## Abstract Insulin receptor associated with the cerebral cortex (CC) has been shown to be involved in brain cognitive functions. Furthermore, deterioration of insulin signaling has been associated with age‐related brain degeneration. We have reported previously that aging stimulates phospholipase
Insulin promotes diacylglycerol kinase activation by different mechanisms in rat cerebral cortex synaptosomes
✍ Scribed by Sandra E. Zulian; Mónica G. Ilincheta de Boschero; Norma M. Giusto
- Publisher
- John Wiley and Sons
- Year
- 2006
- Tongue
- English
- Weight
- 190 KB
- Volume
- 84
- Category
- Article
- ISSN
- 0360-4012
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✦ Synopsis
Abstract
The mechanism by which insulin increases diacylglycerol kinase (DAGK) activity has been studied in cerebral cortex (CC) synaptosomes from adult (3–4 months of age) rats. The purpose of this study was to identify the role of phospholipases C and D (PLC and PLD) in DAGK activation by insulin. Neomycin, an inhibitor of PLC phosphatidylinositol‐bisphosphate (PIP~2~) specific; ethanol, an inhibitor of phosphatidic acid (PA) formation by the promotion of a transphosphatidyl reaction of phosphatidylcholine phospholipase D (PC‐PLD); and DL propranolol, an inhibitor of phosphatidate phosphohydrolase (PAP), were used in this study. Insulin (0.1 μM) shielded an increase in PA synthesis by [^32^P] incorporation using [γ‐^32^P]ATP as substrate and endogenous diacylglycerol (DAG) as co‐substrate. This activated synthesis was strongly inhibited either by ethanol or DL propranolol. Pulse chase experiments also showed a PIP~2~‐PLC activation within 1 min exposure to insulin. When exogenous unsaturated 18:0‐20:4 DAG was present, insulin increased PA synthesis significantly. However, this stimulatory effect was not observed in the presence of exogenous saturated (di‐16:0). In the presence of R59022, a selective DAGK inhibitor, insulin exerted no stimulatory effect on [^32^P]PA formation, suggesting a strong relationship between increased PA formation by insulin and DAGK activity. These data indicate that the increased synthesis of PA by insulin could be mediated by the activation of both a PC‐PLD pathway to provide DAG and a direct DAGK activation that is associated to the use of 18:0‐20:4 DAG species. PIP~2~‐PLC activation may contribute at least partly to the insulin effect on DAGK activity. © 2006 Wiley‐Liss, Inc.
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