功能失调的corin i555(p568)等位基因与收缩期心力衰竭黑人患者脑钠肽加工受损及不良预后相关:心力衰竭遗传风险评估子研究结果
Dysfunctional corin i555(p568) allele is associated with impaired brain natriuretic peptide processing and adverse outcomes in blacks with systolic heart failure: results from the Genetic Risk Assessment in Heart Failure substudy.
作者信息
Rame J Eduardo, Tam S William, McNamara Dennis, Worcel Manuel, Sabolinski Michael L, Wu Alan H, Dries Daniel L
机构信息
Division of Cardiology, University of California San Francisco, San Francisco, California, USA.
出版信息
Circ Heart Fail. 2009 Nov;2(6):541-8. doi: 10.1161/CIRCHEARTFAILURE.109.866822. Epub 2009 Sep 28.
BACKGROUND
Corin, a transmembrane serine protease expressed in cardiomyocytes, cleaves pro-atrial natriuretic peptide and pro-brain natriuretic peptide (BNP) into biologically active peptide hormones. The minor corin I555(P568) allele, defined by the T555I and Q568P mutations, is common in persons of African ancestry and associated with increased risk for hypertension and cardiac concentric hypertrophy. The corin gene product containing the T555I and Q568P mutations has significantly reduced natriuretic peptide processing capacity. We hypothesized that the corin I555(P568) allele would be associated with adverse outcomes and impaired BNP processing in blacks with systolic heart failure.
METHODS AND RESULTS
This is a retrospective study of 354 subjects in the African American Heart Failure Trial Genetic Risk Assessment in Heart Failure substudy. In the corin variant group (n=50) compared with corin nonvariant group (n=300), BNP-32 (amino acids 77 to 108) was lower (190 pg/mL versus 340 pg/mL, P=0.007), but the ratio of unprocessed BNP(1 to 108)/processed BNP-32 was significantly higher (P=0.05). Stratified analyses were conducted because of evidence of significant interaction between the corin I555(P568) allele and treatment assignment. In the placebo arm, multivariable analysis demonstrated that the corin I555(P568) allele was associated with increased risk for death or heart failure hospitalization (relative risk 3.49; 95% CI, 1.45 to 8.39; P=0.005); however, in the treatment arm (fixed-dose combination isosorbide-dinitrate/hydralazine), the corin I555(P568) allele was not associated with adverse outcomes.
CONCLUSIONS
We have identified a pharmacogenomic interaction in blacks with systolic heart failure. The corin I555(P568) allele is associated with an increased risk for death or heart failure hospitalization in patients receiving standard neurohormonal blockade, but the addition of fixed-dose combination isosorbide-dinitrate/hydralazine ameliorates this risk. A plausible mechanism for this pharmacogenomic interaction is the impaired processing of BNP in carriers of the corin I555(P568) allele as compared with noncarriers.
背景
Corin是一种在心肌细胞中表达的跨膜丝氨酸蛋白酶,可将前心钠素和前脑钠肽(BNP)裂解为具有生物活性的肽类激素。由T555I和Q568P突变定义的次要Corin I555(P568)等位基因在非洲裔人群中很常见,且与高血压和心脏向心性肥厚风险增加相关。含有T555I和Q568P突变的Corin基因产物的利钠肽加工能力显著降低。我们推测,Corin I555(P568)等位基因与收缩性心力衰竭黑人患者的不良预后及BNP加工受损有关。
方法与结果
这是一项对非裔美国人心力衰竭试验心力衰竭亚研究中354名受试者的回顾性研究。与Corin非变异组(n = 300)相比,Corin变异组(n = 50)的BNP - 32(氨基酸77至108)水平较低(190 pg/mL对340 pg/mL,P = 0.007),但未加工的BNP(1至108)/加工后的BNP - 32的比值显著更高(P = 0.05)。由于有证据表明Corin I555(P568)等位基因与治疗分配之间存在显著相互作用,因此进行了分层分析。在安慰剂组中,多变量分析表明Corin I555(P568)等位基因与死亡或心力衰竭住院风险增加相关(相对风险3.49;95%可信区间,1.45至8.39;P = 0.005);然而,在治疗组(固定剂量复方硝酸异山梨酯/肼屈嗪)中,Corin I555(P568)等位基因与不良预后无关。
结论
我们在收缩性心力衰竭黑人患者中发现了一种药物基因组相互作用。Corin I555(P568)等位基因与接受标准神经激素阻滞剂治疗的患者死亡或心力衰竭住院风险增加相关,但添加固定剂量复方硝酸异山梨酯/肼屈嗪可改善这种风险。这种药物基因组相互作用的一个合理机制是,与非携带者相比,Corin I555(P568)等位基因携带者的BNP加工受损。
Zotero 插件