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  4. Type 2 diabetes disrupts circadian orchestration of lipid metabolism and membrane fluidity in human pancreatic islets
 
research article

Type 2 diabetes disrupts circadian orchestration of lipid metabolism and membrane fluidity in human pancreatic islets

Petrenko, Volodymyr
•
Sinturel, Flore
•
Loizides-Mangold, Ursula
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August 1, 2022
Plos Biology

Recent evidence suggests that circadian clocks ensure temporal orchestration of lipid homeostasis and play a role in pathophysiology of metabolic diseases in humans, including type 2 diabetes (T2D). Nevertheless, circadian regulation of lipid metabolism in human pancreatic islets has not been explored. Employing lipidomic analyses, we conducted temporal profiling in human pancreatic islets derived from 10 nondiabetic (ND) and 6 T2D donors. Among 329 detected lipid species across 8 major lipid classes, 5% exhibited circadian rhythmicity in ND human islets synchronized in vitro. Two-time point-based lipidomic analyses in T2D human islets revealed global and temporal alterations in phospho- and sphingolipids. Key enzymes regulating turnover of sphingolipids were rhythmically expressed in ND islets and exhibited altered levels in ND islets bearing disrupted clocks and in T2D islets. Strikingly, cellular membrane fluidity, measured by a Nile Red derivative NR12S, was reduced in plasma membrane of T2D diabetic human islets, in ND donors' islets with disrupted circadian clockwork, or treated with sphingolipid pathway modulators. Moreover, inhibiting the glycosphingolipid biosynthesis led to strong reduction of insulin secretion triggered by glucose or KCl, whereas inhibiting earlier steps of de novo ceramide synthesis resulted in milder inhibitory effect on insulin secretion by ND islets. Our data suggest that circadian clocks operative in human pancreatic islets are required for temporal orchestration of lipid homeostasis, and that perturbation of temporal regulation of the islet lipid metabolism upon T2D leads to altered insulin secretion and membrane fluidity. These phenotypes were recapitulated in ND islets bearing disrupted clocks.

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Type
research article
DOI
10.1371/journal.pbio.3001725
Web of Science ID

WOS:000837734300001

Author(s)
Petrenko, Volodymyr
Sinturel, Flore
Loizides-Mangold, Ursula
Montoya, Jonathan Paz
Chera, Simona
Riezman, Howard
Dibner, Charna
Date Issued

2022-08-01

Publisher

PUBLIC LIBRARY SCIENCE

Published in
Plos Biology
Volume

20

Issue

8

Article Number

e3001725

Subjects

Biochemistry & Molecular Biology

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Biology

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Life Sciences & Biomedicine - Other Topics

•

calcium mobilization

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insulin-secretion

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beta-cells

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glucose

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dynamics

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glucosylceramide

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phospholipids

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sphingolipids

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oscillations

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ceramides

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
UPDANGELO  
Available on Infoscience
August 15, 2022
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/190053
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