19 French clinicians believed that bromine was a substitute for iodine, and began using potassium bromide in a variety of disorders without tangible therapeutic effect. In 1857, 31 years after bromine was isolated, Charles Lockock, a London

internist, discovered the anticonvulsant and sedative action of the drug.20 His discovery was one #BMS-354825 datasheet randurls[1|1|,|CHEM1|]# of the many quaint examples of serendipity in which an utterly false theory led to correct, empirical results. Lockock, like most physicians of his time, believed that there was a, cause-effect relationship between masturbation, convulsions, and epilepsy. Bromides were known to curb the sex drive. Lockock’s rationale was to control Inhibitors,research,lifescience,medical epilepsy, ie, convulsions, by reducing the frequency of masturbation.21 The treatment was a success insofar as control of convulsions was concerned. It also brought to attention the sedating properties of the drug. During the second half of the 19th century, potassium bromide and other inorganic bromide salts were widely used as anxiolytic sedatives and anticonvulsants.22 They were undoubtedly effective, although Inhibitors,research,lifescience,medical their relatively low therapeutic efficacy coupled with high toxicity have today all but eliminated them from clinical use.23 Chloral hydrate Similar to potassium bromide, the discovery of the sedative and hypnotic properties of chloral hydrate was also Inhibitors,research,lifescience,medical the result, of an erroneous idea, but, in this case of a,

chemical theory. Chloral, or trichloroacetaldchydc, was first, prepared in 1832 by Justus von Liebig, a professor of chemistry in Giessen (Germany).24 It, was about, 37 years later, in 1 869, that, its hydrate, chloral hydrate, was introduced into clinical therapeutics by Otto Liebreich, a professor of pharmacology Inhibitors,research,lifescience,medical in Berlin.25 Liebreich assumed that one of the components into which chloral hydrate splits in the body is chloroform, and since chloroform induces sleep, so would chloral hydrate. Although no chloroform resulted from the degradation of chloral hydrate, chloral hydrate became the first synthetically produced reliable hypnotic; today, after almost, 140 years, it is still used in clinical practice.17 Lithium Inhibitors,research,lifescience,medical in mood

disorders This discovery and rediscovery of the therapeutic effects of lithium in psychiatry were the result, of false Ketanserin theories about, the etiology of mood disorders. Discovery in the 1880s Lithium is an alkali metal that, was discovered by J. A. Arfvedson in 1817 while analyzing the mineral petalite. The name lithium comes from the Greek “lithos,” stone; it was coined by Jons Jacob Berzelius (1779-1848), who was involved in classifying minerals.26 The substance was first isolated in sufficient, quantity for medical use by R. Bunsscn and A. Mathiesscn, in 1855. Four years later, after the demonstration that lithium carbonate could dissolve urate stones,27 the substance was introduced into medicine for the treatment of gout by Alfred Barring Garrod.