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¡¶ÐÄÔàÔÓÖ¾¡·[ISSN:1009-7236/CN:61-1268/R]

ÆÚÊý:

2005ÄêµÚ6ÆÚ

Ò³Âë:

532-535

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2005-12-05

ÎÄÕÂÐÅÏ¢/Info

Title:

Experimental study of intravascular irradiation phus clopidogel and simvastatin on restenosis

×÷Õß:

Àîºç;  Ф´«Êµ;  ³ÂºÆ

ɽÎ÷Ò½¿Æ´óѧµÚ¶þÒ½ÔºÐÄÄÚ¿Æ, ɽÎ÷ Ì«Ô­ 030001

Author(s):

LI Hong; XIAO Chuanª²shi; CHEN Hao

Department of Cardiology,Sencond Hospital of Shanxi Medical University,Taiyun,Shanxi,030001

¹Ø¼ü´Ê:

ÔÙÏÁÕ­;  Ѫ¹ÜÄÚÕÕÉä;  ÐÁ·¥ËûÍ¡; ÂÈßÁ¸ñÀ×

Keywords:

restenosis;  intravascular irradiation;  simvastatin;  clopidogel

·ÖÀàºÅ:

R543

DOI:

-

ÎÄÏ×±êʶÂë:

A

ÕªÒª:

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Abstract:

AIM To evaluate the preventive effects of intravascular irradiation phus clopidogel and simvastatin on restenosis, and to analyze their synergy. METHODS Male New Zealand rabbit models of restenosis were developed. They were divided into 4 groups: the control group (without any treatment), intravascular irradiation group (ionizing radiation using liquid 32pª²filled balloon catheter), drug group (clopidogel and simvastatin) and combination group (ionizing irradiation combined with clopidogel and simvastatin). At week 2, 4 and 8 after the balloon injury operation, the target vascular sections were cut and stained with HE and histomorphologic changes of the vessels were carefully observed using computer analysis of photomicrograms. ICAMª²1, NFª²¦ÊB and PCNA expressions were detected by inmunohistochemical technique. RESULES Intravascular irradiation treatment significantly inhibited neointimal proliferation. Compared with the control group: lumen area(LA) , intimal thickness (IT), intimal area(IA), and IT/MT and IA/MA ratios of were significantly reduced in a doseª²dependent manner(P<0.05), and PCNA, NFª²¦ÊB and ICAMª²1 expression was also significantly reduced (P<0.05). Compared with combination group: LA, IT, IA, IT/MT and IA/MA of the drug and irradiation group were significantly reduced in a doseª²dependent manner(P<0.05), and PCNA, NFª²kB and ICAMª²1 expressions were significantly lower (P<0.05). CONCLUSION Restenosis can be prevented either by clopidogrel and simvastatin or by intravascular irradiation, while intravascular irradiation combined with medication can exert much better synergistic effects.

²Î¿¼ÎÄÏ×/References

£Û1£ÝWaksman R. Response to radiation therapy in animal restenosis models£ÛJ£Ý. Semin Interv Cardiol, 1997,2:95-101.

£Û2£ÝVerin V, Popowski Y. Intraarterial beta irradiation to reduce restenosis after PTCA. Experimental and clinical experience£ÛJ£Ý. Herz, 1998,23:347-351.

£Û3£ÝWaksman R, Rodriguez JC, Robinson KA, et al. Effect of intravascular irradiation on cell proliferation, apoptosis and vascular remodeling after balloon overstretch injury of porcine coronary arteries£ÛJ£Ý. Circulation, 1997,96:1991-1994.

£Û4£ÝMazur W, Ali MN, Dabaghi SF, et al. High dose rate intracoronary irradiation suppresses neointimal proliferation in the stented and ballooned model of porcine restenosis£ÛJ£Ý. Int J Radiat Oncol Biol Phys,1996,36:777-788.

£Û5£ÝBart J,Smet GL,Klein GL. Metalloproteinase inhibition reduces constructive arterial remodeling after balloon angioplasty£ÛJ£Ý. Circulation, 2000,101:2962-2967.

£Û6£ÝWaksman R, Bhargava B, White L, et al. Intracoronary betaª²radiation therapy inhibits recurrence of inª²stent restenosis£ÛJ£Ý. Circulation, 2000, 101: 1895-1898.

£Û7£ÝFukumoto Y, Libby P, Rabkin E, et al. Statins alter smooth muscle cell accumulation and collagen content in established atheroma of watanabe heritable hyperlipidemic rabbits£ÛJ£Ý. Circulation, 2001,103:993-999.

£Û8£ÝGotto FM, Lipidª²lowering therapy for the primary prevention of coronary heart disease£ÛJ£Ý. J Am Coll Cardiol,1999,33:2078-2088.

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¸üÐÂÈÕÆÚ/Last Update: 2010-01-06