A novel ryanodine receptor mutation and genotype-phenotype correlation in a large malignant hyperthermia New Zealand Maori pedigree

Brown, Rosemary L.; Pollock, Avrum N.; Couchman, Kenneth George; Hodges, Michael; Hutchinson, David; Waaka, Rupene; Lynch, Patrick J.; McCarthy, Tommie V.; Stowell, Kathryn M.

doi:10.1093/hmg/9.10.1515

Cited by 91 publications

(52 citation statements)

References 46 publications

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“…Twenty-three differences in the nucleotide sequence were detected (Table 1). Among these, 19 alterations were silent nucleotide substitutions, 17 of which corresponded to previously reported sequence substitutions (9,15,22,23), and the other three differences were new polymorphisms. None of the 26 previously reported RYR1 mutations associated with MH and/ or CCD (1 -3, 12 -16) was detected in our patients.…”

Section: Screening Of Ryr1 Mutations In the Group 3 Mh Patientsmentioning

confidence: 63%

“…The C-terminal region of RyR1 has been overlooked in the search for MH-associated mutations for some time. Recent sequencing of the complete RyR1 cDNAs from a patient from a Mexican CCD family (14), a patient from a New Zealand Maori MH pedigree (15), and a MH patient from a French family (16) revealed a new region responsible for MH / CCD in the channel region of RyR (MH/ CCD region 3). The novel mutation L4838V in RYR1 found in our MH patients is the first mutation to be located in the transmembrane segment of the channel region, which can be in a broad sense categorized in the MH/CCD region 3.…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, deduced amino acid at position 1832 of RyR1 is Glycine in the human genomic DNA sequence database (accession number AC011469 of DDBJ, EMBL and Genbank). The Q3756E mutation was found only in patient #86, and it was also reported to be a polymorphism not associated with MH (15). Therefore, these two alterations, A1832G and Q3756E, are unlikely to be associated with the MH symptoms.…”

Section: Screening Of Ryr1 Mutations In the Group 3 Mh Patientsmentioning

confidence: 94%

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

Oyamada

Oguchi

Saitoh

et al. 2002

Japanese Journal of Pharmacology

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ABSTRACT-Malignant hyperthermia (MH) is a pharmacogenetical complication of general anesthesia resulting from abnormal Ca 2+ -induced Ca 2+ release (CICR) via the type 1 ryanodine receptor (RyR1) in skeletal muscles. In this study, we analyzed the genomic DNAs prepared for determination of all the 106 exons of the RyR1 gene from blood samples donated by two MH patients with extremely high CICR rates in their biopsied skeletal muscles and a clear history of MH incidence. Two novel point mutations were found in the exons 96 and 101 with alterations in the coded amino acids within the C-terminal channel region, i.e., Pro4668 to Ser and Leu4838 to Val. The latter mutation was found in both MH patients. Rabbit RyR1 channels carrying corresponding mutations were expressed in CHO cells for functional assay. It was found that the L to V but not the P to S mutation of the RyR1 resulted in enhanced Ca 2+ release activity. These results indicate that the L4838V mutation is responsible for the MH incidence. The L4838V mutation is unique because it is the mutation first found within a hydrophobic transmembrane segment of the channel region and should provide further information on the function of the RyR1 as well as for genetic diagnosis of MH.Keywords: Calcium, Sarcoplasmic reticulum, Skeletal muscle, Mutation, General anesthesia Malignant hyperthermia (MH) is a serious complication of general anesthesia triggered by commonly used inhalational anesthetics (1 -3). The typical symptoms include a rapid increase in body temperature and induction of a hypermetabolic state with skeletal muscle rigidity. These symptoms, if not immediately reversed, result in death of the patient. The predisposition to MH is inherited as an autosomal dominant trait. The first hint of the nature of the abnormality in MH patients was obtained when Kalow et al. (4) demonstrated that the patients' muscle has a higher sensitivity than normal muscle to the contracture-inducing action of caffeine applied with or without halothane as a potentiator. It has been shown that caffeine or halothane accelerates the Ca 2+ -induced Ca 2+ release (CICR) mechanism in the sarcoplasmic reticulum (SR) of striated muscle (5, 6). Endo et al. (6) demonstrated that both Ca 2+ sensitivity and the maximum rate of CICR in an MH patient were much higher than those in control human muscles. Thus, induction of muscle contracture due to pharmacological enhancement of CICR by inhalational anesthetics in addition to a genetic basis of CICR acceleration was considered to be the primary cause of elevated body temperature in MH episodes. Furthermore, a cluster analysis based on the rates of CICR in 84 patients suspected of having MH objectively classified the patients into three groups, and a strong correlation was identified between the clinical signs of MH during anesthesia and the acceleration of CICR (7).The channel protein responsible for the CICR was isolated through its high-affinity binding of the plant alkaloid ryanodine; hence it is called the ryanodine receptor (RyR). The...

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Section: Screening Of Ryr1 Mutations In the Group 3 Mh Patientsmentioning

confidence: 63%

Section: Discussionmentioning

confidence: 99%

Section: Screening Of Ryr1 Mutations In the Group 3 Mh Patientsmentioning

confidence: 94%

See 1 more Smart Citation

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

Oyamada

Oguchi

Saitoh

et al. 2002

Japanese Journal of Pharmacology

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“…When more stringent definitions were required to produce an MHS diagnosis from IVCT results, fewer individuals were discordant. When MHS was diagnosed only at an IVCT threshold of 1.2 g contracture in the presence of 2.0 mM caffeine and 1.8 g tension in the presence of 2% halothane, there was no discordance between diagnosis by IVCT and by genotype in this family [19]. Unfortunately, most families do not include such a large number of well-studied individuals.…”

Section: Discordancementioning

confidence: 86%

“…In some cases, discordance has been resolved by redefining the cut-off values for the contracture test results [18,19]. This is a reasonable approach if the family is large enough to evaluate linkage with MHS because the definition of positive contracture threshold was based on a large population of subjects.…”

Section: Discordancementioning

confidence: 99%

The Genetics of Malignant Hyperthermia

Brandom

2005

Anesthesiology Clinics of North America

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A recessive form of central core disease, transiently presenting as multi‐minicore disease, is associated with a homozygous mutation in the ryanodine receptor type 1 gene

Ferreiro

Monnier²,

Romero

et al. 2002

Annals of Neurology

191

138

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Multi-minicore disease is an autosomal recessive congenital myopathy characterized by the presence of multiple, short-length core lesions (minicores) in both muscle fiber types. These lesions being nonspecific and the clinical phenotype being heterogeneous, multi-minicore disease boundaries remain unclear. To identify its genetic basis, we performed a genome-wide screening in a consanguineous Algerian family in which three children presented in infancy with moderate weakness predominant in axial muscles, pelvic girdle and hands, joint hyperlaxity (hand involvement phenotype), and multiple minicores. We mapped the disease to chromosome 19q13 in this family and, subsequently, in three additional families showing a similar phenotype, with a maximum LOD score of 5.19 for D19S570. This locus was excluded in 16 other multi-minicore disease families with predominantly axial weakness, scoliosis, and respiratory insufficiency ("classical" phenotype). In the Algerian family, we identified a novel homozygous missense mutation (P3527S) in the ryanodine receptor type 1 gene, a positional candidate gene responsible for the autosomal dominant congenital myopathy central core disease. New muscle biopsies from the three patients at adulthood demonstrated typical central core disease with rods; no cores were found in the healthy parents. This subgroup of families linked to 19q13 represents the first variant of central core disease with genetically proven recessive inheritance and transient presentation as multi-minicore disease.

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A novel ryanodine receptor mutation and genotype-phenotype correlation in a large malignant hyperthermia New Zealand Maori pedigree

Cited by 91 publications

References 46 publications

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

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

The Genetics of Malignant Hyperthermia

A recessive form of central core disease, transiently presenting as multi‐minicore disease, is associated with a homozygous mutation in the ryanodine receptor type 1 gene

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