1976
DOI: 10.1136/bmj.1.6014.880
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Serum levels of doxycycline in normal subjects after a single oral dose.

Abstract: he was taking a minimum of 256 units daily. Thereafter the dosage dropped progressively, but seven weeks later he still needed up to 188 units daily. He was then transferred to Actrapid MC. In three days his insulin requirement fell by 36 % to 102 units daily. He was stabilised on twice daily Actrapid MC in a total dose of 112-124 units daily and remained well controlled, with a mean mid-morning blood sugar level of 6-1 mmol/l (110 mg/ 100 ml). His

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Cited by 14 publications
(6 citation statements)
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“…Finally, this work suggests the possibility of repurposing DOX as a faster-acting antiparasitic treatment at higher dosing, whose multiple mechanisms would be expected to limit parasite resistance. Prior studies indicate that 500–600 mg doses in humans achieve sustained serum DOX concentrations ≥ 5 µM for 24–48 hr with little or no increase in adverse effects ( Marlin and Cheng, 1979 ; Adadevoh et al, 1976 ). DOX is currently contraindicated for long-term prophylaxis in pregnant women and young children, two of the major at-risk populations for malaria, due to concerns about impacts on fetal development and infant tooth discoloration, respectively, based on observed toxicities for other tetracyclines ( Gaillard et al, 2018 ).…”
Section: Discussionmentioning
confidence: 99%
“…Finally, this work suggests the possibility of repurposing DOX as a faster-acting antiparasitic treatment at higher dosing, whose multiple mechanisms would be expected to limit parasite resistance. Prior studies indicate that 500–600 mg doses in humans achieve sustained serum DOX concentrations ≥ 5 µM for 24–48 hr with little or no increase in adverse effects ( Marlin and Cheng, 1979 ; Adadevoh et al, 1976 ). DOX is currently contraindicated for long-term prophylaxis in pregnant women and young children, two of the major at-risk populations for malaria, due to concerns about impacts on fetal development and infant tooth discoloration, respectively, based on observed toxicities for other tetracyclines ( Gaillard et al, 2018 ).…”
Section: Discussionmentioning
confidence: 99%
“…Tetracyclines are used extensively in tetracycline-controlled transcriptional activation studies [ 22 ]. Blood doxycycline concentrations between 5 and 15 μg/mL have been reported in humans [ 23 , 24 ], but can accumulate in tissue several-fold [ 25 ]. Detailed pharmacokinetics after long-term use in humans are unknown.…”
Section: Introductionmentioning
confidence: 99%
“…The half-life absorption ranges from 1 to 2 hours when administrated while fasting [175], and the peak concentration varies with dose, being 15.3mg/L (~30 μM) after an oral dose of 500mg [176]. Regarding tissue penetration, doxycycline levels are poor in saliva, below those of serum in bone, skin, fat, tendons and muscle [172,177], and highest in the liver, kidney and digestive tract [173].…”
Section: Doxycyline: Pharmacokinetics Pharmacodynamics and Adverse Ementioning
confidence: 99%