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

ÆÚÊý:

2007ÄêµÚ1ÆÚ

Ò³Âë:

53-56

À¸Ä¿:

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³ö°æÈÕÆÚ:

2007-01-01

ÎÄÕÂÐÅÏ¢/Info

Title:

Efficacy and safety of Natroparin in patients undergoing percutaneous coronary intervention

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Author(s):

JI Hui;  JIN LIª²juan;  LI Xueª²qi;  CHEN Song

Department of Cardiology, Fourth Affiliated Hospital, Harbin Medical University, Haerbin 150000, Heilongjiang, China

¹Ø¼ü´Ê:

¸ÎËØ; ÄÇÇü¸ÎËØ; ¾­Æ¤¹Ú×´¶¯Âö½éÈëÖÎÁÆ; Ö÷ÒªÐÄÔàʼþ

Keywords:

Heparin ;  natroparin; percutaneous coronary intervention; major adverse cardiac event

·ÖÀàºÅ:

R5414

DOI:

-

ÎÄÏ×±êʶÂë:

A

ÕªÒª:

Ä¿µÄ ̽ÌÖÄÇÇü¸ÎËØÔÚ¾­Æ¤¹Ú×´¶¯Âö½éÈëÖÎÁÆ(PCI) ÖÐÓ¦ÓõÄÓÐЧÐԺͰ²È«ÐÔ¡£·½·¨ ½«ÎÒÔº2005Äê5ÔÂÖÁ2006 Äê1ÔÂÊÕÖεĹ²172ÀýÐÐPCI ÊõµÄ»¼Õß·ÖΪ2×é¡£A ×éΪPCI ÊõÖÐÓÃÄÇÇü¸ÎËØ(0.1 ml/10 kg),B ×éΪPCIÊõÖÐÓÃÆÕͨ¸ÎËØ(133 ¦Ìkat,1 ¦Ìkat=60 u)¡£A ×é87 (ÄÐ62,Å®25)Àý,ÄêÁä(63¡À3) Ëê¡£B ×é85 (ÄÐ71,Å®14) Àý,ÄêÁä(62¡À2) Ëê¡£PCIÇ°¾²Âö×¢ÉäÄÇÇü¸ÎËØ»òÆÕͨ¸ÎËØ¡£A×éºÍB×éÓÖ·Ö±ð·ÖΪÔñÆںͼ±ÕïPCI¡£³öѪ³Ì¶ÈµÄÅжϸù¾ÝTIMIÑо¿µÄ±ê×¼½øÐС£¹Û²ìËùÓл¼ÕßµÄÐÄÔàʼþ£¨ËÀÍö¡¢ÔÙ¹£ËÀ¡¢ÑªÔËÖؽ¨£©¡£½á¹û Á½×éµÄÒ»°ãÁÙ´²×ÊÁϱȽϲîÒìÎÞÏÔÖøÐÔ¡£A ×éÓëB ×éÊÖÊõ³É¹¦ÂÊ(100 % vs 100%) ; 30 dÄÚÖ÷ÒªÐÄѪ¹Ü²»Á¼Ê¼þ±È½ÏÁ½×é²îÒì¾ùÎÞÏÔÖøÐÔ£»ÔÚÇá΢³öѪ·½ÃæÄÇÇü¸ÎËØÏÔÖøµÍÓÚÆÕͨ¸ÎËØ×é (P<0.05)¡£½áÂÛ ÄÇÇü¸ÎËØÔÚ¼±ÐÔÐļ¡¹£ËÀ»¼ÕßÐÐPCI ÊõÖеÄÓ¦ÓÃÊÇÓÐЧµÄ¡¢°²È«µÄ¡£

Abstract:

AIM To investigate the effectiveness and safety of using Natroparin in PCI. METHODS One hundred and seventyª²two PCI patients, who were hospitalized from May 2005 to January 2006 in the Fourth Affiliated Hospital of Harbin Medical University, were randomly divided into two groups. Natroparin was used in group A (87 patients: 62 males and 25 females, average age 63 ¡À3) and common unfractionated heparin was used in group B (85 patients 71£º males and 14 females, average age 62¡À2). Before PCI, patients in group A were intravenously given Natroparin ( 0.1 ml/10 kg) while those in group B was intravenously given unfractionated heparin (133 ¦Ìkat) for procedural anticoagulation. Bleeding complications were classified according to Thrombolysis in Myocardial Infarction (TIMI) criteria and the bleeding indexes (changes in hemoglobin) were calculated. All the patients were followed up for major adverse clinical events (MACE) such as death, myocardial infarction and need for revascularization for 30 days after PCI. RESULTS No significant difference was found in baseline characteristics between the two groups. The success rate of operation in both groups was 100% (100 % vs 100%). For the 30ª²day followª²up, there was no significant difference in MACE between the two groups but minor hemorrhage in Natroparin group was significantly lower than that in unfractionated heparin group. CONCLUSION The application of Natroparin in PCI is safe and effective.

²Î¿¼ÎÄÏ×/References

£Û1£ÝChoussat R, Montalescot G, Collet JP, et al. A unique, low dose of intravenous enoxaparin in elective percutaneous coronary intervention £ÛJ£Ý. J Am Coll Cardiol, 2002,40(11):1943-1950.

£Û2£ÝKereiakes DJ,Grines C,Fry E,et al.Enoxaparin and abciximab adjunctive pharmacoª²therapy during percutaneous coronary intervention£ÛJ£Ý. J Invasive Cardiol,2001,13(4):272-278.

£Û3£ÝGoodman SG, Fitchett D, Armstrong PW, et al. Randomized evaluation of the safety and efficacy of enoxaparin versus unfractionaª²ted heparin in highª²risk patients with nonª²STª²segment elevation acute coronary syndromª²es receiving the glycoprotein IIb/IIIa inhibitor eptifibatide£ÛJ£Ý. Circulation£¬2003,107(2):238-244.

£Û4£ÝÕÅÏþÁᣬ³Â·½£¬¸ßÔÄ´º,µÈ. µÍ·Ö×Ó¸ÎËØÔÚ¾­Æ¤¹Ú×´¶¯Âö³ÉÐÎÊõÖеÄÓ¦ÓãÛJ£Ý. Öйú½éÈëÐÄÔಡѧÔÓÖ¾,2005,13£¨1£©£º23-24.

£Û5£ÝÖ콨»ª, ÇñÔ­¸Õ, ³Â¾ýÖù,µÈ. ¾­Æ¤¹Ú×´¶¯Âö½éÈëÖÎÁÆÖо²Âö×¢ÉäÄÇÇü¸ÎËصĿ¹ÑªË¨ÁÆЧ¼°°²È«ÐÔÆÀ¼Û£ÛJ£Ý. ÖлªÐÄѪ¹Ü²¡ÔÓÖ¾, 2005,33(4):335-339.

£Û6£ÝHirsh J,Levine MN.Low molecular weight heparin£ÛJ£Ý. Blood,1992,79(1):1-17.

£Û7£ÝHirsh J, Warkentin TE, Raschke R, et al. Heparin and lowª²molecularª²weight heparin: mechanisms of action, pharmacokinetics, dosing considerations, monitoring, efficacy, and safety£ÛJ£Ý. Chest,1998£¬114£¨5£©:489-510.

£Û8£ÝMontalescot G,Philippe F,Ankri A,et al.Early increase of von Willebrand factor predicts adverse outcome in unstable coronary artery diseas beneficial effects of enoxaparin.French Investigators of the ESSENCE Trial£ÛJ£Ý. Circulation,1998,98(4):294-299.

£Û9£ÝFerguson JJ, Antman EM, Bates ER, et al. Combining enoxaparin and IIb/IIIa antagonists in acute coronary syndromes: final results of the National Investigatorsi Collª²aborating on Enoxaparinª²3 (NICE 3) study£ÛJ£Ý. Am Heart J, 2003,146£¨4£© :628-634.

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