JCI Insight (Jul 2021)

A KCNK16 mutation causing TALK-1 gain of function is associated with maturity-onset diabetes of the young

  • Sarah M. Graff,
  • Stephanie R. Johnson,
  • Paul J. Leo,
  • Prasanna K. Dadi,
  • Matthew T. Dickerson,
  • Arya Y. Nakhe,
  • Aideen M. McInerney-Leo,
  • Mhairi Marshall,
  • Karolina E. Zaborska,
  • Charles M. Schaub,
  • Matthew A. Brown,
  • David A. Jacobson,
  • Emma L. Duncan

Journal volume & issue
Vol. 6, no. 13

Abstract

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Maturity-onset diabetes of the young (MODY) is a heterogeneous group of monogenic disorders of impaired pancreatic β cell function. The mechanisms underlying MODY include β cell KATP channel dysfunction (e.g., KCNJ11 [MODY13] or ABCC8 [MODY12] mutations); however, no other β cell channelopathies have been associated with MODY to date. Here, we have identified a nonsynonymous coding variant in KCNK16 (NM_001135105: c.341T>C, p.Leu114Pro) segregating with MODY. KCNK16 is the most abundant and β cell–restricted K+ channel transcript, encoding the two-pore-domain K+ channel TALK-1. Whole-cell K+ currents demonstrated a large gain of function with TALK-1 Leu114Pro compared with TALK-1 WT, due to greater single-channel activity. Glucose-stimulated membrane potential depolarization and Ca2+ influx were inhibited in mouse islets expressing TALK-1 Leu114Pro with less endoplasmic reticulum Ca2+ storage. TALK-1 Leu114Pro significantly blunted glucose-stimulated insulin secretion compared with TALK-1 WT in mouse and human islets. These data suggest that KCNK16 is a previously unreported gene for MODY.

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