TALK-1 channels control β cell endoplasmic reticulum Ca2+ homeostasis.

Vierra, Nicholas C;Dadi, Prasanna K;Milian, Sarah C;Dickerson, Matthew T;Jacobson, David A;et.al.
(2017) Science Signaling — Vol. 10, p. eaan2883 (2017)

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  • Vierra, Nicholas C
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  • Dadi, Prasanna K
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  • Milian, Sarah C
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  • Dickerson, Matthew T
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  • Jacobson, David A
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Abstract
Ca2+ handling by the endoplasmic reticulum (ER) serves critical roles in controlling pancreatic β cell function and becomes perturbed during the pathogenesis of diabetes. ER Ca2+ homeostasis is determined by ion movements across the ER membrane, including K+ flux through K+ channels. We demonstrated that K+ flux through ER-localized TALK-1 channels facilitated Ca2+ release from the ER in mouse and human β cells. We found that β cells from mice lacking TALK-1 exhibited reduced basal cytosolic Ca2+ and increased ER Ca2+ concentrations, suggesting reduced ER Ca2+ leak. These changes in Ca2+ homeostasis were presumably due to TALK-1-mediated ER K+ flux, because we recorded K+ currents mediated by functional TALK-1 channels on the nuclear membrane, which is continuous with the ER. Moreover, overexpression of K+-impermeable TALK-1 channels in HEK293 cells did not reduce ER Ca2+ stores. Reduced ER Ca2+ content in β cells is associated with ER stress and islet dysfunction in diabetes, and islets from TALK-1-deficient mice fed a high-fat diet showed reduced signs of ER stress, suggesting that TALK-1 activity exacerbated ER stress. Our data establish TALK-1 channels as key regulators of β cell ER Ca2+ and suggest that TALK-1 may be a therapeutic target to reduce ER Ca2+ handling defects in β cells during the pathogenesis of diabetes.
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Vierra, N. C., Dadi, P. K., Milian, S. C., Dickerson, M. T., Jordan, K. L., Gilon, P., & Jacobson, D. A. (2017). TALK-1 channels control β cell endoplasmic reticulum Ca2+ homeostasis. Science Signaling, 10, eaan2883. https://doi.org/10.1126/scisignal.aan2883 (Original work published 2017)