AI Article Synopsis

  • Mussels have a highly efficient innate immune system, allowing them to tolerate infections better than other marine species due to diverse antimicrobial peptides (AMPs) that vary greatly among individuals.
  • The CRP-I gene cluster in blue mussels contains about 50 genes and pseudogenes in a small region of chromosome 5 and exhibits significant gene presence/absence variation (PAV) across related species.
  • Although the synthetic CRP-I peptide sCRP-I H1 shows some biological activity, it is unlikely to function as an antimicrobial agent or protease inhibitor, but may help defend against eukaryotic parasites.

Article Abstract

Mussels ( spp.) tolerate infections much better than other species living in the same marine coastal environment thanks to a highly efficient innate immune system, which exploits a remarkable diversification of effector molecules involved in mucosal and humoral responses. Among these, antimicrobial peptides (AMPs) are subjected to massive gene presence/absence variation (PAV), endowing each individual with a potentially unique repertoire of defense molecules. The unavailability of a chromosome-scale assembly has so far prevented a comprehensive evaluation of the genomic arrangement of AMP-encoding loci, preventing an accurate ascertainment of the orthology/paralogy relationships among sequence variants. Here, we characterized the CRP-I gene cluster in the blue mussel , which includes about 50 paralogous genes and pseudogenes, mostly packed in a small genomic region within chromosome 5. We further reported the occurrence of widespread PAV within this family in the species complex and provided evidence that CRP-I peptides likely adopt a knottin fold. We functionally characterized the synthetic peptide sCRP-I H1, assessing the presence of biological activities consistent with other knottins, revealing that mussel CRP-I peptides are unlikely to act as antimicrobial agents or protease inhibitors, even though they may be used as defense molecules against infections from eukaryotic parasites.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10138031PMC
http://dx.doi.org/10.3390/genes14040787DOI Listing

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