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1. Genomic signatures of disease resistance in endangered staghorn corals

   https://doi.org/10.1126/science.adi3601  

   Vollmer, Steven V; Selwyn, Jason D; Despard, Brecia A; Roesel, Charles L (September 2023, Science)

   White band disease (WBD) has caused unprecedented declines in the CaribbeanAcroporacorals, which are now listed as critically endangered species. Highly disease-resistantAcropora cervicornisgenotypes exist, but the genetic underpinnings of disease resistance are not understood. Using transmission experiments, a newly assembled genome, and whole-genome resequencing of 76A. cervicornisgenotypes from Florida and Panama, we identified 10 genomic regions and 73 single-nucleotide polymorphisms that are associated with disease resistance and that include functional protein-coding changes in four genes involved in coral immunity and pathogen detection. Polygenic scores calculated from 10 genomic loci indicate that genetic screens can detect disease resistance in wild and nursery stocks ofA. cervicornisacross the Caribbean. 

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2. Coral Venom and Toxins as Protection Against Crown‐of‐Thorns Sea Star Attack

   https://doi.org/10.1111/mec.70202  

   Gorman, Lucy M; Huffmyer, Ariana S; Byrne, Maria; Mills, Suzanne C; Putnam, Hollie M (November 2025, Molecular Ecology)

   ABSTRACT Crown‐of‐thorns sea star (CoTS) outbreaks are a main cause of hard coral cover decline across the Indo‐Pacific, posing a major threat to the resilience of coral reefs. However, the drivers underlying CoTS feeding on preferred (e.g.,Acroporaspecies) versus non‐preferred (e.g.,Poritesspecies) are poorly understood. We hypothesised that coral venom may influence CoTS prey preferences. To investigate this hypothesis, we compared the coral venom toxin families across the genomes of preferred (A. digitifera,A. hyacinthus,A. milleporaandA. tenuis) and non‐preferred (P. australiensis,P. compressa,P. luteaandP. rus) prey species of CoTS. We also included one species from each genus inhabiting the Caribbean, where CoTS are absent (A. cervicornisandP. astreoides), to broaden our identification of venom constituents shared within each genus and investigate geographic differences. We collected known cnidarian toxins, and along with the cnidarian Tox‐Prot database, used these to identify putative toxins and investigate their phylogeny. The most abundant toxins across all coral species included neurotoxins (kunitz‐type and SCRiPS) and pore‐forming toxins (actinoporins and MAC‐PFs). We found genera‐specific differences with jellyfish toxins (CFXs) only present inPoritesspecies. Similarly, onlyAcroporaspecies harboured pore‐forming toxins with the aerolysin domain. Two toxin homologues only present in Indo‐Pacific corals (CFX and MAC‐PF homologues) showed evidence of positive selection, suggesting their evolution is shaped by environmental pressures, including exposure to CoTS. These findings provide a foundation for future studies of scleractinian venoms, which have direct applications to assessing reef coral's susceptibility to future CoTS outbreaks and active reef management. 

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3. Identification of putative coral pathogens in endangered Caribbean staghorn coral using machine learning

   https://doi.org/10.1111/1462-2920.16700  

   Selwyn, Jason D; Despard, Brecia A; Vollmer, Miles V; Trytten, Emily C; Vollmer, Steven V (September 2024, Environmental Microbiology)

   Abstract Coral diseases contribute to the rapid decline in coral reefs worldwide, and yet coral bacterial pathogens have proved difficult to identify because 16S rRNA gene surveys typically identify tens to hundreds of disease‐associate bacteria as putative pathogens. An example is white band disease (WBD), which has killed up to 95% of the now‐endangered CaribbeanAcroporacorals since 1979, yet the pathogen is still unknown. The 16S rRNA gene surveys have identified hundreds of WBD‐associated bacterial amplicon sequencing variants (ASVs) from at least nine bacterial families with little consensus across studies. We conducted a multi‐year, multi‐site 16S rRNA gene sequencing comparison of 269 healthy and 143 WBD‐infectedAcropora cervicornisand used machine learning modelling to accurately predict disease outcomes and identify the top ASVs contributing to disease. Our ensemble ML models accurately predicted disease with greater than 97% accuracy and identified 19 disease‐associated ASVs and five healthy‐associated ASVs that were consistently differentially abundant across sampling periods. Using a tank‐based transmission experiment, we tested whether the 19 disease‐associated ASVs met the assumption of a pathogen and identified two pathogenic candidate ASVs—ASV25Cysteiniphilum litoraleand ASV8Vibriosp. to target for future isolation, cultivation, and confirmation of Henle‐Koch's postulate via transmission assays. 

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4. Tank-based bacterial profiling identifies basin-wide white band disease pathogen candidate and no bacterial associations with coral disease resistance

   https://doi.org/10.1093/ismeco/ycaf247  

   Trytten, Emily C; Despard, Brecia A; Selwyn, Jason D; Vollmer, Steven V (January 2025, ISME Communications)

   Abstract White band disease (WBD) has decimated the Caribbean staghorn coral, Acropora cervicornis, since its emergence in 1979, but its etiology remains unknown. Numerous WBD pathogen candidates from over nine bacterial families have been implicated, with a multi-year field study recently identifying Cysteiniphilum litorale as the likely pathogen. Here, we use 16S rRNA gene amplicon sequencing to profile changes in the bacterial communities in a tank-based transmission experiment in the Florida Keys using 50 nursery-raised staghorn coral genotypes with varying disease resistances to determine whether any bacteria in the native staghorn coral microbiomes were associated with WBD resistance and to identify bacterial amplicon sequencing variants (ASVs) associated with WBD exposure and transmission. We found no significant associations, positive or negative, between any bacterial ASV, genus, or family and disease resistance in native staghorn coral microbiomes but did identify nine bacterial ASVs strongly associated with disease outcome in the tank-based transmission experiment. ASV 65, classified as Cysteiniphilum litorale, showed strong disease associations consistent with pathogenicity, including being significantly associated with WBD transmission within disease-exposed tanks (i.e. more abundant on diseased fragments) and being significantly more abundant on the diseased experimental dose than the healthy dose. The V3-V4 16S rRNA gene sequence for ASV 65 differed by only 1 of 415 bp from the C. litorale ASV identified as the putative WBD pathogen in the recent multi-year study from Panama, suggesting a rare Caribbean-wide strain-level pathogen association. Eight additional disease-associated ASVs were identified as potential opportunistic pathogens and included ASVs from the families Vibrionaceae and Colwelliaceae. 

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5. Evolution of Plasticity in Response to Ethanol Between Recently Separated Populations of D. melanogaster With Different Ecological Histories

   https://doi.org/10.1002/ece3.72874  

   Boateng‐Sarfo, George; Scherping, Franz; Mammadov, Murad; Signor, Sarah (January 2026, Ecology and Evolution)

   ABSTRACT While there is abundant theoretical work on the evolution of phenotype plasticity, empirical support has lagged. One model for the evolution of phenotype plasticity is by genetic accommodation. Under this model of evolution, when a population encounters a new environment there are widely variable responses among different genotypes, which are then pruned by selection into a single adaptive response. Because of the requirement to replicate genotypes, testing this prediction requires inbred lines as well as populations that are both adapted and not adapted to a resource. We previously demonstrated thatD. melanogasteradapted to ethanol through genetic accommodation usingD. simulansas an ancestral proxy lineage. However, we wondered how generalizable these results were. Here, we used a new population ofD. melanogasterfrom France and an ancestral range population from Zambia and measured behavioral tolerance to ethanol exposure in multiple genotypes from each population, as well as genome‐wide gene expression and alternative splicing in response to ethanol using RNA sequencing. We found that the ZambianD. melanogasterhave lower tolerance to ethanol than the FrenchD. melanogaster, with the Zambian flies becoming sedated while the French flies remain active under the same exposure. At the transcriptional level, Zambian genotypes showed extensive genotype‐specific changes in gene expression and splicing in response to ethanol exposure, while the French genotypes showed relatively modest and fewer genotype‐specific changes, consistent with having a more uniform, population response. We also found that gene expression and splicing appear to evolve independently of one another and that the splicing response to ethanol is largely distinct between populations. Thus, we have independently replicated evidence for evolution by genetic accommodation inD. melanogaster, suggesting that the evolution of plasticity may be an important contributor to the ability to exploit novel resources. 

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