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心力衰竭时钙处理蛋白的调节缺陷。

Defective Ca(2+) handling proteins regulation during heart failure.

机构信息

Department of Biophysics, Second Military Medical University, Shanghai, People's Republic of China.

出版信息

Physiol Res. 2011;60(1):27-37. doi: 10.33549/physiolres.931948. Epub 2010 Oct 15.

DOI:10.33549/physiolres.931948
PMID:20945956
Abstract

Abnormal release of Ca(2+) from sarcoplasmic reticulum (SR) via the cardiac ryanodine receptor (RyR2) may contribute to contractile dysfunction in heart failure (HF). We previously demonstrated that RyR2 macromolecular complexes from HF rat were significantly more depleted of FK506 binding protein (FKBP12.6). Here we assessed expression of key Ca(2+) handling proteins and measured SR Ca(2+) content in control and HF rat myocytes. Direct measurements of SR Ca(2+) content in permeabilized cardiac myocytes demonstrated that SR luminal [Ca(2+)] is markedly lowered in HF (HF: DeltaF/F(0) = 26.4+/-1.8, n=12; control: DeltaF/F(0) = 49.2+/-2.9, n=10; P<0.01). Furthermore, we demonstrated that the expression of RyR2 associated proteins (including calmodulin, sorcin, calsequestrin, protein phosphatase 1, protein phosphatase 2A), Ca(2+) ATPase (SERCA2a), PLB phosphorylation at Ser16 (PLB-S16), PLB phosphorylation at Thr17 (PLB-T17), L-type Ca(2+) channel (Cav1.2) and Na(+)- Ca(2+) exchanger (NCX) were significantly reduced in rat HF. Our results suggest that systolic SR reduced Ca(2+) release and diastolic SR Ca(2+) leak (due to defective protein-protein interaction between RyR2 and its associated proteins) along with reduced SR Ca(2+) uptake (due to down-regulation of SERCA2a, PLB-S16 and PLB-T17), abnormal Ca(2+) extrusion (due to down-regulation of NCX) and defective Ca(2+) -induced Ca(2+) release (due to down-regulation of Cav1.2) could contribute to HF.

摘要

肌浆网(SR)通过心脏兰尼碱受体(RyR2)异常释放 Ca(2+)可能导致心力衰竭(HF)的收缩功能障碍。我们之前的研究表明,HF 大鼠的 RyR2 大分子复合物明显缺乏 FK506 结合蛋白(FKBP12.6)。在这里,我们评估了关键 Ca(2+)处理蛋白的表达,并测量了对照和 HF 大鼠心肌细胞中的 SR Ca(2+)含量。在通透的心肌细胞中直接测量 SR Ca(2+)含量表明,HF 中 SR 腔[Ca(2+)]明显降低(HF:DeltaF/F(0) = 26.4+/-1.8,n=12;对照:DeltaF/F(0) = 49.2+/-2.9,n=10;P<0.01)。此外,我们还证明了 RyR2 相关蛋白(包括钙调蛋白、sorcin、钙调蛋白、蛋白磷酸酶 1、蛋白磷酸酶 2A)、Ca(2+)ATP 酶(SERCA2a)、PLB 丝氨酸 16 位磷酸化(PLB-S16)、PLB 苏氨酸 17 位磷酸化(PLB-T17)、L 型 Ca(2+)通道(Cav1.2)和 Na(+)-Ca(2+)交换体(NCX)的表达在 HF 大鼠中显著降低。我们的结果表明,收缩期 SR 减少了 Ca(2+)释放和舒张期 SR Ca(2+)渗漏(由于 RyR2 与其相关蛋白之间的蛋白-蛋白相互作用缺陷),同时减少了 SR Ca(2+)摄取(由于 SERCA2a、PLB-S16 和 PLB-T17 的下调)、异常的 Ca(2+)外排(由于 NCX 的下调)和缺陷的 Ca(2+)-诱导的 Ca(2+)释放(由于 Cav1.2 的下调)可能导致 HF。

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