Studies on Blood Serum Levels of Rifampicin in Patients with Normal and Impaired Liver Function

Curci, G; Claar, Ernesto; Bergamini, N.; A, Ninni; Claar, Giovanni M.; Ascione, A; Nitti, V

doi:10.1159/000221455

Cited by 7 publications

(6 citation statements)

References 2 publications

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“…The model predictions in cirrhosis population showed an increase in rifampicin exposure that was consistent with the reported clinical data [73]. In cirrhosis (CP-A) population, the observed and predicted AUC 0–∞ after administration of 10 mg/kg dose of rifampicin was 68.8 and 86.2 µg/mL·h, respectively [53]. Moreover, in comparison with the healthy adults, the mean observed and predicted CL/F values were lower in cirrhotic patients.…”

Section: Discussionsupporting

confidence: 76%

“…All of these pathophysiological changes have been incorporated within Simcyp ® cirrhosis populations (CP, A-C) [38]. Since the clinical PK data were only available in CP-A population, the developed rifampicin-cirrhosis model was evaluated only in CP-A population [53]. The model predictions in cirrhosis population showed an increase in rifampicin exposure that was consistent with the reported clinical data [73].…”

Section: Discussionmentioning

confidence: 80%

“…Observed and predicted plasma concentration-time profiles of rifampicin in cirrhosis patients after oral administration. Cirrhosis patients after oral administration ( A ) 4 mg/kg, ( B ) 6 mg/kg, ( C ) 8 mg/kg and ( D ) 10 mg/kg [53]. The observed data are shown as filled colored circles.…”

Section: Figurementioning

confidence: 99%

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Development and Evaluation of Physiologically Based Pharmacokinetic Drug–Disease Models for Predicting Rifampicin Exposure in Tuberculosis and Cirrhosis Populations

et al. 2019

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The physiologically based pharmacokinetic (PBPK) approach facilitates the construction of novel drug–disease models by allowing incorporation of relevant pathophysiological changes. The aim of the present work was to explore and identify the differences in rifampicin pharmacokinetics (PK) after the application of its single dose in healthy and diseased populations by using PBPK drug–disease models. The Simcyp® simulator was used as a platform for modeling and simulation. The model development process was initiated by predicting rifampicin PK in healthy population after intravenous (i.v) and oral administration. Subsequent to successful evaluation in healthy population, the pathophysiological changes in tuberculosis and cirrhosis population were incorporated into the developed model for predicting rifampicin PK in these populations. The model evaluation was performed by using visual predictive checks and the comparison of mean observed/predicted ratios (ratio(Obs/pred)) of the PK parameters. The predicted PK parameters in the healthy population were in adequate harmony with the reported clinical data. The incorporation of pathophysiological changes in albumin concentration in the tuberculosis population revealed improved prediction of clearance. The developed PBPK drug–disease models have efficiently described rifampicin PK in tuberculosis and cirrhosis populations after administering single drug dose, as the ratio(Obs/pred) for all the PK parameters were within a two-fold error range. The mechanistic nature of the developed PBPK models may facilitate their extension to other diseases and drugs.

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Section: Discussionsupporting

confidence: 76%

Section: Discussionmentioning

confidence: 80%

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Development and Evaluation of Physiologically Based Pharmacokinetic Drug–Disease Models for Predicting Rifampicin Exposure in Tuberculosis and Cirrhosis Populations

et al. 2019

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“…Based on comparing multiple-dose studies, examining rifampicin PK in normal hepatic function at 8, 12, and 16 mg/kg biweekly, or in cirrhosis and other chronic liver diseases at 4, 6, 8, and 10 mg/kg biweekly, Curci and colleagues recommend no more than 6 to 8 mg/kg biweekly for those with severe liver impairment [Curci et al , 1973]. In a 7-day study of 13 patients with cirrhosis and 5 healthy volunteers given 600 mg rifampicin daily, total pretreatment bilirubin was a predictor of rifampicin accumulation.…”

Section: Impact Of Liver Disease On the Pharmacokinetics Of Anti-imentioning

confidence: 99%

Relevance of liver failure for anti-infective agents: from pharmacokinetic alterations to dosage adjustments

Büdingen

González

Tucker

et al. 2014

Therapeutic Advances in Infection

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The liver is a complex organ with great ability to influence drug pharmacokinetics. Due to its wide array of function, its impairment has the potential to affect bioavailability, enterohepatic circulation, drug distribution, metabolism, clearance, and biliary elimination. These alterations differ widely depending on the cause of the liver failure, if it is acute or chronic in nature, the extent of impairment, and comorbid conditions. In addition, effects on liver functions do not occur in a proportional or predictable manner for escalating degrees of liver impairment. The ability of hepatic alterations to influence PK is also dependent on drug characteristics, such as administration route, chemical properties, protein binding, and extraction ratio, among others. This complexity makes it difficult to predict what these effects have on drugs. Unlike certain classes of agents, efficacy of anti-infectives is most often dependent on fulfilling pharmacokinetic/pharmacodynamic targets, such as Cmax/MIC, AUC/MIC, T>MIC, IC50/EC50, or T>EC95. Loss of efficacy, or conversely, increased risk of toxicity may occur in certain circumstances of liver injury. Although important to consider these potential alterations and their effects on specific anti-infectives, many lack data to constitute specific dosing adjustments, making it important to monitor patients for effectiveness and toxicities of therapy.

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“…Therapeutic drug monitoring of isoniazid, pyrazinamide, and rifamycins should be performed, at least initially, to ensure achievement of target exposure. Therapeutic drug monitoring should be repeated every week or every other week for rifamycins during the induction phase because of potentially decreased concentrations due to auto-induction [38,47,48]; (vii) fluoroquinolones, ethambutol, cycloserine, or aminoglycosides may be used in case of hepatotoxicity with first-line agents; (viii) maintenance tuberculosis therapy should include isoniazid and a rifamycin as long as tolerability permits; (ix) the optimal duration is not determined and should be considered on a case-by-case basis. An initial induction/intensive 13 phase of two months is advisable with at least three active antituberculosis drugs [8,9,36].…”

Section: Treatment Of Active Tuberculosis With a Focus On Pharmacological Adjustmentsmentioning

confidence: 99%

A practical approach to tuberculosis diagnosis and treatment in liver transplant recipients in a low-prevalence area

Bosch

Valour

Dumitrescu

et al. 2019

Médecine et Maladies Infectieuses

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Studies on Blood Serum Levels of Rifampicin in Patients with Normal and Impaired Liver Function

Cited by 7 publications

References 2 publications

Development and Evaluation of Physiologically Based Pharmacokinetic Drug–Disease Models for Predicting Rifampicin Exposure in Tuberculosis and Cirrhosis Populations

Development and Evaluation of Physiologically Based Pharmacokinetic Drug–Disease Models for Predicting Rifampicin Exposure in Tuberculosis and Cirrhosis Populations

Relevance of liver failure for anti-infective agents: from pharmacokinetic alterations to dosage adjustments

A practical approach to tuberculosis diagnosis and treatment in liver transplant recipients in a low-prevalence area

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