AI Article Synopsis

  • The many-banded krait's venom is connected to important animal neurotoxins, but its detailed genetic information hasn't been clear until now.
  • Scientists created a high-quality genome of the krait, discovering how its venom genes evolved and diversified over time.
  • The study helps us understand how snake venom works better, which could help in making antivenoms and developing new medicines.

Article Abstract

The many-banded krait, , has been recorded as the animal resource of JinQianBaiHuaShe in the . Characterization of its venoms classified chief phyla of modern animal neurotoxins. However, the evolutionary origin and diversification of its neurotoxins as well as biosynthesis of its active compounds remain largely unknown due to the lack of its high-quality genome. Here, we present the 1.58 Gbp genome of assembled into 18 chromosomes with contig/scaffold N50 of 7.53 Mbp/149.8 Mbp. Major bungarotoxin-coding genes were clustered within genome by family and found to be associated with ancient local duplications. The truncation of glycosylphosphatidylinositol anchor in the 3'-terminal of a LY6E paralog released modern three-finger toxins (3FTxs) from membrane tethering before the Colubroidea divergence. Subsequent expansion and mutations diversified and recruited these 3FTxs. After the cobra/krait divergence, the modern unit-B of -bungarotoxin emerged with an extra cysteine residue. A subsequent point substitution in unit-A enabled the -bungarotoxin covalent linkage. The gene expression, chromatin topological organization, and histone modification characteristics were featured by transcriptome, proteome, chromatin conformation capture sequencing, and ChIP-seq. The results highlighted that venom production was under a sophisticated regulation. Our findings provide new insights into snake neurotoxin research, meanwhile will facilitate antivenom development, toxin-driven drug discovery and the quality control of JinQianBaiHuaShe.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10213816PMC
http://dx.doi.org/10.1016/j.apsb.2022.11.015DOI Listing

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