Author: Toto, Angelo; Ma, Sana; Malagrinò, Francesca; Visconti, Lorenzo; Pagano, Livia; Stromgaard, Kristian; Gianni, Stefano
Title: Comparing the binding properties of peptides mimicking the Envelope protein of SARSâ€CoV and SARSâ€CoVâ€2 to the PDZ domain of the tight junctionâ€associated PALS1 protein Cord-id: vn4qa3yc Document date: 2020_8_21
ID: vn4qa3yc
Snippet: The Envelope protein (E) is one of the four structural proteins encoded by the genome of SARSâ€CoV and SARSâ€CoVâ€2 Coronaviruses. It is an integral membrane protein, highly expressed in the host cell, which is known to have an important role in Coronaviruses maturation, assembly and virulence. The E protein presents a PDZâ€binding motif at its Câ€terminus. One of the key interactors of the E protein in the intracellular environment is the PDZ containing protein PALS1. This interaction is k
Document: The Envelope protein (E) is one of the four structural proteins encoded by the genome of SARSâ€CoV and SARSâ€CoVâ€2 Coronaviruses. It is an integral membrane protein, highly expressed in the host cell, which is known to have an important role in Coronaviruses maturation, assembly and virulence. The E protein presents a PDZâ€binding motif at its Câ€terminus. One of the key interactors of the E protein in the intracellular environment is the PDZ containing protein PALS1. This interaction is known to play a key role in the SARSâ€CoV pathology and suspected to affect the integrity of the lung epithelia. In this paper we measured and compared the affinity of peptides mimicking the E protein from SARSâ€CoV and SARSâ€CoVâ€2 for the PDZ domain of PALS1, through equilibrium and kinetic binding experiments. Our results support the hypothesis that the increased virulence of SARSâ€CoVâ€2 compared to SARSâ€CoV may rely on the increased affinity of its Envelope protein for PALS1. This article is protected by copyright. All rights reserved.
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