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Resistance of <i>Argopecten purpuratus</i> scallop larvae to vibriosis is associated with the front-loading of immune genes and enhanced antimicrobial response
Indexado
WoS WOS:000950459700001
Scopus SCOPUS_ID:85150458823
DOI 10.3389/FIMMU.2023.1150280
Año 2023
Tipo artículo de investigación

Citas Totales

Autores Afiliación Chile

Instituciones Chile

% Participación
Internacional

Autores
Afiliación Extranjera

Instituciones
Extranjeras


Abstract



Mass mortality events caused by vibriosis have emerged in hatchery-reared scallop larvae from Chile, threatening scallop aquaculture. In an attempt to mitigate this emerging infectious disease and provide candidates for marker-assisted selective breeding, we tested here the existence of a genetic component of Argopecten purpuratus scallop resistance to the pathogen Vibrio bivalvicida. Through a dual RNA-seq approach we analyzed the basal transcriptome and the transcriptional response to infection in two resistant and two susceptible families as well as the pathogen transcriptomic response to host colonization. The results highlighted a genetic basis in the resistance of scallop larvae to the pathogen. The Vibrio response was characterized by a general metabolic adaptation to the host environment, along with several predicted virulence factors overexpressed in infected scallop larvae with no difference between resistant and susceptible host phenotypes. On the host side, several biological processes were enriched in uninfected resistant larvae. Within these enriched categories, immune-related processes were overexpressed, while morphogenesis, biomineral tissue development, and angiogenesis were under expressed. Particularly, genes involved in immune recognition and antimicrobial response, such as lipopolysaccharide-binding proteins (LBPs), lysozyme, and bactericidal permeability-increasing protein (BPI) were overexpressed in uninfected resistant larvae. As expected, immune-related biological processes were enriched in Vibrio-infected larvae, but they were more numerous in resistant larvae. Overexpressed immune genes in response to infection included several Toll-like receptors, TNF and NF-κB immune signaling genes, and the antimicrobial peptide Big defensin ApBD1. Results strongly suggest that both a front-loading of immune genes and an enhanced antimicrobial response to infection contribute to the resistance, while pathogen infective strategy does not discriminate between host phenotypes. Overall, early expression of host immune genes appears as a strong determinant of the disease outcome that could be used in marker-assisted selective breeding.

Revista



Revista ISSN
Frontiers In Immunology 1664-3224

Métricas Externas



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Disciplinas de Investigación



WOS
Immunology
Scopus
Sin Disciplinas
SciELO
Sin Disciplinas

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Publicaciones WoS (Ediciones: ISSHP, ISTP, AHCI, SSCI, SCI), Scopus, SciELO Chile.

Colaboración Institucional



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Autores - Afiliación



Ord. Autor Género Institución - País
1 JERIA-CASTRO, EDUARDO Hombre Pontificia Universidad Católica de Valparaíso - Chile
2 Oyanedel, D. Hombre Pontificia Universidad Católica de Valparaíso - Chile
3 ROJAS-CARRASCO, RODRIGO ALEJANDRO Hombre Universidad Católica del Norte - Chile
4 Farlora, R. Hombre Universidad de Valparaíso - Chile
5 Lira, German Hombre Universidad Católica del Norte - Chile
6 Mercado, Ana - Universidad Católica del Norte - Chile
7 Muñoz, Katherine Mujer Pontificia Universidad Católica de Valparaíso - Chile
8 Destoumieux-Garzon, Delphine Mujer Université de Montpellier - Francia
Univ Montpellier - Francia
9 BROKORDT-GUZMAN, KATHERINA BERNARDINE Mujer Universidad Católica del Norte - Chile
10 SCHMITT-RIVERA, PAULINA Mujer Pontificia Universidad Católica de Valparaíso - Chile

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Financiamiento



Fuente
FONDECYT
Fondo Nacional de Desarrollo Científico y Tecnológico
Chilean National Fund for Scientific and Technological Development
Chilean National Fund for Scientific and Technological Development, FONDECYT
Beca Doctorado ANID

Muestra la fuente de financiamiento declarada en la publicación.

Agradecimientos



Agradecimiento
This study was supported by the Chilean National Fund for Scientific and Technological Development, FONDECYT #1200129 to PS, RR, RF, and KB. DO was supported by Postdoctorado FONDECYT #3220530. KM was supported by Beca Doctorado ANID # 21201438. Acknowledgments
This study was supported by the Chilean National Fund for Scientific and Technological Development, FONDECYT #1200129 to PS, RR, RF, and KB. DO was supported by Postdoctorado FONDECYT #3220530. KM was supported by Beca Doctorado ANID # 21201438.

Muestra la fuente de financiamiento declarada en la publicación.