AI Article Synopsis

  • The ShK superfamily consists of proteins featuring a conserved ShKT domain, initially found in small venom peptides from sea anemones, which inhibit specific potassium channels.
  • This superfamily includes small toxic peptides as well as larger multifunctional proteins that have various roles, including neurotoxicity and immunosuppression, making them potential treatments for autoimmune diseases.
  • Research on ShKT proteins from the Mediterranean vampire snail shows that these proteins are specifically expressed in salivary glands, suggesting their importance in venom, and they exhibit high variability due to frequent gene duplications.

Article Abstract

Proteins of the ShK superfamily are characterized by a small conserved domain (ShKT), first discovered in small venom peptides produced by sea anemones, and acting as specific inhibitors of voltage-dependent and calcium-activated K⁺ channels. The ShK superfamily includes both small toxic peptides and larger multifunctional proteins with various functions. ShK toxins are often important components of animal venoms, where they perform different biological functions including neurotoxic and immunosuppressive effects. Given their high specificity and effectiveness, they are currently regarded as promising pharmacological lead compounds for the treatment of autoimmune diseases. Here, we report on the molecular analysis of ShKT domain containing proteins produced by the Mediterranean vampire snail , an ectoparasitic gastropod that feeds on benthic fishes. The high specificity of expression of most ShK transcripts in salivary glands identifies them as relevant components of venom. These ShK proteins display various structural architectures, being produced either as single-domain secretory peptides, or as larger proteins combining the ShKT with M12 or CAP domains. Both ShKT-containing genes and their internal ShKT domains undergo frequent duplication events in , ensuring a high level of variability that is likely to play a role in increasing the range of their potential molecular targets.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6409789PMC
http://dx.doi.org/10.3390/toxins11020106DOI Listing

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