Structures of SALSA/DMBT1 SRCR domains reveal the conserved ligand-binding mechanism of the ancient SRCR fold



Reichhardt MP, Loimaranta V, Lea SM, Johnson S

PublisherLIFE SCIENCE ALLIANCE LLC

2020

Life Science Alliance

LIFE SCIENCE ALLIANCE

LIFE SCI ALLIANCE

ARTN e201900502

3

4

10

2575-1077

DOIhttps://doi.org/10.26508/lsa.201900502

https://research.utu.fi/converis/portal/detail/Publication/47792660


The scavenger receptor cysteine-rich (SRCR) family of proteins comprises more than 20 membrane-associated and secreted molecules. Characterised by the presence of one or more copies of the similar to 110 amino-acid SRCR domain, this class of proteins have widespread functions as antimicrobial molecules, scavenger receptors, and signalling receptors. Despite the high level of structural conservation of SRCR domains, no unifying mechanism for ligand interaction has been described. The SRCR protein SALSA, also known as DMBT1/gp340, is a key player in mucosal immunology. Based on detailed structural data of SALSA SRCR domains 1 and 8, we here reveal a novel universal ligand-binding mechanism for SALSA ligands. The binding interface incorporates a dual cation-binding site, which is highly conserved across the SRCR superfamily. Along with the well-described cation dependency on most SRCR domain-ligand interactions, our data suggest that the binding mechanism described for the SALSA SRCR domains is applicable to all SRCR domains. We thus propose to have identified in SALSA a conserved functional mechanism for the SRCR class of proteins.

Last updated on 2024-26-11 at 14:58