Early Development, Identification of Mode of Action, and Use of Dantrolene Sodium

Author:

Pollock Neil A.1,Machon Roslyn G.1,Rosenberg Henry1

Affiliation:

1. From the Department of Anaesthesia and Intensive Care, Midcentral Health, Palmerston North, New Zealand (N.A.P., R.G.M.); and Department of Medical Education and Clinical Research, Saint Barnabas Medical Center, Livingston, New Jersey (H.R.).

Abstract

Abstract Dantrolene—a nitrofurantoin derivative—was developed by Snyder et al. in 1967. After initial discovery of its muscle relaxation potential, investigations in a number of species demonstrated dose-dependent reductions in skeletal muscle tone that were long lasting, relatively nontoxic, and free of adverse effects such as respiratory impairment. Ellis et al. then published a number of papers investigating the means by which dantrolene produced these effects. Using a series of classic physiologic models, Ellis investigated potential sites of action for the new drug, eventually narrowing this down to the intracellular calcium-release mechanism. Ellis went on to play a pivotal role in the discovery of dantrolene’s effectiveness for the treatment of malignant hyperthermia, after reading a scientific bulletin about muscle rigidity in pigs affected by porcine stress syndrome, contacting Gaisford Harrison and sending dantrolene to him for trial.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Anesthesiology and Pain Medicine

Reference48 articles.

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2. The correlation between animal testing procedures and clinical effectiveness of centrally acting muscle relaxants of the mephenesin type.;Ann NY Acad Sci,1956

3. Dantrolene, a direct acting skeletal muscle relaxant.;J Pharm Sci,1973

4. Mechanism of control of skeletal-muscle contraction by dantrolene sodium.;Arch Phys Med Rehabil,1974

5. Effects of dantrolene sodium (F440) on skeletal muscle.;Fed Proc,1971

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