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首页> 美国卫生研究院文献>American Journal of Physiology - Gastrointestinal and Liver Physiology >Cocaine- and amphetamine-regulated transcript is the neurotransmitter regulating the action of cholecystokinin and leptin on short-term satiety in rats
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Cocaine- and amphetamine-regulated transcript is the neurotransmitter regulating the action of cholecystokinin and leptin on short-term satiety in rats

机译:可卡因和苯丙胺调节的转录物是调节胆囊收缩素和瘦素对大鼠短期饱腹感作用的神经递质

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Vagal CCK-A receptors (CCKARs) and leptin receptors (LRbs) interact synergistically to mediate short-term satiety. Cocaine- and amphetamine-regulated transcript (CART) peptide is expressed by vagal afferent neurons. We sought to demonstrate that this neurotransmitter regulates CCK and leptin actions on short-term satiety. We also examined the signal transduction pathways responsible for mediating the CART release from the nodose ganglia (NG). ELISA studies coupled with gene silencing of NG neurons by RNA interference elucidated intracellular signaling pathways responsible for CCK/leptin-stimulated CART release. Feeding studies followed by gene silencing of CART in NG established the role of CART in mediating short-term satiety. Immunohistochemistry was performed on rat NG neurons to confirm colocalization of CCKARs and LRbs; 63% of these neurons contained CART. Coadministration of CCK-8 and leptin caused a 2.2-fold increase in CART release that was inhibited by CCK-OPE, a low-affinity CCKAR antagonist. Transfection of cultured NG neurons with steroid receptor coactivator (SRC) or phosphatidylinositol 3-kinase (PI3K) small-interfering RNA (siRNA) or STAT3 lentiviral short hairpin RNA inhibited CCK/leptin-stimulated CART release. Silencing the expression of the EGR-1 gene inhibited the CCK/leptin-stimulated CART release but had no effect on CCK/leptin-stimulated neuronal firing. Electroporation of NG with CART siRNA inhibited CCK/leptin stimulated c-Fos expression in rat hypothalamus. Feeding studies following electroporation of the NG with CART or STAT3 siRNA abolished the effects of CCK/leptin on short-term satiety. We conclude that the synergistic interaction of low-affinity vagal CCKARs and LRbs mediates CART release from the NG, and CART is the principal neurotransmitter mediating short-term satiety. CART release from the NG involves interaction between CCK/SRC/PI3K cascades and leptin/JAK2/PI3K/STAT3 signaling pathways.
机译:迷走性CCK-A受体(CCKARs)和瘦素受体(LRbs)协同相互作用,介导短期饱腹感。可卡因和苯丙胺调节的转录(CART)肽由迷走神经传入神经元表达。我们试图证明这种神经递质在短期饱腹感时调节CCK和瘦蛋白的作用。我们还检查了负责介导结节神经节(NG)释放CART的信号转导途径。 ELISA研究与RNA干扰对NG神经元的基因沉默相结合,阐明了负责CCK /瘦蛋白刺激的CART释放的细胞内信号传导途径。 NG中CART基因沉默后的进食研究确立了CART在介导短期饱腹感中的作用。在大鼠NG神经元上进行了免疫组织化学,以确认CCKARs和LRbs的共定位。这些神经元中有63%含有CART。 CCK-8和瘦素的共同给药导致CART释放增加2.2倍,而CAG-OPE是一种低亲和力的CCKAR拮抗剂,可抑制CART释放。用类固醇受体共激活剂(SRC)或磷脂酰肌醇3激酶(PI3K)小干扰RNA(siRNA)或STAT3慢病毒短发夹RNA转染培养的NG神经元可抑制CCK /瘦蛋白刺激的CART释放。沉默EGR-1基因的表达可抑制CCK /瘦蛋白刺激的CART释放,但对CCK /瘦蛋白刺激的神经元放电没有影响。用CART siRNA对NG电穿孔可抑制大鼠下丘脑中CCK /瘦素刺激的c-Fos表达。用CART或STAT3 siRNA对NG电穿孔后的进食研究消除了CCK /瘦蛋白对短期饱腹感的影响。我们得出结论,低亲和力迷走神经CCKARs和LRbs的协同相互作用介导了NG释放CART,而CART是介导短期饱腹感的主要神经递质。从NG释放CART涉及CCK / SRC / PI3K级联与瘦素/ JAK2 / PI3K / STAT3信号通路之间的相互作用。

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