From shells to sequences: A proof-of-concept study for on-site analysis of hemolymphatic circulating cell-free DNA from sentinel mussels using Nanopore technology

From shells to sequences: A proof-of-concept study for on-site analysis of hemolymphatic circulating cell-free DNA from sentinel mussels using Nanopore technology

Blue mussels are often abundant and widely distributed in polar marine coastal ecosystems. Because of their wide distribution, ecological importance, and relatively stationary lifestyle, bivalves have long been considered suitable indicators of ecosystem health and changes. Monitoring the population...

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Veröffentlicht in:The Science of the total environment 2024-07, Vol.934, p.172969, Article 172969
Hauptverfasser: Ferchiou, Sophia, Caza, France, Villemur, Richard, Betoulle, Stéphane, St-Pierre, Yves
Format: Artikel
Sprache:eng
Schlagworte:
Biodiversity
biopsy
Chordata
Climate change
environment
environmental health
lifestyle
Liquid biopsy
marine ecosystems
medicine
mitochondrial DNA
mitochondrial genome
Mussels
Mytilus edulis
nanopores
population dynamics
resource management
Self/non-self DNA
species
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Zusammenfassung:Blue mussels are often abundant and widely distributed in polar marine coastal ecosystems. Because of their wide distribution, ecological importance, and relatively stationary lifestyle, bivalves have long been considered suitable indicators of ecosystem health and changes. Monitoring the population dynamics of blue mussels can provide information on the overall biodiversity, species interactions, and ecosystem functioning. In the present work, we combined the concept of liquid biopsy (LB), an emerging concept in medicine based on the sequencing of free circulating DNA, with the Oxford Nanopore Technologies (ONT) platform using a portable laboratory in a remote area. Our results demonstrate that this platform is ideally suited for sequencing hemolymphatic circulating cell-free DNA (ccfDNA) fragments found in blue mussels. The percentage of non-self ccfDNA accounted for >50 % of ccfDNA at certain sampling Sites, allowing the quick, on-site acquisition of a global view of the biodiversity of a coastal marine ecosystem. These ccfDNA fragments originated from viruses, bacteria, plants, arthropods, algae, and multiple Chordata. Aside from non-self ccfDNA, we found DNA fragments from all 14 blue mussel chromosomes, as well as those originating from the mitochondrial genomes. However, the distribution of nuclear and mitochondrial DNA was significantly different between Sites. Similarly, analyses between various sampling Sites showed that the biodiversity varied significantly within microhabitats. Our work shows that the ONT platform is well-suited for LB in sentinel blue mussels in remote and challenging conditions, enabling faster fieldwork for conservation strategies and resource management in diverse settings. [Display omitted] •Analysis of the ccfDNA of sentinel mussels from monitoring marine ecosystems.•Up to 50 % of hemolymphatic ccfDNA has a non-self origin.•Non-self ccfDNA derives from viruses, bacteria, algae, and vertebrates.•The ccfDNA from liquid biopsies is ideally suited to long-read sequencing.•The ONT platform is ideally suited for ccfDNA analysis in remote areas
ISSN:0048-9697
1879-1026
1879-1026
DOI:10.1016/j.scitotenv.2024.172969