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Elucidating the Substrate Envelope of Enterovirus 68-3C Protease: Structural Basis of Specificity and Potential Resistance

Viruses. 2025-10; 
Vincent N. Azzolino; Ala M. Shaqra; Akbar Ali; Nese Kurt Yilmaz; Celia A. Schiffer
Products/Services Used Details Operation
Peptide Synthesis crystallization. 2.2. Protein Crystallization Purified EV68-3C protease, in the inactive form (C147A), and lyophilized substrate peptides purchased from GenScript (Piscataway, NJ, USA) for Biomedical Research were utilized in protein crystallization. Apo crystals of EV68-3C C147A and co-crystals of EV68-3C C147A Get A Quote

摘要

Enterovirus-D68 (EV68) has emerged as a global health concern over the last decade with severe symptomatic infections resulting in long-lasting neurological deficits and death. Unfortunately, there are currently no FDA-approved antiviral drugs for EV68 or any other non-polio enterovirus. One particularly attractive class of potential drugs are small molecules inhibitors, which can target the conserved active site of EV68-3C protease. For other viral proteases, we have demonstrated that the emergence of drug resistance can be minimized by designing inhibitors that leverage the evolutionary constraints of substrate specificity. However, the structural characterization of EV68-3C protease bound to its substrates h... More

关键词

enterovirus, EV68, substrate recognition, protease, drug resistance, protein structure, molecular modeling