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Disease Associated Mutations in KIR Proteins Linked to Aberrant Inward Rectifier Channel Trafficking

  • Eva-Maria Plessl
  • , Muge Qile
  • , Meye Bloothooft
  • , Anna Weinzinger
  • , Marcel van der Heyden

    Publications: Contribution to journalReviewPeer Reviewed

    Abstract

    The ubiquitously expressed family of inward rectifier potassium (K-IR) channels, encoded by KCNJ genes, is primarily involved in cell excitability and potassium homeostasis. Channel mutations associate with a variety of severe human diseases and syndromes, affecting many organ systems including the central and peripheral neural system, heart, kidney, pancreas, and skeletal muscle. A number of mutations associate with altered ion channel expression at the plasma membrane, which might result from defective channel trafficking. Trafficking involves cellular processes that transport ion channels to and from their place of function. By alignment of all K-IR channels, and depicting the trafficking associated mutations, three mutational hotspots were identified. One localized in the transmembrane-domain 1 and immediately adjacent sequences, one was found in the G-loop and Golgi-export domain, and the third one was detected at the immunoglobulin-like domain. Surprisingly, only few mutations were observed in experimentally determined Endoplasmic Reticulum (ER)exit-, export-, or ER-retention motifs. Structural mapping of the trafficking defect causing mutations provided a 3D framework, which indicates that trafficking deficient mutations form clusters. These "mutation clusters" affect trafficking by different mechanisms, including protein stability.

    Original languageEnglish
    Article number650
    Number of pages15
    JournalBiomolecules
    Volume9
    Issue number11
    DOIs
    Publication statusPublished - Nov 2019

    UN SDGs

    This output contributes to the following UN Sustainable Development Goals (SDGs)

    1. SDG 3 - Good Health and Well-being
      SDG 3 Good Health and Well-being

    Austrian Fields of Science 2012

    • 301206 Pharmacology

    Keywords

    • ANDERSEN-TAWIL-SYNDROME
    • ATP CHANNELS
    • ER EXPORT
    • GOLGI EXPORT
    • K-IR
    • KCNJ
    • KIR2.1 CHANNEL
    • KIR4.1
    • RECTIFYING POTASSIUM CHANNEL
    • ROMK
    • SUBUNIT
    • SURFACE EXPRESSION
    • alignment
    • disease
    • inward rectifier channel
    • mutation
    • structure
    • trafficking
    • Disease
    • Trafficking
    • Inward rectifier channel
    • K
    • Alignment
    • Structure
    • Mutation

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