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Information about Malignant Hyperthermia

Malignant hyperthermia
Classification & external resources
ICD-10T88.3
ICD-9995.89
OMIM145600 154275 154276 600467 601887 601888
DiseasesDB7776
MeSHD008305
Malignant hyperthermia (MH or MHS for "malignant hyperthermia syndrome", or "malignant hyperpyrexia due to anaesthesia") is a rare life-threatening condition that is triggered by exposure to drugs used for general anaesthesia, such as volatile anaesthetics or the depolarizing muscle relaxant suxamethonium chloride. In susceptible individuals, these drugs can induce a drastic and uncontrolled increase in skeletal muscle oxidative metabolism which overwhelms the body's capacity to supply oxygen, remove carbon dioxide, and regulate body temperature, eventually leading to circulatory collapse and death if untreated. MH is often inherited as an autosomal dominant disorder, for which there are at least 6 loci of interest. MH is phenotypically and genetically related to central core disease (CCD), an autosomal dominant disorder characterized both by MH symptoms and myopathy. MH is sometimes confused with the neuroleptic malignant syndrome, but the two syndromes are distinct.

Signs, symptoms and diagnosis

The phenomenon presents with muscular rigidity, followed by a hypermetabolic state with increased oxygen consumption, increased carbon dioxide production (hypercarbia), metabolic acidosis, tachycardia, and an increase in body temperature (hyperthermia) at a rate of up to ~2°C per hour. This is followed by a breakdown of muscle cells (rhabdomyolysis), which release their contents such as myoglobin, creatine kinase (CK/CPK) and potassium, into the bloodstream.

Triggers

Halothane, a once popular but now rarely used volatile anaesthetic, has been linked to a large proportion of cases, however, all halogenated volatile anaesthetics are potential triggers of malignant hyperthermia. Succinylcholine, a neuromuscular blocking agent, is also a trigger for MH. MH does not occur with every exposure to triggering agents, and susceptible patients may undergo multiple uneventful episodes of anesthesia before developing an episode of MH. The symptoms usually develop within one hour after exposure to trigger substances, but may even occur several hours later in rare instances.

Susceptibility testing

The standard procedure to test persons suspected of being susceptible is the "caffeine-halothane contracture test", CHCT. A muscle biopsy is carried out at an approved research center, under local anesthesia. The fresh biopsy is bathed in solutions containing caffeine or halothane and observed for contraction; under good conditions, the sensitivity is 97% and the specificity 78%.[1] Negative biopsies are not definitive, so any patient who is suspected of MH by their medical history or that of blood relatives is generally treated with non-triggering anesthetics even if the biopsy was negative. Some researchers advocate the use of the "calcium-induced calcium release" test in addition to the CHCT to make the test more specific.

There is also a protocol for investigating people with a family history of MH, where first-line genetic screening of RYR1 mutations is one of the options.[2]

Pathophysiology

Disease mechanism

Malignant hyperthermia is caused in a large proportion (50-70%) of cases by a mutation of the ryanodine receptor (type 1), located on the sarcoplasmic reticulum (SR), the organelle within skeletal muscle cells that stores calcium.[3][4] RYR1 opens in response to increases in intracellular Ca2+ level mediated by L-type calcium channels, thereby resulting in a drastic increase in intracellular calcium levels and muscle contraction. RYR1 has two sites believed to be important for reacting to changing Ca2+ concentrations: the A-site and the I-site. The A-site is a high affinity Ca2+ binding site that mediates RYR1 opening. The I-site is a lower affinity site that mediates the protein's closing. Caffeine, Halothane, and other triggering agents act by drastically increasing the affinity of the A-site for Ca2+ and concomitantly decreasing the affinity of the I-site in mutant proteins. Mg2+ also affect RYR1 activity, causing the protein to close by acting at either the A- or I-sites. In MH mutant proteins, the affinity for Mg2+ at either or these site is greatly reduced. The end result of these alterations is greatly increased Ca2+ release due to a lowered activation and heightened deactivation threshold.[5][6] The process of reabsorbing this excess Ca2+ consumes large amounts of ATP (adenosine triphosphate), the main cellular energy carrier, and generates the excessive heat (hyperthermia) that is the hallmark of the disease. The muscle cell is damaged by the depletion of ATP and possibly the high temperatures, and cellular constituents "leak" into the circulation, including potassium, myoglobin, creatine and creatine kinase.

The other known causative gene for MH is CACNA1S, which encodes and L-type voltage-gated calcium channel α-subunit. There are two known mutations in this protein, both affecting the same residue, R1086.[7][8] This residue is located in the large intracellular loop connecting domains 3 and 4, a domain possibly involved in negatively regulating RYR1 activity. When these mutant channels are expressed in HEK 293 cells, the resulting channels are 5x more sensitive to activation by caffeine (and presumably Halothane) and activate at 5-10mV more hyperpolarized. Furthermore, cells expressing these channels have an increased basal cytosolic Ca2+ concentration. As these channels interact with and activate RYR1, these alterations result in a drastic increase of intracellular Ca2+, and, thereby, muscle excitability.[9]

In contrast, the neuroleptic malignant syndrome consists of a defect in the central nervous system manifesting in altered responses to dopamine antagonist drugs. Rigidity and hyperthermia can result, but the mechanisms do not involve altered calcium regulation as in MH.

Other chromosomal mutations causing MH have been identified, although in most cases the relevant gene remains to be identified.[2]

Animal model

Research into malignant hyperthermia was limited until the discovery of "porcine stress syndrome" in Landrace pigs, a condition in which stressed pigs develop "pale, soft, exudative" flesh (a manifestation of the effects of malignant hyperthermia) rendering their meat unmarketable at slaughter. This "awake triggering" was not observed in humans, and initially cast doubts on the value of the animal model, but subsequently susceptible humans were discovered to "awake trigger" (develop malignant hyperthermia) in stressful situations. This supported the use of the pig model for research. Pig farmers use halothane cones in swine yards to expose piglets to halothane. Those that die were MH-susceptible, thus saving the farmer the expense of raising a pig whose meat he would not be able to market.

Gillard et al discovered the causative mutation in humans only after similar mutations had first been described in pigs.

Horses also suffer from malignant hyperthermia. It is the Thoroughbred breed that was found to have this etiology. It can be caused by overwork, anesthesia, or stress. An inheritable genetic mutation is found in susceptible animals. [10]

An MH mouse has been constructed, bearing the R163C prevalent in many humans. These mice display symptoms similar to human MH patients, including sensitivity to Halothane (increased respiration, body temperature, and death). Blockade of RYR1 by Dantrolene prevents adverse reaction to Halothane in these mice, as with humans. Muscle from these mice also shows increased K+-induced depolarization and an increased caffeine sensitivity.[11]

Genetics

At least 70 mutations in the ryanodine receptor have been described, which are transmitted in an autosomal dominant fashion. The gene is located on the long arm of the nineteenth chromosome (19q13.1). These mutations tend to cluster in one of three domains within the protein, designated MH1-3. MH1 and MH2 are located in the N-terminus of the protein, which interacts with L-type calcium channels and Ca2+. MH3 is located in the transmembrane forming C-terminus. This region is important for allowing Ca2+ passage through the protein following opening.

Epidemiology

The incidence has been reported to be between 1:4,500 to 1:60,000 procedures involving general anaesthesia. This disorder occurs worldwide and affects all racial groups. Most cases however occur in children and young adults, which might be related to the fact that many older people will have already had surgeries and thus would know about and be able to avoid this condition.

Treatment

The current treatment of choice is the intravenous administration of dantrolene, discontinuation of triggering agents, and supportive therapy directed at correcting hyperthermia, acidosis, and organ dysfunction. Treatment must be instituted rapidly on clinical suspicion of the onset of malignant hyperthermia.

Dantrolene is a muscle relaxant that works directly on the ryanodine receptor to prevent the release of calcium. Pretreatment with dantrolene has been advocated in the past to prevent MH, but this is probably unreliable, and the long half-life of the drug may leave patients weak for extended periods. The only sure way to prevent MH is avoid the use of triggering agents in patients known or suspected of being susceptible to MH.

After the widespread introduction of treatment with dantrolene the mortality of malignant hyperthermia fell from 80% in the 1960s to less than 10%.

The substance azumolene, chemically related to dantrolene, is under investigation for use in MH.

History

The syndrome was first recognized in one affected family by Denborough et al in 1962.[12]

References

1. ^ Allen G, Larach M, Kunselman A (1998). "The sensitivity and specificity of the caffeine-halothane contracture test: a report from the North American Malignant Hyperthermia Registry. The North American Malignant Hyperthermia Registry of MHAUS.". Anesthesiology 88 (3): 579-88. PMID 9523799. 
2. ^ Litman R, Rosenberg H (2005). "Malignant hyperthermia: update on susceptibility testing.". JAMA 293 (23): 2918-24. PMID 15956637. 
3. ^ Gillard E, Otsu K, Fujii J, Khanna V, de Leon S, Derdemezi J, Britt B, Duff C, Worton R, MacLennan D (1991). "A substitution of cysteine for arginine 614 in the ryanodine receptor is potentially causative of human malignant hyperthermia.". Genomics 11 (3): 751-5. PMID 1774074. 
4. ^ Galli L, Orrico A, Lorenzini S, Censini S, Falciani M, Covacci A, Tegazzin V, Sorrentino V (2006). "Frequency and localization of mutations in the 106 exons of the RYR1 gene in 50 individuals with malignant hyperthermia.". Hum Mutat 27 (8): 830. PMID 16835904. 
5. ^ Balog E, Fruen B, Shomer N, Louis C (2001). "Divergent effects of the malignant hyperthermia-susceptible Arg(615)-->Cys mutation on the Ca(2+) and Mg(2+) dependence of the RyR1.". Biophys J 81 (4): 2050-8. PMID 11566777. 
6. ^ Yang T, Ta T, Pessah I, Allen P (2003). "Functional defects in six ryanodine receptor isoform-1 (RyR1) mutations associated with malignant hyperthermia and their impact on skeletal excitation-contraction coupling.". J Biol Chem 278 (28): 25722-30. PMID 12732639. 
7. ^ Monnier N, Procaccio V, Stieglitz P, Lunardi J (1997). "Malignant-hyperthermia susceptibility is associated with a mutation of the alpha 1-subunit of the human dihydropyridine-sensitive L-type voltage-dependent calcium-channel receptor in skeletal muscle.". Am J Hum Genet 60 (6): 1316-25. PMID 9199552. 
8. ^ The R1086C mutant has never been published, but has nevertheless been referenced multiple times in the literature, e.g. Jurkatt-Rott et al. 2000. Jurkat-Rott K, McCarthy T, Lehmann-Horn F (2000). "Genetics and pathogenesis of malignant hyperthermia.". Muscle Nerve 23 (1): 4-17. PMID 10590402. 
9. ^ Weiss R, O'Connell K, Flucher B, Allen P, Grabner M, Dirksen R (2004). "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.". Am J Physiol Cell Physiol 287 (4): C1094-102. PMID 15201141. 
10. ^ Valberg SJ, Mickelson JR, Gallant EM, MacLeay JM, Lentz L, de la Corte F (1999). "Exertional rhabdomyolysis in quarter horses and thoroughbreds: one syndrome, multiple aetiologies". Equine Vet J Suppl 30: 533-8. PMID 10659313. 
11. ^ (2006) "Pharmacologic and Functional Characterization of Malignant Hyperthermia in the R163C RyR1 Knock-in Mouse.". Anesthesiology 105 (6): 1164-1175. PMID 17122579. 
12. ^ DENBOROUGH MA, FORSTER JF, LOVELL RR, MAPLESTONE PA, VILLIERS JD (1962). "Anaesthetic deaths in a family". British journal of anaesthesia 34: 395-6. PMID 13885389. 

External links

    [ e]
Consequences of external causes (, )
General external causesForeign body - Burn - Frostbite
Other external causesRadiation poisoning - Hyperthermia - Hypothermia - Immersion foot - Chilblain - Aerosinusitis - Hypoxia - Barotrauma - Altitude sickness - Chronic mountain sickness - Decompression sickness - Asphyxia - Starvation - maltreatment (Physical abuse, Sexual abuse, Psychological abuse) - Motion sickness (Airsickness, Sea-sickness) - Electric shock - Angioedema - Hypersensitivity (Allergy)
Certain early complications of traumaAir embolism - Fat embolism - Crush syndrome/Rhabdomyolysis - Compartment syndrome - Volkmann's contracture
Complications of surgical and medical careSerum sickness - Malignant hyperthermia
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The International Statistical Classification of Diseases and Related Health Problems (most commonly known by the abbreviation ICD
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List of ICD-10 codes. The version for 2007 is available online at [1]

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III Diseases of the blood and blood-forming organs and certain disorders involving the immune mechanism
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The International Statistical Classification of Diseases and Related Health Problems (most commonly known by the abbreviation ICD
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The following is a list of codes for International Statistical Classification of Diseases and Related Health Problems. These codes are in the public domain.

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Hyperpyrexia, NOS
Classifications and external resources

ICD-10 R 50.9
ICD-9 780.6

In medicine, hyperpyrexia is an excessive and unusual elevation of set body temperature greater than or equal to 41.1° Celsius (106°F), or extremely high fever.
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In modern medical practice, general anaesthesia (AmE: anesthesia) is a state of total unconsciousness resulting from general anaesthetic drugs. A variety of drugs are given to the patient that have different effects with the overall aim of ensuring unconsciousness, amnesia
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The volatile anaesthetics are a class of general anaesthetic drugs. They share the property of being liquid at room temperature, but evaporating easily for administration by inhalation (some experts make a distinction between volatile and gas anesthetics on this basis, but both are
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Please assist in recruiting an expert or [ improve this article] yourself. See the talk page for details. This article has been tagged since March 2007.
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Skeletal muscle is a type of striated muscle, usually attached to the skeleton. Skeletal muscles are used to create movement, by applying force to bones and joints; via contraction.
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Cellular respiration describes the metabolic reactions and processes that take place in a cell or across the cell membrane to obtain biochemical energy from fuel molecules and the release of the cells' waste products.
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2, −1
(neutral oxide)
Electronegativity 3.44 (Pauling scale)
Ionization energies
(more) 1st: 1313.9 kJmol−1
2nd: 3388.3 kJmol−1
3rd: 5300.5 kJmol−1

Atomic radius 60 pm
Atomic radius (calc.
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Carbon dioxide is a chemical compound composed of two oxygen atoms covalently bonded to a single carbon atom. It is a gas at standard temperature and pressure and exists in Earth's atmosphere in this state.
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Thermoregulation is the ability of an organism to keep its body temperature within certain boundaries, even when temperature surrounding is very different. This process is one aspect of homeostasis: a dynamic state of stability between an animal's internal environment and its
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Circulatory System is a psychedelic rock musical ensemble formed by musician/painter Will Cullen Hart, and featuring Hannah Jones, Derek Almstead, Peter Erchick, John Fernandes, and Heather McIntosh.
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dominance relationship refers to how the alleles for a locus interact to produce a phenotype.

There are three main kinds of dominance relationships:
  • Simple dominance or complete dominance (simple Mendelian inheritance) over a recessive trait

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MeSH D009135 In medicine, a myopathy is a neuromuscular disease in which the muscle fibers do not function for any one of many reasons, resulting in muscular weakness. "Myopathy" simply means muscle disease (myo- Greek μυσ "muscle" + -pathy Greek "suffering").
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Neuroleptic malignant syndrome (NMS) is a life-threatening, neurological disorder most often caused by an adverse reaction to neuroleptic or antipsychotic drugs.

Causes


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Skeletal muscle is a type of striated muscle, usually attached to the skeleton. Skeletal muscles are used to create movement, by applying force to bones and joints; via contraction.
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2, −1
(neutral oxide)
Electronegativity 3.44 (Pauling scale)
Ionization energies
(more) 1st: 1313.9 kJmol−1
2nd: 3388.3 kJmol−1
3rd: 5300.5 kJmol−1

Atomic radius 60 pm
Atomic radius (calc.
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Carbon dioxide is a chemical compound composed of two oxygen atoms covalently bonded to a single carbon atom. It is a gas at standard temperature and pressure and exists in Earth's atmosphere in this state.
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Definition: to have more than normal CO2 (Carbon dioxide) levels in the blood. Value is usually obtained while performing a basic Chem-7 blood test, which tests for basic electrolyte levels from a blood sample.
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Metabolic acidosis
Classification & external resources

Davenport diagram
ICD-10 E 87.2
ICD-9 276.2

DiseasesDB 92
MedlinePlus 000335
eMedicine emerg/312   med/1458 ped/15

In medicine, metabolic acidosis
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Tachycardia
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ICD-10 R 00.0
ICD-9 785.0

MeSH D013610 Tachycardia is a form of cardiac arrhythmia which refers to a rapid beating of the heart.
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Heat stroke
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ICD-10 T 67.0
ICD-9 992.0

DiseasesDB 5690
MedlinePlus 000056
eMedicine med/956   Heat exhaustion
Classification & external resources

ICD-10 T 67.3 - T 67.5
ICD-9 992.
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MeSH D012206 Rhabdomyolysis is the rapid breakdown of skeletal muscle tissue due to traumatic injury, either mechanical, physical or chemical. The principal result is a large release of the CK enzymes and other cell byproducts into the blood system and acute renal failure
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Myoglobin is a single-chain globular protein of 153 amino acids, containing a heme (iron-containing porphyrin) prosthetic group in the center around which the remaining apoprotein folds.
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Creatine kinase (CK), also known as phosphocreatine kinase or creatine phosphokinase (CPK) is an enzyme (EC 2.7.3.2 ) expressed by various tissue types. It catalyses the conversion of creatine to phosphocreatine, consuming adenosine triphosphate (ATP) and generating
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Potassium (IPA: /pə(ʊ)ˈtasiəm/, /pə'tæsiəm/) is a chemical element. It has the symbol K (Arabic: al qalja
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