Extrinsic stabilization of antiviral ACE2-Fc fusion proteins targeting SARS-CoV-2.

Commun Biol

Center for Functional Protein Assemblies (CPA) and School of Natural Sciences, Department of Bioscience, Technical University of Munich, 85748, Garching, Germany.

Published: April 2023

AI Article Synopsis

  • The research focuses on ACE2, a viral receptor that allows sarbecoviruses to infect cells, highlighting its importance in viral studies.
  • The study examines the structural stability of fusion proteins made up of ACE2 domains and immunoglobulin Fc, finding that the ACE2 component is less stable than the Fc part and that their movements are interconnected.
  • Chemical compounds like DX600 and MLN4760 can enhance the thermal stability of the ACE2 receptor, suggesting a method to improve the effectiveness of antiviral therapies by stabilizing these vulnerable receptor sections.

Article Abstract

The angiotensin-converting enzyme 2 (ACE2) is a viral receptor used by sarbecoviruses to infect cells. Fusion proteins comprising extracellular ACE2 domains and the Fc part of immunoglobulins exhibit high virus neutralization efficiency, but the structure and stability of these molecules are poorly understood. We show that although the hinge between the ACE2 and the IgG4-Fc is highly flexible, the conformational dynamics of the two ACE2 domains is restricted by their association. Interestingly, the conformational stability of the ACE2 moiety is much lower than that of the Fc part. We found that chemical compounds binding to ACE2, such as DX600 and MLN4760, can be used to strongly increase the thermal stability of the ACE2 by different mechanisms. Together, our findings reveal a general concept for stabilizing the labile receptor segments of therapeutic antiviral fusion proteins by chemical compounds.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10082628PMC
http://dx.doi.org/10.1038/s42003-023-04762-wDOI Listing

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