期刊
DIABETES
卷 54, 期 6, 页码 1698-1705出版社
AMER DIABETES ASSOC
DOI: 10.2337/diabetes.54.6.1698
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资金
- NCCIH NIH HHS [R01 AT001846, R01 AT001846-02, R01-AT001846] Funding Source: Medline
Phosphatidylinositol (PI) 4,5-bisphosphate (PIP2) plays a pivotal role in insulin-stimulated glucose transport as an important precursor to PI 3,4,5-trisphosphate (PIPS) and a key regulator of actin polymerization. Since endothelin (ET)-1 impairs insulin sensitivity and PIP2 is a target of ET-1-induced signaling, we tested whether a change in insulin-stimulated PIPS generation and signaling, PIP2-regulated actin polymerization, or a combination of both accounted for ET-1-induced insulin resistance. Concomitant with a time-dependent loss of insulin sensitivity, ET-1 caused a parallel reduction in plasma membrane PIP2. Despite decreased insulin-stimulated PI 3-kinase activity and PIPS generation, ET-1 did not diminish downstream signaling to Akt-2. Furthermore, addition of exogenous PIP2, but not PIPS, restored insulin-regulated GLUT4 translocation and glucose transport impaired by ET-1. Microscopic and biochemical analyses revealed a PIP2-dependent loss of cortical filamentous actin (F-actin) in ET-1-treated cells. Restoration of insulin sensitivity by PIP2 add-back occurred concomitant with a reestablishment of cortical F-actin. The corrective effect of exogenous PIP2 in ET-1-induced insulin-resistant cells was not present in cells where cortical F-actin remained experimentally depolymerized. These data suggest that ET-1-induced insulin resistance results from reversible changes in PIP2-regulated actin polymerization and not PIP2-dependent signaling.
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