AI Article Synopsis

  • Inwardly rectifying potassium channels (Kir channels) are crucial for maintaining potassium balance and cellular functions, and mutations in these channels can lead to serious diseases.
  • Researchers, using zebrafish as a model, identified and renamed 31 Kir genes, revealing their evolutionary history and how they might have developed through duplications in chordates.
  • The study showed that these Kir genes have distinct expression patterns during early embryonic development, suggesting their roles in embryonic patterning and potential connections to congenital diseases.

Article Abstract

Background: Inwardly rectifying potassium channels are essential for normal potassium homeostasis, maintaining the cellular resting membrane potential, and regulating electrolyte transportation. Mutations in Kir channels have been known to cause debilitating diseases ranging from neurological abnormalities to renal and cardiac failures. Many efforts have been made to understand their protein structures, physiological functions, and pharmacological modifiers. However, their expression and functions during embryonic development remain largely unknown.

Results: Using zebrafish as a model, we identified and renamed 31 kir genes. We also analyzed Kir gene evolution by phylogenetic and syntenic analyses. Our data indicated that the four subtypes of the Kir genes might have already evolved out in chordates. These vertebrate Kir genes most likely resulted from both whole-genome duplications and tandem duplications. In addition, we examined zebrafish kir gene expression during early embryogenesis. Each subgroup's genes showed similar but distinct gene expression domains. The gene expression of ohnologous genes from teleost-specific whole-genome duplication indicated subfunctionalization. Varied temporal gene expression domains suggest that Kir channels may be needed for embryonic patterning or regulation.

Conclusions: Our phylogenetic and developmental analyses of Kir channels shed light on their evolutionary history and potential functions during embryogenesis related to congenital diseases and human channelopathies.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8940742PMC
http://dx.doi.org/10.1002/dvdy.425DOI Listing

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