Mizon-Gérard Frédérique, de Groote Pascal, Lamblin Nicolas, Hermant Xavier, Dallongeville Jean, Amouyel Philippe, Bauters Christophe, Helbecque Nicole
INSERM U508, Institut Pasteur de Lille, 1 rue Calmette, 59019 Lille cedex, France.
Eur Heart J. 2004 Apr;25(8):688-93. doi: 10.1016/j.ehj.2004.01.015.
To assess the possible effect of functional polymorphisms in matrix metalloproteinase (MMP) gene promoters on the clinical outcome of patients with heart failure.
We studied 444 consecutive patients who were referred to our centre for evaluation of left ventricular dysfunction. We extracted genomic DNA from white blood cells and determined the -1306 C >T MMP-2, -1171 5A > 6A MMP-3, and -1562 C >T MMP-9 polymorphisms. Clinical follow-up (median 717 days) was obtained for 443 patients. The MMP-3 polymorphism had a different impact on cardiac survival in HF patients with ischaemic and non-ischaemic cardiomyopathy (interaction p <0.03). The MMP-3 5A/5A genotype was an independent predictor of cardiac mortality (HR 2.92 [1.23-6.69]; p = 0.01) in patients with non-ischaemic HF. In contrast, there was no evidence for any effect of the MMP-3 genotype on cardiac events in patients with ischaemic cardiomyopathy. The MMP-9 polymorphism was associated with cardiac survival (p < 0.03) independently of HF aetiology. In multivariate analysis, the MMP-9 T allele was an independent predictor of cardiac mortality (HR 1.81 [1.09-3.02]; p = 0.02). Finally, there was no evidence for any association between MMP-2 polymorphism and cardiac survival.
MMP-3 and MMP-9 polymorphisms contribute to variability in cardiac survival in HF patients. These data suggest that MMP genotyping could provide important additional information for refining risk stratification in patients with heart failure. MMP genotyping may help to select patients who could benefit from MMP inhibition.
评估基质金属蛋白酶(MMP)基因启动子功能多态性对心力衰竭患者临床结局的可能影响。
我们研究了连续444例因左心室功能障碍转诊至我院的患者。我们从白细胞中提取基因组DNA,并确定-1306 C>T MMP-2、-1171 5A>6A MMP-3和-1562 C>T MMP-9多态性。443例患者获得了临床随访(中位时间717天)。MMP-3多态性对缺血性和非缺血性心肌病心力衰竭患者的心脏生存率有不同影响(交互作用p<0.03)。MMP-3 5A/5A基因型是非缺血性心力衰竭患者心脏死亡的独立预测因素(HR 2.92[1.23-6.69];p=0.01)。相比之下,没有证据表明MMP-3基因型对缺血性心肌病患者的心脏事件有任何影响。MMP-9多态性与心脏生存率相关(p<0.03),与心力衰竭病因无关。在多变量分析中,MMP-9 T等位基因是心脏死亡的独立预测因素(HR 1.81[1.09-3.02];p=0.02)。最后,没有证据表明MMP-2多态性与心脏生存率之间存在任何关联。
MMP-3和MMP-9多态性导致心力衰竭患者心脏生存率的差异。这些数据表明,MMP基因分型可为完善心力衰竭患者的危险分层提供重要的额外信息。MMP基因分型可能有助于选择可能从MMP抑制中获益的患者。
