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无生长追赶SGA幼鼠生长激素和胰岛素受体后信号交联对话的研究
引用本文:黄婷婷,杜敏联,李燕虹,马华梅. 无生长追赶SGA幼鼠生长激素和胰岛素受体后信号交联对话的研究[J]. 中国病理生理杂志, 2008, 24(2): 344-349. DOI: 1000-4718
作者姓名:黄婷婷  杜敏联  李燕虹  马华梅
作者单位:中山大学附属第一医院儿科, 广东 广州 510080
摘    要:目的:在生长激素(GH)和胰岛素(INS)共享受体后PI3K通路基础上探讨无生长追赶的出生低体重(NCU-SGA)幼鼠GH和INS抵抗的受体后机制,以及2者受体后信号通路的交联对话(cross-talk)。方法:取4周龄NCU-SGA雄性大鼠,采用Western印记及免疫共沉淀技术分别测定NCU-SGA幼鼠在基础状态下、胰岛素激发以及先给予GH受体后信号通路JAK2阻滞剂AG490后再行胰岛素激发后(AG490+INS组)肝组织胰岛素受体底物-1(IRS-1)及其下游信号磷酸化Akt(p-Akt)的表达。结果:(1)IRS-1信号表达: SGA鼠基础状态、INS激发后和AG490+INS组,3组间的IRS-1总蛋白及IRS-1磷酸化水平与正常对照组(C组)无显著差异(P>0.05)。(2)p-Akt信号表达: C组基础状态时无p-Akt信号表达,INS刺激后表达明显增强。SGA鼠基础状态时p-Akt已有显著表达(慢性激活),INS刺激后表达较基础状态增加,但增殖显著低于正常对照组(P<0.01);AG490+INS组的p-Akt较JAK2未被阻断时明显增强(P<0.01),但仍显著低于正常对照组(P<0.01),提示GH的信号干扰了INS受体后IRS-1至Akt的信号转导。结论:NCU-SGA幼鼠INS抵抗的发生与IRS-1-Akt通路受损有关,GH抵抗经GH和INS 2者受体后信号通路间的交联对话(cross-talk)使IRS-1至Akt间的信号转导解偶联,诱导和加重了INS抵抗;而PI3K-Akt可能是发生该解偶联的主要交汇点。

关 键 词:小于胎龄儿  大鼠  生长激素抵抗  胰岛素抗药性  信号转导  
文章编号:1000-4718(2008)02-0344-06
收稿时间:2006-09-05
修稿时间:2006-12-26

Post-receptor signaling crosstalk between GH and insulin in non-catch-up growth rats born small for gestational age
HUANG Ting-ting,DU Min-lian,LI Yan-hong,MA Hua-mei. Post-receptor signaling crosstalk between GH and insulin in non-catch-up growth rats born small for gestational age[J]. Chinese Journal of Pathophysiology, 2008, 24(2): 344-349. DOI: 1000-4718
Authors:HUANG Ting-ting  DU Min-lian  LI Yan-hong  MA Hua-mei
Affiliation:Pediatric Department, The First Affiliated Hospital of Sun Yet-sen University, Guangzhou 510080, China. E-mail: szzxsums@163.com
Abstract:AIM:To investigate the post-receptor mechanism of growth hormone (GH) resistance and insulin (INS) resistance and their relationship in non-catch-up growth rats born small for gestational age (NCU-SGA), based on the post-receptor signalling cross-talk between GH and INS at PI3K signaling pathway. METHODS:NCU-SGA rat model was developed by food restriction to pregnant dams. 4 weeks old male NCU-SGA rats were studied. Total and phosphate insulin receptor substrate-1(IRS-1) and its downstream signal Akt levels in liver tissue were measured by Western blotting or immunoprecipitation at baseline, post-stimulating of insulin, and pre-treatment with JAK2 (post-receptor signaling protein of GH) inhibitor AG490 then given insulin stimulation, respectively. RESULTS:(1) Expression levels of total and phosphate IRS-1: No difference between NCU-SGA rats and normal control was observed (P>0.05). (2) Expression levels of Akt : At baseline, Akt was already activated in NCU-SGA rats compared to no Akt activation in normal control rats. However, post- stimulating of insulin, the increase level of phosphate Akt in NCU- SGA rats was remarkably lower than that in control rats (P<0.01). When pre-treatment with JAK2 inhibitor to block GH signaling pathway, the impaired Akt activity was significantly restored (P<0.01), which suggested that the signaling of GH uncouples signal transduction from IRS-1 to Akt in NCU-SGA rats.CONCLUSION:Insulin resistance is related to impaired IRS-1-Akt signaling pathway in NCU-SGA rats. GH resistance mediates and aggrevates INS resistance by uncoupling signal transduction from IRS-1 to Akt via signaling cross-talk at post-receptor level between GH and INS. PI3K/Akt may be the major site for this uncoupling.
Keywords:Small for gestational age   Rats    Grow hormone resistance   Insulin resistance   Signal transduction
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