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纤溶酶原激活物抑制剂-1/组织型纤溶酶原激活物的基因多态性与同种异体移植冠状动脉疾病的发生发展

Gene polymorphisms for plasminogen activator inhibitor-1/tissue plasminogen activator and development of allograft coronary artery disease.

作者信息

Benza R L, Grenett H E, Bourge R C, Kirklin J K, Naftel D C, Castro P F, McGiffin D C, George J F, Booyse F M

机构信息

Department of Medicine, Division of Cardiovascular Disease, University of Alabama at Birmingham, Alabama, USA.

出版信息

Circulation. 1998 Nov 24;98(21):2248-54. doi: 10.1161/01.cir.98.21.2248.

DOI:10.1161/01.cir.98.21.2248
PMID:9826310
Abstract

BACKGROUND

Impaired fibrinolytic activity has been linked to the presence and severity of allograft vasculopathy (Tx CAD). This impairment may be associated with the presence of certain fibrinolytic protein gene polymorphisms.

METHODS AND RESULTS

To investigate the relation between donor-specific fibrinolytic protein genotypes and Tx CAD, we identified donor plasminogen activator inhibitor-1 (PAI-1) HindIII and tissue plasminogen activator (TPA) EcoRI restriction fragment length polymorphisms-based genotypes by Southern blot analysis in 48 recipients of cardiac allografts and correlated these genotypes with the development of CAD. No association was found between donor TPA genotypes and the presence of Tx CAD. Among the 48 patients, 17% were homozygous for the 1/1 PAI-1 genotype, 51% for the 2/2 PAI-1 genotype, and 32% for the 1/2 PAI-1 genotype. The actuarial freedom from any CAD for the recipients with each respective donor PAI-1 genotype at 12 and 24 months was 100% and 100% for the 1/1 PAI-1 genotype, 92% and 92% for the 1/2 PAI-1 genotype, and 75% and 45% for the 2/2 PAI-1 genotype (P=0.03). Recipients with a diseased 2/2 PAI-1 genotyped allograft had longer ischemic times (P=0.02) than those recipients with a Tx CAD-free allograft.

CONCLUSIONS

These data suggest that recipients with a 2/2 PAI-1 genotype are at a significant risk of developing Tx CAD. This genotype may serve as a useful screening tool for predicting the future development of Tx CAD.

摘要

背景

纤溶活性受损与同种异体移植血管病变(移植后冠心病)的发生及严重程度相关。这种损害可能与某些纤溶蛋白基因多态性的存在有关。

方法与结果

为了研究供体特异性纤溶蛋白基因型与移植后冠心病之间的关系,我们通过Southern印迹分析确定了48例心脏移植受者基于纤溶酶原激活物抑制剂-1(PAI-1)HindIII和组织纤溶酶原激活物(TPA)EcoRI限制性片段长度多态性的基因型,并将这些基因型与冠心病的发生情况相关联。未发现供体TPA基因型与移植后冠心病的存在之间存在关联。在48例患者中,17%为PAI-1基因型1/1纯合子,51%为PAI-1基因型2/2纯合子,32%为PAI-1基因型1/2杂合子。具有各供体PAI-1基因型的受者在12个月和24个月时无任何冠心病的精算生存率,PAI-1基因型1/1者为100%和100%,PAI-1基因型1/2者为92%和92%,PAI-1基因型2/2者为75%和45%(P=0.03)。具有患病的PAI-1基因型2/2的同种异体移植物的受者比无移植后冠心病的同种异体移植物的受者缺血时间更长(P=0.02)。

结论

这些数据表明,具有PAI-1基因型2/2的受者发生移植后冠心病的风险显著增加。这种基因型可作为预测移植后冠心病未来发展的有用筛查工具。

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