Knollmann Björn C, Kirchhof Paulus, Sirenko Syevda G, Degen Hubertus, Greene Anne E, Schober Tilmann, Mackow Jessica C, Fabritz Larissa, Potter James D, Morad Martin
Department of Pharmacology, Georgetown University Medical Center, 3900 Reservoir Rd, N.W., Washington, DC 20007, USA.
Circ Res. 2003 Mar 7;92(4):428-36. doi: 10.1161/01.RES.0000059562.91384.1A. Epub 2003 Feb 6.
The cardiac troponin T (TnT) I79N mutation has been linked to familial hypertrophic cardiomyopathy and high incidence of sudden death, despite causing little or no cardiac hypertrophy in patients. Transgenic mice expressing mutant human TnT (I79N-Tg) have increased cardiac contractility, but no ventricular hypertrophy or fibrosis. Enhanced cardiac function has been associated with myofilament Ca2+ sensitization, suggesting altered cellular Ca2+ handling. In the present study, we compare cellular Ca2+ transients and electrophysiological parameters of 64 I79N-Tg and 106 control mice in isolated myocytes, isolated perfused hearts, and whole animals. Ventricular action potentials (APs) measured in isolated I79N-Tg hearts and myocytes were significantly shortened only at 70% repolarization. No significant differences were found either in L-type Ca2+ or transient outward K+ currents, but inward rectifier K+ current (IK1) was significantly decreased. More critically, Ca2+ transients of field-stimulated ventricular I79N-Tg myocytes were reduced and had slow decay kinetics, consistent with increased Ca2+ sensitivity of I79N mutant fibers. AP differences were abolished when myocytes were dialyzed with Ca2+ buffers or after the Na+-Ca2+ exchanger was blocked by Li+. At higher pacing rates or in presence of isoproterenol, diastolic Ca2+ became significantly elevated in I79N-Tg compared with control myocytes. Ventricular ectopy could be induced by isoproterenol-challenge in isolated I79N-Tg hearts and anesthetized I79N-Tg mice. Freely moving I79N-Tg mice had a higher incidence of nonsustained ventricular tachycardia (VT) during mental stress (warm air jets). We conclude that the TnT-I79N mutation causes stress-induced VT even in absence of hypertrophy and/or fibrosis, arising possibly from the combination of AP remodeling related to altered Ca2+ transients and suppression of IK1.
心肌肌钙蛋白T(TnT)I79N突变与家族性肥厚型心肌病及高猝死发生率相关,尽管该突变在患者中几乎不引起或不引起心脏肥大。表达突变型人TnT的转基因小鼠(I79N-Tg)心脏收缩力增强,但无心室肥大或纤维化。心脏功能增强与肌丝Ca2+敏感性增加有关,提示细胞Ca2+处理发生改变。在本研究中,我们比较了64只I79N-Tg小鼠和106只对照小鼠在分离的心肌细胞、离体灌注心脏及整体动物中的细胞Ca2+瞬变和电生理参数。在离体I79N-Tg心脏和心肌细胞中测量的心室动作电位(AP)仅在复极化70%时显著缩短。L型Ca2+电流或瞬时外向K+电流未发现显著差异,但内向整流K+电流(IK1)显著降低。更关键的是,电场刺激的I79N-Tg心室肌细胞的Ca2+瞬变减少且衰减动力学缓慢,这与I79N突变纤维的Ca2+敏感性增加一致。当用Ca2+缓冲液透析心肌细胞或用Li+阻断Na+-Ca2+交换器后,AP差异消失。在更高的起搏频率或异丙肾上腺素存在的情况下,与对照心肌细胞相比,I79N-Tg心肌细胞的舒张期Ca2+显著升高。异丙肾上腺素刺激可在离体I79N-Tg心脏和麻醉的I79N-Tg小鼠中诱发室性早搏。自由活动的I79N-Tg小鼠在精神应激(暖空气喷射)期间非持续性室性心动过速(VT)的发生率更高。我们得出结论,即使在没有肥大和/或纤维化的情况下,TnT-I79N突变也会导致应激诱导的VT,这可能是由与Ca2+瞬变改变相关的AP重塑和IK1抑制共同作用引起的。
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