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2. Fasciite nécrosante abdominale secondaire à des auto-injections de produits amincissants achetés sur internet

Author

Grodner, C., primary, Bernigaud, C., additional, Lapadula, S., additional, Beringuer, H., additional, Billiet, P.A., additional, Woerther, P.L., additional, Billon, R., additional, Derhy, H., additional, Haye, B., additional, Hotz, C., additional, Pressiat, C., additional, Vodovar, D., additional, Rodriguez, C., additional, Fabresse, N., additional, Hua, C., additional, De Prost, N., additional, and Chosidow, O., additional

Published
2019
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6. Health products e‐sale should be regulated: a case of necrotizing soft‐tissue infection of the abdomen linked to self‐injection of slimming products purchased on the internet

Author

Lionel Nakad, Jean-Winoc Decousser, Barbara Hersant, Raphaelle Billon, Raphaël Lepeule, Claire Hotz, Saskia Oro, Camille Gomart, Christophe Rodriguez, Simone Lapadula, Claire Pressiat, Pierre‐Antoine Billiet, Camille Hua, Paul-Louis Woerther, Nicolas de Prost, Henri Derhy, Charlotte Bernigaud, Nicolas Fabresse, Cécile Maud Champy, Romain Bosc, Oliver Chosidow, Benjamin Haye, Dominique Vodovar, Jean‐Michel Gracies, Helene Beringuer, Nicola de’ Angelis, Alain Luciani, Camille Grodner, Grodner, C., Bernigaud, C., La Padula, S., Beringuer, H., Billiet, P. -A., Woerther, P. -L., Billon, R., Derhy, H., Haye, B., Hotz, C., Pressiat, C., Vodovar, D., Rodriguez, C., Fabresse, N., de Prost, N., Hua, C., Chosidow, O., Bosc, R., Champy, C., De Angelis, N., Decousser, J. -W., Gomart, C., Gracies, J. -M., Hersant, B., Lepeule, R., Luciani, A., Nakad, L., and Oro, S.

Subjects
medicine.medical_specialty, medicine.anatomical_structure, business.industry, medicine, Abdomen, Self injection, The Internet, Soft tissue infection, Dermatology, business, Surgery
Published
2021
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8. The impact of extracorporeal membrane oxygenation on antifungal pharmacokinetics: A systematic review.

Author

Jendoubi A, Pressiat C, De Roux Q, Hulin A, Ghaleh B, Tissier R, Kohlhauer M, and Mongardon N

Subjects
Humans, Caspofungin, Critical Illness therapy, Micafungin, Antifungal Agents pharmacokinetics, Extracorporeal Membrane Oxygenation
Abstract

Background and Objective: The use of extracorporeal membrane oxygenation (ECMO) as a cardiocirculatory or respiratory support has tremendously increased in critically ill patients. In the setting of ECMO support, invasive fungal infections are a severe cause of morbidity and mortality. This vulnerable population is at risk of suboptimal antifungal exposure due to an increased volume of distribution (Vd), drug sequestration and decreased clearance. Here, we aimed to summarize ex-vivo and clinical studies on the potential impact of ECMO on the pharmacokinetics (PK) of antifungal agents and dosing requirements., Methods: A systematic search of the literature within electronic databases PubMed and EMBASE was conducted from database inception to 30 April 2023. Inclusion criteria were as follows: critically ill patients receiving ECMO regardless of age and reporting at least one PK parameter., Results: Thirty-six studies met inclusion criteria, including seven ex-vivo experiments and 29 clinical studies evaluating three classes of antifungals: polyenes, triazoles and echinocandins. Based on the available ex-vivo PK data, we found a significant sequestration of highly lipophilic and protein-bound antifungals within the ECMO circuit such as voriconazole, posaconazole and micafungin but the PK of several antifungals remains to be addressed such as amphotericin B, isavuconazole and anidulafungin. Most clinical studies have shown increased Vd of some antifungals like fluconazole and micafungin, particularly in the pediatric population. Conflicting data exist about caspofungin exposure., Conclusions: The available literature on the antifungal PK changes in ECMO setting is scarce. Whenever possible, therapeutic drug monitoring is highly advised to personalize antifungal therapy., (Copyright © 2023 Elsevier Ltd and International Society of Antimicrobial Chemotherapy. All rights reserved.)

Published
2024
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9. The novel cyclophilin inhibitor C105SR reduces hepatic ischaemia-reperfusion injury via mitoprotection.

Author

Kheyar A, Ahnou N, Ahmed-Belkacem A, Hulin A, Pressiat C, Ghaleh B, Guichou JF, Morin D, Pawlotsky JM, and Teixeira-Clerc F

Abstract

Background & Aims: Mitochondrial permeability transition pore (mPTP) opening is critical for mediating cell death during hepatic ischaemia-reperfusion injury (IRI). Blocking mPTP opening by inhibiting cyclophilin D (CypD) is a promising pharmacological approach for the treatment of IRI. Here, we show that diastereoisomers of a new class of small-molecule cyclophilin inhibitors (SMCypIs) have properties that make them attractive candidates for the development of therapeutic agents against liver IRI., Methods: Derivatives of the parent SMCypI were synthesised and evaluated for their ability to inhibit CypD peptidyl-prolyl cis - trans isomerase (PPIase) activity and for their mitoprotective properties, evaluated by measuring mitochondrial swelling and calcium retention capacity in liver mitochondria. The ability of the selected compounds to inhibit mPTP opening was evaluated in cells subjected to hypoxia/reoxygenation using a calcein/cobalt assay. Their ability to inhibit cell death was evaluated in cells subjected to hypoxia/reoxygenation by measuring lactate dehydrogenase (LDH) release, propidium iodide staining, and cell viability. The compound performing best in vitro was selected for in vivo efficacy evaluation in a mouse model of hepatic IRI., Results: The two compounds that showed the strongest inhibition of CypD PPIase activity and mPTP opening, C105 and C110, were selected. Their SR diastereoisomers carried the activity of the racemic mixture and exhibited mitoprotective properties superior to those of the known macrocyclic cyclophilin inhibitors cyclosporin A and alisporivir. C105SR was more potent than C110SR in inhibiting mPTP opening and prevented cell death in a model of hypoxia/reoxygenation. Finally, C105SR substantially protected against hepatic IRI in vivo by reducing hepatocyte necrosis and apoptosis., Conclusions: We identified a novel cyclophilin inhibitor with strong mitoprotective properties both in vitro and in vivo that represents a promising candidate for cellular protection in hepatic IRI., Impact and Implications: Hepatic ischaemia-reperfusion injury (IRI) is one of the main causes of morbidity and mortality during or after liver surgery. However, no effective therapies are available to prevent or treat this devastating syndrome. An attractive strategy to prevent hepatic IRI aims at reducing cell death by targeting mitochondrial permeability transition pore opening, a phenomenon regulated by cyclophilin D. Here, we identified a new small-molecule cyclophilin inhibitor, and demonstrated the enhanced mitoprotective and hepatoprotective properties of one of its diastereoisomers both in vitro and in vivo , making it an attractive lead compound for subsequent clinical development., Competing Interests: The authors have no conflict of interest to disclose. Please refer to the accompanying ICMJE disclosure forms for further details., (© 2023 The Authors.)

Published
2023
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10. JAK Inhibition in Aicardi-Goutières Syndrome: a Monocentric Multidisciplinary Real-World Approach Study.

Author

Frémond ML, Hully M, Fournier B, Barrois R, Lévy R, Aubart M, Castelle M, Chabalier D, Gins C, Sarda E, Al Adba B, Couderc S, D' Almeida C, Berat CM, Durrleman C, Espil C, Lambert L, Méni C, Périvier M, Pillet P, Polivka L, Schiff M, Todosi C, Uettwiller F, Lepelley A, Rice GI, Seabra L, Sanquer S, Hulin A, Pressiat C, Goldwirt L, Bondet V, Duffy D, Moshous D, Bader-Meunier B, Bodemer C, Robin-Renaldo F, Boddaert N, Blanche S, Desguerre I, Crow YJ, and Neven B

Subjects
Humans, Signal Transduction, Genetic Testing, Autoimmune Diseases of the Nervous System diagnosis, Autoimmune Diseases of the Nervous System drug therapy, Autoimmune Diseases of the Nervous System genetics, Nervous System Malformations diagnosis, Nervous System Malformations drug therapy, Nervous System Malformations genetics
Abstract

The paradigm type I interferonopathy Aicardi-Goutières syndrome (AGS) is most typically characterized by severe neurological involvement. AGS is considered an immune-mediated disease, poorly responsive to conventional immunosuppression. Premised on a chronic enhancement of type I interferon signaling, JAK1/2 inhibition has been trialed in AGS, with clear improvements in cutaneous and systemic disease manifestations. Contrastingly, treatment efficacy at the level of the neurological system has been less conclusive. Here, we report our real-word approach study of JAK1/2 inhibition in 11 patients with AGS, providing extensive assessments of clinical and radiological status; interferon signaling, including in cerebrospinal fluid (CSF); and drug concentrations in blood and CSF. Over a median follow-up of 17 months, we observed a clear benefit of JAK1/2 inhibition on certain systemic features of AGS, and reproduced results reported using the AGS neurologic severity scale. In contrast, there was no change in other scales assessing neurological status; using the caregiver scale, only patient comfort, but no other domain of everyday-life care, was improved. Serious bacterial infections occurred in 4 out of the 11 patients. Overall, our data lead us to conclude that other approaches to treatment are urgently required for the neurologic features of AGS. We suggest that earlier diagnosis and adequate central nervous system penetration likely remain the major factors determining the efficacy of therapy in preventing irreversible brain damage, implying the importance of early and rapid genetic testing and the consideration of intrathecal drug delivery., (© 2023. The Author(s).)

Published
2023
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11. Impaired Pharmacokinetics of Amiodarone under Veno-Venous Extracorporeal Membrane Oxygenation: From Bench to Bedside.

Author

Lescroart M, Pressiat C, Péquignot B, Tran N, Hébert JL, Alsagheer N, Gambier N, Ghaleh B, Scala-Bertola J, and Levy B

Abstract

Background: Adjusting drug therapy under veno-venous extracorporeal membrane oxygenation (VV ECMO) is challenging. Although impaired pharmacokinetics (PK) under VV ECMO have been reported for sedative drugs and antibiotics, data about amiodarone are lacking. We evaluated the pharmacokinetics of amiodarone under VV ECMO both in vitro and in vivo., Methods: In vitro: Amiodarone concentration decays were compared between closed-loop ECMO and control stirring containers over a 24 h period. In vivo: Potassium-induced cardiac arrest in 10 pigs with ARDS, assigned to either control or VV ECMO groups, was treated with 300 mg amiodarone injection under continuous cardiopulmonary resuscitation. Pharmacokinetic parameters C max , T max AUC and F were determined from both direct amiodarone plasma concentrations observation and non-linear mixed effects modeling estimation., Results: An in vitro study revealed a rapid and significant decrease in amiodarone concentrations in the closed-loop ECMO circuitry whereas it remained stable in control experiment. In vivo study revealed a 32% decrease in the AUC and a significant 42% drop of C max in the VV ECMO group as compared to controls. No difference in T max was observed. VV ECMO significantly modified both central distribution volume and amiodarone clearance. Monte Carlo simulations predicted that a 600 mg bolus of amiodarone under VV ECMO would achieve the amiodarone bioavailability observed in the control group., Conclusions: This is the first study to report decreased amiodarone bioavailability under VV ECMO. Higher doses of amiodarone should be considered for effective amiodarone exposure under VV ECMO.

Published
2022
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12. Health products e-sale should be regulated: a case of necrotizing soft-tissue infection of the abdomen linked to self-injection of slimming products purchased on the internet.

Author

Grodner C, Bernigaud C, Lapadula S, Beringuer H, Billiet PA, Woerther PL, Billon R, Derhy H, Haye B, Hotz C, Pressiat C, Vodovar D, Rodriguez C, Fabresse N, de Prost N, Hua C, and Chosidow O

Subjects
Abdomen, Commerce, Humans, Internet, Fasciitis, Necrotizing, Soft Tissue Infections drug therapy
Published
2022
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13. Population Pharmacokinetics of Amikacin in Patients on Veno-Arterial Extracorporeal Membrane Oxygenation.

Author

Pressiat C, Kudela A, De Roux Q, Khoudour N, Alessandri C, Haouache H, Vodovar D, Woerther PL, Hutin A, Ghaleh B, Hulin A, and Mongardon N

Abstract

Veno-arterial extracorporeal membrane oxygenation (V-A ECMO) support leads to complex pharmacokinetic alterations, whereas adequate drug dosing is paramount for efficacy and absence of toxicity in critically ill patients. Amikacin is a major antibiotic used in nosocomial sepsis, especially for these patients. We aimed to describe amikacin pharmacokinetics on V-A ECMO support and to determine relevant variables to improve its dosing. All critically ill patients requiring empirical antimicrobial therapy, including amikacin for nosocomial sepsis supported or not by V-A ECMO, were included in a prospective population pharmacokinetic study. This population pharmacokinetic analysis was built with a dedicated software, and Monte Carlo simulations were performed to identify doses achieving therapeutic plasma concentrations. Thirty-nine patients were included (control n = 15, V-A ECMO n = 24); 215 plasma assays were performed and used for the modeling process. Patients received 29 (24-33) and 32 (30-35) mg/kg of amikacin in control and ECMO groups, respectively. Data were best described by a two-compartment model with first-order elimination. Inter-individual variabilities were observed on clearance, central compartment volume (V 1 ) , and peripherical compartment volume (V 2 ). Three significant covariates explained these variabilities: Kidney Disease Improving Global Outcomes (KDIGO) stage on amikacin clearance, total body weight on V 1, and ECMO support on V 2 . Our simulations showed that the adequate dosage of amikacin was 40 mg/kg in KDIGO stage 0 patients, while 25 mg/kg in KDIGO stage 3 patients was relevant. V-A ECMO support had only a secondary impact on amikacin pharmacokinetics, as compared to acute kidney injury.

Published
2022
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14. Pharmacokinetics/Pharmacodynamics of Caspofungin in Plasma and Peritoneal Fluid of Liver Transplant Recipients.

Author

Pressiat C, Ait-Ammar N, Daniel M, Hulin A, Botterel F, and Levesque E

Subjects
Antifungal Agents pharmacokinetics, Antifungal Agents therapeutic use, Caspofungin, Echinocandins pharmacokinetics, Echinocandins therapeutic use, Humans, Lipopeptides pharmacology, Lipopeptides therapeutic use, Microbial Sensitivity Tests, Ascitic Fluid, Liver Transplantation
Abstract

The weaker diffusion of echinocandins in the peritoneal fluid (PF) could promote Candida -resistant isolates. The aim of this study was to analyze the pharmacokinetics (PK)/pharmacodynamics (PD) of caspofungin in plasma and PF samples from liver transplant recipients. Liver transplant patients received caspofungin as postoperative prophylaxis. Caspofungin concentrations were quantified in plasma and PF samples on days 1, 3, and 8. Data were analyzed using nonlinear mixed-effect modeling and Monte Carlo simulations. Area under the curve (AUC) values for plasma and PF were simulated under three dosing regimens. Probabilities of target attainment (PTAs) were calculated using area under the unbound plasma concentration-time curve from 0 to 24 h at steady state ( f AUC 0-24 )/MIC ratios, with MICs ranging from 0.008 to 8 mg/L. All of the patients included were monitored weekly for Candida colonization and for Candida infections. Twenty patients were included. The median daily dose of caspofungin was 0.81 mg/kg. Plasma ( n  = 395) and PF ( n  = 50) concentrations at steady state were available. A two-compartment model with first-order absorption and elimination was described. Our two-compartment model with first-order absorption and elimination produced an effective PK/PD relationship in plasma, achieving a PTA of ≥90% with MICs ranging from 0.008 to 0.12 mg/L for Candida albicans and Candida glabrata. In PF, PTAs at D8 were optimal only for a MIC of 0.008 mg/L in patients weighing 60 kg under the three dosing regimens. Among the 16 patients colonized, all MIC values were below the maximal concentration ( C max ) in plasma but not in PF. PF concentrations of caspofungin were low. Simulations showed that the PTAs for Candida spp. in PF were not optimal, which might suggest a potential risk of resistance.

Published
2022
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16. Comparison of three galenic forms of lamivudine in young West African children living with Human Immunodeficiency Virus.

Author

Pressiat C, Dainguy E, Tréluyer JM, Yonaba C, Urien S, Eboua F, Foissac F, Dahourou DL, Bouazza N, Malateste K, Desmonde S, Pruvost A, Leroy V, Hirt D, and Study Group TMA

Subjects
Child, Child, Preschool, Humans, Lamivudine pharmacokinetics, Lamivudine therapeutic use, Tablets therapeutic use, Anti-HIV Agents pharmacokinetics, Anti-HIV Agents therapeutic use, HIV Infections drug therapy, HIV-1
Abstract

Background: Few pharmacokinetic data were reported on dispersible tablets despite their increasing use. One hundred fifty HIV-infected children receiving lamivudine were enrolled in the MONOD ANRS 12,206 trial. Three galenic forms were administered: liquid formulation, tablet form and dispersible scored tablet., Method: HIV-infected children <4 years old were enrolled in the MONOD ANRS 12,206 trial designed to assess the simplification of a successful 12-months lopinavir-based antiretroviral treatment with efavirenz. Lamivudine plasma concentrations were analysed using nonlinear mixed effects modelling approach., Results: One hundred and fifty children (age: 2.5 years (1.9-3.2), weight 11.1 (9.5-12.5) kg (median (IQR)) were included in this study. Over the study period, 79 received only the syrup form, 29 children switched from syrup form to tablet 3TC/AZT form, 36 from syrup to the orodispersible ABC/3TC form and two from the 3TC/AZT form to the orodispersible ABC/3TC form. The 630 lamivudine concentrations were best described by a two-compartment model allometrically scaled. Galenic form had no significant effect on 3TC pharmacokinetic., Conclusion: This trial provided an opportunity to compare three galenic forms (liquid formulation, tablet form and dispersible scored tablet) of lamivudine in the target population of young HIV-1-infected children. Galenic form had no significant effect on lamivudine pharmacokinetics.

Published
2021
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17. Impact of renal function on hydroxyurea exposure in sickle-cell disease patients.

Author

Pressiat C, Rakotoson MG, Habibi A, Barau C, Arrouasse R, Galactéros F, Stehlé T, Audard V, Hulin A, and Bartolucci P

Subjects
Antisickling Agents, Humans, Kidney physiology, Prospective Studies, Anemia, Sickle Cell drug therapy, Hydroxyurea
Abstract

Aims: This prospective study aimed to develop a population pharmacokinetics (PK) model of hydroxyurea (HU) in patients with sickle cell disease. This model can be used to determine the impact of glomerular filtration rate (GFR) on HU kinetics., Methods: We included 30 patients. They underwent HU pharmacokinetics analyses of plasma and urine. Six underwent PK analyses in 2 periods with and without angiotensin-converting enzyme inhibitor. HU was assayed with a validated high-performance liquid chromatography-UV method. Noncompartmental PK analysis was conducted and a population PK model built with Monolix. This model was validated externally on another 56 patients. HU PK was simulated as a function of GFR., Results: The HU PK model was constructed as a 2-compartment model with first-order absorption and elimination. The quality criteria were good, including for external validation. We found that estimated GFR (eGFR) and body weight affected HU PK, with lower eGFR or body weight associated with a higher HU area under the curve. We recommend the monitoring of HU through eGFR and body weight, which together account for 47% of its variability. Urinary HU fractions and renal clearance were higher in the glomerular hyperfiltration group and lower in the moderate chronic kidney disease group, respectively. No differences in nonrenal HU clearance were observed., Conclusion: Estimated GFR has an impact on the kinetics of hydroxyurea, and HU dose should be adapted accordingly. Angiotensin-converting enzyme inhibitor seems to have minor effect on HU PK in adults with sickle cell disease., (© 2020 British Pharmacological Society.)

Published
2021
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18. Life-Saving, Dose-Adjusted, Targeted Therapy in a Patient with a STAT3 Gain-of-Function Mutation.

Author

Sarfati E, Hadjadj J, Fusaro M, Klifa R, Grimaud M, Berteloot L, Hadchouel A, Godot C, Stolzenberg MC, Frémond ML, Pressiat C, Molina T, Fischer A, Picard C, Renolleau S, Rieux-Laucat F, Blanche S, and Neven B

Subjects
Alleles, Disease Management, Genetic Association Studies, Genotype, Germ-Line Mutation, Humans, Immune System Diseases diagnosis, Janus Kinase Inhibitors administration & dosage, Janus Kinase Inhibitors adverse effects, Janus Kinase Inhibitors therapeutic use, Phenotype, Tomography, X-Ray Computed, Treatment Outcome, Gain of Function Mutation, Genetic Predisposition to Disease, Immune System Diseases drug therapy, Immune System Diseases etiology, Molecular Targeted Therapy methods, STAT3 Transcription Factor genetics
Published
2021
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19. [Improvement of the pre-examination phase of medical biology exams at the Henri Mondor University Hospitals: a pilot study].

Author

Breijo S, Pelisse C, Theveny A, Traigneau F, Schabad C, Agbovon O, Salmon P, Arronis Y, Goulas E, Cassereau C, Pressiat C, Challine D, and Bastard JP

Subjects
Accreditation, Allergy and Immunology education, Allergy and Immunology standards, Biology methods, Biology standards, Clinical Laboratory Techniques methods, Cytodiagnosis methods, Cytodiagnosis nursing, Cytodiagnosis standards, Education, Distance standards, Education, Nursing methods, Education, Nursing standards, Educational Status, France, Hospitals, University standards, Humans, Job Satisfaction, Laboratories standards, Nephrology Nursing education, Nephrology Nursing standards, Pilot Projects, Pre-Analytical Phase methods, Specimen Handling methods, Specimen Handling nursing, Students, Nursing, Clinical Laboratory Techniques standards, Pre-Analytical Phase standards, Quality Assurance, Health Care standards, Quality Improvement standards, Specimen Handling standards
Abstract

The medical and university department of biology pathology at Henri Mondor hospital in Créteil has been engaged in an NF EN ISO 15189 accreditation process since 2014. One of the elements of this process concerns the quality of handling of samples and their transportation to laboratories, including the implementation place requires fighting against pre-examination non-conformities, which are the source of many dysfunctions. The pre-examination group has implemented several actions in a targeted care service. Thanks to these, the rate of non-conformities has halved in 18 months. In parallel, a work project targeting student nurses on internship was born to follow up on the results of a statistical study carried out by the pre-examination group on non-conformities. The objective of the project was to include nursing students on internship in a full support course on good sampling practices and pre-analytical non-conformities. This was based on the realization of two knowledge quizzes (before and after training), theoretical training, and visits to several laboratories. This study lasted 10 months with the participation of 37 students. The results showed a marked improvement in knowledge of pre-analytics as well as total satisfaction of all students. Our approach has helped to better understand the needs of laboratories and demonstrates the usefulness of training students in good sampling practices in order to ensure better patient care as well as an improvement in their comfort and well-being.

Published
2020
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20. JAK Inhibition in the Aicardi-Goutières Syndrome.

Author

Neven B, Al Adba B, Hully M, Desguerre I, Pressiat C, Boddaert N, Duffy D, Rice GI, Seabra L, Frémond ML, Blanche S, and Crow YJ

Subjects
Humans, Janus Kinases, Autoimmune Diseases of the Nervous System, Nervous System Malformations genetics
Published
2020
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21. Paracetamol absorption test to detect poor enteric absorption of oseltamivir in intensive care unit patients with severe influenza: a pilot study.

Author

May F, Peytavin G, Fourati S, Pressiat C, Carteaux G, Razazi K, Mekontso Dessap A, and de Prost N

Subjects
Acetaminophen blood, Acetaminophen therapeutic use, Antiviral Agents therapeutic use, Humans, Influenza, Human complications, Influenza, Human physiopathology, Intensive Care Units organization & administration, Intensive Care Units statistics & numerical data, Pilot Projects, Acetaminophen analysis, Gastric Absorption, Influenza, Human blood
Published
2019
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22. Development and Validation of a Simultaneous Quantification Method of Ruxolitinib, Vismodegib, Olaparib, and Pazopanib in Human Plasma Using Liquid Chromatography Coupled With Tandem Mass Spectrometry.

Author

Pressiat C, Huynh HH, Plé A, Sauvageon H, Madelaine I, Chougnet C, Le Maignan C, Mourah S, and Goldwirt L

Subjects
Angiogenesis Inhibitors blood, Chromatography, Liquid methods, Chromatography, Liquid standards, Humans, Indazoles, Nitriles, Poly(ADP-ribose) Polymerase Inhibitors blood, Reproducibility of Results, Anilides blood, Phthalazines blood, Piperazines blood, Pyrazoles blood, Pyridines blood, Pyrimidines blood, Sulfonamides blood, Tandem Mass Spectrometry methods, Tandem Mass Spectrometry standards
Abstract

Background: A simple, rapid, and sensitive liquid chromatography coupled with tandem mass spectrometry method has been developed and validated for the quantification of ruxolitinib, olaparib, vismodegib, and pazopanib in human plasma., Methods: After a simple protein precipitation of plasma samples, the chromatographic separation was performed using an ultraperformance liquid chromatography system coupled with mass tandem spectrometry in a positive ionization mode. The mobile phase consisted of a gradient elution of 10-mmol/L formate ammonium buffer containing 0.1% (vol/vol) formic acid (phase A) and acetonitrile with 0.1% (vol/vol) formic acid (phase B) at a flow rate at 300 µL/min., Results: Analysis time was 5.0 minutes per run, and all analytes and internal standards eluted within 1.5-1.73 minutes. The calibration curves were linear over the range from 10 to 2500 ng/mL for ruxolitinib and from 100 to 100,000 ng/mL for olaparib, vismodegib, and pazopanib with coefficients of correlation above 0.99 for all analytes. The intraday and interday coefficients of variation were below 14.26% and 14.81%, respectively, for lower concentration and below 9.94% and 6.37%, respectively, for higher concentration., Conclusions: Using liquid chromatography coupled with tandem mass spectrometry, we have developed and validated a simple and rapid assay for the simultaneous quantification of olaparib, vismodegib, pazopanib, and ruxolitinib in human plasma. This method is now part of our therapeutic drug monitoring service provision and is currently used clinically to manage patients prescribed these drugs.

Published
2018
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23. Decreased darunavir concentrations during once-daily co-administration with maraviroc and raltegravir: OPTIPRIM-ANRS 147 trial.

Author

Pressiat C, Hirt D, Treluyer JM, Zheng Y, Morlat P, Naqvi A, Tran L, Viard JP, Avettand-Fenoel V, Rouzioux C, Meyer L, and Cheret A

Subjects
Adult, Anti-HIV Agents administration & dosage, Darunavir administration & dosage, Female, HIV Infections drug therapy, HIV-1 isolation & purification, Humans, Male, Maraviroc administration & dosage, Middle Aged, Models, Statistical, Raltegravir Potassium administration & dosage, Ritonavir administration & dosage, Ritonavir pharmacokinetics, Viral Load, Young Adult, Anti-HIV Agents pharmacokinetics, Darunavir pharmacokinetics, Maraviroc pharmacokinetics, Plasma chemistry, Raltegravir Potassium pharmacokinetics
Abstract

Background: The OPTIPRIM-ANRS 147 trial compared intensive combination ART (darunavir/ritonavir, tenofovir disoproxil fumarate/emtricitabine, raltegravir and maraviroc) started early during primary HIV-1 infection with standard tritherapy with darunavir/ritonavir, tenofovir disoproxil fumarate and emtricitabine. From month 6 to 18, the percentage of viral load values <50 copies/mL was lower in the pentatherapy arm than in the tritherapy arm. Here we compared antiretroviral drug concentrations between the two arms., Methods: Plasma samples were collected from 50 patients at various times after drug administration. A Bayesian approach based on published population pharmacokinetic models was used to estimate residual drug concentrations (Ctrough) and exposures (AUC) in each patient. A mixed linear regression model was then used to compare the AUC and Ctrough values of each drug used in both groups., Results: Published models adequately described our data and could be used to predict Ctrough and AUC. No significant difference in tenofovir disoproxil fumarate, emtricitabine and ritonavir parameters was found between the two arms. However, darunavir Ctrough and AUC were significantly lower in the pentatherapy arm than in the tritherapy arm (P = 0.03 and P = 0.04, respectively)., Conclusions: Adding maraviroc and raltegravir to darunavir-based tritherapy decreased darunavir concentrations. Compliance issues, maraviroc-darunavir interaction and raltegravir-darunavir interaction were suspected and may affect the kinetics of viral decay during pentatherapy. A specific pharmacokinetic interaction study is needed to explore the interactions between darunavir and maraviroc and raltegravir.

Published
2018
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24. Suboptimal cotrimoxazole prophylactic concentrations in HIV-infected children according to the WHO guidelines.

Author

Pressiat C, Mea-Assande V, Yonaba C, Treluyer JM, Dahourou DL, Amorissani-Folquet M, Blanche S, Eboua F, Ye D, Lui G, Malateste K, Zheng Y, Leroy V, and Hirt D

Subjects
AIDS-Related Opportunistic Infections immunology, AIDS-Related Opportunistic Infections microbiology, Administration, Oral, Anti-Bacterial Agents blood, Anti-Bacterial Agents pharmacokinetics, Burkina Faso, Child, Preschool, Coinfection, Computer Simulation, Cote d'Ivoire, Female, HIV Infections immunology, Humans, Infant, Male, Metabolic Clearance Rate, Models, Biological, Nonlinear Dynamics, Pneumonia, Pneumocystis immunology, Pneumonia, Pneumocystis microbiology, Trimethoprim, Sulfamethoxazole Drug Combination blood, Trimethoprim, Sulfamethoxazole Drug Combination pharmacokinetics, AIDS-Related Opportunistic Infections prevention & control, Anti-Bacterial Agents administration & dosage, HIV Infections drug therapy, HIV Protease Inhibitors therapeutic use, Lopinavir therapeutic use, Pneumonia, Pneumocystis prevention & control, Practice Guidelines as Topic, Trimethoprim, Sulfamethoxazole Drug Combination administration & dosage, World Health Organization
Abstract

Aims: A clinical study was conduct in HIV-infected children to evaluate the prophylactic doses of cotrimoxazole [sulfamethoxazole (SMX) and trimethoprim (TMP)] advised by the WHO., Methods: Children received lopinavir-based antiretroviral therapy with cotrimoxazole prophylaxis (200 mg of SMX/40 mg of TMP once daily). A nonlinear mixed effects modelling approach was used to analyse plasma concentrations. Factors that could impact the pharmacokinetic profile were investigated. The model was subsequently used to simulate individual exposure and evaluate different administration schemes., Results: The cohort comprised 136 children [average age: 1.9 years (range: [0.7-4]), average weight: 9.5 kg (range: [6-16.3])]. A dose per kg was justified by the significant influence of implementing an allometrically scaled body size covariate on SMX and TMP pharmacokinetics. SMX and TPM clearance were estimated at 0.49 l h -1 /9.5 kg and 3.06 l h -1 /9.5 kg, respectively. The simulated exposures obtained after administration of oral dosing recommended by the WHO for children from 10 to 15 kg were significantly lower than in adults for SMX and TMP. This could induce a reduction of effectiveness of cotrimoxazole. Simulations show that regimens of 30 mg kg -1 of SMX and 6 mg kg -1 of TMP in the 5-10 kg group and 25 mg kg -1 of SMX and 5 mg kg -1 of TMP in the 10-15 kg group are more suitable doses., Conclusions: In this context of high prevalence of opportunistic infections, a lower exposure to cotrimoxazole in children than adults was noted. To achieve comparable exposure to adults, a dosing scheme per kg was proposed., (© 2017 The British Pharmacological Society.)

Published
2017
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25. Pharmacokinetics of Efavirenz at a High Dose of 25 Milligrams per Kilogram per Day in Children 2 to 3 Years Old.

Author

Pressiat C, Amorissani-Folquet M, Yonaba C, Treluyer JM, Dahourou DL, Eboua F, Blanche S, Mea-Assande V, Bouazza N, Foissac F, Malateste K, Ouedraogo S, Lui G, Leroy V, and Hirt D

Subjects
Alkynes, Anti-HIV Agents therapeutic use, Bayes Theorem, Benzoxazines therapeutic use, Child, Preschool, Cyclopropanes, Drug Administration Schedule, Female, Humans, Lopinavir therapeutic use, Male, Anti-HIV Agents pharmacokinetics, Benzoxazines pharmacokinetics, Lopinavir pharmacokinetics
Abstract

The MONOD ANRS 12206 trial was designated to assess simplification of a successful lopinavir (LPV)-based antiretroviral treatment in HIV-infected children younger than 3 years of age using efavirenz (EFV; 25 mg/kg of body weight/day) to preserve the class of protease inhibitors for children in that age group. In this substudy, EFV concentrations were measured to check the consistency of an EFV dose of 25 mg/kg and to compare it with the 2016 FDA recommended dose. Fifty-two children underwent blood sampling for pharmacokinetic study at 6 months and 12 months after switching to EFV. We applied a Bayesian approach to derive EFV pharmacokinetic parameters using the nonlinear mixed-effect modeling (NONMEM) program. The proportion of midinterval concentrations 12 h after drug intake ( C 12 h ) corresponding to the EFV therapeutic pharmacokinetic thresholds (1 to 4 mg/liter) was assessed according to different dose regimens (25 mg/kg in the MONOD study versus the 2016 FDA recommended dose). With both the 25 mg/kg/day dose and the 2016 FDA recommended EFV dose, simulations showed that the majority of C 12 h values were within the therapeutic range (62.6% versus 62.8%). However, there were more children underexposed with the 2016 FDA recommended dose (11.6% versus 1.2%). Conversely, there were more concentrations above the threshold of toxicity with the 25 mg/kg dose (36.2% versus 25.6%), with C 12 h values of up to 15 mg/liter. Only 1 of 52 children was switched back to LPV because of persistent sleeping disorders, but his C 12 h value was within therapeutic ranges. A high EFV dose of 25 mg/kg per day in children under 3 years old achieved satisfactory therapeutic effective levels. However, the 2016 FDA recommended EFV dose appeared to provide more acceptable safe therapeutic profiles. (This study has been registered at ClinicalTrials.gov under identifier NCT01127204.)., (Copyright © 2017 American Society for Microbiology.)

Published
2017
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26. A Physiologically-Based Pharmacokinetic Model to Predict Human Fetal Exposure for a Drug Metabolized by Several CYP450 Pathways.

Author

De Sousa Mendes M, Lui G, Zheng Y, Pressiat C, Hirt D, Valade E, Bouazza N, Foissac F, Blanche S, Treluyer JM, Urien S, and Benaboud S

Subjects
Female, Fetus drug effects, Forecasting, Humans, Male, Placenta drug effects, Placenta physiology, Pregnancy, Reverse Transcriptase Inhibitors pharmacokinetics, Signal Transduction drug effects, Cytochrome P-450 Enzyme System metabolism, Fetus physiology, Models, Biological, Nevirapine pharmacokinetics, Signal Transduction physiology
Abstract

Background: Pregnant women and their fetuses are exposed to numerous drugs; however, they are orphan populations with respect to the safety and efficacy of drugs. Therefore, the prediction of maternal and fetal drug exposure prior to administration would be highly useful., Methods: A physiologically-based pharmacokinetic (PBPK) model for nevirapine, which is metabolized by the cytochrome P450 (CYP) 3A4, 2B6 and 2D6 pathways, was developed to predict maternal and fetal pharmacokinetics (PK). The model was developed in both non-pregnant and pregnant women, and all physiological and enzymatic changes that could impact nevirapine PK were taken into account. Transplacental parameters estimated from ex vivo human placenta perfusion experiments were included in this PBPK model. To validate the model, observed maternal and cord blood concentrations were compared with predicted concentrations, and the impact of fetal clearance on fetal PK was investigated., Results: By implementing physiological changes, including CYP3A4, 2D6 and 2B6 inductions, we predicted a clearance increase of 21 % in late pregnancy. The PBPK model successfully predicted the disposition for both non-pregnant and pregnant populations. Parameters obtained from the ex vivo experiments allowed the prediction of nevirapine concentrations that matched observed cord blood concentrations. The fetal-to-maternal area under the curve ratio (0-24 h interval) was 0.77, and fetal metabolism had no significant effect on fetal PK., Conclusions: The PBPK approach is a useful tool for quantifying a priori the drug exposure of metabolized drugs during pregnancy, and can be applied to evaluate alternative dosing regimens to optimize drug therapy. This approach, including ex vivo human placental perfusion parameters, is a promising approach for predicting human fetal exposure.

Published
2017
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27. Development and Validation of a Simultaneous Quantification Method of 14 Tyrosine Kinase Inhibitors in Human Plasma Using LC-MS/MS.

Author

Huynh HH, Pressiat C, Sauvageon H, Madelaine I, Maslanka P, Lebbé C, Thieblemont C, Goldwirt L, and Mourah S

Subjects
Antineoplastic Agents administration & dosage, Drug Monitoring methods, Humans, Protein Kinase Inhibitors administration & dosage, Reproducibility of Results, Antineoplastic Agents blood, Chromatography, High Pressure Liquid methods, Protein Kinase Inhibitors blood, Tandem Mass Spectrometry methods
Abstract

Background: A sensitive liquid chromatography coupled with tandem mass spectrometry (MS/MS) method for the analysis in a small volume of plasma of 14 tyrosine kinase inhibitors currently used (imatinib, dasatinib, ibrutinib, ponatinib, trametinib, sunitinib, cobimetinib, dabrafenib, erlotinib, lapatinib, nilotinib, bosutinib, sorafenib, and vemurafenib) has been developed and validated. This multianalyte liquid chromatography coupled with MS/MS assay is of interest for anticancer drug combination therapy., Methods: After a simple protein precipitation of plasma samples, the chromatographic separation was performed using an ultra performance liquid chromatography system coupled with MS/MS in a positive ionization mode. The mobile phase consisted of a gradient elution of 10 mmol/L formate ammonium buffer containing 0.1% (vol/vol) formic acid (phase A) and acetonitrile with 0.1% (vol/vol) formic acid (phase B) at a flow rate of 300 μL/min., Results: The analysis time was 5.0 minutes per run, and all analytes and internal standard eluted within 1.45-1.79 minutes. The calibration curves were linear over the range from 1 to 500 ng/mL for bosutinib, cobimetinib, dasatinib, ibrutinib, and trametinib, from 5 to 500 ng/mL for ponatinib and sunitinib; from 50 to 2500 ng/mL for lapatinib; from 750 to 100,000 ng/mL for vemurafenib, and from 10 to 2500 ng/mL for dabrafenib, erlotinib, imatinib, nilotinib, and sorafenib, with coefficients of correlation above 0.99 for all analytes. The intra- and interday imprecisions were below 14.36%., Conclusions: This method was successfully applied to therapeutic drug monitoring in clinical practice.

Published
2017
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28. Prediction of human fetal pharmacokinetics using ex vivo human placenta perfusion studies and physiologically based models.

Author

De Sousa Mendes M, Hirt D, Vinot C, Valade E, Lui G, Pressiat C, Bouazza N, Foissac F, Blanche S, Lê MP, Peytavin G, Treluyer JM, Urien S, and Benaboud S

Subjects
Anti-HIV Agents administration & dosage, Anti-HIV Agents blood, Computer Simulation, Emtricitabine administration & dosage, Emtricitabine blood, Emtricitabine pharmacokinetics, Female, Fetal Blood, Humans, Perfusion, Predictive Value of Tests, Pregnancy, Tenofovir administration & dosage, Tenofovir blood, Tenofovir pharmacokinetics, Anti-HIV Agents pharmacokinetics, Fetus metabolism, Maternal-Fetal Exchange physiology, Models, Biological, Placenta metabolism, Placental Circulation physiology
Abstract

Aims: Pregnant women can be exposed to numerous drugs during the gestational period. For obvious ethical reasons, in vivo studies of fetal exposure to drugs are limited. Information about the transplacental transfer of drugs prior to their administration to pregnant women would be highly useful. In the present study, a novel approach was developed quantitatively predict or to predict the fetal exposure to drugs administered to the mother quantitatively., Methods: Transplacental parameters estimated from ex vivo human placenta perfusion experiments were implemented in pregnancy-physiologically based pharmacokinetic (p-PBPK) models in order to predict fetal PK. Thereafter, fetal PK profiles for two antiretroviral drugs, tenofovir (TFV) and emtricitabine (FTC) were simulated. These predictions were then compared to observed cord blood concentrations, to validate these models., Results: Parameters obtained from the ex vivo experiments enabled a good prediction of observed cord blood concentrations without additional a scaling factor. Moreover, a sensitivity analysis showed that fetal predictions were sensitive to changes in transplacental parameters values obtained ex vivo., Conclusion: The integration of ex vivo human placental perfusion parameters in a p-PBPK model should be a promising new approach for predicting human fetal exposure to xenobiotics., (© 2015 The British Pharmacological Society.)

Published
2016
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29. Population approach to analyze the pharmacokinetics of free and total lopinavir in HIV-infected pregnant women and consequences for dose adjustment.

Author

Fauchet F, Treluyer JM, Illamola SM, Pressiat C, Lui G, Valade E, Mandelbrot L, Lechedanec J, Delmas S, Blanche S, Warszawski J, Urien S, Tubiana R, and Hirt D

Subjects
Adult, Anti-HIV Agents administration & dosage, Anti-HIV Agents therapeutic use, Female, Genotyping Techniques, HIV Infections drug therapy, Humans, Lopinavir administration & dosage, Lopinavir therapeutic use, Pregnancy, Pregnancy Complications, Infectious drug therapy, Young Adult, Anti-HIV Agents pharmacokinetics, Lopinavir pharmacokinetics
Abstract

The aims of this study were to describe the unbound and total lopinavir (LPV) pharmacokinetics in pregnant women in order to evaluate if a dosing adjustment is necessary during pregnancy. Lopinavir placental transfer is described, and several genetic covariates were tested to explain its variability. A total of 400 maternal, 79 cord blood, and 48 amniotic fluid samples were collected from 208 women for LPV concentration determinations and pharmacokinetics analysis. Among the maternal LPV concentrations, 79 samples were also used to measure the unbound LPV concentrations. Population pharmacokinetics models were developed by using NONMEM software. Two models were developed to describe (i) unbound and total LPV pharmacokinetics and (ii) LPV placental transfer. The pharmacokinetics was best described by a one-compartment model with first-order absorption and elimination. A pregnancy effect was found on maternal clearance (39% increase), whereas the treatment group (monotherapy versus triple therapy) or the genetic polymorphisms did not explain the pharmacokinetics or placental transfer of LPV. Efficient unbound LPV concentrations in nonpregnant women were similar to those measured during the third trimester of pregnancy. Our study showed a 39% increase of maternal total LPV clearance during pregnancy, whereas unbound LPV concentrations were similar to those simulated in nonpregnant women. The genetic polymorphisms selected did not influence the LPV pharmacokinetics or placental transfer. Thus, we suggest that the LPV dosage should not be increased during pregnancy., (Copyright © 2015, American Society for Microbiology. All Rights Reserved.)

Published
2015
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30. Complete remission of Schnitzler syndrome and Waldenström macroglobulinemia under rituximab-cyclophosphamide-dexamethasone.

Author

Aouba A, Pressiat C, Pricopi M, Georgin-Lavialle S, Boue F, Lievre-Castilla MA, Marfaing-Koka A, Prevot S, and Decottignies A

Subjects
Antibodies, Monoclonal, Murine-Derived administration & dosage, Cyclophosphamide administration & dosage, Dexamethasone administration & dosage, Female, Humans, Interleukin 1 Receptor Antagonist Protein therapeutic use, Middle Aged, Remission Induction, Rituximab, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Schnitzler Syndrome drug therapy, Waldenstrom Macroglobulinemia drug therapy
Abstract

In Schnitzler syndrome, which is mostly diagnosed with a low and asymptomatic monoclonal peak, anakinra has always exhibited a complete but only transient control of the auto-inflammatory signs, which are induced by interleukin (IL)-1 auto-activation. We focused on the treatment of a case of Schnitzler syndrome with moderate macroglobulinemia peak. Anakinra failed to improve the severe inflammatory anaemia and the dysglobulinemia, but rituximab-dexamethasone-cyclophosphamide chemotherapy alone allowed a complete response. The correlation between the clinical, pro-inflammatory cytokines and dysglobulinemia complete controls with chemotherapy proves the following: (1) the dual action of this treatment in both the auto-inflammatory and dysglobulinemia components of the syndrome and (2) a different but entangled cytokine network in the pathogenesis of the auto-inflammatory and dysglobulinemia components of the syndrome., (© 2014 S. Karger AG, Basel.)

Published
2015
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