4.6 Article

Shared and distinct lipid-lipid interactions in plasma and affected tissues in a diabetic mouse model

期刊

JOURNAL OF LIPID RESEARCH
卷 59, 期 2, 页码 173-183

出版社

ELSEVIER
DOI: 10.1194/jlr.M077222

关键词

diabetes; eye; kidney; mass spectrometry; nerve; systems biology

资金

  1. National Institutes of Health, National Institute of Diabetes and Digestive and Kidney Diseases [DK094292, DK089503, DK082841, DK081943, DK097153]
  2. National Eye Institute Grant [EY20582]
  3. Michigan Institute for Clinical and Health Research CTSA Award from the National Center for Advancing Translational Sciences [2UL1TR000433]
  4. American Diabetes Association
  5. Program for Neurology Research and Discovery
  6. Juvenile Diabetes Research Foundation
  7. Taubman Institute at the University of Michigan
  8. Novo Nordisk Grant [NNF14SA0006]
  9. Novo Nordisk Fonden [NNF14OC0011633] Funding Source: researchfish

向作者/读者索取更多资源

Lipids are ubiquitous metabolites with diverse functions; abnormalities in lipid metabolism appear to be related to complications from multiple diseases, including type 2 diabetes. Through technological advances, the entire lipidome has been characterized and researchers now need computational approaches to better understand lipid network perturbations in different diseases. Using a mouse model of type 2 diabetes with microvascular complications, we examined lipid levels in plasma and in renal, neural, and retinal tissues to identify shared and distinct lipid abnormalities. We used correlation analysis to construct interaction networks in each tissue, to associate changes in lipids with changes in enzymes of lipid metabolism, and to identify overlap of coregulated lipid subclasses between plasma and each tissue to define subclasses of plasma lipids to use as surrogates of tissue lipid metabolism. Lipid metabolism alterations were mostly tissue specific in the kidney, nerve, and retina; no lipid changes correlated between the plasma and all three tissue types. However, alterations in diacylglycerol and in lipids containing arachidonic acid, an inflammatory mediator, were shared among the tissue types, and the highly saturated cholesterol esters were similarly coregulated between plasma and each tissue type in the diabetic mouse. Our results identified several patterns of altered lipid metabolism that may help to identify pathogenic alterations in different tissues and could be used as biomarkers in future research into diabetic microvascular tissue damage.

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