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1.
Mol Ecol ; 31(3): 736-751, 2022 02.
Artigo em Inglês | MEDLINE | ID: mdl-34192383

RESUMO

Transmissible cancers are parasitic malignant cell lineages that have acquired the ability to infect new hosts from the same species, or sometimes related species. First described in dogs and Tasmanian devils, transmissible cancers were later discovered in some marine bivalves affected by a leukaemia-like disease. In Mytilus mussels, two lineages of bivalve transmissible neoplasia (BTN) have been described to date (MtrBTN1 and MtrBTN2), both of which emerged in a Mytilus trossulus founder individual. Here, we performed extensive screening of genetic chimerism, a hallmark of transmissible cancer, by genotyping 106 single nucleotide polymorphisms of 5,907 European Mytilus mussels. Genetic analysis allowed us to simultaneously obtain the genotype of hosts - Mytilus edulis, M. galloprovincialis or hybrids - and the genotype of tumours of heavily infected individuals. In addition, a subset of 222 individuals were systematically genotyped and analysed by histology to screen for possible nontransmissible cancers. We detected MtrBTN2 at low prevalence in M. edulis, and also in M. galloprovincialis and hybrids although at a much lower prevalence. No MtrBTN1 or new BTN were found, but eight individuals with nontransmissible neoplasia were observed at a single polluted site on the same sampling date. We observed a diversity of MtrBTN2 genotypes that appeared more introgressed or more ancestral than MtrBTN1 and reference healthy M. trossulus individuals. The observed polymorphism is probably due to somatic null alleles caused by structural variations or point mutations in primer-binding sites leading to enhanced detection of the host alleles. Despite low prevalence, two sublineages divergent by 10% fixed somatic null alleles and one nonsynonymous mtCOI (mitochondrial cytochrome oxidase I) substitution are cospreading in the same geographical area, suggesting a complex diversification of MtrBTN2 since its emergence and host species shift.


Assuntos
Mytilus edulis , Mytilus , Neoplasias , Animais , Cães , Europa (Continente) , Mytilus/genética , Mytilus edulis/genética , Prevalência
2.
J Invertebr Pathol ; 170: 107308, 2020 02.
Artigo em Inglês | MEDLINE | ID: mdl-31857123

RESUMO

In 2014, a high and unusual mass mortality of mussels occurred in several important production areas along the French coasts of the Atlantic and English Channel. In the first quarter of 2016, mass mortalities hit farms on the west coast of the country once again. These heterogeneous mortality events elicited a multi-parametric study conducted during the 2017 mussel season in three sites in northern Brittany (Brest, Lannion and St. Brieuc). The objective was to assess the health status of these mussels, follow mortality and attempt to identify potential causes of the abnormal high mortality of farmed mussels in northern Brittany. Brest was the most affected site with 70% cumulative mortality, then Lannion with 40% and finally St. Brieuc with a normal value of 15%. We highlighted a temporal 'mortality window' that opened throughout the spring season, and concerned the sites affected by mortality of harmful parasites (including pathogenic bacteria), neoplasia, metal contamination, and tissue alterations. Likely, the combination of all these factors leads to a weakening of mussels that can cause death.


Assuntos
Interações Hospedeiro-Patógeno , Mytilus edulis , Poluentes Químicos da Água/toxicidade , Animais , França , Longevidade , Mytilus edulis/efeitos dos fármacos , Mytilus edulis/microbiologia , Mytilus edulis/parasitologia , Mytilus edulis/virologia
3.
J Fish Dis ; 41(11): 1759-1769, 2018 Nov.
Artigo em Inglês | MEDLINE | ID: mdl-30151980

RESUMO

The acute course of disease in young oysters infected by OsHV-1 and the rapid tissue degradation often preclude histological examination of specimens collected during outbreaks in field. Herein, live spat originated from two geographical areas were sampled just at the onset of a mortality event that occurred in Normandy (France) in June 2016. The lesions, associated with high OsHV-1 DNA quantities, were characterized by severe and diffuse haemocytosis mainly involving blast-like cells, myocyte degeneration and large, irregularly shaped degenerate eosinophilic cells in the connective tissue. The herpesvirus was identified by negative staining TEM and real-time PCR. Sequencing of the C region and ORFs 42/43 confirmed that the variants met the definition of OsHV-1 µVar. We sequenced 30 other ORFs in twenty OsHV-1-positive individuals and compared them to the µVar specimens isolated between 2009 and 2011. The ORFs encoding putative membrane proteins showed the highest number of variations. Seven different genotypes were identified, confirming the presence of relevant genetic diversity. Phylogenetic analysis provided evidence for a well-separated µVar new group, with an evolutionary divergence estimated at 0.0013 from the other µVar variants. The geographical distribution of these newly described variants and their effective virulence should be investigated in future.


Assuntos
Crassostrea/virologia , Vírus de DNA/fisiologia , Animais , Vírus de DNA/classificação , Vírus de DNA/genética , DNA Viral/análise , França , Microscopia Eletrônica de Transmissão , Filogenia , Reação em Cadeia da Polimerase em Tempo Real , Análise de Sequência de DNA
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