Impaired oxidation of debrisoquine in patients with perhexiline neuropathy.

Shah, Rahul; Oates, N S; Idle, Jeffrey R.; Smith, Richard L.; Lockhart, J. D. F.

doi:10.1136/bmj.284.6312.295

Cited by 204 publications

(80 citation statements)

References 25 publications

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“…It has been shown that perhexiline-induced liver disease and neuropathy are more frequent in poor hydroxylators when tested with debrisoquine or sparteine (Shah et al, 1982;Morgan et al, 1984). This observation is paralleled by an increased phospholipid accumulation in nervous tissue of rats with a similar genetic hydroxylation defect (Meier et al, 1986).…”

Section: Introductionsupporting

confidence: 53%

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Differences in hepatic drug accumulation and enzyme induction after chronic amiodarone feeding of two rat strains: role of the hydroxylator phenotype?

Pirovino

Honegger

Müller

et al. 1990

British J Pharmacology

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It has previously been shown that the extent of hepatic phospholipidosis induced by chronic amiodarone treatment correlates with the degree of drug accumulation in liver tissue. To investigate a possible influence of pharmacogenetic factors, biochemical and morphological investigations were carried out in two rat strains differing in debrisoquine hydroxylation. Plasma and liver tissue concentrations of amiodarone and its main metabolite, desethyl‐amiodarone, were significantly higher in rats with deficient hydroxylation. Microsomal enzyme induction, drug cytochrome P‐450 complex formation and typical ultrastructural features of phospholipidosis were only seen in rats with deficient hydroxylation and in a more sensitive species, the guinea‐pig. It remains to be seen whether deficient debrisoquine hydroxylation in man is associated with an increased susceptibility to amioadarone side effects.

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Section: Introductionsupporting

confidence: 53%

“…However, the fact that drug accumulation and metabolism are so different in the two rat strains studied, points to a possible influence of pharmacogenetic factors on the susceptibility to amiodarone side effects in man. This has been demonstrated for drugs such as perhexiline (Shah et al, 1982;Morgan et al, 1984;Meier et al, 1986).…”

Section: Discussionmentioning

confidence: 99%

Differences in hepatic drug accumulation and enzyme induction after chronic amiodarone feeding of two rat strains: role of the hydroxylator phenotype?

Pirovino

Honegger

Müller

et al. 1990

British J Pharmacology

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“…The advantage of these modifications is that phenotyping can be offered on a same-day basis. This would be of considerable value when used in a clinical context such as the need to prescribe perhexiline, a drug known to be metabolised by debrisoquine pathway and having significant neurological and hepatic toxicity -0.7 (Shah et al, 1982). The fact that debrisoquine is highly water soluble and is excreted unchanged by the kidneys as well as undergoing extensive first pass metabolism in EM subjects, makes it an ideal drug for population surveys.…”

Section: Discussionmentioning

confidence: 99%

Debrisoquine oxidation in an Australian population.

Peart¹,

Boutagy²,

Shenfield³

1986

Brit J Clinical Pharma

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1 The standard laboratory method for determination of debrisoquine phenotype has been modified and shortened with no loss of sensitivity. Debrisoquine metabolic ratios (MR) at 4 and 8 h showed excellent correlation indicating that collection time can also be shortened. Same day phenotyping is therefore possible. 2 One hundred normal, Caucasian Australian subjects were phenotyped (46 males, 54 females) and 6% were poor metabolisers (PM) of debrisoquine. 3 Fifty of the original subjects were also acetylation phenotyped and 34% were fast and 66% slow acetylators. One PM of debrisoquine was a fast acetylator of sulphadimidine and four PM were slow acetylators. This was a non-significant association.

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“…In addition to debrisoquine, this isoenzyme is responsible for the genetic polymorphic oxidation of 30 other drugs, including dextromethorphan and perhexiline maleate (Eichelbaum, 1982;Larrey, 1986 (Eichelbaum, 1982;Larrey, 1986). There is a clear association between impairment of debrisoquine oxidation and susceptibility to perhexiline neuropathy (Shah et al, 1982).…”

Section: Introductionmentioning

confidence: 99%

Extensive oxidative metabolism of dextromethorphan in patients with almitrine neuropathy.

Bélec¹,

Larrey²,

Crémoux³

et al. 1989

Brit J Clinical Pharma

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Almitrine bismesylate can induce a stereotypical sensory peripheral neuropathy probably through a toxic mechanism. High plasma concentrations of almitrine have been reported in a patient with neuropathy. Since large inter‐individual variations in plasma drug concentrations are found it is possible that the development of toxicity may be linked to genetically determined polymorphic oxidation of the drug. Oxidation phenotyping was performed in fifteen patients with almitrine neuropathy using dextromethorphan, a test compound subject to oxidative metabolism similar to that of debrisoquine. All patients were of the extensive metaboliser phenotype. This result shows that, in contrast to perhexiline neuropathy, almitrine neuropathy is not related to slow oxidation of the compound with regard to the particular P‐450 iso‐enzyme involved in dextromethorphan and debrisoquine metabolism.

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Impaired oxidation of debrisoquine in patients with perhexiline neuropathy.

Cited by 204 publications

References 25 publications

Differences in hepatic drug accumulation and enzyme induction after chronic amiodarone feeding of two rat strains: role of the hydroxylator phenotype?

Differences in hepatic drug accumulation and enzyme induction after chronic amiodarone feeding of two rat strains: role of the hydroxylator phenotype?

Debrisoquine oxidation in an Australian population.

Extensive oxidative metabolism of dextromethorphan in patients with almitrine neuropathy.

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