Viruses of a key coral symbiont exhibit temperature-driven productivity across a reefscape

Author:

Howe-Kerr Lauren I1ORCID,Grupstra Carsten G B12ORCID,Rabbitt Kristen M13ORCID,Conetta Dennis1ORCID,Coy Samantha R14ORCID,Klinges J Grace5ORCID,Maher Rebecca L6ORCID,McConnell Kaitlin M7ORCID,Meiling Sonora S8ORCID,Messyasz Adriana9ORCID,Schmeltzer Emily R7ORCID,Seabrook Sarah710ORCID,Sims Jordan A111ORCID,Veglia Alex J1ORCID,Thurber Andrew R7ORCID,Thurber Rebecca L Vega7ORCID,Correa Adrienne M S1ORCID

Affiliation:

1. Department of BioSciences, Rice University , Houston, TX, USA

2. Department of Biology, Boston University , Boston, MA, USA

3. Department of Marine and Environmental Sciences, Northeastern University , Boston, MA, USA

4. Department of Oceanography, Texas A & M University , College Station, TX, USA

5. Mote Marine Laboratory, Elizabeth Moore International Center for Coral Reef Research & Restoration , Summerland Key, FL, USA

6. Institute of Ecology and Evolution, University of Oregon , Eugene, OR, USA

7. Oregon State University , Corvallis, OR, USA

8. University of the Virgin Islands , St. Thomas, US Virgin Islands, USA

9. Rutgers School of Environmental and Biological Sciences , New Brunswick, NJ, USA

10. National Institute of Water and Atmospheric Research , Wellington, New Zealand

11. Environmental Science and Policy, George Mason University , Fairfax, VA, USA

Abstract

Abstract Viruses can affect coral health by infecting their symbiotic dinoflagellate partners (Symbiodiniaceae). Yet, viral dynamics in coral colonies exposed to environmental stress have not been studied at the reef scale, particularly within individual viral lineages. We sequenced the viral major capsid protein (mcp) gene of positive-sense single-stranded RNA viruses known to infect symbiotic dinoflagellates (‘dinoRNAVs’) to analyze their dynamics in the reef-building coral, Porites lobata. We repeatedly sampled 54 colonies harboring Cladocopium C15 dinoflagellates, across three environmentally distinct reef zones (fringing reef, back reef, and forereef) around the island of Moorea, French Polynesia over a 3-year period and spanning a reef-wide thermal stress event. By the end of the sampling period, 28% (5/18) of corals in the fringing reef experienced partial mortality versus 78% (14/18) of corals in the forereef. Over 90% (50/54) of colonies had detectable dinoRNAV infections. Reef zone influenced the composition and richness of viral mcp amino acid types (‘aminotypes’), with the fringing reef containing the highest aminotype richness. The reef-wide thermal stress event significantly increased aminotype dispersion, and this pattern was strongest in the colonies that experienced partial mortality. These findings demonstrate that dinoRNAV infections respond to environmental fluctuations experienced in situ on reefs. Further, viral productivity will likely increase as ocean temperatures continue to rise, potentially impacting the foundational symbiosis underpinning coral reef ecosystems.

Funder

Lewis and Clark Grant for Exploration, Wagoner Foreign Study award, American Society for Microbiology Goldschmidt Award

National Science Foundation

Publisher

Oxford University Press (OUP)

Subject

General Medicine

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