4.5 Article

Spatially Organized β-Cell Subpopulations Control Electrical Dynamics across Islets of Langerhans

Journal

BIOPHYSICAL JOURNAL
Volume 113, Issue 5, Pages 1093-1108

Publisher

CELL PRESS
DOI: 10.1016/j.bpj.2017.07.021

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Funding

  1. National Institutes of Health (NIH) [R0l DK102950, R01 DK106412]
  2. Juvenile Diabetes Research Foundation [5-CDA-2014-198-A-N, F31 DK107043]
  3. University of Colorado Anschutz Medical Campus Advance Light Microscopy Core [P30 NS048154, UL1 TR001082]
  4. Barbara Davis Center Islet Core [P30 DK057516]
  5. National Science Foundation (NSF) [CNS-08217944]
  6. University of Colorado

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Understanding how heterogeneous cells within a multicellular system interact and affect overall function is difficult without a means of perturbing individual cells or subpopulations. Here we apply optogenetics to understand how subpopulations of beta-cells control the overall [Ca2+]i response and insulin secretion dynamics of the islets of Langerhans. We spatiotempdrally perturbed electrical activity in beta-cells of channelrhodopsin2-expressing islets, mapped the [Ca2+]i response, and correlated this with the cellular metabolic activity and an in silico electrophysiology model. We discovered organized regions of metabolic activity across the islet, and these affect the way in which beta-cells electrically interact. Specific regions acted as pacemakers by initiating calcium wave propagation. Our findings reveal the functional architecture of the islet, and show how distinct subpopulations of cells can disproportionality affect function. These results also suggest ways in which other neuroendocrine systems can be regulated, and demonstrate how optogenetic tools can discern their functional architecture.

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