Dörner Andrea, Giessen Stefanie, Gaub Regina, Grosse Siestrup Helga, Schwimmbeck Peter L, Hetzer Roland, Poller Wolfgang, Schultheiss Heinz-Peter
Charité University Medicine, Campus Benjamin Franklin, Department of Cardiology, Berlin, Germany.
Eur J Heart Fail. 2006 Jan;8(1):81-9. doi: 10.1016/j.ejheart.2005.05.003. Epub 2005 Aug 16.
Impaired mitochondrial ADP/ATP transport and altered adenine nucleotide translocase (ANT) isoform expression characterized by enhanced ANT1 and decreased ANT2 expression have been implicated in the pathophysiology of dilated cardiomyopathy (DCM). It is still unknown whether restricted ANT function results from exogenous factors, or mutations in the ANT genes, or whether the imbalance in the isoform composition causes the reduced ADP/ATP transport. We performed DNA mutation screening of ANT genes and analyzed the kinetic properties of ANT protein isolated from DCM hearts and controls in a reconstituted system excluding natural environmental influences.
A G1409T polymorphism in ANT2 leads to an exchange from Arg111 to Leu111 in healthy blood donors (n = 60) with allele frequencies of 76% and 24%. This polymorphism was neither associated with DCM (74%, 26%; n = 93) nor with altered myocardial ANT isoform expression or restricted ANT function (89%, 11%; n = 8). However, there was a remarkable reduction in the maximum transport activity (v(max)) of reconstituted ANT from DCM hearts with altered ANT isoform expression (498 +/- 113 micromol min(-1) g(-1) incorporated protein vs. 1112 +/- 178 micromol min(-1) g(-1) incorporated protein, p < 0.01). Moreover, the substrate affinity of DCM myocardial ANT to ATP was slightly reduced with an increased K(m) value of 104.3 +/- 2.4 microM vs. 90.4 +/- 2.9 microM in controls (p < 0.03).
The altered isoform expression in DCM hearts entails changes in the kinetic properties of total ANT protein restricting ANT function and contributing to disturbed energy metabolism in DCM.
线粒体 ADP/ATP 转运受损以及腺嘌呤核苷酸转位酶(ANT)亚型表达改变,其特征为 ANT1 增强和 ANT2 表达降低,已被认为与扩张型心肌病(DCM)的病理生理学有关。目前尚不清楚 ANT 功能受限是由外源性因素、ANT 基因突变导致的,还是亚型组成的失衡导致 ADP/ATP 转运减少。我们对 ANT 基因进行了 DNA 突变筛查,并在排除自然环境影响的重组系统中分析了从 DCM 心脏和对照中分离出的 ANT 蛋白的动力学特性。
在健康献血者(n = 60)中,ANT2 基因的 G1409T 多态性导致 Arg111 替换为 Leu111,等位基因频率分别为 76%和 24%。这种多态性既与 DCM(74%,26%;n = 93)无关,也与心肌 ANT 亚型表达改变或 ANT 功能受限无关(89%,11%;n = 8)。然而,在 ANT 亚型表达改变的 DCM 心脏中,重组 ANT 的最大转运活性(v(max))显著降低(掺入蛋白为 498±113 μmol min⁻¹ g⁻¹ 对比掺入蛋白为 1112±178 μmol min⁻¹ g⁻¹,p < 0.01)。此外,DCM 心肌 ANT 对 ATP 的底物亲和力略有降低,K(m)值增加,对照中为 90.4±2.9 μM,DCM 中为 104.3±2.4 μM(p < 0.03)。
DCM 心脏中 ANT 亚型表达的改变导致总 ANT 蛋白动力学特性发生变化,限制了 ANT 功能,并导致 DCM 能量代谢紊乱。
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