J.-M. Besson scite author profile

J.-M. Besson

3Publications

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876Citation Statements Given

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Study of urinary excretion of butobarbitone in man in relation to the percentage of ideal body weight.

Cheymol¹,

Bernheim²,

Besson³

et al. 1979

Brit J Clinical Pharma

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I Thirty-three patients with no evidence of endocrine disease, hepatic or renal insufficiency or sleep disorders, were classified in groups 1 to 4 in order of increasing of percentage of ideal body weight (IBW) respectively: < 90% of IBW, 90-120%, 120-180%, and > 180% of IBW. After oral administration of 200 mg butobarbitone, concentration of the intact drug was measured by gas liquid chromatographic assay in urine samples collected during 72 h and at three times in blood. 2 A highly significant negative relationship was found between the cumulative excretion of butobarbitone with urine and the logarithm of the percentage of IBW. In contrast for a given weight, excretion of the drug with urine was found to be weakly correlated with the diuresis. 3 The cumulative urinary elimination of butobarbitone was significantly different between the groups studied, except of the difference between the group 2 and 3 of the patients. No significant difference was found between the renal clearances ofbutobarbitone in the four groups of subjects. 4 We conclude that redistribution of butobarbitone into adipose tissues can explain the obtained results and that obesity modifies the pharmacokinetics of the drug.

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Neurology: Behavioral confirmation of ‘diffuse noxious inhibitory controls’ (DNIC) and evidence for a role of endogenous opiates

Kraus¹,

LeBars²,

Besson³

1982

Pain

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The Pharmacology of Pain

Dickenson¹,

Besson²

1997

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J.-M. Besson

Study of urinary excretion of butobarbitone in man in relation to the percentage of ideal body weight.

Neurology: Behavioral confirmation of ‘diffuse noxious inhibitory controls’ (DNIC) and evidence for a role of endogenous opiates

The Pharmacology of Pain

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