瑞舒伐他汀对代谢综合征患者血清血管生成素-2和超敏C反应蛋白的影响

The impact of rosuvastatin on serum Ang-2 and hs-CRP in patients with metabolic syndrome

导出

摘要目的观察瑞舒伐他汀对代谢综合征（MS）患者血清血管生成素-2（Ang-2）和超敏C反应蛋白（hs-CRP）的影响及其安全性。方法将80例MS患者分为治疗组40例和对照组40例。两组均给予降压治疗，同时治疗组加用瑞舒伐他汀10mg／d口服，疗程8周。对照组不用任何调脂药。治疗前和治疗后8周分别检测血清Ang-2、hs-CRP浓度及肝、肾功能，比较两组治疗前、后各相关指标的差异。结果（1）治疗组治疗8周后Ang-2和hs-CRP浓度较治疗前显著降低[（1．81±0．47）μg／L降至（0．30±0．01）μg／L，（6．32±1．28）mg／L降至（2．02±0．26）mg／L；t=9．02、t=5．75，P均〈0．01]；而对照组上述指标在治疗前后比较差异均无统计学意义[（1．80±0．45）μg/L与（1．79±0．48）μg／L，（6．28±1．34）mg／L与（6．20±1．42）mg／L；t=0．19、t=0．23，P均〉0．05]。（2）治疗8周后治疗组的Ang-2和hs-CRP浓度与对照组相比明显降低[（0．30±0．01）μg／L与（1．79±0．48）μg／L，（2．02±0．26）mg／L与（6．20±1．42）mg／L；t=2．34、t=2．58，P均〈0．05]。（3）治疗组不良反应少，安全性好。结论瑞舒伐他汀可降低MS患者血清Ang-2和hs-CRP浓度，改善胰岛素抵抗，其安全性良好。 Objective To observe the impact of rosuvastatin on serum Ang-2 and hs-CRP in patients with metabolic syndrome （MS） to collect data on safety of rosuvastatin in treating MS. Methods Eighty MS patients were enrolled and divided into the treatment group （ n = 40 ） and the control group （ n = 40 ） . The treatment group received both antihypertensive therapy and rosuvastatin with a dose of 10 mg/d. While the control group were only given antihypertensive therapy and but not any lipid-lowering drugs. The levels of plasma Ang-2 and hs-CRP and liver and kidney functions were measured and compared before and after 8-week treatment. Results （1） The levels of plasma Ang-2 and hs-CRP were significantly lower after 8 weeks than before treatment in the treatment groups [ Ang-2 ：（ 0. 30 ± 0. 01 ） μg/L vs. （ 1.81 ± 0. 47 ） μg/L, t = 9.02, P 〈 0. 01 ;hs-CRP：（ 2.02 ± 0. 26 ） mg,/L vs. （ 6. 32 ± 1.28 ） mg/L, t = 5.75, P 〈 0.01 ] . Whereas statistical difference was not found in the control group [ Ang-2 ：（ 1.80 ± 0.45 ） μg/L vs. （ 1.79 ± 0. 48 ） μg/L, t = 0. 19, P 〉0. 05 ;hs-CRP：（6. 28 ± 1.34 ） mg/L vs. （ 6. 20 ± 1.42 ） mg/L, t = 0. 23, P 〉 0.05 ]. （ 2 ） After 8 weeks＇ treatment, the levels of plasma Ang-2 and hs-CRP were significantly lower in the treatment group than in the control group [ Ang-2 ：（0. 30 ± 0. 01 ） μg/L vs. （ 1.79 ± 0. 48）μg/L, t = 2. 34, P 〈 0. 05 ; （2. 02 ± 0. 26） mg/L vs. （6. 20 ± 1.42）mg/L,t = 2. 58 ,P 〈 0.05 ]. （3）The adverse reaction in the treatment group was fewer than the control group and the security of rosuvastatin treatment on MS was fine. Conclusion Rosuvastatin can reduce plasma Ang-2 and hs-CRP levels and improve insulin resistance in patients with MS. Its security is fine.

作者李波刘微微沃金善

机构地区青岛大学医学院附属医院海阳分院心内科青岛大学医学院附属医院心内科

出处《中国综合临床》 2012年第8期845-848,共4页 Clinical Medicine of China

关键词瑞舒伐他汀代谢综合征胰岛素抵抗血管生成素-2 超敏C反应蛋白 Rosuvastatin Metabolic syndrome Insulin resistance Angiopoietin-2 High- sensitivity C-reactive protein

分类号 R589 [医药卫生—内分泌]

引文网络
相关文献

参考文献18

1Soares R, Costa C. Oxidative stress, inflammation and angiogenesis in the metabolic syndrome [ M ]. Germany : Springer verlag, 2009 : 163.
2翟斐,李素梅.胰岛素抵抗与血管内皮功能障碍共同发病机制的研究进展[J].国际内科学杂志,2008,35(7):390-393. 被引量：10
3Du X, Edelstein D, Brownlee M. Oral benfotiamine plus alpha-lipoic acid normalises complication-causing pathways in type 1 diabetes [ J]. Diabetologia,2008,51 (10) :1930-1932.
4Gonzalez AS, Guerrero DB, Soto MB, et al. Metabolic syndrome, insulin resistance and the inflammation markers C-reactive protein and ferritin [J]. Eur J Clin Nutr,2006,60(6) :802-809.
5Rodilla E,Costa JA, Mares S, et al. Impact of metabolic syndrome on CRP levels [ J ]. Rev Clin Esp ,2006,206 (8) :363-368.
6Iwasaki T, Nakajima A, Yoneda M, et al. Relationship between the serum concentrations of C-reaetive protein and parameters of adiposity and insulin resistance in patients with type 2 diabetes mellitus [ J]. Endocr J,2006,53 (3) :345-356.
7Fornengo P, Bosio A, Epifani G, et al. Prevalence of silent myocardial ischaemia in new-onset middle-aged Type 2 diabetic patients without other cardiovascular risk factors [ J]. Diabet Med, 2006,23 (7) :775-779.
8Goldin A, Beckman JA, Schmidt AM, et al. Advanced glyeation end products : sparking the development of diabetic vascular injury [ J ]. Circulation ,2006,114 (6) :597-605.
9Jandeleit-Dahm K, Cooper ME. The role of AGEs in cardiovascular disease [ J]. Curr Pharm Des,2008,14(10) :979-986.
10乔平,王圣,吴忠,陈关良,马建林,苏哲坦.冠心病并代谢综合征患者血清糖基化终末产物的水平及其临床意义[J].临床心血管病杂志,2008,24(9):662-664. 被引量：4

二级参考文献144

1李雷,夏勇,杨煜,史春志,田乃亮,蒋文龙,李东野.肱动脉血流介导的舒张功能与冠状动脉病变的关系[J].临床心血管病杂志,2006,22(5):288-290. 被引量：11
2麦劲壮,李河,方积乾,刘小清,饶栩栩.Meta分析中失安全系数的估计[J].循证医学,2006,6(5):297-300. 被引量：140
3李中东,焦正,王宏图.胆固醇吸收抑制剂——依折麦布[J].中国药学杂志,2007,42(10):797-798. 被引量：9
4王朝晖.对代谢综合征防治模式的新思考[J].临床心血管病杂志,2007,23(6):401-402. 被引量：4
5Expert panel on detection, evaluation and treatment of high blood cholesterol in adults. Executive summary of the third report of the national cholesterol education program (ncep) expert panel on detection, evaluation, and treatment of high blood cholesterol in adults (adult treatment panel III)[J]. JAMA, 2001, 285; 2486--2497.
6HAFFNER S M, MIETTNEN H, STERN M P, et al. The homestasis model in the san antonio heart study[J].Diabetes Care, 1997, 20 : 1087-- 1092.
7KANAUCHI M, TSUJIMOTO N, HASHIMOTO T. Advancedglycation end products in nondiabetic patients with coronary artery disease[J]. Diabetes Care, 2001,24 :1620-- 1623.
8PEPPA M, URIBARRI J, VLASSARA H. The role of advancedglycation end products in the development of atherosclerosis[J]. Curr Diab Rep, 2004,4:31 -- 36.
9TANAKA N, YONEKURA H, YAMAGISHI S, et al. The receptor for advanced glycation end products is induced by the glycation products themselves and tumor necrosis factor alpha through nuclear factor kappa B, and by 17beta estradiol through Sp21 in human vascular endothelial cells[J]. J Biol Chem, 2000, 275:25781--25790.
10YAMAGISHI S, INAGAKI Y, OKAMOTO T, et al. Advancedglycation end product2induced apoptosis and overexpression of vascular endothelial growth factor and monocyte chemoattractant protein21 in human cultured mesangial cells[J]. J Biol Chem, 2002, 277 :20309--20315.

共引文献60

1田娜.他汀类药物在糖尿病血管病变应用的新进展[J].慢性病学杂志,2013,13(11):840-842. 被引量：4
2余婧,王伟,黄建华.腹主动脉瘤药物干预的研究进展[J].中国血管外科杂志（电子版）,2016,8(2):160-163. 被引量：1
3柳岚,吴静,雷闽湘.胰岛素抵抗和2型糖尿病大鼠主动脉内皮功能的变化及罗格列酮的影响[J].国际内科学杂志,2009,36(6):311-314.
4朱馨媛,郭彩霞,张立克,杜凤和.血浆内源性sRAGE、esRAGE、cRAGE对冠心病及其并发急性心肌梗死的诊断价值[J].临床心血管病杂志,2010,26(7):517-520. 被引量：8
5潘俏凤.他汀类药物在稳定动脉粥样硬化斑块的作用机制[J].中国现代药物应用,2011,5(8):10-11. 被引量：1
6滕秋叶,唐召力,覃碧云,张治坤,唐海莲,陈海玉.服药疗程对血脂康与辛伐他汀调脂效果的影响[J].中国综合临床,2011,27(9):910-913. 被引量：1
7田文华,杨禹娟,张小兰.国产普伐他汀钠治疗高脂血症的疗效观察[J].中国医药,2011,6(11):1310-1311. 被引量：4
8李波,刘微微,沃金善.瑞舒伐他汀对代谢综合征患者血清血管生成素2和炎症因子水平的影响[J].中国全科医学,2012,15(21):2402-2404. 被引量：6
9陈康.他汀类药物防治相关疾病研究现状[J].武警后勤学院学报（医学版）,2012,21(10):836-840. 被引量：10
10谢燕,唐巧云,郑海建,张威,王进红.2型糖尿病肾病凝血异常相关因素分析[J].中国综合临床,2012,28(10):1009-1012. 被引量：8

1李少军,张永红,韩冬,刘璐,朱燕亭,冯维,李凤娟,李满祥.COPD急性加重期血浆Ang-2的变化及临床意义[J].中华肺部疾病杂志（电子版）,2015,8(3):5-9. 被引量：2
2方唯一.调脂药在急性冠脉综合征的预防和治疗作用[J].医师进修杂志,2002,25(2):11-13. 被引量：1
3容凯.调脂治疗的新进展及合理用药[J].引进国外医药技术与设备,1998,4(1):99-101.
4邹晓波.调脂药物的合理应用[J].国际医药卫生导报,2002,8(02B):133-135. 被引量：1
5调脂药可以治疗不稳定型心绞痛吗[J].求医问药,2005,0(10):22-22.
6常建.如何防治糖尿病并发症 (八)并发血脂异常的糖尿病患者如何治疗[J].求医问药,2011(11):11-11.
7叶卫军,周伟全,杜凌超.瑞舒伐他汀治疗代谢综合征的疗效观察[J].海峡药学,2015,27(10):143-144. 被引量：1
8徐济民.高血压伴高脂血症病人怎样选用调脂药？[J].家庭用药,2002(6):19-19.
9徐济民.高血压伴高脂血症怎样选用调脂药[J].江苏卫生保健（今日保健）,2006(1):26-27.
10陈炳汀,林义兆.血脂康对高脂血症的疗效[J].心血管康复医学杂志,2004,13(3):278-279. 被引量：3

中国综合临床

2012年第8期

浏览历史

内容加载中请稍等...

瑞舒伐他汀对代谢综合征患者血清血管生成素-2和超敏C反应蛋白的影响

参考文献18

二级参考文献144

共引文献60

相关作者

相关机构

相关主题

浏览历史