Differential routing and disposition of the long-chain saturated fatty acid palmitate in rodent vs human beta-cells

Patricia Thomas; Catherine Arden; Jenna Corcoran; Christian Hacker; Hannah J Welters; Noel G Morgan

doi:10.1038/s41387-022-00199-y

Differential routing and disposition of the long-chain saturated fatty acid palmitate in rodent vs human beta-cells

Nutr Diabetes. 2022 Apr 20;12(1):22. doi: 10.1038/s41387-022-00199-y.

Authors

Patricia Thomas¹, Catherine Arden², Jenna Corcoran³, Christian Hacker⁴, Hannah J Welters⁵, Noel G Morgan⁵

Affiliations

¹ Institute of Metabolism and Systems Research, Birmingham Medical School, University of Birmingham, Birmingham, UK. p.thomas@bham.ac.uk.
² Biosciences Institute, The Medical School, Newcastle University, Newcastle upon Tyne, UK.
³ Department of Biosciences, University of Exeter, Geoffrey Pope Building, Exeter, UK.
⁴ Bioimaging Centre, College of Life and Environmental Sciences, University of Exeter, Exeter, UK.
⁵ Institute of Biomedical and Clinical Research, College of Medicine and Health, University of Exeter, Exeter, UK.

Abstract

Background: Rodent and human β-cells are differentially susceptible to the "lipotoxic" effects of long-chain saturated fatty acids (LC-SFA) but the factors accounting for this are unclear. Here, we have studied the intracellular disposition of the LC-SFA palmitate in human vs rodent β-cells and present data that reveal new insights into the factors regulating β-cell lipotoxicity.

Methods: The subcellular distribution of the LC-SFA palmitate was studied in rodent (INS-1E and INS-1 823/13 cells) and human (EndoC-βH1) β-cells using confocal fluorescence and electron microscopy (EM). Protein expression was assessed by Western blotting and cell viability, by vital dye staining.

Results: Exposure of INS-1 cells to palmitate for 24 h led to loss of viability, whereas EndoC-βH1 cells remained viable even after 72 h of treatment with a high concentration (1 mM) of palmitate. Use of the fluorescent palmitate analogue BODIPY FL C₁₆ revealed an early localisation of the LC-SFA to the Golgi apparatus in INS-1 cells and this correlated with distention of intracellular membranes, visualised under the EM. Despite this, the PERK-dependent ER stress pathway was not activated under these conditions. By contrast, BODIPY FL C₁₆ did not accumulate in the Golgi apparatus in EndoC-βH1 cells but, rather, co-localised with the lipid droplet-associated protein, PLIN2, suggesting preferential routing into lipid droplets. When INS-1 cells were treated with a combination of palmitate plus oleate, the toxic effects of palmitate were attenuated and BODIPY FL C₁₆ localised primarily with PLIN2 but not with a Golgi marker.

Conclusion: In rodent β-cells, palmitate accumulates in the Golgi apparatus at early time points whereas, in EndoC- βH1 cells, it is routed preferentially into lipid droplets. This may account for the differential sensitivity of rodent vs human β-cells to "lipotoxicity" since manoeuvres leading to the incorporation of palmitate into lipid droplets is associated with the maintenance of cell viability in both cell types.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Fatty Acids / metabolism
Humans
Insulin-Secreting Cells* / metabolism
Oleic Acid / metabolism
Palmitates* / metabolism
Palmitates* / pharmacology
Rodentia / metabolism

Substances

Fatty Acids
Palmitates
Oleic Acid

Abstract

Publication types

MeSH terms

Substances

Grants and funding