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Diversity analysis of sea anemone peptide toxins in different tissues of Heteractis crispa based on transcriptomics
Guo, Q.; Fu, J.; Yuan, L.; Liao, Y.; Li, M.; Li, X.; Yi, B.; Zhang, J.; Gao, B. (2024). Diversity analysis of sea anemone peptide toxins in different tissues of Heteractis crispa based on transcriptomics. NPG Scientific Reports 14(1): 7684. https://dx.doi.org/10.1038/s41598-024-58402-2
In: Scientific Reports (Nature Publishing Group). Nature Publishing Group: London. ISSN 2045-2322; e-ISSN 2045-2322, more
Peer reviewed article  

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Keywords
    Radianthus crispa (Hemprich & Ehrenberg in Ehrenberg, 1834) [WoRMS]
    Marine/Coastal

Authors  Top 
  • Guo, Q.
  • Fu, J.
  • Yuan, L.
  • Liao, Y.
  • Li, M.
  • Li, X.
  • Yi, B.
  • Zhang, J.
  • Gao, B.

Abstract
    Peptide toxins found in sea anemones venom have diverse properties that make them important research subjects in the fields of pharmacology, neuroscience and biotechnology. This study used high-throughput sequencing technology to systematically analyze the venom components of the tentacles, column, and mesenterial filaments of sea anemone Heteractis crispa, revealing the diversity and complexity of sea anemone toxins in different tissues. A total of 1049 transcripts were identified and categorized into 60 families, of which 91.0% were proteins and 9.0% were peptides. Of those 1049 transcripts, 416, 291, and 307 putative proteins and peptide precursors were identified from tentacles, column, and mesenterial filaments respectively, while 428 were identified when the datasets were combined. Of these putative toxin sequences, 42 were detected in all three tissues, including 33 proteins and 9 peptides, with the majority of peptides being ShKT domain, β-defensin, and Kunitz-type. In addition, this study applied bioinformatics approaches to predict the family classification, 3D structures, and functional annotation of these representative peptides, as well as the evolutionary relationships between peptides, laying the foundation for the next step of peptide pharmacological activity research.

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