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首页> 外文期刊>Basic Research in Cardiology >Novel insights into the mechanisms mediating the local antihypertrophic effects of cardiac atrial natriuretic peptide: role of cGMP-dependent protein kinase and RGS2
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Novel insights into the mechanisms mediating the local antihypertrophic effects of cardiac atrial natriuretic peptide: role of cGMP-dependent protein kinase and RGS2

机译:介导心脏心钠素的局部抗肥厚作用的机制的新见解:cGMP依赖性蛋白激酶和RGS2的作用

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Cardiac atrial natriuretic peptide (ANP) locally counteracts cardiac hypertrophy via the guanylyl cyclase-A (GC-A) receptor and cGMP production, but the downstream signalling pathways are unknown. Here, we examined the influence of ANP on β-adrenergic versus Angiotensin II (Ang II)-dependent (Gs vs. Gαq mediated) modulation of Ca2+ i-handling in cardiomyocytes and of hypertrophy in intact hearts. L-type Ca2+ currents and Ca2+ i transients in adult isolated murine ventricular myocytes were studied by voltage-clamp recordings and fluorescence microscopy. ANP suppressed Ang II-stimulated Ca2+ currents and transients, but had no effect on isoproterenol stimulation. Ang II suppression by ANP was abolished in cardiomyocytes of mice deficient in GC-A, in cyclic GMP-dependent protein kinase I (PKG I) or in the regulator of G protein signalling (RGS) 2, a target of PKG I. Cardiac hypertrophy in response to exogenous Ang II was significantly exacerbated in mice with conditional, cardiomyocyte-restricted GC-A deletion (CM GC-A KO). This was concomitant to increased activation of the Ca2+/calmodulin-dependent prohypertrophic signal transducer CaMKII. In contrast, β-adrenoreceptor-induced hypertrophy was not enhanced in CM GC-A KO mice. Lastly, while the stimulatory effects of Ang II on Ca2+-handling were absent in myocytes of mice deficient in TRPC3/TRPC6, the effects of isoproterenol were unchanged. Our data demonstrate a direct myocardial role for ANP/GC-A/cGMP to antagonize the Ca2+ i-dependent hypertrophic growth response to Ang II, but not to β-adrenergic stimulation. The selectivity of this interaction is determined by PKG I and RGS2-dependent modulation of Ang II/AT1 signalling. Furthermore, they strengthen published observations in neonatal cardiomyocytes showing that TRPC3/TRPC6 channels are essential for Ang II, but not for β-adrenergic Ca2+ i-stimulation in adult myocytes.
机译:心脏心钠素(ANP)通过鸟苷酸环化酶-A(GC-A)受体和cGMP产生局部抵消心脏肥大,但下游信号传导途径尚不清楚。在这里,我们研究了ANP对β-肾上腺素与血管紧张素II(Ang II)依赖性(G s 与G αq介导)对Ca 的调节的影响。心肌细胞的2 + i 处理和完整心脏的肥大。通过电压钳记录和荧光显微镜研究了成年鼠离体心肌细胞中L型Ca 2 + 电流和Ca 2 + i 瞬变。 ANP抑制Ang II刺激的Ca 2 + 电流和瞬变,但对异丙肾上腺素刺激无影响。在缺乏GC-A的小鼠的心肌细胞,环状GMP依赖性蛋白激酶I(PKG I)或G蛋白信号转导因子(RGS)2(PKG I的靶标)的调节剂中,取消了ANP对Ang II的抑制作用。在有条件的,心肌细胞限制性的GC-A缺失(CM GC-A KO)的小鼠中,对外源性Ang II的应答明显加剧。这伴随着Ca 2 + /钙调蛋白依赖性肥厚性信号转导剂CaMKII的激活增加。相反,在CM GC-A KO小鼠中,β-肾上腺素受体诱导的肥大并未增强。最后,虽然在缺乏TRPC3 / TRPC6的小鼠心肌细胞中没有Ang II对Ca 2 + 处理的刺激作用,但异丙肾上腺素的作用没有改变。我们的数据表明,ANP / GC-A / cGMP可以直接拮抗Ca 2 + i 依赖于Ang II的肥大性生长反应,但不能拮抗β-肾上腺素刺激。这种相互作用的选择性取决于Ang II / AT 1 信号的PKG I和RGS2依赖性调节。此外,他们加强了在新生儿心肌细胞中发表的观察结果,表明TRPC3 / TRPC6通道对Ang II至关重要,但对成年心肌细胞的β-肾上腺素Ca 2 + i 刺激不是必需的。

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