Sultiame Explained

Verifiedfields:changed
Verifiedrevid:470474738
Iupac Name:4-(1,1-dioxothiazinan-2-yl)benzenesulfonamide
Aan:Sulthiame
Usan:sulthiame
Tradename:Ospolot
Pregnancy Au:D
Legal Au:S4
Legal Uk:POM
Legal Us:Rx-only
Routes Of Administration:Oral
Bioavailability:100% (oral)
Protein Bound:29%
Metabolism:Hepatic secretion
Elimination Half-Life:24 hours
Excretion:Fecal (10%) and renal (90%)
Cas Number:61-56-3
Atc Prefix:N03
Atc Suffix:AX03
Pubchem:5356
Drugbank:DB08329
Chemspiderid:5163
Unii:I00Q766CZ2
Kegg:D01787
Chembl:328560
C:10
H:14
N:2
O:4
S:2
Smiles:O=S2(=O)N(c1ccc(cc1)S(=O)(=O)N)CCCC2
Stdinchi:1S/C10H14N2O4S2/c11-18(15,16)10-5-3-9(4-6-10)12-7-1-2-8-17(12,13)14/h3-6H,1-2,7-8H2,(H2,11,15,16)
Stdinchikey:HMHVCUVYZFYAJI-UHFFFAOYSA-N

Sultiame (or sulthiame) is a sulfonamide and inhibitor of the enzyme carbonic anhydrase. It is used as an anticonvulsant.

History

Sultiame was first synthesised in the laboratories of Bayer AG in the mid-1950s and eventually launched as Ospolot in Europe and other markets the early 1960s. It never became a registered drug in the United States. The brand was transferred to Desitin GmbH in 1993 and is sold in several European countries, in Israel, Japan, and Australia.

Sultiame became established as a second-line drug for treatment of partial epilepsy in the 1960s and 1970s and was often used in combination with the established anticonvulsant phenytoin. Temporal lobe seizures appeared particularly responsive to sultiame. Doubts subsequently arose as to whether sultiame has intrinsic anticonvulsant properties. After discovering sultiame's ability to raise the blood levels of phenytoin,[1] it was assumed that sultiame would only act in combination with phenytoin. This finding, together with the equivocal results of a study in the US, resulted in a quick decline of sultiame's use. It was only in 1988, that the German child neurologist Hermann Doose discovered its specific effects in benign focal epilepsies of childhood.[2] Today, sulthiame is the drug of choice for benign focal epilepsies of childhood (such as benign rolandic epilepsy) in the German-speaking countries and Israel.[3] [4]

Indications

Historically, sultiame has been used to treat partial seizures. In Australia, it is currently registered for behavioural disorders associated with epilepsy; hyperkinetic behaviour; temporal lobe epilepsy; myoclonic seizures; grand mal attacks; and Jacksonian seizures.[5] In contrast to other sulfonamide drugs, sultiame is devoid of antibacterial activity.

Adverse effects

The more common adverse effects are ataxia, paraesthesia of face and limbs, hyperpnoea, dyspnoea, and anorexia. Less common adverse effects include giddiness, rash, Stevens–Johnson syndrome, nausea, weight loss, leukopenia, headache, psychic changes, depression, drooling, increased pain, frequency of fits, insomnia, status epilepticus. Disturbances in calcium and vitamin D metabolism have been occasionally reported after long-term use.

Interactions

Sultiame taken together with primidone may lead to severe side-effects, including psychotic reactions. The addition of sulthiame to phenytoin therapy has shown to be followed by a rise in the serum levels of phenytoin. Sultiame may also lead to a rise of phenobarbitone blood levels. Alcohol must not be consumed during treatment.

Overdose

Vomiting, hypotension, headache, vertigo, ataxia, metabolic acidosis with hyperpnoea and catatonic state may occur. There is no specific antidote. It is not known whether dialysis may help in case of overdose.

Synthesis

Sulfanilamide can be reacted with ω-chlorobutylsulfonyl chloride and aqueous sodium carbonate to form the presumed intermediate (middle), which spontaneously cyclizes to give the drug.

Notes and References

  1. Hansen JM, Kristensen M, Skovsted L . Sulthiame (Ospolot) as inhibitor of diphenylhydatoin metabolism . Epilepsia . 9 . 1 . 17–22 . March 1968 . 4386877 . 10.1111/j.1528-1157.1968.tb04954.x . 20168357 .
  2. Doose H, Baier WK, Ernst JP, Tuxhorn I, Völzke E . Benign partial epilepsy--treatment with sulthiame . Developmental Medicine and Child Neurology . 30 . 5 . 683–4 . October 1988 . 2906619 . 10.1111/j.1469-8749.1988.tb04809.x . 37726714 .
  3. Debus OM, Kurlemann G . Sulthiame in the primary therapy of West syndrome: a randomized double-blind placebo-controlled add-on trial on baseline pyridoxine medication . Epilepsia . 45 . 2 . 103–8 . February 2004 . 14738417 . 10.1111/j.0013-9580.2004.19003.x . free .
  4. Koepp MJ, Patsalos PN, Sander JW . Sulthiame in adults with refractory epilepsy and learning disability: an open trial . Epilepsy Research . 50 . 3 . 277–82 . August 2002 . 12200218 . 10.1016/s0920-1211(02)00054-2 . 13220334 .
  5. http://www.pharmalab.com.au/resources/5/Ospolot%20PI%20TAB002%20TAB003%20Version0804.pdf Pharmalab Pty Ltd. Product Information Ospolot (Sulthiame).