Dataset: Metagenome and metatranscriptome sequences from deep-sea hydrothermal vent microbial communities

Name: Metagenome and metatranscriptome sequences from deep-sea hydrothermal vent microbial communities collected on cruises AT42-22, TN405, and NA108 from May 2019 to Jun 2022
Published: 2024-10-10
Keywords: deep-sea hydrothermal vents, metagenome, metatranscriptome, deep-sea microbial ecology, microbial interactions, biota, oceans

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Spatial Extent: N:45.9 E:-81.7 S:18.13 W:-126.7

Mid-Cayman Rise, Axial Seamount, Gorda Ridge

Temporal Extent: 2013-09 - 2022-07

Project:

Collaborative Research: Microbes need frenemies: unveiling microbial relationships with protists and viruses that support deep-sea hydrothermal vent food webs (frenemies)

Principal Investigator:

Sarah K. Hu (Woods Hole Oceanographic Institution, WHOI)

Co-Principal Investigator:

Rika Anderson (Carleton College)

Julie Huber (Woods Hole Oceanographic Institution, WHOI)

BCO-DMO Data Manager:

Audrey Mickle (Woods Hole Oceanographic Institution, WHOI BCO-DMO)

Version:

Version Date:

2024-10-10

Restricted:

Current State:

Preliminary and in progress

Metagenome and metatranscriptome sequences from deep-sea hydrothermal vent microbial communities collected on cruises AT42-22, TN405, and NA108 from May 2019 to Jun 2022

Abstract:

This dataset is a collection of sample collection metadata, sample identifier information, and NCBI accession information for samples and sequence runs produced as part of the frenemies project. This project examines trophic interactions among microbial eukaryotes, viruses, bacteria, and archaea at deep-sea hydrothermal vents using metagenomics and metatranscriptomics and characterizes these ecologically-significant interactions, such as mutualism, predator-prey, or virus-host. We sequenced samples collected during the 2020 expedition AT42-22 to the Mid-Cayman Rise hydrothermal vent fields, as well as from the 2019 expedition NA108 to the Gorda Ridge and the 2022 expedition TN405 to the Axial seamount. Sequencing targeted archaea, bacteria, and viruses with metagenomics and microbial eukaryotes with metatranscriptomics. We plan to use these data to identify ecologically-significant interactions among protists, viruses, bacteria, and archaea, with a specific emphasis on microbial mortality via viral lysis and eukaryotic grazing.

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Methods & Sampling

All samples were collected via ROVs, where an intake valve was positioned at the location of active diffuse flow (<100C) and collected into bags, bottles, or a filter directly. If collected into a bag or bottle, fluid was filtered immediately upon recovery. All filters had a pore size of 0.2µm and were composed of PES material.

Samples collected at the Mid-Cayman Rise and the Axial Seamount locations utilized the ROV Jason HOG sampler. Samples collected at the Gorda Ridge used the ROV Hercules SUPR sampler.

Metatranscriptomics

Messenger RNA (mRNA) was subset from previously extracted RNA from all sites and grazing experiments (Qiagen RNA mini kit). Then metatranscriptome libraries were prepared from the mRNA. Library was prepped with NEBNext Ultra II Directional RNA Library Prep Kit for Illumina #E7760S; with a Poly(A) mRNA magnetic isolation module first. For fragmentation, samples were incubated at 94C for 10 minutes. PCR cycles done until enough was isolated, range of 16-28. Mainly 20 or 22 cycles total. Input total RNA for metatranscriptome libraries was either 100 ng or 10 ng. However, with mRNA content ranging from 1-5% of the total RNA, the PCR amplification steps needed to be modified for the estimated input mRNA.

Libraries were sequenced with NovaSeq at the Northwest Genomics Sequence Center (Seattle, WA). Sequenced with NovaSeq S2 300 cycles. An average of 100 million sequences per sample were recovered from the metatranscriptome sequencing.

Metagenomics

Duplicate samples (other half of filter) from in situ sites at Mid-Cayman Rise were extracted for DNA (n = 12), then prepared as metagenome libraries, and sent for NovaSeq sequencing (data received January 2023). DNA extracted with MasterPure Complete DNA and RNA Purification Kit (Lucigen MC85200). Input DNA diluted to 50 ng total, or all DNA input (For low concentration samples) and sheared to target 400 bps with Covaris M220 focused-ultrasonicator, utilizing SonoLab 7.2. For 70 sections, 200 cycles (bursts) at 50 watts (Peak incident power), duty factor = 10%, and average incident power was 5 watts. Min temp: 18C, setpoint: 20C, and max: 22C.

Libraries were prepped with Ovation Ultralow System V2 (from Nugen). Library amplification was done at 15 cycles, and pooled. Sequencing was done with a NovaSeq S2 300 Cycle (UW Genomics NWGC). Over 80 million sequences per sample were recovered, to ensure sufficient sequencing depth.

BCO-DMO Processing

- Imported submitted file "bco-dmo_Frenemies.csv" into the BCO-DMO system.
- Split lat_lon field into separate fields
- Converted lon to lon W, (West is negative)
- Created YEAR field in format YYYY by pulling the year from FIELDYR
- Added a CRUISE_ID field with corresponding cruise IDs given in submission by year
- Exported dataset as 936069_v1_frenemies_accession_metadata.csv

More Information about this dataset

Funding Sources

Funding Source	Award Number
NSF Division of Ocean Sciences	OCE-2327203

Deployments

Deployment	Start Date	Platform	Investigator
AT42-22	2020-01-14	R/V Atlantis	Jeffrey S. Seewald (Chief Scientist)	data info
NA108	2019-05-24	E/V Nautilus	Darlene Lim (Co-Chief Scientist)	data info
TN405	2022-07-08	R/V Thomas G. Thompson	Julie Huber (Chief Scientist)	data info

Instruments

Automated DNA Sequencer

Supplied Name: Illumina NovaSeq 6000

Supplied Description:

Libraries were sequenced with NovaSeq at the Northwest Genomics Sequence Center (Seattle, WA).

Instrument Type

Generic Name: Automated DNA Sequencer

Acronym: Automated Sequencer

Generic Description:

General term for a laboratory instrument used for deciphering the order of bases in a strand of DNA. Sanger sequencers detect fluorescence from different dyes that are used to identify the A, C, G, and T extension reactions. Contemporary or Pyrosequencer methods are based on detecting the activity of DNA polymerase (a DNA synthesizing enzyme) with another chemoluminescent enzyme. Essentially, the method allows sequencing of a single strand of DNA by synthesizing the complementary strand along it, one base pair at a time, and detecting which base was actually added at each step.

Hydrothermal Organic Geochemistry Sampler

Supplied Name: ROV Jason, HOG sampler

Supplied Description:

Instrument Type

Generic Name: Hydrothermal Organic Geochemistry Sampler

Acronym: HOG sampler

Generic Description:

The Hydrothermal Organic Geochemistry (HOG) sampler is designed to collect large volume (2–9 L) fluid samples with minimal introduction of organic or microbial contamination, and to be powered and deployed in real time from a submersible. Additional design constraints include utilizing materials appropriate for sampling fluids with elevated temperatures, fitting the sampler into the space available on the submersible, and minimizing the time needed to remove samples and prepare the sampler for re-deployment between dives.

ultrasonic cell disrupter (sonicator)

Supplied Name: Covaris M220 focused-ultrasonicator

Supplied Description:

Input DNA diluted to 50 ng total, or all DNA input (For low concentration samples) and sheared to target 400 bps with Covaris M220 focused-ultrasonicator

Instrument Type

Generic Name: ultrasonic cell disrupter (sonicator)

Generic Description:

Instrument that applies sound energy to agitate particles in a sample.

Parameters

Date and time formats are described in python strftime() syntax.

Supplied Name	Supplied description	Supplied Units	Standard Name
SAMPLE_ID	Complete sample ID associated with fastq files	unitless	sample
SHORT_SAMPLE_ID	Short name sample identifier associated with cruise ID	unitless	sample
SAMPLE_NAME	Related sample name associated with vent site	unitless	sample
LAB_NUM	Internal number for sample inventory	unitless	sample
CRUISE_ID	Identifer of cruise during which sample was collected	unitless	cruise_id
FIELD_REGION	Region of hydrothermal vent field	unitless	site
YEAR	Year of sample collection Format: %Y	unitless	date
FIELD_YEAR	Hydrothermal vent field with year of collection	unitless	site_descrip
VENT	Name of individual vent site or sample origin	unitless	site
LAT	Latitude of site where samples were collected. Negative values indicate South.	Decimal Degrees	lat
LON	Longitude of site where samples were collected. Negative values indicate West.	Decimal Degrees	lon
ORIGIN_TYPE	Origin of the sample, either in situ or grazing experiment	unitless	sample_descrip
ORIGIN_DESCRIPTION	Collection method description	unitless	sample_descrip
FRENEMIES_PROJ	Associated project	unitless	project
LIBRARY	Type of fastq sequence file	unitless	sample_descrip
RUN	SRR number in NCBI	unitless	SRA_run
BIOSAMPLE	Biosample ID number in NCBI	unitless	BioSample
BASES	Total number of bps in giga base pairs (Gb)	Giga base pairs (Gb)	genetic_conc
BYTES	Total size of the sequence file in Gigabytes (GB)	Gigabytes	file_size
EXPERIMENT	Experiment ID for locating sequences in NCBI	unitless	SRA_experiment
LIBRARY_NAME	Sample identifer for fastq files	unitless	sample
LIBRARY_SELECTION	Amplication used in library prep	unitless	sampling_method
geo_loc_name_country	Geo location name for SRA metadata	unitless	site
geo_loc_name_country_continent	Geo location associated with continent	unitless	site
geo_loc_name	Geo location name for site of vent field	unitless	site

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Database

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Dataset: Metagenome and metatranscriptome sequences from deep-sea hydrothermal vent microbial communities