4.5 Article Proceedings Paper

Stress Stimulates Production of Catecholamines in Rat Adipocytes

Journal

CELLULAR AND MOLECULAR NEUROBIOLOGY
Volume 32, Issue 5, Pages 801-813

Publisher

SPRINGER/PLENUM PUBLISHERS
DOI: 10.1007/s10571-012-9822-6

Keywords

Mesenteric adipocytes; Stromal vascular fraction; Catecholamine production; Immobilization; Cold; Novel stressors

Funding

  1. Slovak Research and Development Agency [APVV-0088-10, 0148-06]
  2. TRANSMED 2 [ITMS: 26240120030]
  3. VEGA [2/0188/09, 2/0036/11]
  4. EFSD

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The sympathoadrenal system is the main source of catecholamines (CAs) in adipose tissues and therefore plays the key role in the regulation of adipose tissue metabolism. We recently reported existence of an alternative CA-producing system directly in adipose tissue cells, and here we investigated effect of various stressors-physical (cold) and emotional stress (immobilization) on dynamics of this system. Acute or chronic cold exposure increased intracellular norepinephrine (NE) and epinephrine (EPI) concentration in isolated rat mesenteric adipocytes. Gene expression of CA biosynthetic enzymes did not change in adipocytes but was increased in stromal vascular fraction (SVF) after 28 day cold. Exposure of rats to a single IMO stress caused increases in NE and EPI levels, and also gene expression of CA biosynthetic enzymes in adipocytes. In SVF changes were similar but more pronounced. Animals adapted to a long-term cold exposure (28 days, 4A degrees C) did not show those responses found after a single IMO stress either in adipocytes or SVF. Our data indicate that gene machinery accommodated in adipocytes, which is able to synthesize NE and EPI de novo, is significantly activated by stress. Cold-adapted animals keep their adaptation even after an exposure to a novel stressor. These findings suggest the functionality of CAs produced endogenously in adipocytes. Taken together, the newly discovered CA synthesizing system in adipocytes is activated in stress situations and might significantly contribute to regulation of lipolysis and other metabolic or thermogenetic processes.

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