Your search keyword '"Tomokazu Tajiri"' showing total 8 results

1. Biowaiver Monograph for Immediate-Release Solid Oral Dosage Forms: Sitagliptin Phosphate Monohydrate

Author

Rodrigo Cristofoletti, Mehul Mehta, Tomokazu Tajiri, Jennifer B. Dressman, Peter Langguth, James E. Polli, Naseem A. Charoo, Hassan A. Hassan, Daud Baraka Abdallah, Ahmed Abdalla Bakheit, Bertil Abrahamsson, Vinod P. Shah, Kashif Ul Haque, and Alan F. Parr

Subjects

Dosage Forms, Drug, business.industry, media_common.quotation_subject, Sitagliptin Phosphate, Administration, Oral, Biological Availability, Pharmaceutical Science, Pharmacology, Bioequivalence, Biopharmaceutics Classification System, Permeability, Dosage form, Biopharmaceutics, Bioavailability, Solubility, Therapeutic Equivalency, Pharmacokinetics, Sitagliptin, Pharmacodynamics, medicine, Humans, business, medicine.drug, media_common

Abstract

Sitagliptin is an antihyperglycemic drug used in adults for the treatment of diabetes Type 2. Literature data and in-house experiments were applied in this monograph to assess whether methods based on the Biopharmaceutics Classification System (BCS) could be used to assess the bioequivalence of solid immediate-release (IR) oral dosage forms containing sitagliptin phosphate monohydrate, as an alternative to a pharmacokinetic study in human volunteers. The solubility and permeability characteristics of sitagliptin were reviewed according to the BCS, along with dissolution, therapeutic index, therapeutic applications, pharmacokinetics, pharmacodynamic characteristics, reports of bioequivalence (BE) / bioavailability problems, data on interactions between the drug and excipients and other data germane to the subject. All data reviewed in this monograph unambiguously support classification of sitagliptin as a BCS Class 1 drug. In light of its broad therapeutic index and lack of severe adverse effects, the clinical risks associated with moderately supraoptimal doses were deemed inconsequential, as were the risks associated with moderately suboptimal doses. Taking all evidence into consideration, it was concluded that the BCS-based biowaiver can be implemented for solid IR oral drug products containing sitagliptin phosphate monohydrate, provided (a) the test product is formulated solely with excipients commonly present in solid IR oral drug products approved in ICH or associated countries and used in amounts commonly applied in this type of product, (b) data in support of the BCS-based biowaiver are obtained using the methods recommended by the WHO, FDA, EMA or ICH and (c) the test product and the comparator product (which is the innovator product in this case) meet all in vitro dissolution specifications provided in the WHO, FDA, EMA or ICH guidance.

Published

2022

2. A Novel In Vitro Membrane Permeability Methodology Using Three-dimensional Caco-2 Tubules in a Microphysiological System Which Better Mimics In Vivo Physiological Conditions

Author

Linda Gijzen, Kouichi Yoshinari, Niels Ouwerkerk, Kei Motonaga, Marleen Bokkers, Yuki Hagiwara, Remko van Vught, Harumi Kumagai, Tomokazu Tajiri, Rumaisha Annida, and Yoshifumi Katakawa

Subjects

Cell Membrane Permeability, Bile acid, Membrane permeability, Chemistry, medicine.drug_class, Human gastrointestinal tract, Pharmaceutical Science, Permeability, In vitro, Intestinal fluid, Bile Acids and Salts, Gastrointestinal Tract, medicine.anatomical_structure, Intestinal Absorption, Caco-2, Permeability (electromagnetism), In vivo, medicine, Biophysics, Humans, Caco-2 Cells

Abstract

The aim of this study was to develop an in vitro drug permeability methodology which mimics the gastrointestinal environment more accurately than conventional 2D methodologies through a three-dimensional (3D) Caco-2 tubules using a microphysiological system. Such a system offers significant advantages, including accelerated cellular polarization and more accurate mimicry of the in vivo environment. This methodology was confirmed by measuring the permeability of propranolol as a model compound, and subsequently applied to those of solifenacin and bile acids for a comprehensive understanding of permeability for the drug product in the human gastrointestinal tract. To protect the Caco-2 tubules from bile acid toxicity, a mucus layer was applied on the surface of Caco-2 tubules and it enables to use simulated intestinal fluid. The assessment using propranolol reproduced results equivalent to those obtained from conventional methodology, while that using solifenacin indicated fluctuations in the permeability of solifenacin due to various factors, including interaction with bile acids. We therefore suggest that this model will serve as an alternative testing system for measuring drug absorption in an environment closely resembling that of the human gastrointestinal tract.

Published

2022

3. Novel Dissolution Approach for Tacrolimus-Loaded Microspheres Using a Dialysis Membrane for in Vitro–in Vivo Correlation

Author

Shin-ichiro Kimura, Masanori Kaihara, Yasunori Iwao, Yoshifumi Katakawa, Kei Motonaga, Kazuhiro Hojo, Hiromu Kondo, Takatsune Yoshida, Tomokazu Tajiri, and Atsushi Kambayashi

Subjects

010405 organic chemistry, Chemistry, General Chemistry, General Medicine, 010402 general chemistry, 01 natural sciences, 0104 chemical sciences, Microsphere, Dialysis tubing, Pharmacokinetics, In vivo, Drug Discovery, Paddle, Dissolution testing, In vitro in vivo, Dissolution, Biomedical engineering

Abstract

The aim of this study was to establish a novel approach to in vitro dissolution evaluation using a combination of the paddle method and a dialysis membrane, both to predict the overall in vivo performance of tacrolimus microspheres and also to identify a suitable dissolution test method to describe the in vivo initial burst phenomenon. This new dissolution method for evaluating the release of tacrolimus from microspheres consisted of rotating a customized paddle inside a dialysis membrane using a conventional paddle apparatus. Findings were compared with a method in which the paddle was rotated outside the dialysis membrane, the conventional paddle method, and the flow-through cell method. We concluded that the paddle method with a dialysis membrane and internal agitation, which was designed to mimic in vivo conditions, predicted the overall pharmacokinetic (PK) profile of tacrolimus microspheres whereas the conventional paddle method described the initial burst. These findings suggest that it may not be possible to predict both the PK profile and initial burst using a single analysis method. We therefore recommend that evaluation of the initial burst be performed separately. In conclusion, we propose that combination of the paddle method with a dialysis membrane and internal agitation to evaluate the overall PK profile, together with the paddle method to describe the in vivo initial burst, represents a novel approach to in vitro dissolution evaluation for microsphere formulations.

Published

2019

4. Biowaiver Monographs for Immediate Release Solid Oral Dosage Forms: Cephalexin Monohydrate

Author

Bertil Abrahamsson, Paul M. Quizon, Gerlinde F. Plöger, Rodrigo Cristofoletti, Alan F. Parr, D.W. Groot, Tomokazu Tajiri, Vinod P. Shah, Jennifer B. Dressman, Mehul Mehta, James E. Polli, and Peter Langguth

Subjects

Drug, media_common.quotation_subject, Pharmaceutical Science, Excipient, Administration, Oral, Biological Availability, 02 engineering and technology, Bioequivalence, Pharmacology, 030226 pharmacology & pharmacy, Dosage form, Permeability, Biopharmaceutics, 03 medical and health sciences, 0302 clinical medicine, medicine, Biopharmaceutics Classification System (BCS), Humans, Regulatory science, LADME characteristics, media_common, Active ingredient, cephalexin monohydrate, Dosage Forms, bioequivalence, Cephalexin, excipients, business.industry, 021001 nanoscience & nanotechnology, Biopharmaceutics Classification System, Solubility, Therapeutic Equivalency, regulatory science, 0210 nano-technology, business, medicine.drug

Abstract

Literature data and results of experimental studies relevant to the decision to allow waiver of bioequivalence studies in humans for the approval of immediate release solid oral dosage forms containing cephalexin monohydrate are presented. Solubility studies were performed in accordance with the current biowaiver guidelines of the Food and Drug Administration, World Health Organization and European Medicines Agency, taking the degradation at some pH values into consideration. Together with solubility and permeability data for cephalexin monohydrate from the literature, it was demonstrated to be a Biopharmaceutics Classification System Class 1 drug. The pharmacokinetic behavior, results of bioequivalence studies published in the literature, as well as the therapeutic uses, potential toxicity and potential excipient effects on bioavailability were also assessed. Cephalexin has a wide therapeutic index and no bioequivalence problems have been reported. Dissolution studies were run under Biopharmaceutics Classification System-biowaiver conditions for the pure drug and 2 generic formulations available on the German market. Considering all relevant aspects, it was concluded that a biowaiver-based approval for products containing cephalexin monohydrate as the single active pharmaceutical ingredient is scientifically justified, provided that well-established excipients are used in usual amounts and that both test and reference dosage forms meet the guideline criteria of either "rapidly dissolving" or "very rapidly dissolving."

Published

2019

5. Biowaiver Monograph for Immediate-Release Solid Oral Dosage Forms: Ondansetron

Author

Alan F. Parr, Tomokazu Tajiri, Bertil Abrahamsson, Jennifer B. Dressman, Mangal S. Nagarsenker, Vinod P. Shah, Rodrigo Cristofoletti, James E. Polli, Peter Langguth, Mehul Mehta, Gopal Singh Rajawat, D.W. Groot, and Tejashree Belubbi

Subjects

Nausea, Pharmaceutical Science, Administration, Oral, Biological Availability, dissolution, 02 engineering and technology, Bioequivalence, Pharmacology, 030226 pharmacology & pharmacy, Dosage form, Biopharmaceutics, Ondansetron, Excipients, 03 medical and health sciences, ondansetron hydrochloride dihydrate, 0302 clinical medicine, Pharmacokinetics, Medicine, Humans, Dissolution testing, Dosage Forms, Ondansetron hydrochloride, business.industry, biopharmaceutics classification system (BCS), solubility, 021001 nanoscience & nanotechnology, Biopharmaceutics Classification System, biowaiver, Therapeutic Equivalency, medicine.symptom, permeability, 0210 nano-technology, business, medicine.drug, Tablets

Abstract

Literature data pertaining to the physicochemical, pharmaceutical, and pharmacokinetic properties of ondansetron hydrochloride dihydrate are reviewed to arrive at a decision on whether a marketing authorization of an immediate release (IR) solid oral dosage form can be approved based on a Biopharmaceutics Classification System (BCS)-based biowaiver. Ondansetron, a 5HT3 receptor antagonist, is used at doses ranging from 4 mg to 24 mg in the management of nausea and vomiting associated with chemotherapy, radiotherapy, and postoperative treatment. It is a weak base and thus exhibits pH-dependent solubility. However, it is able to meet the criteria of "high solubility" as well as "high permeability" and can therefore be classified as a BCS class I drug. Furthermore, ondansetron hydrochloride 8 mg IR tablets (Zofran® 8 mg) and multiples thereof (16 mg = Zofran® 8 mg × 2 tablets and 24 mg = Zofran® 8 mg × 3 tablets) meet the criteria of "rapidly dissolving" in dissolution testing. Ondansetron hydrochloride has a wide therapeutic window and is well-tolerated after oral administration. Based on its favorable physicochemical properties, pharmacokinetic data and the minimal risks associated with an incorrect bioequivalence decision, the BCS-based biowaiver procedure can be recommended for ondansetron hydrochloride dihydrate IR tablets.

Published

2019

6. Novel Dissolution Approach for Tacrolimus-Loaded Microspheres Using a Dialysis Membrane for in Vitro-in Vivo Correlation

Author

Masanori, Kaihara, Kazuhiro, Hojo, Tomokazu, Tajiri, Atsushi, Kambayashi, Takatsune, Yoshida, Yoshifumi, Katakawa, Kei, Motonaga, Shin-Ichiro, Kimura, Yasunori, Iwao, and Hiromu, Kondo

Subjects

Drug Carriers, Drug Liberation, Models, Chemical, Polylactic Acid-Polyglycolic Acid Copolymer, Solubility, Chemistry, Pharmaceutical, Polyesters, Membranes, Artificial, Equipment Design, Immunosuppressive Agents, Microspheres, Tacrolimus

Abstract

The aim of this study was to establish a novel approach to in vitro dissolution evaluation using a combination of the paddle method and a dialysis membrane, both to predict the overall in vivo performance of tacrolimus microspheres and also to identify a suitable dissolution test method to describe the in vivo initial burst phenomenon. This new dissolution method for evaluating the release of tacrolimus from microspheres consisted of rotating a customized paddle inside a dialysis membrane using a conventional paddle apparatus. Findings were compared with a method in which the paddle was rotated outside the dialysis membrane, the conventional paddle method, and the flow-through cell method. We concluded that the paddle method with a dialysis membrane and internal agitation, which was designed to mimic in vivo conditions, predicted the overall pharmacokinetic (PK) profile of tacrolimus microspheres whereas the conventional paddle method described the initial burst. These findings suggest that it may not be possible to predict both the PK profile and initial burst using a single analysis method. We therefore recommend that evaluation of the initial burst be performed separately. In conclusion, we propose that combination of the paddle method with a dialysis membrane and internal agitation to evaluate the overall PK profile, together with the paddle method to describe the in vivo initial burst, represents a novel approach to in vitro dissolution evaluation for microsphere formulations.

Published

2019

7. The mechanism of solifenacin release from a pH-responsive ion-complex oral suspension in the fasted upper gastrointestinal lumen

Author

Maria Vertzoni, Kei Motonaga, Niels Ouwerkerk, Christos Reppas, Yoshifumi Katakawa, Daisuke Murayama, Yosuke Yamamoto, Moe Haneda, Tomokazu Tajiri, and Harumi Kumagai

Subjects

food.ingredient, Administration, Oral, Pharmaceutical Science, Lumen (anatomy), 02 engineering and technology, 030226 pharmacology & pharmacy, Lecithin, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, food, Suspensions, Intestine, Small, medicine, Humans, Particle Size, Ion-exchange resin, Chromatography, Solifenacin, Chemistry, technology, industry, and agriculture, Cationic polymerization, Fasting, Solifenacin Succinate, Hydrogen-Ion Concentration, 021001 nanoscience & nanotechnology, Taurocholic acid, Small intestine, Drug Liberation, medicine.anatomical_structure, Intestinal Absorption, Solubility, Gastric Mucosa, Particle size, 0210 nano-technology, medicine.drug

Abstract

The main objective of this study was to investigate the mechanism of solifenacin release from a pH-responsive ion-complex oral resinate suspension under conditions simulating the environment in the upper gastrointestinal lumen. A secondary objective was to propose an appropriate in vitro methodology for evaluating the quality of orally administered solifenacin suspensions. The mechanism of solifenacin release from polacrilin potassium resin (Amberlite® IRP88) was investigated using biorelevant media and compendial setups (USP Apparatus 2 and USP Apparatus 4) and using newer, recently validated in vitro methodologies [biorelevant gastrointestinal transfer (BioGIT) system]. We evaluated the impact of particle size and concentration of the resin; thickener concentration (carbomer homopolymer, type B); and the impact of pH, cationic strength, agitation intensity and level of simulation of contents in the upper gastrointestinal lumen. Data suggested that solifenacin release from the resinate was determined by the resin particle size, the medium pH, cationic strength (when the conditions in the upper small intestine are simulated) and the level of simulation of contents in the upper small intestine. The interaction of solifenacin with taurocholic acid/lecithin aggregates was significant, but unlikely to affect the degree of solifenacin absorption, as a BCS Class I compound. Under acidic conditions, solifenacin was dissociated and released from the pH-responsive resin rapidly. Under conditions simulating the contents of the upper small intestine, solifenacin was replaced by cations from the testing media and diffused through the resin matrix. All three in vitro systems with or without a pH gradient are useful in distinguishing solifenacin release characteristics from resinate suspensions with different particle sizes. Because of this drug release mechanism, USP Apparatus 2 with fixed pH media demonstrated equivalent or slightly higher discriminative sensitivity than the other setups and appears to be appropriate for product quality control.

Published

2020

8. The BioGIT System: a Valuable In Vitro Tool to Assess the Impact of Dose and Formulation on Early Exposure to Low Solubility Drugs After Oral Administration

Author

Vicky Barmpatsalou, Christer Tannergren, Patrick Augustijns, Joerg Rosenberg, Alexandros Kourentas, Mira Symillides, Stefania Beato, James Butler, Maria Vertzoni, Tomokazu Tajiri, René Holm, Neils Ouwerkerk, and Christos Reppas

Subjects

Posaconazole, Drug Compounding, Pharmaceutical Science, Administration, Oral, Capsules, 02 engineering and technology, In Vitro Techniques, 030226 pharmacology & pharmacy, Models, Biological, 03 medical and health sciences, 0302 clinical medicine, Nifedipine, Suspensions, Oral administration, medicine, Solubility, Active ingredient, Chromatography, Fenofibrate, Dose-Response Relationship, Drug, Chemistry, Capsule, 021001 nanoscience & nanotechnology, Pharmaceutical Preparations, Gastrointestinal Absorption, Area Under Curve, 0210 nano-technology, Weak base, medicine.drug, Tablets

Abstract

The purpose of this study was to evaluate the usefulness of the in vitro biorelevant gastrointestinal transfer (BioGIT) system in assessing the impact of dose and formulation on early exposure by comparing in vitro data with previously collected human plasma data of low solubility active pharmaceutical ingredients. Eight model active pharmaceutical ingredients were tested; Lu 35-138C (salt of weak base in a HP-beta-CD solution, three doses), fenofibrate (solid dispersion, tablet, two doses), AZD2207 EQ (salt of weak base, capsule, three doses), posaconazole (Noxafil® suspension, two doses), SB705498 (weak base, tablets vs. capsules), cyclosporine A (Sandimmun® vs. Sandimmun® Neoral), nifedipine (Adalat® capsule vs. Macorel® tablet), and itraconazole (Sporanox® capsule vs. Sporanox® solution). AUC0–0.75h values were calculated from the apparent concentration versus time data in the duodenal compartment of the BioGIT system. Differences in AUC0–0.75h values were evaluated versus differences in AUC0–1h and in AUC0–2h values calculated from previously collected plasma data in healthy adults. Ratios of mean AUC0–0.75h, mean AUC0–1h, and mean AUC0–2h values were estimated using the lowest dose or the formulation with the lower AUC0–0.75h value as denominator. The BioGIT system qualitatively identified the impact of dose and of formulation on early exposure in all cases. Log-transformed mean BioGIT AUC0–0.75h ratios correlated significantly with log-transformed mean plasma AUC0–1h ratios. Based on this correlation, BioGIT AUC0–0.75h ratios between 0.3 and 10 directly reflect corresponding plasma AUC0–1h ratios. BioGIT system is a valuable tool for the assessment of the impact of dose and formulation on early exposure to low solubility drugs.

Published

2018