Your search keyword '"Brain penetration"' showing total 12 results

1. Panobinostat penetrates the blood–brain barrier and achieves effective brain concentrations in a murine model.

Author

Homan, Morgan J., Franson, Andrea, Ravi, Karthik, Roberts, Holly, Pai, Manjunath P., Liu, Cai, He, Miao, Matvekas, Aleksas, Koschmann, Carl, and Marini, Bernard L.

Subjects

*BLOOD-brain barrier, *BRAIN tumors, *CELL lines, *BLOOD sampling, *PHARMACOKINETICS

Abstract

Purpose: Panobinostat, an orally bioavailable pan-HDAC inhibitor, has demonstrated potent activity in multiple malignancies, including pediatric brain tumors such as DIPG, with increased activity against H3K27M mutant cell lines. Given limited evidence regarding the CNS penetration of panobinostat, we sought to characterize its BBB penetration in a murine model. Methods: Panobinostat 15 mg/kg was administered IV to 12 CD-1 female mice. At specified time points, mice were euthanized, blood samples were collected, and brains were removed. LC–MS was performed to quantify panobinostat concentrations. Cmax and AUC were estimated and correlated with previously published pharmacokinetic analyses and reports of IC-50 values in DIPG cell lines. Results: Mean panobinostat plasma concentrations (ng/mL) were 27.3 ± 2.5 at 1 h, 7.56 ± 1.8 at 2 h, 1.48 ± 0.56 at 4 h, and 2.33 ± 1.18 at 7 h. Mean panobinostat brain concentrations (ng/g) were 60.5 ± 6.1 at 1 h, 42.9 ± 5.4 at 2 h, 33.2 ± 6.1 at 4 h, and 28.1 ± 4.3 at 7 h. Brain-to-plasma ratio at 1 h was 2.22 and the brain to plasma AUC ratio was 2.63. Based on the published human pharmacokinetic data, the anticipated Cmax in humans is expected to be significantly higher than the IC-50 identified in DIPG models. Conclusion: It is expected that panobinostat would be effective in CNS tumors where the IC-50 is in the low nanomolar range. Thus, our data demonstrate panobinostat crosses the BBB and achieves concentrations above the IC-50 for DIPG and other brain tumors and should be explored further for clinical efficacy. [ABSTRACT FROM AUTHOR]

Published

2021

2. Assessing extent of brain penetration in vivo (Kp,uu,brain) in Göttingen minipig using a diverse set of reference drugs.

Author

Langthaler, Kristine, Jones, Christopher R., Brodin, Birger, and Bundgaard, Christoffer

Subjects

*MEDICATION safety, *DRUGS, *P-glycoprotein, *MONKEYS, *BLOOD-brain barrier

Abstract

• Successful determination of minipig K p,uu,brain was achieved by cassette dosing, employing a pseudo steady-state approach. • Brain penetration data are presented for the first time in Göttingen minipig for a large set of reference compounds. • Results support use of Göttingen minipig as a non-rodent drug safety model for CNS drug candidates. • Transporter substrates gave the most pronounced difference in K p,uu,brain comparing across minipig, dog, monkey and human. The application of Göttingen minipigs for non-rodent pharmacokinetics (PK) and drug safety testing has seen a dramatic increase in recent years. The aim of this study was to determine the total and unbound brain-to-plasma ratios (K p,brain and K p,uu,brain) for a diverse set of reference compounds in female Göttingen minipigs and compare these with K p,uu,brain values from other species to assess the suitability of Göttingen minipigs as a model for CNS drug safety testing and brain PK in clinical translation. The reference set consisted of 17 compounds with varying physico-chemical properties and included known human P-glycoprotein (P-gp) substrates. The results of the study showed, that minipig K p,brain and K p,uu,brain values for the tested compounds were in the range 0.03–86 and 0.02–2.4 (n = 3–4) respectively. The K p,uu,brain values were comparable between minipig and rat for a large proportion of the compounds (71% within 2-fold, n = 17). Comparisons of brain penetration across several species for a subset of reference compounds revealed that minipig values were quite similar to those of rat, dog, monkey and human. The study highlighted that the largest K p,uu,brain species differences were observed for compounds classified as transporter substrates (e.g. cimetidine, risperidone, Way-100635 and altanserin). In conclusion these brain penetration data add substantially to the available literature on PK and drug disposition for minipigs and support use of Göttingen minipig as a non-rodent drug safety model for CNS drug candidates and as a brain PK model for clinical translation. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

3. In vivo real time non invasive monitoring of brain penetration of chemicals with near-infrared spectroscopy: Concomitant PK/PD analysis.

Author

Crespi, Francesco, Cattini, Stefano, Donini, Maurizio, Bandera, Andrea, and Rovati, Luigi

Subjects

*NEAR infrared spectroscopy, *OXYGENATION (Chemistry), *HEMOGLOBINS, *LABORATORY rats, *BRAIN physiology

Abstract

Background Near-infrared spectroscopy (NIRS) is a non-invasive technique that monitors changes in oxygenation of haemoglobin. The absorption spectra of near-infrared light differ for the oxygenation–deoxygenation states of haemoglobin (oxygenate (HbO 2 ) and deoxygenate (Hb), respectively) so that these two states can be directly monitored. Comparison with existing method(s) Different methodologies report different basal values of HbO 2 and Hb absolute concentrations in brain. Here, we attempt to calculate basal HbO 2 levels in rat CNS via evaluation of the influence of exogenous oxygen or exogenous carbon dioxide on the NIRS parameters measured in vivo. New method Furthermore the possibility that changes of haemoglobin oxygenation in rat brain as measured by NIRS might be a useful index of brain penetration of chemical entities has been investigated. Different compounds from different chemical classes were selected on the basis of parallel ex vivo and in vivo pharmacokinetic (PK/PD) studies of brain penetration and overall pharmacokinetic profile. Results It appeared that NIRS might contribute to assess brain penetration of chemical entities, i.e. significant changes in NIRS signals could be related to brain exposure, conversely the lack of significant changes in relevant NIRS parameters could be indicative of low brain exposure. Conclusions This work is proposing a further innovation on NIRS preclinical applications i.e. a “chemical” NIRS [chNIRS] approach for determining penetration of drugs in animal brain. Therefore, chNIRS could became a non invasive methodology for studies on neurobiological processes and psychiatric diseases in preclinical but also a translational strategy from preclinical to clinical investigations. [ABSTRACT FROM AUTHOR]

Published

2016

4. Application of an in Vitro Blood–Brain Barrier Model in the Selection of Experimental Drug Candidates for the Treatment of Huntington’s Disease

Author

Mark Rose, Odalys Gonzalez Paz, Giulio Auciello, Annalise Di Marco, Todd Herbst, Ignacio Muñoz-Sanjuán, Domenico Vignone, Edith Monteagudo, Vinod Khetarpal, Matteo Zini, Maria Rosaria Battista, Laura Orsatti, Vincenzo Summa, Celia Dominguez, Leticia M Toledo-Sherman, Ivan Fini, Antonella Cellucci, Di Marco, A., Gonzalez Paz, O., Fini, I., Vignone, D., Cellucci, A., Battista, M. R., Auciello, G., Orsatti, L., Zini, M., Monteagudo, E., Khetarpal, V., Rose, M., Dominguez, C., Herbst, T., Toledo-Sherman, L., Summa, V., and Munoz-Sanjuan, I.

Subjects

Swine, Pharmaceutical Science, 02 engineering and technology, Pharmacology, efflux transporter, 030226 pharmacology & pharmacy, brain penetration, Rats, Sprague-Dawley, 0302 clinical medicine, Drug Discovery, Electric Impedance, Coculture Technique, Cells, Cultured, Cerebral Cortex, Endothelial Cell, Tight junction, Tight Junction, Drug discovery, Chemistry, Huntington's disease, Biological activity, 021001 nanoscience & nanotechnology, Huntington Disease, medicine.anatomical_structure, Blood-Brain Barrier, Molecular Medicine, Central Nervous System Agent, CNS, Astrocyte, 0210 nano-technology, ATP-Binding Cassette Transporter, Central nervous system, Blood–brain barrier, Models, Biological, Permeability, Tight Junctions, Capillary Permeability, 03 medical and health sciences, In vivo, Huntingtin Protein, medicine, Animals, Solute Carrier Protein, Solute Carrier Proteins, Animal, Endothelial Cells, medicine.disease, Coculture Techniques, Rats, Astrocytes, transport, Rat, ATP-Binding Cassette Transporters, Central Nervous System Agents

Abstract

Huntington's disease (HD) is a neurodegenerative disease caused by polyglutamine expansion in the huntingtin protein. For drug candidates targeting HD, the ability to cross the blood-brain barrier (BBB) and reach the site of action in the central nervous system (CNS) is crucial for achieving pharmacological activity. To assess the permeability of selected compounds across the BBB, we utilized a two-dimensional model composed of primary porcine brain endothelial cells and rat astrocytes. Our objective was to use this in vitro model to rank and prioritize compounds for in vivo pharmacokinetic and brain penetration studies. The model was first characterized using a set of validation markers chosen based on their functional importance at the BBB. It was shown to fulfill the major BBB characteristics, including functional tight junctions, high transendothelial electrical resistance, expression, and activity of influx and efflux transporters. The in vitro permeability of 54 structurally diverse known compounds was determined and shown to have a good correlation with the in situ brain perfusion data in rodents. We used this model to investigate the BBB permeability of a series of new HD compounds from different chemical classes, and we found a good correlation with in vivo brain permeation, demonstrating the usefulness of the in vitro model for optimizing CNS drug properties and for guiding the selection of lead compounds in a drug discovery setting. ©

Published

2019

5. P-glycoprotein (MDR1/ABCB1) and Breast Cancer Resistance Protein (BCRP/ABCG2) limit brain accumulation of the FLT3 inhibitor quizartinib in mice

Author

Wang, Jing, Gan, Changpei, Retmana, Irene A., Sparidans, Rolf W., Li, Wenlong, Lebre, Maria C., Beijnen, Jos H., Schinkel, Alfred H., Pharmacoepidemiology and Clinical Pharmacology, Afd Pharmacoepi & Clinical Pharmacology, Afd Chemical Biology and Drug Discovery, Chemical Biology and Drug Discovery, Pharmacoepidemiology and Clinical Pharmacology, Afd Pharmacoepi & Clinical Pharmacology, Afd Chemical Biology and Drug Discovery, and Chemical Biology and Drug Discovery

Subjects

Genetically modified mouse, ATP Binding Cassette Transporter, Subfamily B, Abcg2, ABCG2, Biological Availability, Pharmaceutical Science, Antineoplastic Agents, Mice, Transgenic, 02 engineering and technology, Pharmacology, 030226 pharmacology & pharmacy, Madin Darby Canine Kidney Cells, Mice, 03 medical and health sciences, chemistry.chemical_compound, Dogs, 0302 clinical medicine, Pharmacokinetics, In vivo, Oral administration, CYP3A enzymes, ATP Binding Cassette Transporter, Subfamily G, Member 2, Animals, Humans, Tissue Distribution, Benzothiazoles, FLT3, P-glycoprotein, Quizartinib, Mice, Knockout, Brain penetration, biology, Phenylurea Compounds, Brain, ABCB1, 021001 nanoscience & nanotechnology, Neoplasm Proteins, fms-Like Tyrosine Kinase 3, chemistry, biology.protein, Female, 0210 nano-technology, FLT3 Inhibitor

Abstract

Quizartinib, a second-generation FLT3 inhibitor, is in clinical development for the treatment of acute myeloid leukemia. We studied its pharmacokinetic interactions with the multidrug efflux transporters ABCB1 and ABCG2 and the multidrug metabolizing enzyme CYP3A, using in vitro transport assays and knockout and transgenic mouse models. Quizartinib was transported by human ABCB1 in vitro, and by mouse (m)Abcb1 and mAbcg2 in vivo. Upon oral administration, the brain accumulation of quizartinib was 6-fold decreased by mAbcb1 and 2-fold by mAbcg2 (together: 12-fold). Unexpectedly, the absence of mAbcb1 resulted in a ∼2-fold lower plasma exposure in Abcb1a/1b−/− and Abcb1a/1b;Abcg2−/− mice, suggesting that loss of mAbcb1 causes compensatory alterations in alternative quizartinib elimination or uptake systems. mAbcb1 and mAbcg2 themselves did not appear to restrict quizartinib oral availability. Oral and intravenous pharmacokinetics of quizartinib were not substantially altered between wild-type, Cyp3a knockout and CYP3A4-humanized mice. All three strains showed relatively high (33–51%) oral bioavailability. If this also applies in humans, this would suggest a limited risk of CYP3A-related inter-individual variation in exposure for this drug. Our results provide a possible rationale for using pharmacological ABCB1/ABCG2 inhibitors together with quizartinib when treating malignant lesions situated in part or in whole behind the blood-brain barrier.

Published

2019

6. Brain penetration assessment in vivo: A reliable and simple method in anesthetized rats at steady state.

Author

Andersen, Claus A., Perfetti, Paolo, Nibbio, Martina, Bellini, Marta, Angelini, Roberto, and Fornasier, Massenzio

Subjects

*INTRAVENOUS anesthesia, *LABORATORY rats, *PHARMACOKINETICS, *BLOOD plasma, *CENTRAL nervous system, *DRUG development

Abstract

Highlights: [•] Brain penetration is measured in a robust and efficient manner at steady state. [•] CNS drug discovery improved by simplified brain/plasma-ratio method in rats. [•] Steady state method robust with respect to variable plasma–brain equilibration rate. [•] One day experiment yielding brain/plasma-ratio in triplicates with simple equipment. [•] The 3Rs benefits: animal reduction and steady state model refinement. [ABSTRACT FROM AUTHOR]

Published

2014

7. Quantitative microdialysis using modified ultraslow microdialysis: Direct rapid and reliable determination of free brain concentrations with the MetaQuant technique

Author

Cremers, Thomas I.F.H., de Vries, Martin G., Huinink, Kirsten D., Loon, Jan Paul van, Hart, Marieke v.d., Ebert, Bjarke, Westerink, Ben H.C., and De Lange, Elizabeth C.M.

Subjects

*MICRODIALYSIS, *QUANTITATIVE research, *BLOOD-brain barrier, *BLOOD testing, *CEREBRAL circulation, *FLUID dynamics, *BRAIN chemistry, *CENTRAL nervous system stimulants

Abstract

Abstract: The only method to quantify free extracellular levels of drugs in the brain of living animals is microdialysis. However, quantitative microdialysis has been hampered by methodological issues for decades. The problems arise from the need to establish the in vivo recovery for appropriate quantitation. In dealing with these issues the “dynamic no-net-flux” (DNNF) method seemed to be the experimental method of choice. Major disadvantages were, however, the need for a very high degree of bioanalytical precision and accuracy and the need for a large number of animals. Moreover, today we know that the experimental data are not always straightforward. To improve robustness and practicality of quantitative microdialysis sampling we modified the ultraslow microdialysis approach. Ultraslow microdialysis uses very low microdialysis flow rates (<200nl/min) which increase recovery (both in vivo and in vitro) to over 90%. However, new practical issues arise when attempting to work with these flow rates. The resulting very low volumes and long lag times make this method very impractical for general application. In the modified version, addition of a carrier flow after the dialysis process has been completed, which negates the problems of long lag times and low volumes. The resulting dilution of the dialysis sample concentration can simply be mathematically corrected. In the current study we measured the free brain levels of two CNS compounds using the classic DNNF and the new modified ultraslow dialysis method. Modified ultraslow microdialysis was shown to generate robust data with the use of only small numbers of rats. The method is a promising tool for common straightforward screening of blood–brain barrier penetration of compounds into the brain. [Copyright &y& Elsevier]

Published

2009

8. An improved, scalable synthesis of Notum inhibitor LP-922056 using 1-chloro-1,2-benziodoxol-3-one as a superior electrophilic chlorinating agent

Author

George Papageorgiou, Paul V. Fish, Elliott D. Bayle, David Steadman, Benjamin N. Atkinson, Nicky J. Willis, and William Mahy

Subjects

01 natural sciences, Full Research Paper, brain penetration, Negative regulator, lcsh:QD241-441, 03 medical and health sciences, Carboxylesterase, lp-922056, lcsh:Organic chemistry, In vivo, lcsh:Science, electrophilic chlorination, 030304 developmental biology, Chemical Biology & High Throughput, 0303 health sciences, 010405 organic chemistry, Drug discovery, Chemistry, 1-chloro-1,2-benziodoxol-3-one, Organic Chemistry, Wnt signaling pathway, Notum, 0104 chemical sciences, Cell biology, notum inhibitor, Electrophile, lcsh:Q, Efflux, Structural Biology & Biophysics

Abstract

Background: The carboxylesterase Notum has been shown to act as a key negative regulator of the Wnt signalling pathway by mediating the depalmitoleoylation of Wnt proteins. LP-922056 (1) is an orally active inhibitor of Notum. We are investigating the role of Notum in modulating Wnt signalling in the central nervous system and wished to establish if 1 would serve as a peripherally restricted control. An accessible and improved synthetic route would allow 1 to become more readily available as a chemical tool to explore the fundamental biology of Notum and build target validation to underpin new drug discovery programs. Results: An improved, scalable synthesis of 1 is reported. Key modifications include: (1) the introduction of the C7-cyclopropyl group was most effectively achieved with a Suzuki–Miyaura cross-coupling reaction with MIDA-boronate 11 (5 → 6); and (2) C6 chlorination was performed with 1-chloro-1,2-benziodoxol-3-one (12) (6 → 7) as a mild selective electrophilic chlorination agent. This 7-step route has been reliably performed on large scale to produce multigram quantities of 1 in good efficiency and high purity. Pharmacokinetic studies in mouse showed CNS penetration of 1 is very low with brain:plasma concentration ratio of just 0.01. A small library of amides 17 were prepared from acid 1 to explore if 1 could be modified to deliver a CNS penetrant tool by capping off the acid as an amide. Although significant Notum inhibition activity could be achieved, none of these amides demonstrated the required combination of metabolic stability along with cell permeability without evidence of P-gp mediated efflux. Conclusion: Mouse pharmacokinetic studies demonstrate that 1 is unsuitable for use in models of disease where brain penetration is an essential requirement of the compound but would be an ideal peripherally restricted control. These data will contribute to the understanding of drug levels of 1 to overlay with appropriate in vivo efficacy endpoints, i.e. the PK-PD relationship. The identification of a suitable analogue of 1 (or 17) which combines Notum inhibition with CNS penetration would be a valuable chemical probe for investigating the role of Notum in disease models.

Published

2019

9. Improved Controlled Release and Brain Penetration of the Small Molecule S14 Using PLGA Nanoparticles

Author

Daniel I. Perez, Ana Martínez, Elisa Rojas-Prats, Inés Maestro, Vanesa Nozal, Carmen Gil, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Ministerio de Educación, Cultura y Deporte (España), European Commission, Nozal, Vanesa [0000-0001-5260-5683], Rojas-Prats, Elisa [0000-0002-5747-8764], Maestro, Inés [0000-0002-5026-5803], Gil, Carmen [0000-0002-3882-6081], Pérez, Daniel I. [0000-0003-1774-4471], Martínez, Ana [0000-0002-2707-8110], Nozal, Vanesa, Rojas-Prats, Elisa, Maestro, Inés, Gil, Carmen, Pérez, Daniel I., and Martínez, Ana

Subjects

0301 basic medicine, phosphodiesterase 7 inhibitor, Druggability, 02 engineering and technology, brain penetration, lcsh:Chemistry, Mice, chemistry.chemical_compound, Nanoparticle, Polylactic Acid-Polyglycolic Acid Copolymer, Controlled release, lcsh:QH301-705.5, Spectroscopy, Drug Carriers, Brain penetration, Molecular Structure, Chemistry, Phosphodiesterase 7 inhibitor, nanoparticle, Brain, PLGA, Phosphodiesterase, General Medicine, 021001 nanoscience & nanotechnology, Small molecule, 3. Good health, Computer Science Applications, 0210 nano-technology, Cell Survival, Drug Compounding, Permeability, Article, Catalysis, nanoprecipitation, Inorganic Chemistry, 03 medical and health sciences, In vivo, Animals, Humans, Cyclic adenosine monophosphate, Particle Size, Physical and Theoretical Chemistry, Molecular Biology, Quinazolinones, Cyclic Nucleotide Phosphodiesterases, Type 7, Organic Chemistry, In vitro, Drug Liberation, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Delayed-Action Preparations, Biophysics, Nanoparticles, Nanoprecipitation, controlled release

Abstract

14 p.-8 fig.-4 tab., Phosphodiesterase 7 (PDE7) is an enzyme responsible for the degradation of cyclic adenosine monophosphate (cAMP), an important cellular messenger. PDE7’s role in neurotransmission, expression profile in the brain and the druggability of other phosphodiesterases have motivated the search for potent inhibitors to treat neurodegenerative and inflammatory diseases. Different heterocyclic compounds have been described over the years; among them, phenyl-2-thioxo-(1H)-quinazolin-4-one, called S14, has shown very promising results in different in vitro and in vivo studies. Recently, polymeric nanoparticles have been used as new formulations to target specific organs and produce controlled release of certain drugs. In this work, we describe poly(lactic-co-glycolic acid) (PLGA)-based polymeric nanoparticles loaded with S14. Their preparation, optimization, characterization and in vivo drug release profile are here presented as an effort to improve pharmacokinetic properties of this interesting PDE7 inhibitor., This research was supported by MINECO (grant RTC-2015-3439-1 and PID2019-105600RB-I00), ISCiii CIBERNED (CB18/05/00040), MECD (FPU14-00204 to E.R.-P. and FPU16-04466 to V.N.) and H2020-MSCA-ITN-2017 (grant no. 765912 to I.M.).

Published

2021

10. In vivo real time non invasive monitoring of brain penetration of chemicals with near-infrared spectroscopy: Concomitant PK/PD analysis

Author

Luigi Rovati, Stefano Cattini, Francesco Crespi, Andrea Bandera, and Maurizio Donini

Subjects

Pathology, medicine.medical_specialty, Brain penetration, CO(2), Hb, HbO(2), In vivo, NIRS, Non invasive, O(2), PK/PD, Rat brain, Pharmacology, 01 natural sciences, 010309 optics, Hemoglobins, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, 0103 physical sciences, medicine, Animals, PK/PD models, Spectroscopy, Near-Infrared, Chemistry, General Neuroscience, Near-infrared spectroscopy, Brain, Penetration (firestop), Oxygenation, Carbon Dioxide, Rats, Oxygen, 030217 neurology & neurosurgery, Ex vivo

Abstract

Background Near-infrared spectroscopy (NIRS) is a non-invasive technique that monitors changes in oxygenation of haemoglobin. The absorption spectra of near-infrared light differ for the oxygenation–deoxygenation states of haemoglobin (oxygenate (HbO 2 ) and deoxygenate (Hb), respectively) so that these two states can be directly monitored. Comparison with existing method(s) Different methodologies report different basal values of HbO 2 and Hb absolute concentrations in brain. Here, we attempt to calculate basal HbO 2 levels in rat CNS via evaluation of the influence of exogenous oxygen or exogenous carbon dioxide on the NIRS parameters measured in vivo. New method Furthermore the possibility that changes of haemoglobin oxygenation in rat brain as measured by NIRS might be a useful index of brain penetration of chemical entities has been investigated. Different compounds from different chemical classes were selected on the basis of parallel ex vivo and in vivo pharmacokinetic (PK/PD) studies of brain penetration and overall pharmacokinetic profile. Results It appeared that NIRS might contribute to assess brain penetration of chemical entities, i.e. significant changes in NIRS signals could be related to brain exposure, conversely the lack of significant changes in relevant NIRS parameters could be indicative of low brain exposure. Conclusions This work is proposing a further innovation on NIRS preclinical applications i.e. a “chemical” NIRS [chNIRS] approach for determining penetration of drugs in animal brain. Therefore, chNIRS could became a non invasive methodology for studies on neurobiological processes and psychiatric diseases in preclinical but also a translational strategy from preclinical to clinical investigations.

Published

2016

11. In Vitro and In Vivo Evaluation of the Antifungal Activity of APX001A/APX001 against Candida auris

Author

Karen J. Shaw, Fatima Zohra Abidi, Christopher L. Hager, Lisa Long, Emily L Larkin, and Mahmoud A. Ghannoum

Subjects

0301 basic medicine, APX001, efficacy, 030106 microbiology, yeast, survival, brain penetration, Microbiology, 03 medical and health sciences, In vivo, Amphotericin B, Medicine, Experimental Therapeutics, Pharmacology (medical), infection model, Pharmacology, Kidney, Fungal protein, business.industry, APX001A, susceptibility testing, antifungal susceptibility testing, Candida auris, In vitro, 3. Good health, Infectious Diseases, medicine.anatomical_structure, Anidulafungin, business, Fluconazole, medicine.drug

Abstract

Candida auris is an emerging multidrug-resistant yeast that has been responsible for invasive infections associated with high morbidity and mortality. C. auris strains often demonstrate high fluconazole and amphotericin B MIC values, and some strains are resistant to all three major antifungal classes. We evaluated the susceptibility of 16 C. auris clinical strains, isolated from a wide geographical area, to 10 antifungal agents, including APX001A, a novel agent that inhibits the fungal protein Gwt1 (glycosylphosphatidylinositol-anchored wall transfer protein 1). APX001A demonstrated significantly lower MIC 50 and MIC 90 values (0.004 and 0.031 μg/ml, respectively) than all other agents tested. The efficacy of the prodrug APX001 was evaluated in an immunocompromised murine model of disseminated C. auris infection. Significant efficacy (80 to 100% survival) was observed in all three APX001 treatment groups versus 50% survival for the anidulafungin treatment group. In addition, APX001 showed a significant log reduction in CFU counts in kidney, lung, and brain tissue (1.03 to 1.83) versus the vehicle control. Anidulafungin also showed a significant log reduction in CFU in the kidneys and lungs (1.5 and 1.62, respectively) but did not impact brain CFU. These data support further clinical evaluation of this new antifungal agent.

Published

2018

12. Quantitative microdialysis using modified ultraslow microdialysis

Author

Jan Paul van Loon, Martin G. de Vries, Thomas I. F. H. Cremers, Marieke C. G. van der Hart, Ben H.C. Westerink, Bjarke Ebert, Kirsten D. Huinink, Elizabeth C. M. de Lange, Biomonitoring and Sensoring, and Medicinal Chemistry and Bioanalysis (MCB)

Subjects

Male, Microdialysis, PHARMACOKINETICS, BLOOD, INTRACEREBRAL MICRODIALYSIS, INVIVO, Analytical chemistry, Prefrontal Cortex, RETRODIALYSIS, Citalopram, CEREBROSPINAL-FLUID, Recovery, In vivo, Intracerebral microdialysis, Animals, Rats, Wistar, CALIBRATION, Brain penetration, Chemistry, General Neuroscience, Brain, P-GLYCOPROTEIN, Isoxazoles, IN-VITRO, TRANSPORT, Rats, Dialysis method, Brain concentrations, Ultraslow, Extracellular Space, Central Nervous System Agents, Biomedical engineering, Quantitative

Abstract

The only method to quantify free extracellular levels of drugs in the brain of living animals is microdialysis. However, quantitative microdialysis has been hampered by methodological issues for decades. The problems arise from the need to establish the in vivo recovery for appropriate quantitation. In dealing with these issues the "dynamic no-net-flux" (DNNF) method seemed to be the experimental method of choice. Major disadvantages were, however, the need for a very high degree of bioanalytical precision and accuracy and the need for a large number of animals. Moreover, today we know that the experimental data are not always straightforward. To improve robustness and practicality of quantitative microdialysis sampling we modified the ultraslow microdialysis approach. Ultraslow microdialysis uses very low microdialysis flow rates (

Published

2009