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  1. Article ; Online: Population Pharmacokinetic Modeling and Determination of Individual Exposure to Avalglucosidase Alfa in Adolescent and Adult Patients With Late-Onset Pompe Disease: Analysis of Pooled Data From Phase I to III Clinical Trials.

    Tuffal, Gilles / Tiraboschi, Gilles / Hurbin, Fabrice / Boittet, Pascale / Palmer, Rachel / Martinez, Jean-Marie / Fabre, David

    Therapeutic drug monitoring

    2023  Volume 45, Issue 5, Page(s) 644–652

    Abstract: Background: Pompe disease is a rare genetic disorder caused by a deficiency of a lysosomal enzyme called acid alpha-glucosidase and is classified into infantile and late-onset forms. Since 2006, an enzyme replacement therapy involving alglucosidase alfa ...

    Abstract Background: Pompe disease is a rare genetic disorder caused by a deficiency of a lysosomal enzyme called acid alpha-glucosidase and is classified into infantile and late-onset forms. Since 2006, an enzyme replacement therapy involving alglucosidase alfa has been available. In 2021, a new enzyme replacement therapy involving avalglucosidase alfa demonstrated improved clinical benefits. In this article, the authors describe the pharmacokinetics of avalglucosidase alfa using a population pharmacokinetic approach.
    Methods: The population pharmacokinetic model was developed using a data set that included 75 patients and 2042 plasma drug concentrations determined through enzymatic activity assay from 3 studies (phases I/II and III) and involved 3 dose levels (5, 10, and 20 mg/kg). The analysis was performed using NONMEM software.
    Results: Two sequences were observed in the plasma drug concentration profile: the first kinetic driving exposure, and after 12 hours postdose, a slight rebound addressing very low concentrations that lasted up to 2 weeks. Following model screening, a model with a central compartment with parallel linear and nonlinear elimination and 2 concatenated peripheral compartments was proposed. A putative back-redistribution of a marginal fraction of the drug from the second peripheral compartment to the central compartment may explain the slight rebound in concentration. The final model's mean bias and precision for individual predictions were -2.66% and 30.7%, respectively, and -0.433% and 38.9%, respectively, for population predictions.
    Conclusions: A concatenated 3-compartment model was developed to describe the avalglucosidase alfa concentrations in patients with late-onset Pompe disease. None of the covariates tested could explain the interindividual variability.
    MeSH term(s) Adolescent ; Adult ; Humans ; Enzyme Replacement Therapy ; Glycogen Storage Disease Type II/drug therapy ; Glycogen Storage Disease Type II/etiology ; Kinetics ; Clinical Trials, Phase I as Topic ; Clinical Trials, Phase II as Topic ; Clinical Trials, Phase III as Topic
    Language English
    Publishing date 2023-08-01
    Publishing country United States
    Document type Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 424443-6
    ISSN 1536-3694 ; 0163-4356
    ISSN (online) 1536-3694
    ISSN 0163-4356
    DOI 10.1097/FTD.0000000000001086
    Database MEDical Literature Analysis and Retrieval System OnLINE

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    In stock of ZB MED Cologne/Königswinter

    Zs.A 1503: Show issues Location:
    Je nach Verfügbarkeit (siehe Angabe bei Bestand)
    bis Jg. 1994: Bestellungen von Artikeln über das Online-Bestellformular
    Jg. 1995 - 2021: Lesesall (1.OG)
    ab Jg. 2022: Lesesaal (EG)

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  2. Article ; Online: Population pharmacokinetic modeling and dosing simulation of avalglucosidase alfa for selecting alternative dosing regimen in pediatric patients with late-onset pompe disease.

    Tiraboschi, Gilles / Marchionni, David / Tuffal, Gilles / Fabre, David / Martinez, Jean-Marie / Haack, Kristina An / Miossec, Patrick / Kittner, Barbara / Daba, Nadia / Hurbin, Fabrice

    Journal of pharmacokinetics and pharmacodynamics

    2023  Volume 50, Issue 6, Page(s) 461–474

    Abstract: Avalglucosidase alfa (AVAL) was approved in the United States (2021) for patients with late-onset Pompe disease (LOPD), aged ≥ 1 year. In the present study, pharmacokinetic (PK) simulations were conducted to propose alternative dosing regimens for ... ...

    Abstract Avalglucosidase alfa (AVAL) was approved in the United States (2021) for patients with late-onset Pompe disease (LOPD), aged ≥ 1 year. In the present study, pharmacokinetic (PK) simulations were conducted to propose alternative dosing regimens for pediatric LOPD patients based on a bodyweight cut-off. Population PK (PopPK) analysis was performed using nonlinear mixed effect modeling approach on pooled data from three clinical trials with LOPD patients, and a phase 2 study (NCT03019406) with infantile-onset Pompe disease (IOPD: 1-12 years) patients. A total of 2257 concentration-time points from 91 patients (LOPD, n = 75; IOPD, n = 16) were included in the analysis. The model was bodyweight dependent allometric scaling with time varying bodyweight included on clearance and distribution volume. Simulations were performed for two dosing regimens (20 mg/kg or 40 mg/kg) with different bodyweight cut-off (25, 30, 35 and 40 kg) by generating virtual pediatric (1-17 years) and adult patients. Corresponding simulated individual exposures (maximal concentration, C
    MeSH term(s) Adult ; Humans ; Child ; United States ; Glycogen Storage Disease Type II/drug therapy ; Glycogen Storage Disease Type II/chemically induced ; Glycogen Storage Disease Type II/epidemiology ; alpha-Glucosidases/adverse effects ; alpha-Glucosidases/metabolism ; Body Weight ; Kinetics
    Chemical Substances alpha-Glucosidases (EC 3.2.1.20)
    Language English
    Publishing date 2023-08-03
    Publishing country United States
    Document type Journal Article
    ZDB-ID 2041601-5
    ISSN 1573-8744 ; 1567-567X
    ISSN (online) 1573-8744
    ISSN 1567-567X
    DOI 10.1007/s10928-023-09874-8
    Database MEDical Literature Analysis and Retrieval System OnLINE

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    Zs.A 980: Show issues Location:
    Je nach Verfügbarkeit (siehe Angabe bei Bestand)
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    Jg. 1995 - 2021: Lesesall (1.OG)
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  3. Article ; Online: Rational design of potent GSK3beta inhibitors with selectivity for Cdk1 and Cdk2.

    Lesuisse, Dominique / Dutruc-Rosset, Gilles / Tiraboschi, Gilles / Dreyer, Matthias K / Maignan, Sébastien / Chevalier, Alain / Halley, Frank / Bertrand, Philippe / Burgevin, Marie-Claude / Quarteronet, Dominique / Rooney, Thomas

    Bioorganic & medicinal chemistry letters

    2010  Volume 20, Issue 6, Page(s) 1985–1989

    Abstract: From an HTS hit, a series of potent and selective inhibitors of GSK3beta have been designed based on a Cdk2-homology model and with the help of several crystal structures of the compounds within Cdk2. ...

    Abstract From an HTS hit, a series of potent and selective inhibitors of GSK3beta have been designed based on a Cdk2-homology model and with the help of several crystal structures of the compounds within Cdk2.
    MeSH term(s) CDC2 Protein Kinase/antagonists & inhibitors ; Cyclin-Dependent Kinase 2/antagonists & inhibitors ; Drug Design ; Glycogen Synthase Kinase 3/antagonists & inhibitors ; Glycogen Synthase Kinase 3 beta ; Models, Molecular ; Protein Kinase Inhibitors/chemistry ; Protein Kinase Inhibitors/pharmacology ; Substrate Specificity
    Chemical Substances Protein Kinase Inhibitors ; Glycogen Synthase Kinase 3 beta (EC 2.7.11.1) ; CDC2 Protein Kinase (EC 2.7.11.22) ; Cyclin-Dependent Kinase 2 (EC 2.7.11.22) ; Glycogen Synthase Kinase 3 (EC 2.7.11.26)
    Language English
    Publishing date 2010-03-15
    Publishing country England
    Document type Journal Article
    ZDB-ID 1063195-1
    ISSN 1464-3405 ; 0960-894X
    ISSN (online) 1464-3405
    ISSN 0960-894X
    DOI 10.1016/j.bmcl.2010.01.114
    Database MEDical Literature Analysis and Retrieval System OnLINE

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    In stock of ZB MED Cologne/Königswinter

    Zs.A 3203: Show issues Location:
    Je nach Verfügbarkeit (siehe Angabe bei Bestand)
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  4. Article ; Online: Design of potent and selective GSK3beta inhibitors with acceptable safety profile and pharmacokinetics.

    Lesuisse, Dominique / Tiraboschi, Gilles / Krick, Alain / Abecassis, Pierre-Yves / Dutruc-Rosset, Gilles / Babin, Didier / Halley, Frank / Châtreau, Fabienne / Lachaud, Sylvette / Chevalier, Alain / Quarteronet, Dominique / Burgevin, Marie-Claude / Amara, Céline / Bertrand, Philippe / Rooney, Thomas

    Bioorganic & medicinal chemistry letters

    2010  Volume 20, Issue 7, Page(s) 2344–2349

    Abstract: From potent and selective inhibitors of GSK3beta displaying CYP1A2 inhibition and poor PK properties, mostly linked to metabolic instability and in vivo hydrolysis of the amide bond, we were able to obtain safe and orally available inhibitors with good ... ...

    Abstract From potent and selective inhibitors of GSK3beta displaying CYP1A2 inhibition and poor PK properties, mostly linked to metabolic instability and in vivo hydrolysis of the amide bond, we were able to obtain safe and orally available inhibitors with good half lives.
    MeSH term(s) Animals ; Cytochrome P-450 CYP1A2/metabolism ; Cytochrome P-450 CYP1A2 Inhibitors ; Glycogen Synthase Kinase 3/antagonists & inhibitors ; Glycogen Synthase Kinase 3/metabolism ; Glycogen Synthase Kinase 3 beta ; Humans ; Mice ; Models, Molecular ; Protein Kinase Inhibitors/chemistry ; Protein Kinase Inhibitors/pharmacokinetics ; Protein Kinase Inhibitors/pharmacology
    Chemical Substances Cytochrome P-450 CYP1A2 Inhibitors ; Protein Kinase Inhibitors ; Cytochrome P-450 CYP1A2 (EC 1.14.14.1) ; GSK3B protein, human (EC 2.7.11.1) ; Glycogen Synthase Kinase 3 beta (EC 2.7.11.1) ; Gsk3b protein, mouse (EC 2.7.11.1) ; Glycogen Synthase Kinase 3 (EC 2.7.11.26)
    Language English
    Publishing date 2010-04-01
    Publishing country England
    Document type Journal Article
    ZDB-ID 1063195-1
    ISSN 1464-3405 ; 0960-894X
    ISSN (online) 1464-3405
    ISSN 0960-894X
    DOI 10.1016/j.bmcl.2010.01.132
    Database MEDical Literature Analysis and Retrieval System OnLINE

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    In stock of ZB MED Cologne/Königswinter

    Zs.A 3203: Show issues Location:
    Je nach Verfügbarkeit (siehe Angabe bei Bestand)
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    Jg. 1995 - 2021: Lesesall (2.OG)
    ab Jg. 2022: Lesesaal (EG)

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