Novel Mutations in C-terminal Channel Region of the Ryanodine Receptor in Malignant Hyperthermia Patients

Oyamada, Hideto; Oguchi, K; Saitoh, Naoto; Yamazawa, Toshiko; Hirose, Keikichi; Kawana, Yoko; Wakatsuki, Kazunao; Oguchi, Katsuji; Tagami, Minoru; Hanaoka, Kazuo; Endo, Makoto; Iino, Masamitsu

doi:10.1254/jjp.88.159

Cited by 32 publications

(15 citation statements)

References 38 publications

(26 reference statements)

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“…Using showing much stronger uorescent signal in the cytoplasm than in the nucleus, as previously reported [12][13][14] . These results indicated highly reproducible expression of exogenous RyR1 at the expected location from cell to cell and from clone to clone using this experimental system.…”

Section: Establishment Of Stable Hek293 Cell Lines Induced To Expresssupporting

confidence: 73%

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The Role of a Brain-specific Splice Variant of Ryanodine Receptor Type 1

Hayashi

Oyamada

Yamazawa

et al. 2010

Showa Univ J Med Sci

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Section: Establishment Of Stable Hek293 Cell Lines Induced To Expresssupporting

confidence: 73%

“…View, CA or pBI bidirectional expression vector Clontech 13 . However, the nal size of these expression vectors 250,000 bp was too large for the ef cient expression of both recombinant proteins.…”

Section: Resultsmentioning

confidence: 99%

The Role of a Brain-specific Splice Variant of Ryanodine Receptor Type 1

Hayashi

Oyamada

Yamazawa

et al. 2010

Showa Univ J Med Sci

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“…10 The p.Val4847Leu that co-segregated well with an MHS phenotype within a large French-Canadian family, C-27, is positioned within the putative transmembrane segment and maps to the HS3b ''mutation hot spot'' region in RyR1. 13,38 At least three other closely spaced MH/CCD mutations are located within the same transmembrane segment 33,39,40 (Fig. 3).…”

Section: Discussionmentioning

confidence: 98%

Ryanodine receptor type 1 gene mutations found in the Canadian malignant hyperthermia population

Kraeva

Riazi

Loke

et al. 2011

Can J Anesth/J Can Anesth

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Purpose Malignant hyperthermia (MH) is an autosomal dominant pharmacogenetic disorder that is manifested on exposure of susceptible individuals to halogenated anesthetics or succinylcholine. Since MH is associated primarily with mutations in the ryanodine receptor type 1 (RYR1) gene, the purpose of this study was to determine the distribution and frequency of MH causative RyR1 mutations in the Canadian MH susceptible (MHS) population. Methods In this study, we screened a representative cohort of 36 unrelated Canadian MHS individuals for RYR1 mutations by sequencing complete RYR1 transcripts and selected regions of CACNA1S transcripts. We then analyzed the correlation between caffeine-halothane contracture test (CHCT) results and RYR1 genotypes within MH families. Results Eighty-six percent of patients had at least one RyR1 mutation (31 out of 36), five of which were unrelated individuals who were double-variant carriers. Fifteen of the 27 mutations identified in RYR1 were novel. Eight novel mutations, involving highly conserved amino acid residues, were predicted to be causal. Two of the mutations co-segregated with the MHS phenotype within two large independent families (a total of 79 individuals). Fourteen percent of MHS individuals (five out of 36) carried neither RYR1 nor known CACNA1S mutations. Conclusions The distribution and frequency of MH causative RyR1 mutations in the Canadian MHS population are close to those of European MHS populations. Novel mutations described in this study will contribute to the worldwide pool of MH-associated mutations in the RYR1 gene, ultimately increasing the value of MH genetic diagnostic testing. RésuméObjectif L'hyperthermie maligne (HM) est une maladie pharmacoge´ne´tique he´re´ditaire dominante autosomique qui se manifeste lors de l'exposition des personnes susceptibles a`des anesthe´siques haloge´ne´s ou à la succinylcholine. E´tant donne´que l'HM est principalement associe´e aux mutations au niveau du ge`ne des re´cepteurs de ryanodine de type 1 (RYR1), l'objectif de cette e´tude e´tait de de´terminer la distribution et la fre´quence des mutations RyR1 causant une HM chez la population canadienne susceptible a`l'HM (SHM). Méthode Dans cette e´tude, nous avons examine´une cohorte repre´sentative de 36 personnes canadiennes SHM This article is accompanied by an editorial. Please see Can J Anesth 2011; 58: 6.

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“…Certain MH mutations are believed to cause partial domain unzipping and to destabilize the channel (4,183). However, mutations in the COOH-terminal region, which is probably not directly related to the domain switch, also cause MH (17,179,208).…”

Section: B Malignant Hyperthermiamentioning

confidence: 99%

Calcium-Induced Calcium Release in Skeletal Muscle

Endo¹

2009

Physiological Reviews

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Calcium-induced calcium release (CICR) was first discovered in skeletal muscle. CICR is defined as Ca2+ release by the action of Ca2+ alone without the simultaneous action of other activating processes. CICR is biphasically dependent on Ca2+ concentration; is inhibited by Mg2+, procaine, and tetracaine; and is potentiated by ATP, other adenine compounds, and caffeine. With depolarization of the sarcoplasmic reticulum (SR), a potential change of the SR membrane in which the luminal side becomes more negative, CICR is activated for several seconds and is then inactivated. All three types of ryanodine receptors (RyRs) show CICR activity. At least one RyR, RyR1, also shows non-CICR Ca2+ release, such as that triggered by the t-tubule voltage sensor, by clofibric acid, and by SR depolarization. Maximum rates of CICR, at the optimal Ca2+ concentration in the presence of physiological levels of ATP and Mg2+ determined in skinned fibers and fragmented SR, are much lower than the rate of physiological Ca2+ release. The primary event of physiological Ca2+ release, the Ca2+ spark, is the simultaneous opening of multiple channels, the coordinating mechanism of which does not appear to be CICR because of the low probability of CICR opening under physiological conditions. The coordination may require Ca2+, but in that case, some other stimulus or stimuli must be provided simultaneously, which is not CICR by definition. Thus CICR does not appear to contribute significantly to physiological Ca2+ release. On the other hand, CICR appears to play a key role in caffeine contracture and malignant hyperthermia. The potentiation of voltage-activated Ca2+ release by caffeine, however, does not seem to occur through secondary CICR, although the site where caffeine potentiates voltage-activated Ca2+ release might be the same site where caffeine potentiates CICR.

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Novel Mutations in C-terminal Channel Region of the Ryanodine Receptor in Malignant Hyperthermia Patients

Cited by 32 publications

References 38 publications

The Role of a Brain-specific Splice Variant of Ryanodine Receptor Type 1

The Role of a Brain-specific Splice Variant of Ryanodine Receptor Type 1

Ryanodine receptor type 1 gene mutations found in the Canadian malignant hyperthermia population

Calcium-Induced Calcium Release in Skeletal Muscle

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