Abstract

Obesity, in particular abdominal obesity, alters the composition of plasma and tissue fatty acids (FAs), which contributes to inflammation and insulin resistance. FA metabolism is modulated by desaturases and may affect adipokine and insulin secretion. Therefore, we examined relationships between adipokines, a marker of insulin production, and plasma FA desaturase enzyme activity estimates (EAEs) in obesity. Plasma phospholipid (PPL) FAs were isolated from 126 males (ages 48 to 65 years), derivatized, and analyzed using gas chromatography. Delta-6 desaturase (D6D) and delta-5 desaturase (D5D) EAEs were calculated as the ratio of PPL 20:3/18:2 and 20:4/20:3, respectively. In body mass index (BMI) and waist circumference (WC) adjusted polytomous logistic regression analyses, PPL FAs and FA desaturase EAEs were associated with C-peptide and adiponectin. Individuals with elevated D6D EAEs were less likely (OR 0.33) to have serum adiponectin concentrations > 5.37 μg/mL, compared with adiponectin concentrations ≤ 3.62 μg/mL. Individuals with increased D5D EAEs were less likely (OR 0.8) to have C-peptide concentrations ≥ 3.32 ng/mL, and > 1.80 and ≤ 3.29 ng/mL, compared with those with C-peptide ≤ 1.76 ng/mL. The proinflammatory cytokine tumor necrosis factor-α (TNF- α) was positively associated with C-peptide, but TNF- α was not associated with the D5D EAE. C-peptide and adiponectin concentrations are associated with specific PPL FAs and FA desaturase EAEs. The relationship between C-peptide concentrations and D5D EAEs remained significant after adjusting for BMI, WC, and TNF-α. Thus, future research should investigate whether D5D inhibition may occur through a C-peptide mediated pathway.

Highlights

  • Obesity is a chronic disease affecting over one-third of US adults [1]

  • Serum adiponectin concentrations were significantly associated with PPL fatty acid (FA) (Tables 2 and 3)

  • Fatty acids expressed as percent of total phospholipids

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Summary

Introduction

Obesity is a chronic disease affecting over one-third of US adults [1]. Obesity is associated with excess lipid storage in white adipose tissue (WAT), adipokine dysregulation, insulin resistance, and chronic low-grade inflammation [2]. Adipokines are adipose-derived cytokines, which have functions in regulating metabolism and inflammation. The expansion of WAT alters adipokine secretion and fatty acid (FA) metabolism, and influences low-grade inflammation associated with insulin resistance and type-2 diabetes (T2D) [3]. PLOS ONE | DOI:10.1371/journal.pone.0149305 March 29, 2016

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