Structural and functional characterization of NEMO cleavage by SARS-CoV-2 3CLpro

Author:

Hameedi Mikhail Ali,Prates Erica T.,Garvin Michael R.,Mathews Irimpan,Kirtley Amos B,Demerdash Omar,Bechthold Mark,Iyer Mamta,Rahighi Simin,Kneller Daniel W.,Kovalevsky AndreyORCID,Irle Stephan,Vuong Van-Quan,Mitchell Julie C.,Labbe Audrey,Galanie Stephanie,Wakatsuki Soichi,Jacobson DanielORCID

Abstract

AbstractIn addition to its essential role in viral polyprotein processing, the SARS-CoV-2 3C-like (3CLpro) protease can cleave human immune signaling proteins, like NF-κB Essential Modulator (NEMO) and deregulate the host immune response. Here, in vitro assays show that SARS-CoV-2 3CLpro cleaves NEMO with fine-tuned efficiency. Analysis of the 2.14 Å resolution crystal structure of 3CLpro C145S bound to NEMO226-235 reveals subsites that tolerate a range of viral and host substrates through main chain hydrogen bonds while also enforcing specificity using side chain hydrogen bonds and hydrophobic contacts. Machine learning- and physics-based computational methods predict that variation in key binding residues of 3CLpro- NEMO helps explain the high fitness of SARS-CoV-2 in humans. We posit that cleavage of NEMO is an important piece of information to be accounted for in the pathology of COVID-19.

Publisher

Cold Spring Harbor Laboratory

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