| 瘦素通过其受体刺激小鼠血管平滑肌细胞增殖而促进动脉内膜增生 |
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| 引用本文: | 沈粤春,何兆初,陆东风,区碧如,潘洁贞,王晓明,李君.瘦素通过其受体刺激小鼠血管平滑肌细胞增殖而促进动脉内膜增生[J].中华心血管病杂志,2009,37(7). |
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| 作者姓名: | 沈粤春 何兆初 陆东风 区碧如 潘洁贞 王晓明 李君 |
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| 作者单位: | 1. 广州医学院第一附属医院心血管内科,510120
2. 广州医学院第一附属医院外科,510120 |
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| 摘 要: | 目的 探讨瘦素是否影响动脉内膜的增生及其发生机制.方法 利用野生型(Wt)、瘦素基因缺陷(Lep-/-)、瘦素受体基冈缺陷(LepR-/-)小鼠,通过股动脉内膜损伤及瘦素疗法,结合组织学特性,分析瘦素影响动脉内膜增生情况及其机制.结果 动脉内膜损伤后4周,Lep-/-和LepR-/-小鼠的内膜面积与中层面积比值(I/M)均小于Wt小鼠,差异均有统计学意义(Lep-/-小鼠比Wt小鼠为0.80±0.14比1.50±0.22,P<0.01;LepR-/-小鼠比Wt小鼠为0.55±0.20比1.50 ±0.22,P<0.05).Lep-/-和LepR-/-小鼠经动脉内膜损伤并同时给予瘦素治疗后,前者的I/M显著增加,而后者的I/M无明显变化.α-肌动蛋白和5-溴-2-脱氧尿嘧啶染色显示,二者在各组动脉增生内膜的阳性率分布趋势与内膜增厚程度一致.结论 瘦素缺乏或瘦素受体缺乏防止动脉内膜增生,外源性瘦素恢复Lep-/-小鼠动脉内膜增生,但对LepR-/-小鼠内膜无影响.本研究从动物模型上证明,高瘦素血症是动脉内膜增生的高危因素,并说明瘦素通过瘦素受体刺激血管平滑肌细胞增殖而促进动脉内膜增生.
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| 关 键 词: | 动脉粥样硬化 瘦素 血管内膜 |
Leptin promotes neointimal formation by stimulating vascular smooth muscle cell proliferation through leptin receptor |
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| SHEN Yue-chun,HE Zhao-chu,LU Dong-feng,OU Bi-ru,PAN Jie-zhen,WANG Xiao-ming,LI Jun.Leptin promotes neointimal formation by stimulating vascular smooth muscle cell proliferation through leptin receptor[J].Chinese Journal of Cardiology,2009,37(7). |
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| Authors: | SHEN Yue-chun HE Zhao-chu LU Dong-feng OU Bi-ru PAN Jie-zhen WANG Xiao-ming LI Jun |
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| Abstract: | Objective To evaluate the role of leptin in neointimal formation and related mechanisms.Methods Femoral arterial injury was induced in wild-type (Wt,n = 10),leptin-deficient (Lep -/-,n = 12),and ieptin receptor-deficient (LepR -/- ,n = 10) mice.Leptin treatment studies (tail vein injection of adenovirus expressing murine ieptin on the RSV promoter,ad-leptin) were performed on Lep -/- (n = 5) and LepR -/- (n = 4) mice.Intimal (I) and medial (M) areas were measured and the ratio of I/M was calculated.Smooth muscle cells were detected by smooth muscle α-actin staining using an α-actin monoclonal antibody.Cellular proliferation was analyzed with BrdU Staining Kit and the number of BrdU-positive cells was counted manually.Plasma leptin level was measured by ELISA.Results The I/M ratio of Lep -/- and LepR -/- mice was significantly lower than that in Wt separately (Lep -/- vs.Wt = 0.80±0.14 vs.1.50±0.22,P<0.01; LepR-/- vs.Wt=0.55±0.20 vs.1.50±0.22,P<0.05).Plasma leptin level was significantly increased in Lep-/- and LepR -/- mice post leptin treatment.I/M was significantly increased in Lep -/- mice receiving ad-leptin compared with untreated Lep -/- mice (P < 0.05),while I/M was similar between LepR -/- mice with and without ad-leptin treatment (P > 0.05).The changes on number of positive α-actin and BrdU stained smooth muscle cells were consistent with the neointimal formation findings in various groups.Conclusions Mice lacking leptin or the ieptin receptor were protected from neointimal formation following vascular injury.Leptin treatment increased neointimsl formation in Lep-/- but not in LepR-/- mice,suggesting leptin receptor activation and vascular smooth muscle cell proliferation played a pivotal role on neointimal formation post-injury in this model,giving an evidence that high plasma leptin level is a risk factor for neointimal formation. |
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| Keywords: | Atherosclerosis Leptin Tunica intima |
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