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首页> 外文期刊>The Journal of Physiology >Calsequestrin-1: a new candidate gene for malignant hyperthermia and exertional/environmental heat stroke.
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Calsequestrin-1: a new candidate gene for malignant hyperthermia and exertional/environmental heat stroke.

机译:Calsequestrin-1:恶性高热和劳累性/环境性中暑的新候选基因。

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摘要

Malignant hyperthermia (MH) and exertional/environmental heat stroke (EHS) in humans present as similar life threatening crises triggered by volatile anaesthetics and strenuous exercise and/or high temperature, respectively. Many families (70-80%) diagnosed with MH susceptibility (MHS), and a few with EHS, are linked to mutations in the gene for the ryanodine receptor type-1 (RyR1), Ca(2+) release channel of the sarcoplasmic reticulum (SR) of skeletal muscle and a key protein in excitation-contraction (EC) coupling. However, mutations in the RyR1 gene are not found in all MH families, suggesting that alternative genes remain to be identified. In our laboratory we have recently characterized a novel knockout model lacking skeletal muscle calsequestrin (CASQ1), a SR Ca(2+)-binding protein that modulates RyR1 function, and investigated whether these mice present a MH/EHS-like phenotype. Ablation of CASQ1 results in remodelling of the EC coupling apparatus and functional changes, which in male mice causes a striking increase in the rate of spontaneous mortality and susceptibility to trigger MH-like lethal episodes in response to halothane and heat stress. The demonstration that ablation of CASQ1 results in MH- and EHS-like lethal episodes validates CASQ1 as a viable candidate gene for linkage analysis in MH and EHS families where mutations in RyR1 are excluded.
机译:人体的恶性高热(MH)和运动/环境中暑(EHS)分别是由挥发性麻醉剂和剧烈运动和/或高温引发的类似威胁生命的危机。许多被诊断患有MH易感性(MHS)的家庭(70-80%),以及一些具有EHS的家庭,与肌浆蛋白1型ryanodine受体(RyR1),Ca(2+)释放通道的基因突变相关骨骼肌网状结构(SR)和兴奋收缩(EC)耦合中的关键蛋白。但是,并非在所有MH家族中都发现RyR1基因的突变,这表明仍有待鉴定的替代基因。在我们的实验室中,我们最近表征了一种新型的基因敲除模型,该模型缺乏骨骼肌钙网蛋白(CASQ1),后者是一种可调节RyR1功能的SR Ca(2+)结合蛋白,并研究了这些小鼠是否表现出MH / EHS样表型。 CASQ1的消融导致EC耦合装置的重塑和功能改变,这在雄性小鼠中引起自发死亡率的增加,以及对氟烷和热应激的反应容易触发MH类致死性发作的易感性。 CASQ1消融导致MH和EHS样致命事件的证明证明CASQ1是在MH和EHS家族中进行连锁分析的可行候选基因,其中RyR1的突变被排除在外。

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