde Inhibitors of Human Cathepsin L Are Potent Anti-CoV-2 Agents

Front Chem. 2022-07; 
Jiyun Zhu, Linfeng Li, Aleksandra Drelich, Bala C Chenna, Drake M Mellott, Zane W Taylor, Vivian Tat, Christopher Z Garcia, Ardala Katzfuss, Chien-Te K Tseng, Thomas D Meek
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Gene Synthesis … -AMC) was purchased from EMD Millipore or GenScript. The methods for the synthesis and … K777 c NA Me-Pip An external file that holds a picture, illustration, etc. Object name is fchem… Get A Quote

摘要

Cysteine proteases comprise an important class of drug targets, especially for infectious diseases such as Chagas disease (cruzain) and COVID-19 (3CL protease, cathepsin L). Peptide aldehydes have proven to be potent inhibitors for all of these proteases. However, the intrinsic, high electrophilicity of the aldehyde group is associated with safety concerns and metabolic instability, limiting the use of aldehyde inhibitors as drugs. We have developed a novel class of compounds, self-masked aldehyde inhibitors (SMAIs) which are based on the dipeptide aldehyde inhibitor (Cbz-Phe-Phe-CHO, ), for which the P Phe group contains a 1'-hydroxy group, effectively, an -tyrosinyl aldehyde (Cbz-Phe--Tyr-CHO, ; (Li (2021) ... More

關(guān)鍵詞

COVID-19, SARS coronavirus-2, cathepsin L, cysteine proteases, reversible covalent inactivation, self-masked aldehydes
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