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《心脏杂志》[ISSN:1009-7236/CN:61-1268/R]

期数:

2017年第5期

页码:

529-533

栏目:

基础研究

出版日期:

2017-03-25

文章信息/Info

Title:

Adiponectin improves hypoxia-induced pulmonary microvascular endothelial cell dysfunction and its mechanism

作者:

徐海军¹; 4; 张存娟¹; 张 娟¹; 吴海霞¹; 苏 慧²; 张海峰³; 孙 新¹

（第四军医大学：1.西京医院儿科，2.西京医院老年病科，3.教学实验中心,陕西 西安 710032；
4.杨凌示范区医院儿科,陕西 杨凌 712100）

Author(s):

XU Hai-jun¹; 4;  ZHANG Cun-juan¹;  ZHANG Juan¹;  WU Hai-xia¹;  SU Hui²;  ZHANG Hai-feng³;  SUN Xin¹

(1.Department of Pediatrics, 2.Department of Geriatrics, Xijing Hospital, 3.Experiment Teaching Center, Fourth Military Medical University, Xi’an 710032, Shaanxi, China；
4.Department of Pediatrics, Hospital of Yangling Demonstration District, Yangling 712100, Shaanxi, China)

关键词:

肺动脉内皮细胞; 脂联素; 内皮细胞功能障碍

Keywords:

pulmonary artery endothelialcell;  adiponectin;  endothelial dysfunction

分类号:

R589.2

DOI:

-

文献标识码:

A

摘要:

目的 研究重组人球状脂联素（APN）改善低氧诱导的大鼠肺微血管内皮细胞（PMVECs）功能障碍，探讨其潜在的分子机制。方法 取SD雄性大鼠PMVECs原代培养，传至第三代行细胞鉴定；PMVECs分3组，常氧（210 ml/L O2,37℃）组；低氧（20 ml/L O2,37℃）组；低氧（20 ml/L O2,37℃）+APN（1 μg/ml）处理组，分别培养3 h、6 h、9 h和12 h，收集细胞上清测NO浓度；3组PMVEC行RT- PCR测定eNOS基因表达；BCA法测定各组总蛋白含量；行Western blot检测AMPK/p-AMPK、PI3K/p-PI3K、Akt/p-Akt和eNOS/p-eNOS表达。结果 ①鉴定培养细胞为PMVECs；②在相应时间点，与正常组比较，低氧诱导的NO浓度、eNOS mRNA表达水平、总蛋白表达显著下降（P<0.01）；与低氧组对比，低氧+APN组显著增加了低氧诱导的NO浓度、eNOS mRNA表达水平、总蛋白表达（P<0.01）；③3组AMPK、PI3K、Akt和eNOS总蛋白表达水平不变；与正常组比较，低氧诱导的AMPK、PI3K、Akt、eNOS磷酸化表达水平下降（P<0.05）；与低氧组对比，低氧+APN组增加了低氧诱导的AMPK、PI3K、Akt、eNOS磷酸化表达水平（P<0.05）。结论 在细胞水平上，APN能改善低氧条件下诱导的PMVECs功能障碍，促进肺血管具有舒张作用的NO产生，其可能机制可能是伴随着AMPK/PI3K/Akt/eNOS /NO信号通路的激活，APN可能成为潜在治疗低氧性肺动脉高压的辅助药物。

Abstract:

AIM To investigate the effect and molecular mechanism of adiponectin in improving hypoxia-induced dysfunction of rat pulmonary microvascular endothelial cells (PMVECs). METHODS The third passage of primary cultured PMVECs from SD rats were identified by immunohistochemical method and were divided into three groups. The three groups were cultured respectively under normoxia condition (210 ml/L O2, 37℃), hypoxia condition (20 ml/L O2, 37℃) or hypoxia condition (20 ml/L O2, 37℃) with treatment of APN (1 μg/ml). Supernatant and cell lysate were collected at different time intervals at 3 h, 6 h, 9 h and 12 h. NO concentration in supernatant was determined by nitrate reductive enzymatic method, the expression of eNOS-mRNA was observed by RT-PCR, the total protein concentration was detected by the method of BCA, and protein levels of AMPK/p-AMPK, PI3K/p-PI3K,Akt/p-Akt and eNOS/p-eNOS were respectively detected by Western blot from 12 h cells in each group. RESULTS Primary culture of PMVECs was successful. At the same time interval, NO production, mRNA of eNOS and total protein levels in the hypoxia group decreased significantly compared with those in the normoxia group (P<0.01). No production, eNOS mRNA and total protein levels in the hypoxia+ANP group were significantly higher than those in the hypoxia group (P<0.01). There was no significant difference in total protein levels of AMPK, PI3K,Akt and eNOS among the three groups. Phosphorylated AMPK, PI3K,Akt and eNOS decreased significantly（P<0.05） in the hypoxia group compared with those in the normoxia group. Phosphorylated AMPK, PI3K,Akt and eNOS increased significantly（P<0.05） in the hypoxia+ANP group compared with those in the hypoxia group. CONCLUSION APN improves hypoxia-induced dysfunction of PMVECs at cellular levels. It can increase the production of NO possibly through the activation of AMPK/PI3K/Akt/eNOS/NO signaling pathway. APN is a potential ancillary drug for the treatment of hypoxia pulmonary hypertension.

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备注/Memo

备注/Memo:

收稿日期：2016-09-26.
基金项目：国家自然基金项目资助（81270330,30700345,31371151和31271219）；陕西省科技厅国际合作课题项目资助（2013KW30-02）；陕西省科学技术研究发展计划项目资助（2013Kkjxx-89）
通讯作者：孙新，副教授，主要从事肺动脉高压研究 Email:sunxin6@fmmu.edu.cn
作者简介：徐海军，硕士生 Emai:navy800628@163.com

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更新日期/Last Update: 2017-04-20