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《心脏杂志》[ISSN:1009-7236/CN:61-1268/R]

期数:

2011年第1期

页码:

56-58,64

栏目:

基础研究

出版日期:

2010-10-27

文章信息/Info

Title:

rhCD40L induces expression of matrix metalloproteinases in cultured U937 cells by cyclooxygenase-2 pathway

作者:

李岚¹; 樊民²; 杨靖²; 汪沁沁²

1.解放军第411医院内4科，上海 200081；2.第二军医大学长征医院心内科，上海 200003

Author(s):

LI Lan¹;  FAN Min²;  YANG Jing²;  WANG Qin-qin²

1.Fourth Medical Department, PLA 411 Hospital, Shanghai 200081, China; 2.Department of Cardiovasology, Changzheng Hospital, Second Military Medical University, Shanghai 200003, China

关键词:

CD40配体; 诱导型环氧合酶-2; 基质金属蛋白酶; 单核细胞系U937

Keywords:

CD40 ligand;  cyclooxygenase-2;  matrix metalloproteinases;  monocyte

分类号:

Q559

DOI:

-

文献标识码:

A

摘要:

目的: 探讨重组人CD40配体（rhCD40L）诱导U937细胞中基质金属蛋白酶（MMPs）表达的作用及其与诱导型环氧合酶-2(COX-2)途径的关系。方法： 体外培养U937细胞，以不同浓度（0.1、0.2、0.4 mg/L）的rhCD40L和不同浓度（10-5 mol/L、10^-4 mol/L、10^-3 mol/L）的COX-2特异性抑制剂(NS-398)分别刺激24 h。在加入终浓度为0.4 mg/L rhCD40L的基础上，加入终浓度为10^-4 mol/L的NS-398，共同刺激U937细胞24 h后，收集培养上清液，用酶谱法测定MMPs的活性。结果： rhCD40L可使MMP-2和MMP-9的活性明显增加（P<0.01），且呈剂量依赖性；NS-398可抑制MMP-2和MMP-9的活性，且抑制作用随剂量的增加而增强（P<0.05）。结论： rhCD40L以浓度依赖的方式诱导MMPs表达，rhCD40L对MMPs的诱导作用可能与COX-2途径有关。

Abstract:

AIM: To evaluate matrix metalloproteinase (MMP) expression induced by rhCD40L in cultured U937 cell and possible effects of cyclooxygenase-2 (COX-2). METHODS: U937 cells were treated with rhCD40L and NS-398 in different concentrations, respectively, and on the basis of the treatment with rhCD40L, U937 cells were cocultured with NS-398 and aspirin. The supernatant of the U937 cells cultures was collected. Zymography was performed by SDS-PAGE in 10% gels containing 0.1% (w/v) gelatin (denatured collagen) at 4℃. The activities of MMPs were detected by the grey level of the band. RESULTS: rhCD40L increased the activity of MMPs in a dose-dependent manner, whereas NS-398 significantly inhibited the activity of MMPs. NS-398 significantly inhibited the activity of MMPs induced by rhCD40L. CONCLUSION: rhCD40L can induce U937 cells to secrete MMPs in a dose-dependent manner, which may be related to COX-2 pathway.

参考文献/References

[1]Schonbeck U, Libby P. CD40 signaling and plaque instability[J]. Circ Res, 2001, 89(12):1092-1103.

[2]Nagashima H, Aoka Y, Sakomura Y, et al. Matrix metalloproteinase 2 is suppressed by trapidil, a CD40-CD40 ligand pathway inhibitor, in human abdominal aortic aneurysm wall[J]. J Vasc Surg, 2004, 39(2):447-453.

[3]Smola-Hess S, Schnitzler R, Hadaschik D, et al. CD40L induces matrix-metalloproteinase-9 but not tissue inhibitor of metalloproteinases-1 in cervical carcinoma cells: imbalance between NF-kappaB and STAT3 activation[J]. Exp Cell Res, 2001, 267(2):205-215.

[4]Santovito D, Mezzetti A, Cipollone F. Cyclooxygenase and prostaglandin synthases: roles in plaque stability and instability in humans[J]. Curr Opin Lipidol, 2009, 20(5):402-408.

[5]Bujold K, Rhainds D, Jossart C, et al. CD36-mediated cholesterol efflux is associated with PPARgamma activation via a MAPK-dependent COX-2 pathway in macrophages[J]. Cardiovasc Res, 2009, 83(3):457-464.

[6]Rival Y, Puech L, Taillandier T, et al. PPAR activators and COX inhibitors selectively block cytokine-induced COX-2 expression and activity in human aortic smooth muscle cells[J]. Eur J Pharmacol, 2009, 606(1-3):121-129.

[7]Rupp J, Berger M, Reiling N, et al. Cox-2 inhibition abrogates Chlamydia pneumoniae-induced PGE2 and MMP-1 expression[J]. Biochem Biophys Res Commun, 2004, 320(3):738-744.

[8]Choi YA, Lee DJ, Lim HK, et al. Interleukin-1beta stimulates matrix metalloproteinase-2 expression via a prostaglandin E2-dependent mechanism in human chondrocytes[J]. Exp Mol Med, 2004, 36(3):226-232.

[9]Cipollone F, Fazia M, Iezzi A, et al. Blockade of the angiotensin II type 1 receptor stabilizes atherosclerotic plaques in humans by inhibiting prostaglandin E2-dependent matrix metalloproteinase activity[J]. Circulation, 2004, 109(12):1482-1488.

[10]Pillinger MH, Rosenthal PB, Tolani SN, et al. Cyclooxygenase-2-derived E prostaglandins down-regulate matrix metalloproteinase-1 expression in fibroblast-like synoviocytes via inhibition of extracellular signal-regulated kinase activation[J]. J Immunol, 2003, 171(11):6080-6089.

备注/Memo

备注/Memo:

收稿日期：2010-01-19.基金项目：上海市卫生局科研课题资助（2007105） 通讯作者：樊民，教授，主要从事冠心病临床及基础研究 Email:fanmin@medmail.com.cn 作者简介：李岚，主治医师，硕士Email：lilan0824@sina.com.cn

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更新日期/Last Update: 2010-10-27