Effects of caffeine, halothane, and 4-chloro-m-cresol on skeletal muscle lactate and pyruvate in malignant hyperthermia-susceptible and normal swine as assessed by microdialysis.

Abstract	BACKGROUND: Skeletal muscle fibers from malignant hyperthermia (MH)-susceptible humans and swine are markedly more sensitive to ryanodine receptor (RyR1) agonists than those from normal individuals. Reproducible shifts in the dose-response of skeletal muscle to caffeine and halothane are the basis of the current in vitro diagnostic caffeine-halothane contracture test. In an attempt to develop a less invasive MH diagnostic test, the authors determined the effects of RyR1 agonists (caffeine, 4-chloro-m-cresol [4CmC], and halothane) on the adductor muscle with respect to the lactate-pyruvate (L/P) system that was percutaneously dialyzed using a microdialysis technique in homozygous MH-susceptible compared with normal swine. METHODS: Animals were anesthetized (ketamine-propofol) and artificially ventilated. Sets of six CMA/20 microdialysis catheters were implanted; each catheter was perfused with different RyR1 agonist concentrations. After a 30-min equilibration after implantation, one of the catheters was perfused (2 microl/min) with vehicle (0.9% saline or lipid emulsion), and the other five were perfused with caffeine (1-64 mM), 4CmC (0.1-8 mM), or halothane (prepared in lipid emulsion; 10-500 mM). Outflow dialysate fractions collected at 10-min intervals and L/P parameters were measured enzymatically. RESULTS: Only in the MH-susceptible group did all RyR1 agonists increase dialysate L/P in a dose-dependent manner. The dose-effect relations were most prominent with 4CmC. With the halothane lipid emulsion, data scatter was high compared with that of the caffeine group and especially the 4CmC group. There were no signs of global muscle rigidity, systemic hypermetabolism, or a clinical MH episode during microdialysis RyR1 perfusion. CONCLUSIONS: The authors data demonstrate that the in vivo muscle microdialysis of the porcine L/P system reveals distinct differences between MH-susceptible and MH-normal muscle, especially in response to highly specific RyR1 agonists such as 4CmC. The microdialysis L/P technique seems to have an MH diagnostic potential in the clinical setting.
Authors	Saiid Bina, George Cowan, John Karaian, Sheila Muldoon, Paul Mongan, Rolf Bünger
Journal	Anesthesiology (Anesthesiology) Vol. 104 Issue 1 Pg. 90-100 (Jan 2006) ISSN: 0003-3022 [Print] United States
PMID	16394695 (Publication Type: Journal Article, Research Support, Non-U.S. Gov't)
Chemical References	Anesthetics, Dissociative Anesthetics, Inhalation Anesthetics, Intravenous Central Nervous System Stimulants Cresols Electrolytes Ryanodine Receptor Calcium Release Channel Lactic Acid chlorocresol Caffeine Ketamine Pyruvic Acid Creatine Kinase Glucose Halothane Propofol
Topics	Anesthesia, General Anesthetics, Dissociative Anesthetics, Inhalation (pharmacology) Anesthetics, Intravenous Animals Blood Gas Analysis Caffeine (pharmacology) Central Nervous System Stimulants (pharmacology) Creatine Kinase (blood) Cresols (pharmacology) Dose-Response Relationship, Drug Electrolytes (metabolism) Glucose (metabolism) Halothane (pharmacology) Ketamine Lactic Acid (metabolism) Malignant Hyperthermia (genetics, metabolism) Microdialysis Muscle, Skeletal (drug effects, metabolism) Propofol Pyruvic Acid (metabolism) Ryanodine Receptor Calcium Release Channel (drug effects) Swine

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