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Exclusion of defects in the skeletal muscle specific regions of the DHPR alpha 1 subunit as frequent causes of malignant hyperthermia.

机译：排除DHPR alpha 1亚基骨骼肌特定区域的缺陷是恶性高热的常见原因。

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摘要

The molecular defect predisposing to the majority of malignant hyperthermia (MH) cases is unknown, although various point mutations in the ryanodine receptor gene (RYR1) have been associated with susceptibility in a small proportion of cases. We report here that one of these, the Arg163Cys substitution, does not cosegregate with MH susceptibility. Comparison of cDNA sequences encoding the skeletal muscle specific components of the dihydropyridine receptor alpha 1 subunit between MH susceptible (MHS) and MH non-susceptible (MHN) patients was made in subjects without the reported MH linked RYR1 mutations. There were no differences within the sequence encoding the II-III loop or the IS3/IS3-IS4 segment, excluding defects in these functional segments of the alpha 1 subunit as frequent causes of MH.

机译：尽管在少数病例中，赖氨酸受体基因（RYR1）的各种点突变与易感性相关，但大多数恶性高热（MH）病例的分子缺陷尚不清楚。我们在这里报告，其中之一，Arg163Cys替代，不与MH敏感性共分离。在没有报道MH连锁的RYR1突变的受试者中比较了MH易感（MHS）和MH不敏感（MHN）患者之间编码二氢吡啶受体α1亚基的骨骼肌特定成分的cDNA序列。在编码II-III环或IS3 / IS3-IS4片段的序列内没有差异，除了作为MH常见原因的alpha 1亚基的这些功能片段中的缺陷。

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期刊名称 Journal of Medical Genetics
作者
R O OBrien; N L Taske; P M Hansbro; K I Matthaei; S P Hogan; M A Denborough; P S Foster;
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作者单位

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年(卷),期 1995(32),11
年度 1995
页码 913–914
总页数 2
原文格式 PDF
正文语种
中图分类遗传学;
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专利

1. Amino Acid Residues 489–503 of Dihydropyridine Receptor (DHPR) β1a Subunit Are Critical for Structural Communication between the Skeletal Muscle DHPR Complex and Type 1 Ryanodine Receptor [J] . Jose Eltit, Clara Franzini-Armstrong, Claudio Perez The Journal of biological chemistry . 2014,第52期

机译：二氢吡啶受体（DHPR）β1a亚基的氨基酸残基489-503对于骨骼肌DHPR络合物和1型ryanodine受体之间的结构通信至关重要
2. Multiple regions of the porcine alpha-skeletal actin gene modulate muscle-specific expression in cell culture and directly injected skeletal muscle. [J] . Reecy JM, Bidwell CA, Andrisani OM, Animal Biotechnology . 1998,第2期

机译：猪α-骨架肌动蛋白基因的多个区域调节细胞培养物中的肌肉特异性表达，并直接注射骨骼肌。
3. Functional analysis of the R1086H malignant hyperthermia mutation in the DHPR reveals an unexpected influence of the III-IV loop on skeletal muscle EC coupling. [J] . Weiss RG, OConnell KM, Flucher BE, American Journal of Physiology . 2004,第4期

机译：DHPR中R1086H恶性热疗突变的功能分析揭示了III-IV环对骨骼肌EC耦合的意外影响。
4. Changes in the expression of selected proteins elucidate skeletal muscle type-specific resistance to glucocorticoid-induced muscle cachexia [C] . P. Pawlikowska, M. Lokociejewska, J.F. Hocquette, International Symposium on Energy and Protein Metabolism and Nutrition . 2007

机译：所选蛋白质表达的变化阐明骨骼肌型特异性对糖皮质激素诱导的肌肉恶病症的抗性
5. Skeletal Muscle Metabolic Dysfunction in Patients with Malignant Hyperthermia. [D] . Thompson, Sara J. 2016

机译：恶性高热患者的骨骼肌代谢功能障碍。
6. Amino Acid Residues 489–503 of Dihydropyridine Receptor (DHPR) β1a Subunit Are Critical for Structural Communication between the Skeletal Muscle DHPR Complex and Type 1 Ryanodine Receptor [O] . Jose M. Eltit, Clara Franzini-Armstrong, Claudio F. Perez 2014

机译：二氢吡啶受体（DHPR）β1a亚基的氨基酸残基489–503对骨骼肌DHPR复合体与1型Ryanodine受体之间的结构通讯至关重要
7. Exclusion of defects in the skeletal muscle specific regions of the DHPR alpha 1 subunit as frequent causes of malignant hyperthermia. [O] . O'Brien, R O, Taske, N L, Hansbro, P M, 1995

机译：排除DHPR alpha 1亚基骨骼肌特定区域的缺陷是恶性高热的常见原因。

Exclusion of defects in the skeletal muscle specific regions of the DHPR alpha 1 subunit as frequent causes of malignant hyperthermia.

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