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Mechanisms involved in the cytotoxic and cytoprotective actions of saturated versus monounsaturated long-chain fatty acids in pancreatic β-cells

  • Peninsula Medical School, Universities of Exeter and Plymouth
    ,
  • University of Southampton
Research Output: Contribution to journal Article Peer-review

Sustainable Development Goals

  • SDG 3 - Good Health and Well-being
    SDG 3 Good Health and Well

Abstract

Long-chain saturated and monounsaturated fatty acids differ in their propensity to induce β-cell death in vitro with palmitate (C16:0) being cytotoxic, whereas palmitoleate (C16:1n-7) is cytoprotective. We now show that this cytoprotective capacity extends to a poorly metabolised C16:1n-7 derivative, methyl-palmitoleate (0.25 mM palmitate alone: 92±4% death after 18 h; palmitate plus 0.25 mM methyl-palmitoleate: 12±2%; P<0.001). Palmitoleate and its methylated derivative also acted as mitogens in cultured β-cells (5-bromo-2-deoxyuridine incorporation - control: 0.15±0.01 units; 0.25 mM palmitoleate: 0.22±0.01 units; P<0.05). It has been proposed that alterations in neutral lipid synthesis (particularly triacylglycerol (TAG) formation) might mediate the differential responses to saturated and unsaturated fatty acids and we have examined this proposition. Palmitate and palmitoleate both promoted β-cell phospholipid remodelling and increased TAG formation (control: 0.9± 0.1 nmol TAG/106 cells; 0.25 mM palmitate: 1.55±0.07; 0.25 mM palmitoleate: 1.4±0.05; palmitate plus palmitoleate: 2.3±0.1). By contrast, methyl-palmitoleate failed to influence TAG levels (0.25 mM methyl-palmitoleate alone: 0.95±0.06 nmol TAG/106 cells; methyl-palmitoleate plus palmitate: 1.5±0.05) or its fatty acid composition in β-cells exposed to palmitate. The results suggest that monounsaturated fatty acids can promote cell viability and mitogenesis by a mechanism that does not require their metabolism and is independent of alterations in TAG formation.

Publication Information

Output type

Research Output: Contribution to journal Article Peer-review

Original language

English

Pages from-to (Number of pages)

Pages 283-291 (9 pages)

Journal (Volume, Issue Number)

Journal of Endocrinology (Volume 194, Issue 2)

Publication milestones

  • Published - 22/05/2007

Publication status

Published - 22/05/2007

ISSN

0022-0795

External Publication IDs

  • Scopus: 34547888676
  • PubMed: 17641278