Literature DB >> 10612272

Anticonvulsant hypersensitivity syndrome: incidence, prevention and management.

S R Knowles1, L E Shapiro, N H Shear.   

Abstract

Although the anticonvulsant hypersensitivity syndrome was first described in 1950, confusion still abounds regarding the syndrome. The triad of fever, rash and internal organ involvement occurring 1 to 8 weeks after exposure to an anticonvulsant heralds this rare (1 in 1,000 to 10,000 exposures) but serious reaction. Aromatic anticonvulsants [phenytoin, phenobarbital (phenobarbitone) and carbamazepine] are the most frequently involved drugs; however, there have also been several cases of anticonvulsant hypersensitivity syndrome associated with lamotrigine. Fever, in conjunction with malaise and pharyngitis, is often the first sign. This is followed by a rash which can range from a simple exanthem to toxic epidermal necrolysis. Internal organ involvement usually involves the liver, although other organs such as the kidney, CNS or lungs may be involved. Hypothyroidism may be a complication in these patients approximately 2 months after occurrence of symptoms. The aromatic anticonvulsants are metabolised to hydroxylated aromatic compounds, such as arene oxides. If detoxification of this toxic metabolite is insufficient, the toxic metabolite may bind to cellular macromolecules causing cell necrosis or a secondary immunological response. Cross-reactivity among the aromatic anticonvulsants may be as high as 75%. In addition, there is a familial tendency to hypersensitivity to anticonvulsants. Discontinuation of the anticonvulsant is essential in patients who develop symptoms compatible with anticonvulsant hypersensitivity syndrome. A minimum battery of laboratory tests, such as liver transaminases, complete blood count and urinalysis and serum creatinine, should be performed. Corticosteroids are usually administered if symptoms are severe. Patients with anticonvulsant hypersensitivity syndrome should avoid all aromatic anticonvulsants; benzodiazepines, valproic acid (sodium valproate) or one of the newer anticonvulsants can be used for seizure control. However, valproic acid should be used very cautiously in the presence of hepatitis. There is no evidence that lamotrigine cross-reacts with aromatic anticonvulsants. In addition, family counselling is a vital component of patient management.

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Year:  1999        PMID: 10612272     DOI: 10.2165/00002018-199921060-00005

Source DB:  PubMed          Journal:  Drug Saf        ISSN: 0114-5916            Impact factor:   5.606


  105 in total

1.  Cross sensitivity of skin rashes with antiepileptic drugs.

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Journal:  Can J Neurol Sci       Date:  1997-08       Impact factor: 2.104

2.  Lymphocyte-stimulation tests and patch tests to carbamazepine hypersensitivity.

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Journal:  Clin Exp Immunol       Date:  1977-08       Impact factor: 4.330

3.  Fatal course of toxic epidermal necrolysis under treatment with lamotrigine.

Authors:  M Sterker; J Berrouschot; D Schneider
Journal:  Int J Clin Pharmacol Ther       Date:  1995-11       Impact factor: 1.366

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Journal:  Am J Clin Pathol       Date:  1980-10       Impact factor: 2.493

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9.  The anticonvulsant hypersensitivity syndrome.

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Journal:  Br J Dermatol       Date:  1993-08       Impact factor: 9.302

10.  Mycosis fungoides-like lesions associated with phenytoin therapy.

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Journal:  Arch Dermatol       Date:  1985-09
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  49 in total

1.  Should celecoxib be contraindicated in patients who are allergic to sulfonamides?

Authors:  Bengt-Erik Wiholm
Journal:  Drug Saf       Date:  2002       Impact factor: 5.606

Review 2.  Reactive metabolites and adverse drug reactions: clinical considerations.

Authors:  Sandra R Knowles; Lori E Shapiro; Neil H Shear
Journal:  Clin Rev Allergy Immunol       Date:  2003-06       Impact factor: 8.667

3.  Phenobarbital-induced bullous lesions in a non-comatose patient.

Authors:  Michael Keng; Maritza Lagos; Michael R Liepman; Kimberly Trever
Journal:  Psychiatry (Edgmont)       Date:  2006-12

4.  [DRESS syndrome after carbamazepine].

Authors:  G Wurpts; H Ott; A Schlüter; M Häusler
Journal:  Hautarzt       Date:  2007-11       Impact factor: 0.751

5.  Establishing causality in pediatric adverse drug reactions: use of the Naranjo probability scale.

Authors:  Marina Avner; Yaron Finkelstein; Dan Hackam; Gideon Koren
Journal:  Paediatr Drugs       Date:  2007       Impact factor: 3.022

6.  Is it time for drug sensitivity genetic screening?

Authors:  Carl W Bazil
Journal:  Curr Neurol Neurosci Rep       Date:  2009-07       Impact factor: 5.081

7.  Adverse Cutaneous Drug Reactions Associated with Old- and New- Generation Antiepileptic Drugs Using the Japanese Pharmacovigilance Database.

Authors:  Keiko Hosohata; Ayaka Inada; Saki Oyama; Iku Niinomi; Tomohito Wakabayashi; Kazunori Iwanaga
Journal:  Clin Drug Investig       Date:  2019-04       Impact factor: 2.859

8.  Evaluation of the patients diagnosed with Stevens Johnson syndrome and toxic epidermal necrolysis: a single center experience.

Authors:  Şükrü Çekiç; Yakup Canıtez; Nihat Sapan
Journal:  Turk Pediatri Ars       Date:  2016-09-01

Review 9.  Anticonvulsant hypersensitivity syndrome in children: incidence, prevention and management.

Authors:  Alberto Verrotti; Daniela Trotta; Carmela Salladini; Francesco Chiarelli
Journal:  CNS Drugs       Date:  2002       Impact factor: 5.749

10.  Drug hypersensitivity to previously tolerated phenytoin by carbamazepine-induced DRESS syndrome.

Authors:  Cheol-Woo Kim; Gwang-Seong Choi; Chang-Ho Yun; Deok-In Kim
Journal:  J Korean Med Sci       Date:  2006-08       Impact factor: 2.153

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