Your search keyword '"Yasuhiro Tsume"' showing total 75 results

1. An In Vivo Predictive Dissolution Methodology (iPD Methodology) with a BCS Class IIb Drug Can Predict the In Vivo Bioequivalence Results: Etoricoxib Products

Author

Isabel Gonzalez-Alvarez, Marival Bermejo, Yasuhiro Tsume, Alejandro Ruiz-Picazo, Marta Gonzalez-Alvarez, Bart Hens, Alfredo Garcia-Arieta, Greg E. Amidon, and Gordon L. Amidon

Subjects

gastrointestinal simulator, in vitro dissolution, BCS class II, weak base, dissolution modelling, Pharmacy and materia medica, RS1-441

Abstract

The purpose of this study was to predict in vivo performance of three oral products of Etoricoxib (Arcoxia® as reference and two generic formulations in development) by conducting in vivo predictive dissolution with GIS (Gastro Intestinal Simulator) and computational analysis. Those predictions were compared with the results from previous bioequivalence (BE) human studies. Product dissolution studies were performed using a computer-controlled multicompartmental dissolution device (GIS) equipped with three dissolution chambers, representing stomach, duodenum, and jejunum, with integrated transit times and secretion rates. The measured dissolved amounts were modelled in each compartment with a set of differential equations representing transit, dissolution, and precipitation processes. The observed drug concentration by in vitro dissolution studies were directly convoluted with permeability and disposition parameters from literature to generate the predicted plasma concentrations. The GIS was able to detect the dissolution differences among reference and generic formulations in the gastric chamber where the drug solubility is high (pH 2) while the USP 2 standard dissolution test at pH 2 did not show any difference. Therefore, the current study confirms the importance of multicompartmental dissolution testing for weak bases as observed for other case examples but also the impact of excipients on duodenal and jejunal in vivo behavior.

Published

2021

2. A Mechanistic Physiologically-Based Biopharmaceutics Modeling (PBBM) Approach to Assess the In Vivo Performance of an Orally Administered Drug Product: From IVIVC to IVIVP

Author

Marival Bermejo, Bart Hens, Joseph Dickens, Deanna Mudie, Paulo Paixão, Yasuhiro Tsume, Kerby Shedden, and Gordon L. Amidon

Subjects

oral absorption, in silico modeling, gastroplus, phoenix winnonlin, pharmacokinetics, clinical studies, ibuprofen, manometry, gastrointestinal, mechanistic modeling, pbpk, pbbm, Pharmacy and materia medica, RS1-441

Abstract

The application of in silico modeling to predict the in vivo outcome of an oral drug product is gaining a lot of interest. Fully relying on these models as a surrogate tool requires continuous optimization and validation. To do so, intraluminal and systemic data are desirable to judge the predicted outcomes. The aim of this study was to predict the systemic concentrations of ibuprofen after oral administration of an 800 mg immediate-release (IR) tablet to healthy subjects in fasted-state conditions. A mechanistic oral absorption model coupled with a two-compartmental pharmacokinetic (PK) model was built in Phoenix WinNonlinWinNonlin® software and in the GastroPlus™ simulator. It should be noted that all simulations were performed in an ideal framework as we were in possession of a plethora of in vivo data (e.g., motility, pH, luminal and systemic concentrations) in order to evaluate and optimize these models. All this work refers to the fact that important, yet crucial, gastrointestinal (GI) variables should be integrated into biopredictive dissolution testing (low buffer capacity media, considering phosphate versus bicarbonate buffer, hydrodynamics) to account for a valuable input for physiologically-based pharmacokinetic (PBPK) platform programs. While simulations can be performed and mechanistic insights can be gained from such simulations from current software, we need to move from correlations to predictions (IVIVC → IVIVP) and, moreover, we need to further determine the dynamics of the GI variables controlling the dosage form transit, disintegration, dissolution, absorption and metabolism along the human GI tract. Establishing the link between biopredictive in vitro dissolution testing and mechanistic oral absorption modeling (i.e., physiologically-based biopharmaceutics modeling (PBBM)) creates an opportunity to potentially request biowaivers in the near future for orally administered drug products, regardless of its classification according to the Biopharmaceutics Classification System (BCS).

Published

2020

3. The Dipeptide Monoester Prodrugs of Floxuridine and Gemcitabine—Feasibility of Orally Administrable Nucleoside Analogs

Author

Yasuhiro Tsume, Blanca Borras Bermejo, and Gordon L. Amidon

Subjects

gemcitabine prodrug, floxuridine prodrug, mouse in situ perfusion, pancreatic tumor cells, dipeptide, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Dipeptide monoester prodrugs of floxuridine and gemcitabine were synthesized. Their chemical stability in buffers, enzymatic stability in cell homogenates, permeability in mouse intestinal membrane along with drug concentration in mouse plasma, and anti-proliferative activity in cancer cells were determined and compared to their parent drugs. Floxuridine prodrug was more enzymatically stable than floxuridine and the degradation from prodrug to parent drug works as the rate-limiting step. On the other hand, gemcitabine prodrug was less enzymatically stable than gemcitabine. Those dipeptide monoester prodrugs exhibited 2.4- to 48.7-fold higher uptake than their parent drugs in Caco-2, Panc-1, and AsPC-1 cells. Floxuridine and gemcitabine prodrugs showed superior permeability in mouse jejunum to their parent drugs and exhibited the higher drug concentration in plasma after in situ mouse perfusion. Cell proliferation assays in ductal pancreatic cancer cells, AsPC-1 and Panc-1, indicated that dipeptide prodrugs of floxuridine and gemcitabine were more potent than their parent drugs. The enhanced potency of nucleoside analogs was attributed to their improved membrane permeability. The prodrug forms of 5¢-L-phenylalanyl-l-tyrosyl-floxuridine and 5¢-L-phenylalanyl-L-tyrosyl-gemcitabine appeared in mouse plasma after the permeation of intestinal membrane and the first-pass effect, suggesting their potential for the development of oral dosage form for anti-cancer agents.

Published

2014

4. Exploring Bioequivalence of Dexketoprofen Trometamol Drug Products with the Gastrointestinal Simulator (GIS) and Precipitation Pathways Analyses

Author

Marival Bermejo, Gislaine Kuminek, Jozef Al-Gousous, Alejandro Ruiz-Picazo, Yasuhiro Tsume, Alfredo Garcia-Arieta, Isabel González-Alvarez, Bart Hens, Gregory E. Amidon, Nair Rodriguez-Hornedo, Gordon L. Amidon, and Deanna Mudie

Subjects

gastrointestinal absorption, dexketoprofen, gastrointestinal simulator, microscopy imaging, liquid–liquid phase separation, oral absorption, in vitro dissolution, Pharmacy and materia medica, RS1-441

Abstract

The present work aimed to explain the differences in oral performance in fasted humans who were categorized into groups based on the three different drug product formulations of dexketoprofen trometamol (DKT) salt—Using a combination of in vitro techniques and pharmacokinetic analysis. The non-bioequivalence (non-BE) tablet group achieved higher plasma Cmax and area under the curve (AUC) than the reference and BE tablets groups, with only one difference in tablet composition, which was the presence of calcium monohydrogen phosphate, an alkalinizing excipient, in the tablet core of the non-BE formulation. Concentration profiles determined using a gastrointestinal simulator (GIS) apparatus designed with 0.01 N hydrochloric acid and 34 mM sodium chloride as the gastric medium and fasted state simulated intestinal fluids (FaSSIF-v1) as the intestinal medium showed a faster rate and a higher extent of dissolution of the non-BE product compared to the BE and reference products. These in vitro profiles mirrored the fraction doses absorbed in vivo obtained from deconvoluted plasma concentration–time profiles. However, when sodium chloride was not included in the gastric medium and phosphate buffer without bile salts and phospholipids were used as the intestinal medium, the three products exhibited nearly identical concentration profiles. Microscopic examination of DKT salt dissolution in the gastric medium containing sodium chloride identified that when calcium phosphate was present, the DKT dissolved without conversion to the less soluble free acid, which was consistent with the higher drug exposure of the non-BE formulation. In the absence of calcium phosphate, however, dexketoprofen trometamol salt dissolution began with a nano-phase formation that grew to a liquid–liquid phase separation (LLPS) and formed the less soluble free acid crystals. This phenomenon was dependent on the salt/excipient concentrations and the presence of free acid crystals in the salt phase. This work demonstrated the importance of excipients and purity of salt phase on the evolution and rate of salt disproportionation pathways. Moreover, the presented data clearly showed the usefulness of the GIS apparatus as a discriminating tool that could highlight the differences in formulation behavior when utilizing physiologically-relevant media and experimental conditions in combination with microscopy imaging.

Published

2019

5. The Feasibility of Enzyme Targeted Activation for Amino Acid/Dipeptide Monoester Prodrugs of Floxuridine; Cathepsin D as a Potential Targeted Enzyme

Author

Gordon L. Amidon and Yasuhiro Tsume

Subjects

prodrugs, Capan-2 cell, cathepsin, enzymatic activation, cell proliferation assay, Organic chemistry, QD241-441

Abstract

The improvement of therapeutic efficacy for cancer agents has been a big challenge which includes the increase of tumor selectivity and the reduction of adverse effects at non-tumor sites. In order to achieve those goals, prodrug approaches have been extensively investigated. In this report, the potential activation enzymes for 5¢-amino acid/dipeptide monoester floxuridine prodrugs in pancreatic cancer cells were selected and the feasibility of enzyme specific activation of prodrugs was evaluated. All prodrugs exhibited the range of 3.0–105.7 min of half life in Capan-2 cell homogenate with the presence and the absence of selective enzyme inhibitors. 5¢-O-L-Phenylalanyl-L-tyrosyl-floxuridine exhibited longer half life only with the presence of pepstatin A. Human cathepsin B and D selectively hydrolized 5¢-O-L-phenylalanyl-L-tyrosylfloxuridine and 5¢-O-L-phenylalanyl-L-glycylfloxuridine compared to the other tested prodrugs. The wide range of growth inhibitory effect by floxuridine prodrugs in Capan-2 cells was observed due to the different affinities of prodrug promoieties to enyzmes. In conclusion, it is feasible to design prodrugs which are activated by specific enzymes. Cathepsin D might be a good candidate as a target enzyme for prodrug activation and 5¢-O-L-phenylalanyl-L-tyrosylfloxuridine may be the best candidate among the tested floxuridine prodrugs.

Published

2012

6. Enhanced Absorption and Growth Inhibition with Amino Acid Monoester Prodrugs of Floxuridine by Targeting hPEPT1 Transporters

Author

Gordon L. Amidon, Chandrasekharan Ramachandran, John M. Hilfinger, Christopher P. Landowski, Jing Sun, Balvinder S. Vig, and Yasuhiro Tsume

Subjects

5-FU, floxuridine, prodrugs, Caco-2 permeability, cell proliferation assays, oligopeptide transporter 1 (PEPT1), Organic chemistry, QD241-441

Abstract

A series of amino acid monoester prodrugs of floxuridine was synthesized and evaluated for the improvement of oral bioavailability and the feasibility of target drug delivery via oligopeptide transporters. All floxuridine 5′-amino acid monoester prodrugs exhibited PEPT1 affinity, with inhibition coefficients of Gly-Sar uptake (IC50) ranging from 0.7 – 2.3 mM in Caco-2 and 2.0 – 4.8 mM in AsPC-1 cells, while that of floxuridine was 7.3 mM and 6.3 mM, respectively. Caco-2 membrane permeabilities of floxuridine prodrugs (1.01 – 5.31 x 10-6 cm/sec) and floxuridine (0.48 x 10-6 cm/sec) were much higher than that of 5-FU (0.038 x 10-6 cm/sec). MDCK cells stably transfected with the human oligopeptide transporter PEPT1 (MDCK/hPEPT1) exhibited enhanced cell growth inhibition in the presence of the prodrugs. This prodrug strategy offers great potential, not only for increased drug absorption but also for improved tumor selectivity and drug efficacy.

Published

2008

7. Potential Development of Tumor-Targeted Oral Anti-Cancer Prodrugs: Amino Acid and Dipeptide Monoester Prodrugs of Gemcitabine

Author

Yasuhiro Tsume, Adam J. Drelich, David E. Smith, and Gordon L. Amidon

Subjects

gemcitabine prodrugs, stroma cells, pancreatic cancer, metabolism, cytosine deaminase, Organic chemistry, QD241-441

Abstract

One of the main obstacles for cancer therapies is to deliver medicines effectively to target sites. Since stroma cells are developed around tumors, chemotherapeutic agents have to go through stroma cells in order to reach tumors. As a method to improve drug delivery to the tumor site, a prodrug approach for gemcitabine was adopted. Amino acid and dipeptide monoester prodrugs of gemcitabine were synthesized and their chemical stability in buffers, resistance to thymidine phosphorylase and cytidine deaminase, antiproliferative activity, and uptake/permeability in HFF cells as a surrogate to stroma cells were determined and compared to their parent drug, gemcitabine. The activation of all gemcitabine prodrugs was faster in pancreatic cell homogenates than their hydrolysis in buffer, suggesting enzymatic action. All prodrugs exhibited great stability in HFF cell homogenate, enhanced resistance to glycosidic bond metabolism by thymidine phosphorylase, and deamination by cytidine deaminase compared to their parent drug. All gemcitabine prodrugs exhibited higher uptake in HFF cells and better permeability across HFF monolayers than gemcitabine, suggesting a better delivery to tumor sites. Cell antiproliferative assays in Panc-1 and Capan-2 pancreatic ductal cell lines indicated that the gemcitabine prodrugs were more potent than their parent drug gemcitabine. The transport and enzymatic profiles of gemcitabine prodrugs suggest their potential for delayed enzymatic bioconversion and enhanced resistance to metabolic enzymes, as well as for enhanced drug delivery to tumor sites, and cytotoxic activity in cancer cells. These attributes would facilitate the prolonged systemic circulation and improved therapeutic efficacy of gemcitabine prodrugs.

Published

2017

8. Selection of Suitable Prodrug Candidates for in vivo Studies via in vitro Studies; The Correlation of Prodrug Stability in Between Cell Culture Homogenates and Human Tissue Homogenates

Author

Yasuhiro Tsume and Gordon L Amidon

Subjects

Therapeutics. Pharmacology, RM1-950, Pharmacy and materia medica, RS1-441

Abstract

Purpose. To determine the correlations/discrepancies of drug stabilities between in the homogenates of human culture cells and of human tissues. Methods. Amino acid/dipeptide monoester prodrugs of floxuridine were chosen as the model drugs. The stabilities (half-lives) of floxuridine prodrugs in human tissues (pancreas, liver, and small intestine) homogenates were obtained and compared with ones in cell culture homogenates (AcPC-1, Capan-2, and Caco-2 cells) as well as human liver microsomes. The correlations of prodrug stability in human small bowel tissue homogenate vs. Caco-2 cell homogenate, human liver tissue homogenate vs. human liver microsomes, and human pancreatic tissue homogenate vs. pancreatic cell, AsPC-1 and Capan-2, homogenates were examined. Results. The stabilities of floxuridine prodrugs in human small bowel homogenate exhibited the great correlation to ones in Caco-2 cell homogenate (slope = 1.0-1.3, r2 = 0.79-0.98). The stability of those prodrugs in human pancreas tissue homogenate also exhibited the good correlations to ones in AsPC-1 and Capan-2 cells homogenates (slope = 0.5-0.8, r2 = 0.58-0.79). However, the correlations of prodrug stabilities between in human liver tissue homogenates and in human liver microsomes were weaker than others (slope = 1.3-1.9, r2 = 0.07-0.24). Conclusions. The correlations of drug stabilities in cultured cell homogenates and in human tissue homogenates were compared. Those results exhibited wide range of correlations between in cell homogenate and in human tissue homogenate (r2 = 0.07 – 0.98). Those in vitro studies in cell homogenates would be good tools to predict drug stabilities in vivo and to select drug candidates for further developments. In the series of experiments, 5′-O-D-valyl-floxuridine and 5′-O-L-phenylalanyl-L-tyrosyl-floxuridine would be selected as candidates of oral drug targeting delivery for cancer chemotherapy due to their relatively good stabilities compared to other tested prodrugs. This article is open to POST-PUBLICATION REVIEW. Registered readers (see “For Readers”) may comment by clicking on ABSTRACT on the issue’s contents page.

Published

2012

9. Harmonizing Biopredictive Methodologies Through the Product Quality Research Institute (PQRI) Part I: Biopredictive Dissolution of Ibuprofen and Dipyridamole Tablets

Author

Yasuhiro Tsume, Lee Ashworth, Marival Bermejo, Joan Cheng, Vincent Cicale, Jennifer Dressman, Masahiro Fushimi, Isabel Gonzalez-Alvarez, Yiwang Guo, Corinne Jankovsky, Xujin Lu, Kazuki Matsui, Sanjaykumar Patel, Natalie Sanderson, Changquan Calvin Sun, Naveen K. Thakral, Miki Yamane, and Laurin Zöller

Subjects

Pharmaceutical Science

Abstract

Assessing in vivo performance to inform formulation selection and development decisions is an important aspect of drug development. Biopredictive dissolution methodologies for oral dosage forms have been developed to understand in vivo performance, assist in formulation development/optimization, and forecast the outcome of bioequivalence studies by combining them with simulation tools to predict plasma profiles in humans. However, unlike compendial dissolution methodologies, the various biopredictive methodologies have not yet been harmonized or standardized. This manuscript presents the initial phases of an effort to develop best practices and move toward standardization of the biopredictive methodologies through the Product Quality Research Institute (PQRI, https://pqri.org) entitled “The standardization of in vitro predictive dissolution methodologies and in silico bioequivalence study Working Group.” This Working Group (WG) is comprised of participants from 10 pharmaceutical companies and academic institutes. The project will be accomplished in a total of five phases including assessing the performance of dissolution protocols designed by the individual WG members, and then building “best practice” protocols based on the initial dissolution profiles. After refining the “best practice” protocols to produce equivalent dissolution profiles, those will be combined with physiologically based biopharmaceutics models (PBBM) to predict plasma profiles. In this manuscript, the first two of the five phases are reported, namely generating biopredictive dissolution profiles for ibuprofen and dipyridamole and using those dissolution profiles with PBBM to match the clinical plasma profiles. Key experimental parameters are identified, and this knowledge will be applied to build the “best practice” protocol in the next phase. Graphical Abstract

Published

2023

10. Evaluation and prediction of oral drug absorption and bioequivalence with food-druginteraction

Author

Yasuhiro Tsume

Subjects

Pharmacology, Pharmaceutical Science, Pharmacology (medical)

Published

2023

11. The Introduction of a New Flexible In Vivo Predictive Dissolution Apparatus, GIS-Alpha (GIS-α), to Study Dissolution Profiles of BCS Class IIb Drugs, Dipyridamole and Ketoconazole

Author

Andre Hermans, Michael Wang, Filippos Kesisoglou, Sanjaykumar Patel, and Yasuhiro Tsume

Subjects

Drug, media_common.quotation_subject, Administration, Oral, Pharmaceutical Science, 02 engineering and technology, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, In vivo, medicine, Dissolution testing, Solubility, Dissolution, media_common, Chromatography, Chemistry, Reproducibility of Results, Dipyridamole, Hydrogen-Ion Concentration, 021001 nanoscience & nanotechnology, Ketoconazole, Intestinal Absorption, Pharmaceutical Preparations, 0210 nano-technology, Oral retinoid, medicine.drug

Abstract

The physiological pH changes and peristalsis activities in gastrointestinal (GI) tract have big impact on the dissolution of oral drug products, when those oral drug products include APIs with pH-dependent solubility. It is well documented that predicting the bioperformance of those oral drug products can be challenging using compendial methods. To overcome this limitation, in vivo predictive dissolution apparatuses, such as the transfer model, have been developed to predict bioperformance of oral formulation candidates and drug products. In this manuscript we utilize a new transfer-model dissolution apparatus, the gastrointestinal simulator-α (GIS-α), to characterize its behavior in terms of transfer kinetics and pH, assess its reproducibility and adaptability to mimic different transfer conditions, as well as study dissolution of ketoconazole and dipyridamole as model BCS class IIb compounds. Availability of commercially available dissolution transfer systems with similar configuration to compendial dissolution apparatus, may be helpful to simplify and standardize in vivo predictive dissolution methodologies for BCS class IIb compounds in the future.

Published

2020

12. Dissolution Challenges Associated with the Surface pH of Drug Particles: Integration into Mechanistic Oral Absorption Modeling

Author

Bart, Hens, Nidhi, Seegobin, Marival, Bermejo, Yasuhiro, Tsume, Nicola, Clear, Mark, McAllister, Gregory E, Amidon, and Gordon L, Amidon

Subjects

Drug Liberation, Solubility, Therapeutic Equivalency, Chemistry, Pharmaceutical, Administration, Oral, Humans, Pharmaceutical Science, Computer Simulation, Ibuprofen, Hydrogen-Ion Concentration, Models, Biological

Abstract

The present work aimed to differentiate between in vitro dissolution profiles of ibuprofen as input for GastroPlus™ and to see the impact on systemic exposure. In vitro dissolution profiles of ibuprofen obtained under low- and high-buffered dissolution media were used as input using the z-factor approach. In a second step, a customized surface pH calculator was applied to predict the surface pH of ibuprofen under these low- and high-buffered dissolution conditions. These surface pH values were adopted in GastroPlus™ and simulations were performed to predict the systemic outcome. Simulated data were compared with systemic data of ibuprofen obtained under fasted state conditions in healthy subjects. The slower dissolution rate observed when working under low-buffered conditions nicely matched with the slower dissolution rate as observed during the clinical aspiration study and was in line with the systemic exposure of the drug. Finally, a population simulation was performed to explore the impact of z-factor towards bioequivalence (BE) criteria (so-called safe space). Concerning future perspectives, the customized calculator should be developed in such a way to make it possible to predict the dissolution rate (being informed by the particle size distribution) which, in its turn, can be used as a surrogate to predict the USP2 dissolution curve. Subsequently, validation can be done by using this profile as input for PBPK platforms.

Published

2022

13. Linking the Gastrointestinal Behavior of Ibuprofen with the Systemic Exposure between and within Humans—Part 2: Fed State

Author

Duxin Sun, Bo Wen, Bart Hens, Jianghong Fan, Gregory E. Amidon, Joseph Dickens, Allen Lee, Gail Benninghoff, Marival Bermejo, Gordon L. Amidon, Jeffrey Wysocki, Paulo Paixão, Raimar Löbenberg, William L. Hasler, Arjang Talattof, Niloufar Salehi, Jason Baker, Alex Yu, Robert Lionberger, Yasuhiro Tsume, Ann Frances, Mark J. Koenigsknecht, and Kerby Shedden

Subjects

Male, BIOAVAILABILITY, Administration, Oral, Datasets as Topic, Pharmaceutical Science, Ibuprofen, 02 engineering and technology, Research & Experimental Medicine, buffer capacity, Pharmacology, 030226 pharmacology & pharmacy, Food-Drug Interactions, CALORIC CONTENT, 0302 clinical medicine, Oral administration, oral absorption, Drug Discovery, ABSORPTION, VITRO, Pharmacology & Pharmacy, IN-VIVO DISSOLUTION, ibuprofen, Biological Variation, Individual, Stomach, immediate release, Hydrogen-Ion Concentration, Middle Aged, Postprandial Period, 021001 nanoscience & nanotechnology, Healthy Volunteers, Postprandial, Medicine, Research & Experimental, Area Under Curve, Molecular Medicine, Female, MEAL, 0210 nano-technology, Life Sciences & Biomedicine, Tablets, medicine.drug, Adult, in vivo dissolution, Cmax, Biological Availability, Bioequivalence, Models, Biological, DOSAGE FORMS, Article, in vivo study, Young Adult, 03 medical and health sciences, Pharmacokinetics, In vivo, MOTILITY, medicine, Humans, Computer Simulation, Gastric Absorption, bioequivalence, Science & Technology, business.industry, manometry, fed state, Bioavailability, Drug Liberation, Biological Variation, Population, Gastric Emptying, Solubility, LIQUIDS, local drug concentration in the GI tract, business, TRACT

Abstract

Exploring the intraluminal behavior of an oral drug product in the human gastrointestinal (GI) tract remains challenging. Many in vivo techniques are available to investigate the impact of GI physiology on oral drug behavior in fasting state conditions. However, little is known about the intraluminal behavior of a drug in postprandial conditions. In a previous report, we described the mean solution and total concentrations of ibuprofen after oral administration of an immediate-release (IR) tablet in fed state conditions. In parallel, blood samples were taken to assess systemic concentrations. The purpose of this work was to statistically evaluate the impact of GI physiology (e.g., pH, contractile events) within and between individuals (intra and intersubject variability) for a total of 17 healthy subjects. In addition, a pharmacokinetic (PK) analysis was performed by noncompartmental analysis, and PK parameters were correlated with underlying physiological factors (pH, time to phase III contractions postdose) and study parameters (e.g., ingested amount of calories, coadministered water). Moreover, individual plasma profiles were deconvoluted to assess the fraction absorbed as a function of time, demonstrating the link between intraluminal and systemic behavior of the drug. The results demonstrated that the in vivo dissolution of ibuprofen depends on the present gastric pH and motility events at the time of administration. Both intraluminal factors were responsible for explaining 63% of plasma Cmax variability among all individuals. For the first time, an in-depth analysis was performed on a large data set derived from an aspiration/motility study, quantifying the impact of physiology on systemic behavior of an orally administered drug product in fed state conditions. The data obtained from this study will help us to develop an in vitro biorelevant dissolution approach and optimize in silico tools in order to predict the in vivo performance of orally administered drug products, especially in fed state conditions. ispartof: MOLECULAR PHARMACEUTICS vol:15 issue:12 pages:5468-5478 ispartof: location:United States status: published

Published

2018

14. Highlights from the 2020 AAPS 360 Annual Meeting

Author

Vivian A. Gray, Jennifer B. Dressman, Dorys Argelia Diaz, Yasuhiro Tsume, Nikoletta Fotaki, and Publica

Subjects

Pharmaceutical Science

Published

2021

15. Summary of the In Vivo Predictive Dissolution (iPD) - Oral Drug Delivery (ODD) Conference 2018

Author

Luca Marciani, Gregory E. Amidon, Joseph Dickens, Paulo Paixão, Duxin Sun, Alex Yu, Gordon L. Amidon, Yasuhiro Tsume, Hans Lennernäs, Kai Wang, Niloufar Salehi, Bart Hens, Kerby Shedden, William L. Hasler, Arjang Talattof, Robert M. Ziff, Jozef Al-Gousous, Marival Bermejo, Peter Langguth, Raimar Löbenberg, James G. Brasseur, and Gail Benninghoff

Subjects

business.industry, education, Pharmaceutical Science, Pharmacology, bacterial infections and mycoses, 030226 pharmacology & pharmacy, stomatognathic diseases, 03 medical and health sciences, 0302 clinical medicine, In vivo, 030220 oncology & carcinogenesis, mental disorders, Medicine, business, Dissolution, Oral retinoid

Abstract

Summary of the In Vivo Predictive Dissolution (iPD) - Oral Drug Delivery (ODD) Conference 2018

Published

2018

16. The Combination of GIS and Biphasic to Better Predict In Vivo Dissolution of BCS Class IIb Drugs, Ketoconazole and Raloxifene

Author

Gregory E. Amidon, Naoto Igawa, Yasuhiro Tsume, Gordon L. Amidon, and Adam J. Drelich

Subjects

In vitro dissolution, Chemistry, Pharmaceutical, Pharmaceutical Science, 02 engineering and technology, Pharmacology, Models, Biological, 030226 pharmacology & pharmacy, Permeability, 03 medical and health sciences, 0302 clinical medicine, In vivo, medicine, Humans, Computer Simulation, Raloxifene, Dissolution testing, Dissolution, Chemistry, 021001 nanoscience & nanotechnology, Gastrointestinal Tract, Drug Liberation, Ketoconazole, Biopharmaceutical, Intestinal Absorption, Solubility, Raloxifene Hydrochloride, In vitro system, 0210 nano-technology, medicine.drug

Abstract

The formulation developments and the in vivo assessment of Biopharmaceutical Classification System (BCS) class II drugs are challenging due to their low solubility and high permeability in the human gastrointestinal (GI) tract. Since the GI environment influences the drug dissolution of BCS class II drugs, the human GI characteristics should be incorporated into the in vitro dissolution system to predict bioperformance of BCS class II drugs. An absorptive compartment may be important in dissolution apparatus for BCS class II drugs, especially for bases (BCS IIb) because of high permeability, precipitation, and supersaturation. Thus, the in vitro dissolution system with an absorptive compartment may help predicting the in vivo phenomena of BCS class II drugs better than compendial dissolution apparatuses. In this study, an absorptive compartment (a biphasic device) was introduced to a gastrointestinal simulator. This addition was evaluated if this in vitro system could improve the prediction of in vivo dissolution for BCS class IIb drugs, ketoconazole and raloxifene, and subsequent absorption. The gastrointestinal simulator is a practical in vivo predictive tool and exhibited an improved in vivo prediction utilizing the biphasic format and thus a better tool for evaluating the bioperformance of BCS class IIb drugs than compendial apparatuses.

Published

2018

17. Oral product input to the GI tract: GIS an oral product performance technology

Author

Yasuhiro Tsume and Gordon L. Amidon

Subjects

Drug, Active ingredient, Gastric emptying, Computer science, General Chemical Engineering, media_common.quotation_subject, 02 engineering and technology, Pharmacology, 021001 nanoscience & nanotechnology, 030226 pharmacology & pharmacy, Systemic circulation, Dosage form, 03 medical and health sciences, 0302 clinical medicine, Dissolution testing, Biochemical engineering, 0210 nano-technology, Magic bullet, Oral Product, media_common

Abstract

The patient receives a pharmaceutical product, not a drug. The pharmaceutical products are formulated with a drug, an active ingredient to produce the maximum therapeutic effect after oral absorption. Therefore, it is the product we must optimize for the patients. In order to assure the safety and efficacy of pharmaceutical products, we need an in vivo predictive tool for oral product performance in patients. Currently, we are a surprisingly long way from accomplishing that objective. If the 20th century was the ‘age of the drug’, i.e., the ‘magic bullet’, the 21st century must become the ‘age of the guided missile’, i.e., the delivery system, including the form of the active pharmaceutical ingredient (API) (‘drug’). The physical form of the drug and the delivery system must be optimized to maximize the therapeutic benefits of pharmaceutical products for humans. Oral immediate release (IR) dosage forms cannot be optimal for all drugs or likely even any drugs (APIs). Still, the formulation of pharmaceutical products has to be optimized for patients. But how do we optimize oral delivery of drugs? It is usually through ‘trial and error’, in humans! We need a better way to optimize the oral dosage forms. We have suggested to select different dissolution methodologies for this optimization based on BCS Subclasses. In this article, we present the predicted in vivo drug dissolution profile of ketoconazole as a model drug from our laboratory utilizing a gastrointestinal simulator (GIS), which is an adaptation of the ASD system. GIS consists of three chambers representing stomach, duodenum, and jejunum, to create the human gastrointestinal tract-like environment and enable the control the gastric emptying rate. This dissolution system allows the monitoring of the drug dissolution phenomena and the observation of the supersaturation and the precipitation of pharmaceutical products, which is useful information to predict in vivo dissolution of pharmaceutical products. This system can provide the actual input needed to accurately predict the input into the systemic circulation required by many of the absorption prediction packages available today.

Published

2017

18. The impact of supersaturation level for oral absorption of BCS class IIb drugs, dipyridamole and ketoconazole, using in vivo predictive dissolution system: Gastrointestinal Simulator (GIS)

Author

Gregory E. Amidon, Amanda L. Searls, Yasuhiro Tsume, Susumu Takeuchi, Duxin Sun, Kazuki Matsui, and Gordon L. Amidon

Subjects

Administration, Oral, Pharmaceutical Science, 02 engineering and technology, Absorption (skin), Pharmacology, Models, Biological, 030226 pharmacology & pharmacy, Dosage form, 03 medical and health sciences, 0302 clinical medicine, In vivo, medicine, Animals, Chemical Precipitation, Computer Simulation, Dissolution testing, Dissolution, Simulation, Supersaturation, Chemistry, Dipyridamole, 021001 nanoscience & nanotechnology, Gastrointestinal Tract, Mice, Inbred C57BL, Drug Liberation, Ketoconazole, Intestinal Absorption, Solubility, 0210 nano-technology, medicine.drug

Abstract

The development of formulations and the assessment of oral drug absorption for Biopharmaceutical Classification System (BCS) class IIb drugs is often a difficult issue due to the potential for supersaturation and precipitation in the gastrointestinal (GI) tract. The physiological environment in the GI tract largely influences in vivo drug dissolution rates of those drugs. Thus, those physiological factors should be incorporated into the in vitro system to better assess in vivo performance of BCS class IIb drugs. In order to predict oral bioperformance, an in vitro dissolution system with multiple compartments incorporating physiologically relevant factors would be expected to more accurately predict in vivo phenomena than a one-compartment dissolution system like USP Apparatus 2 because, for example, the pH change occurring in the human GI tract can be better replicated in a multi-compartmental platform. The Gastrointestinal Simulator (GIS) consists of three compartments, the gastric, duodenal and jejunal chambers, and is a practical in vitro dissolution apparatus to predict in vivo dissolution for oral dosage forms. This system can demonstrate supersaturation and precipitation and, therefore, has the potential to predict in vivo bioperformance of oral dosage forms where this phenomenon may occur. In this report, in vitro studies were performed with dipyridamole and ketoconazole to evaluate the precipitation rates and the relationship between the supersaturation levels and oral absorption of BCS class II weak base drugs. To evaluate the impact of observed supersaturation levels on oral absorption, a study utilizing the GIS in combination with mouse intestinal infusion was conducted. Supersaturation levels observed in the GIS enhanced dipyridamole and ketoconazole absorption in mouse, and a good correlation between their supersaturation levels and their concentration in plasma was observed. The GIS, therefore, appears to represent in vivo dissolution phenomena and demonstrate supersaturation and precipitation of dipyridamole and ketoconazole. We therefore conclude that the GIS has been shown to be a good biopredictive tool to predict in vivo bioperformance of BCS class IIb drugs that can be used to optimize oral formulations.

Published

2017

19. Utilization of Gastrointestinal Simulator, an in Vivo Predictive Dissolution Methodology, Coupled with Computational Approach To Forecast Oral Absorption of Dipyridamole

Author

Amanda L. Searls, Susumu Takeuchi, Gordon L. Amidon, Kazuki Matsui, and Yasuhiro Tsume

Subjects

Male, Absorption (pharmacology), In silico, Administration, Oral, Pharmaceutical Science, 02 engineering and technology, Models, Biological, 030226 pharmacology & pharmacy, Intestinal absorption, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, In vivo, Drug Discovery, medicine, Humans, Dissolution testing, Simulation, Aged, Gastric emptying, Chemistry, Dipyridamole, Hydrogen-Ion Concentration, 021001 nanoscience & nanotechnology, Gastrointestinal Tract, Kinetics, Gastric Emptying, Intestinal Absorption, Solubility, Molecular Medicine, Administration, Intravenous, Female, 0210 nano-technology, medicine.drug

Abstract

Weakly basic drugs exhibit a pH-dependent dissolution profile in the gastrointestinal (GI) tract, which makes it difficult to predict their oral absorption profile. The aim of this study was to investigate the utility of the gastrointestinal simulator (GIS), a novel in vivo predictive dissolution (iPD) methodology, in predicting the in vivo behavior of the weakly basic drug dipyridamole when coupled with in silico analysis. The GIS is a multicompartmental dissolution apparatus, which represents physiological gastric emptying in the fasted state. Kinetic parameters for drug dissolution and precipitation were optimized by fitting a curve to the dissolved drug amount-time profiles in the United States Pharmacopeia apparatus II and GIS. Optimized parameters were incorporated into mathematical equations to describe the mass transport kinetics of dipyridamole in the GI tract. By using this in silico model, intraluminal drug concentration-time profile was simulated. The predicted profile of dipyridamole in the duodenal compartment adequately captured observed data. In addition, the plasma concentration-time profile was also predicted using pharmacokinetic parameters following intravenous administration. On the basis of the comparison with observed data, the in silico approach coupled with the GIS successfully predicted in vivo pharmacokinetic profiles. Although further investigations are still required to generalize, these results indicated that incorporating GIS data into mathematical equations improves the predictability of in vivo behavior of weakly basic drugs like dipyridamole.

Published

2017

20. Linking the Gastrointestinal Behavior of Ibuprofen with the Systemic Exposure between and within Humans-Part 1: Fasted State Conditions

Author

Yasuhiro Tsume, William L. Hasler, Gail Benninghoff, Paulo Paixão, Gordon L. Amidon, Gregory E. Amidon, Joseph Dickens, Duxin Sun, Bo Wen, Naír Rodríguez-Hornedo, Allen Lee, Jianghong Fan, Raimar Löbenberg, Marival Bermejo, Jason Baker, Katie L. Cavanagh, Kerby Shedden, Niloufar Salehi, Alex Yu, Arjang Talattof, Mark J. Koenigsknecht, Ann Frances, Gislaine Kuminek, Robert Lionberger, Bart Hens, and Jeffrey Wysocki

Subjects

Male, PHARMACOKINETICS, WEAK ACID, Administration, Oral, Datasets as Topic, Pharmaceutical Science, Ibuprofen, 02 engineering and technology, Pharmacology, Research & Experimental Medicine, 030226 pharmacology & pharmacy, 0302 clinical medicine, Oral administration, Drug Discovery, Healthy volunteers, Medicine, Pharmacology & Pharmacy, DRUG, IN-VIVO DISSOLUTION, ibuprofen, Biological Variation, Individual, ORAL ABSORPTION, Fasting, Hydrogen-Ion Concentration, Middle Aged, immediate release, 021001 nanoscience & nanotechnology, Healthy Volunteers, Pharmacokinetic analysis, Fasted state, Medicine, Research & Experimental, motility, Area Under Curve, Molecular Medicine, Female, 0210 nano-technology, Life Sciences & Biomedicine, Tablets, medicine.drug, Adult, in vivo dissolution, Biological Availability, SIMULATOR, Bioequivalence, Models, Biological, Article, Young Adult, 03 medical and health sciences, Humans, bioequivalence, Science & Technology, business.industry, aspiration/motility study, organic chemicals, Plasma levels, manometry, PANCREATIC-SECRETION, Bioavailability, Gastrointestinal Tract, Drug Liberation, Biological Variation, Population, Solubility, Gastrointestinal Absorption, local drug concentration in the GI tract, MIGRATING MOTOR COMPLEX, business, bioavailability

Abstract

The goal of this project was to explore and to statistically evaluate the responsible gastrointestinal (GI) factors that are significant factors in explaining the systemic exposure of ibuprofen, between and within human subjects. In a previous study, we determined the solution and total concentrations of ibuprofen as a function of time in aspirated GI fluids, after oral administration of an 800 mg IR tablet (reference standard) of ibuprofen to 20 healthy volunteers in fasted state conditions. In addition, we determined luminal pH and motility pressure recordings that were simultaneously monitored along the GI tract. Blood samples were taken to determine ibuprofen plasma levels. In this work, an in-depth statistical and pharmacokinetic analysis was performed to explain which underlying GI variables are determining the systemic concentrations of ibuprofen between (inter-) and within (intra-) subjects. In addition, the obtained plasma profiles were deconvoluted to link the fraction absorbed with the fraction dissolved. Multiple linear regressions were performed to explain and quantitatively express the impact of underlying GI physiology on systemic exposure of the drug (in terms of plasma Cmax/AUC and plasma Tmax). The exploratory analysis of the correlation between plasma Cmax/AUC and the time to the first phase III contractions postdose (TMMC-III) explains ∼40% of the variability in plasma Cmax for all fasted state subjects. We have experimentally shown that the in vivo intestinal dissolution of ibuprofen is dependent upon physiological variables like, in this case, pH and postdose phase III contractions. For the first time, this work presents a thorough statistical analysis explaining how the GI behavior of an ionized drug can explain the systemic exposure of the drug based on the individual profiles of participating subjects. This creates a scientifically based and rational framework that emphasizes the importance of including pH and motility in a predictive in vivo dissolution methodology to forecast the in vivo performance of a drug product. Moreover, as no extensive first-pass metabolism is considered for ibuprofen, this study demonstrates how intraluminal drug behavior is reflecting the systemic exposure of a drug. ispartof: MOLECULAR PHARMACEUTICS vol:15 issue:12 pages:5454-5467 ispartof: location:United States status: published

Published

2018

21. The Evaluation of In Vitro Drug Dissolution of Commercially Available Oral Dosage Forms for Itraconazole in Gastrointestinal Simulator With Biorelevant Media

Author

Yasuhiro Tsume, Gregory E. Amidon, Gordon L. Amidon, and Kazuki Matsui

Subjects

Drug, Antifungal Agents, Itraconazole, media_common.quotation_subject, Pharmaceutical Science, Capsules, 02 engineering and technology, Pharmacology, Models, Biological, 030226 pharmacology & pharmacy, Epithelium, Permeability, Intestinal absorption, Dosage form, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, medicine, Humans, Dissolution testing, Dissolution, Simulation, media_common, Chromatography, Chemistry, 021001 nanoscience & nanotechnology, Biopharmaceutics Classification System, Pharmaceutical Solutions, Intestinal Absorption, Solubility, Gastric Mucosa, Area Under Curve, Caco-2 Cells, 0210 nano-technology, medicine.drug

Abstract

The purpose of this study was to assess the feasibility of a multicompartmental in vitro dissolution apparatus, gastrointestinal simulator (GIS), in assessing the drug dissolution of 2 commercially available oral dosage forms for itraconazole (ICZ). The GIS consists of 3 chambers, mimicking the upper gastrointestinal tract. In vitro dissolution of ICZ capsule or oral solution was evaluated in United States Pharmacopeia apparatus II and GIS. To investigate the suitability of fasted state simulated intestinal fluid (FaSSIF) to predict better in vivo, FaSSIF as well as phosphate buffer were used as dissolution media. Area under the dissolved drug amount-time curve (AUDC) was calculated for each dosage form in each apparatus, and the ratios of AUDCoral solution to AUDCcapsule were compared with human pharmacokinetic data. Based on this comparison, GIS with FaSSIF can adequately distinguish the pharmacokinetic profiles of 2 oral dosage forms for ICZ. Additionally, Caco-2 cell transepithelial transport study in combination with GIS revealed that improved drug dissolution by formulations resulted in enhanced permeation of ICZ through cell monolayer, suggesting the observed ICZ concentration in the GIS will directly reflect systemic exposure. These results indicate GIS would be a powerful tool to assess the formulations of ICZ as well as other Biopharmaceutics Classification System class II drug formulations.

Published

2016

22. The in vivo predictive dissolution for immediate release dosage of donepezil and danazol, BCS class IIc drugs, with the GIS and the USP II with biphasic dissolution apparatus

Author

Yasuhiro Tsume, Hao Ruan, Gordon L. Amidon, Gregory E. Amidon, Naoto Igawa, and Adam J. Drelich

Subjects

Danazol, Chemistry, Pharmaceutical Science, 02 engineering and technology, Pharmacology, 021001 nanoscience & nanotechnology, 030226 pharmacology & pharmacy, 03 medical and health sciences, 0302 clinical medicine, Biopharmaceutical, In vivo, medicine, Dissolution testing, Immediate release, Solubility, 0210 nano-technology, Donepezil, Dissolution, medicine.drug

Abstract

The formulation developments and the in vivo assessment of Biopharmaceutical Classification System (BCS) class II drugs are challenging due to their low solubility and high permeability in the human gastrointestinal (GI) tract. Since the pH change in the GI environment influences the drug dissolution of BCS class IIa and IIb drugs but not for IIc drugs, the incorporation of the human GI characteristics into the in vitro dissolution system may not be crucial for BCS class IIc drugs to predict their bioperformance. An absorptive compartment in dissolution apparatus would be important to predict bioperformance of BCS class IIc drugs due to their physicochemical characteristics, low solubility and high permeability. In this study, an absorptive compartment (biphasic system) was introduced to a gastrointestinal simulator (GIS) and USP dissolution apparatus II for the evaluation of in vivo prediction for BCS class IIc drugs. Those in vitro systems with the biphasic phase were evaluated for the prediction of in vivo dissolution of BCS class IIc drugs, donepezil and danazol, and subsequent absorption. For the evaluation of in vivo dissolution of BCS class IIc drugs, simpler dissolution apparatus, USP II, with the absorptive phase might be adequate a dissolution method to predict in vivo.

Published

2020

23. Report from the '3rd International Symposium on BA/BE of Oral Drug Products: Biopharmaceutics meets Galenics'

Author

P. Paixão, K. Moribe, J.A. Morais, Shinji Yamashita, Kohsaku Kawakami, Yasuhiro Tsume, N. Silva, M. Bermejo, and Gordon L. Amidon

Subjects

Biopharmaceutics, Pharmaceutical Science, Library science, 02 engineering and technology, 021001 nanoscience & nanotechnology, 030226 pharmacology & pharmacy, language.human_language, 03 medical and health sciences, 0302 clinical medicine, Biopharmaceutical, Political science, Agency (sociology), language, Portuguese, 0210 nano-technology, Oral retinoid

Abstract

The “3rd International Symposium on BA/BE of Oral Drug Products – Biopharmaceutics meets Galenics (BA/BE 2018)” was held during 11–12th of October 2018 at INFARMED, the Portuguese regulatory medicines agency, in Lisbon, Portugal. Summary of this meeting and perspective/directions of biopharmaceutical researches are discussed in this opinion paper.

Published

2020

24. Biopredictive in vitro testing methods to assess intestinal drug absorption from supersaturating dosage forms

Author

Kohsaku Kawakami, Makoto Kataoka, Yasuhiro Tsume, Keisuke Ueda, Bart Hens, Shinji Yamashita, Ping Gao, and Patrick Augustijns

Subjects

Absorption (pharmacology), Drug, In vitro dissolution, Chemistry, media_common.quotation_subject, Pharmaceutical Science, 02 engineering and technology, 021001 nanoscience & nanotechnology, 030226 pharmacology & pharmacy, Dosage form, 03 medical and health sciences, 0302 clinical medicine, Biochemical engineering, 0210 nano-technology, media_common

Abstract

The discovery pipelines in pharmaceutical companies are highly populated with poorly soluble compounds, demanding for an appropriate solution to overcome this problem. Generating supersaturated concentrations for these drugs in the gastrointestinal (GI) tract has been put forward as a promising strategy to assure sufficient systemic exposure after oral intake of the drug. Numerous publications have shown to which extent supersaturating dosage forms can create supersaturated concentrations by testing these formulations in in vitro dissolution models. The obtained dissolution profiles can serve as a valuable input for computational software programs to simulate the systemic outcome of the drug. To improve our fundamental knowledge and understanding of the impact of supersaturation/precipitation on oral absorption, attempts have been made to develop biopredictive in vitro dissolution systems such as the Gastrointestinal Simulator (GIS), the dissolution/permeation system, and the biphasic test system. Moreover, aspiration studies in humans have been performed throughout the years to measure simultaneously GI and systemic concentrations of the drug in order to directly envisage the impact of supersaturation on systemic exposure. This manuscript aims to provide a comprehensive review with respect to the predictive power of in vitro tools towards the in vivo performance of supersaturating dosage forms. Different case studies will be thoroughly presented where a plethora of supersaturating formulations was tested applying a biopredictive setting. Recent investigations on liquid-liquid phase separation of supersaturated solutions, which makes comprehension of the dissolution process of supersaturating dosage forms extremely challenging, are also discussed.

Published

2020

25. Formulation predictive dissolution (fPD) testing to advance oral drug product development: an introduction to the US FDA funded ‘21st Century BA/BE’ project

Author

Gordon L. Amidon, Bart Hens, Gail Benninghoff, Jozef Al-Gousous, Duxin Sun, Yasuhiro Tsume, William L. Hasler, Hans Lennernäs, Patrick D. Sinko, Arjang Talattof, Paulo Paixão, Alex Yu, James G. Brasseur, Meagan Dean, Luca Marciani, Gregory E. Amidon, Joseph Dickens, Kerby Shedden, Robert M. Ziff, Nicholas Job, Niloufar Salehi, Marival Bermejo, and Peter Langguth

Subjects

Physiologically based pharmacokinetic modelling, Bioavailability, Computer science, Manometry, Drug Compounding, Administration, Oral, Pharmaceutical Science, 02 engineering and technology, Bioequivalence, Computational fluid dynamics, 030226 pharmacology & pharmacy, Article, DOSAGE FORMS, INDUCED VARIABILITY, 03 medical and health sciences, 0302 clinical medicine, BIOPHARMACEUTICS CLASSIFICATION-SYSTEM, ABSORPTION, Humans, Dissolution testing, Oral absorption, Pharmacology & Pharmacy, Dissolution, IN-VIVO DISSOLUTION, In vivo dissolution, Science & Technology, WORKSHOP REPORT, United States Food and Drug Administration, business.industry, GASTROINTESTINAL SIMULATOR GIS, VITRO DISSOLUTION, 021001 nanoscience & nanotechnology, Biopharmaceutics Classification System, United States, MODEL, Drug Liberation, New product development, Predictive power, DIFFUSION-CONTROLLED DISSOLUTION, Biochemical engineering, 0210 nano-technology, business, Life Sciences & Biomedicine, Oral retinoid, MRI

Abstract

Over the past decade, formulation predictive dissolution (fPD) testing has gained increasing attention. Another mindset is pushed forward where scientists in our field are more confident to explore the in vivo behavior of an oral drug product by performing predictive in vitro dissolution studies. Similarly, there is an increasing interest in the application of modern computational fluid dynamics (CFD) frameworks and high-performance computing platforms to study the local processes underlying absorption within the gastrointestinal (GI) tract. In that way, CFD and computing platforms both can inform future PBPK-based in silico frameworks and determine the GI-motility-driven hydrodynamic impacts that should be incorporated into in vitro dissolution methods for in vivo relevance. Current compendial dissolution methods are not always reliable to predict the in vivo behavior, especially not for biopharmaceutics classification system (BCS) class 2/4 compounds suffering from a low aqueous solubility. Developing a predictive dissolution test will be more reliable, cost-effective and less time-consuming as long as the predictive power of the test is sufficiently strong. There is a need to develop a biorelevant, predictive dissolution method that can be applied by pharmaceutical drug companies to facilitate marketing access for generic and novel drug products. In 2014, Prof. Gordon L. Amidon and his team initiated a far-ranging research program designed to integrate (1) in vivo studies in humans in order to further improve the understanding of the intraluminal processing of oral dosage forms and dissolved drug along the gastrointestinal (GI) tract, (2) advancement of in vitro methodologies that incorporates higher levels of in vivo relevance and (3) computational experiments to study the local processes underlying dissolution, transport and absorption within the intestines performed with a new unique CFD based framework. Of particular importance is revealing the physiological variables determining the variability in in vivo dissolution and GI absorption from person to person in order to address (potential) in vivo BE failures. This paper provides an introduction to this multidisciplinary project, informs the reader about current achievements and outlines future directions. ispartof: INTERNATIONAL JOURNAL OF PHARMACEUTICS vol:548 issue:1 pages:120-127 ispartof: location:Netherlands status: published

Published

2018

26. Effect of Biphenyl Hydrolase-Like (BPHL) Gene Disruption on the Intestinal Stability, Permeability and Absorption of Valacyclovir in Wildtype and Bphl Knockout Mice

Author

David Smith, Daniel Epling, Jian Shi, Gordon L. Amidon, Hao Jie Zhu, Yongjun Hu, Yasuhiro Tsume, and Feifeng Song

Subjects

0301 basic medicine, Proteases, Administration, Oral, Biochemistry, Antiviral Agents, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, In vivo, Animals, Pharmacology, Mice, Knockout, Oligopeptide, Chemistry, Wild type, virus diseases, Serine hydrolase, Transporter, Prodrug, Molecular biology, 030104 developmental biology, 030220 oncology & carcinogenesis, Area Under Curve, Valacyclovir, Knockout mouse, Injections, Intravenous, Carboxylic Ester Hydrolases, Half-Life

Abstract

Biphenyl hydrolase-like protein (BPHL) is a novel human serine hydrolase that was originally cloned from a breast carcinoma cDNA library and shown to convert valacyclovir to acyclovir and valganciclovir to ganciclovir. However, the exclusivity of this process has not been determined and, indeed, it is possible that a number of esterases/proteases may mediate the hydrolysis of valacyclovir and similar prodrugs. The objectives of the present study were to evaluate the in situ intestinal permeability and stability of valacyclovir in wildtype (WT) and Bphl knockout (KO) mice, as well as the in vivo oral absorption and intravenous disposition of valacyclovir and acyclovir in the two mouse genotypes. We found that Bphl knockout mice had no obvious phenotype and that Bphl ablation did not alter the jejunal permeability of valacyclovir during in situ perfusions (i.e., 0.54 × 10−4 in WT vs. 0.53 × 10−4 cm/s in KO). Whereas no meaningful changes occurred between genotypes in the gene expression of proton-coupled oligopeptide transporters (i.e., PepT1, PepT2, PhT1, PhT2), enzymatic upregulation of Cyp3a11, Cyp3a16, Abhd14a and Abhd14b was observed in some tissues of Bphl knockout mice. Most importantly, we found that valacyclovir was rapidly and efficiently hydrolyzed to acyclovir in the absence of BPHL, and that hydrolysis was more extensive after the oral vs. intravenous route of administration (for both genotypes). Taken as a whole, BPHL is not obligatory for the conversion of valacyclovir to acyclovir either presystemically or systemically.

Published

2018

27. Gastric emptying and intestinal appearance of nonabsorbable drugs phenol red and paromomycin in human subjects: A multi-compartment stomach approach

Author

William L. Hasler, Ann Frances, Gregory E. Amidon, Joseph Dickens, Alex Yu, Jeffrey Wysocki, Paulo Paixão, Jianghong Fan, Bo Wen, Gail Benninghoff, Raimar Löbenberg, Bart Hens, Allen Lee, Marival Bermejo, Niloufar Salehi, Yasuhiro Tsume, Arjang Talattof, Robert Lionberger, Kerby Shedden, Gordon L. Amidon, Mark J. Koenigsknecht, Jason Baker, and Duxin Sun

Subjects

Male, INDICATORS, Bioavailability, Paromomycin, Administration, Oral, Pharmaceutical Science, 02 engineering and technology, Pharmacology, 030226 pharmacology & pharmacy, Phenolsulfonphthalein, chemistry.chemical_compound, 0302 clinical medicine, Intestine, Small, ABSORPTION, VITRO, Pharmacology & Pharmacy, Antrum, IN-VIVO DISSOLUTION, In vivo dissolution, ORAL DOSAGE FORMS, Bioequivalence, Phenol red, Stomach, digestive, oral, and skin physiology, Fasting, General Medicine, Middle Aged, Postprandial Period, 021001 nanoscience & nanotechnology, Healthy Volunteers, medicine.anatomical_structure, Female, 0210 nano-technology, Life Sciences & Biomedicine, Nonabsorbable marker, Biotechnology, Adult, Gastrointestinal, Human gastric emptying, POORLY ABSORBABLE DRUG, Models, Biological, Article, Aspiration/motility study, Young Adult, 03 medical and health sciences, HUMAN GASTROINTESTINAL-TRACT, Pharmacokinetics, Gastrointestinal mass transport model, MOTILITY, medicine, Humans, Oral absorption, Migrating motor complex, Science & Technology, Gastric emptying, Small intestine, MODEL, Gastric Emptying, Intestinal Absorption, Solubility, chemistry, Duodenum

Abstract

The goal of this study was to create a mass transport model (MTM) model for gastric emptying and upper gastrointestinal (GI) appearance that can capture the in vivo concentration-time profiles of the nonabsorbable drug phenol red in solution in the stomach and upper small intestine by direct luminal measurement while simultaneously recording the contractile activity (motility) via manometry. We advanced from a one-compartmental design of the stomach to a much more appropriate, multi-compartmental 'mixing tank' gastric model that reflects drug distribution along the different regions of the stomach as a consequence of randomly dosing relative to the different contractile phases of the migrating motor complex (MMC). To capture the intraluminal phenol red concentrations in the different segments of the GI tract both in fasted and fed state conditions, it was essential to include a bypass flow compartment ('magenstrasse') to facilitate the transport of the phenol red solution directly to the duodenum (fasted state) or antrum (fed state). The fasted and fed state models were validated with external reference data from an independent aspiration study using another nonabsorbable marker (paromomycin). These results will be essential for the development and optimization of computational programs for GI simulation and absorption prediction, providing a realistic gastric physiologically-based pharmacokinetic (PBPK) model based on direct measurement of gastric concentrations of the drug in the stomach. ispartof: EUROPEAN JOURNAL OF PHARMACEUTICS AND BIOPHARMACEUTICS vol:129 pages:162-174 ispartof: location:Netherlands status: published

Published

2018

28. Measuring the Impact of Gastrointestinal Variables on the Systemic Outcome of Two Suspensions of Posaconazole by a PBPK Model

Author

Raimar Löbenberg, Arjang Talattof, Yasuhiro Tsume, Bart Hens, Marival Bermejo, Paulo Paixão, and Gordon L. Amidon

Subjects

Posaconazole, Physiologically based pharmacokinetic modelling, medicine.medical_specialty, Antifungal Agents, Pharmaceutical Science, Context (language use), Bioequivalence, 030226 pharmacology & pharmacy, Gastroenterology, Bile Acids and Salts, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Internal medicine, Intestine, Small, Humans, Medicine, Dissolution testing, Gastric emptying, business.industry, Organ Size, Hydrogen-Ion Concentration, Models, Theoretical, Triazoles, Pharmacometrics, Gastrointestinal Tract, Gastric Emptying, 030220 oncology & carcinogenesis, business, medicine.drug

Abstract

For the last two decades, the application of physiologically based pharmacokinetic (PBPK) models has grown exponentially in the field of oral absorption and in a regulatory context. Although these models are widely used, their predictive power should be validated and optimized in order to rely on these models and to know exactly what is going on "under the hood". In this study, an automated sensitivity analysis (ASA) was performed for 11 gastrointestinal (GI) variables that are integrated into the PBPK software program Simcyp®. The model of interest was a previously validated workspace that was able to predict the intraluminal and systemic behavior of two different suspensions of posaconazole in the Simcyp® Simulator. The sensitivity of the following GI parameters was evaluated in this model: gastric and duodenal pH, gastric and duodenal bicarbonate concentrations (reflecting buffer capacity), duodenal bile salts concentration, gastric emptying, the interdigestive migrating motor complex (IMMC), small intestinal transit time (SITT), gastric and jejunal volumes, and permeability. The most sensitive parameters were gastric/duodenal pH and gastric emptying, for both suspensions. The outcome of the sensitivity analyses highlights the important GI variables that must be integrated into an in vivo predictive dissolution test to help and create a rational and scientific framework/design for product development of novel and generic drug products. ispartof: The AAPS Journal vol:20 issue:3 pages:57-57 ispartof: location:United States status: published

Published

2018

29. Evaluation and optimized selection of supersaturating drug delivery systems of posaconazole (BCS class 2b) in the gastrointestinal simulator (GIS): An in vitro-in silico-in vivo approach

Author

Gislaine Kuminek, Yasuhiro Tsume, Bart Hens, Isabel González-Álvarez, Gail Benninghoff, Gordon L. Amidon, Jianghong Fan, Hao Ruan, Gregory E. Amidon, Katie L. Cavanagh, Kazuki Matsui, Naír Rodríguez-Hornedo, and Marival Bermejo

Subjects

Posaconazole, Computer science, In silico, Chemistry, Pharmaceutical, Pharmaceutical Science, Administration, Oral, Biological Availability, 02 engineering and technology, Bioequivalence, 030226 pharmacology & pharmacy, Permeability, Biopharmaceutics, 03 medical and health sciences, 0302 clinical medicine, Drug Delivery Systems, In vivo, medicine, Computer Simulation, Simulation, Triazoles, 021001 nanoscience & nanotechnology, Biopharmaceutics Classification System, Pharmacometrics, Bioavailability, Gastrointestinal Tract, Intestinal Absorption, Solubility, Drug delivery, 0210 nano-technology, medicine.drug

Abstract

Supersaturating drug delivery systems (SDDS) have been put forward in the recent decades in order to circumvent the issue of low aqueous solubility. Prior to the start of clinical trials, these enabling formulations should be adequately explored in in vitro/in silico studies in order to understand their in vivo performance and to select the most appropriate and effective formulation in terms of oral bioavailability and therapeutic outcome. The purpose of this work was to evaluate the in vivo performance of four different oral formulations of posaconazole (categorized as a biopharmaceutics classification system (BCS) class 2b compound) based on the in vitro concentrations in the gastrointestinal simulator (GIS), coupled with an in silico pharmacokinetic model to predict their systemic profiles. Recently published intraluminal and systemic concentrations of posaconazole for these formulations served as a reference to validate the in vitro and in silico results. Additionally, the morphology of the formed precipitate of posaconazole was visualized and characterized by optical microscopy studies and thermal analysis. This multidisciplinary work demonstrates an in vitro-in silico-in vivo approach that provides a scientific basis for screening SDDS by a user-friendly formulation predictive dissolution (fPD) device in order to rank these formulations towards their in vivo performance. ispartof: European Journal of Pharmaceutical Sciences vol:115 pages:258-269 ispartof: location:Netherlands status: published

Published

2018

30. In Vivo Dissolution and Systemic Absorption of Immediate Release Ibuprofen in Human Gastrointestinal Tract under Fed and Fasted Conditions

Author

Ann Frances, Barry E. Bleske, Xinyuan Zhang, Alex Yu, William L. Hasler, Manjunath P. Pai, Duxin Sun, Yasuhiro Tsume, Mark J. Koenigsknecht, Gordon L. Amidon, Huixia Zhang, Robert Lionberger, Allen Lee, Ting Zhao, Bo Wen, and Jason Baker

Subjects

Adult, Male, Pharmaceutical Science, Administration, Oral, Biological Availability, Ibuprofen, 02 engineering and technology, Pharmacology, 030226 pharmacology & pharmacy, Article, Biopharmaceutics, Jejunum, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Pharmacokinetics, In vivo, Drug Discovery, medicine, Humans, Dissolution testing, business.industry, Stomach, Human gastrointestinal tract, Fasting, Middle Aged, 021001 nanoscience & nanotechnology, Postprandial Period, Healthy Volunteers, Absorption, Physiological, Gastrointestinal Tract, Drug Liberation, medicine.anatomical_structure, Gastric Emptying, Intestinal Absorption, Solubility, Duodenum, Molecular Medicine, Female, 0210 nano-technology, business, medicine.drug, Tablets

Abstract

In vivo drug dissolution in the gastrointestinal (GI) tract is largely unmeasured. The purpose of this clinical study was to evaluate the in vivo drug dissolution and systemic absorption of the BCS class IIa drug ibuprofen under fed and fasted conditions by direct sampling of stomach and small intestinal luminal content. Expanding current knowledge of drug dissolution in vivo will help to establish physiologically relevant in vitro models predictive of drug dissolution. A multilumen GI catheter was orally inserted into the GI tract of healthy human subjects. Subjects received a single oral dose of ibuprofen (800 mg tablet) with 250 mL of water under fasting and fed conditions. The GI catheter facilitated collection of GI fluid from the stomach, duodenum, and jejunum. Ibuprofen concentration in GI fluid supernatant and plasma was determined by LC–MS/MS. A total of 23 subjects completed the study, with 11 subjects returning for an additional study visit (a total of 34 completed study visits). The subjects were primarily white (61%) and male (65%) with an average age of 30 years. The subjects had a median [min, max] weight of 79 [52, 123] kg and body mass index of 25.7 [19.4, 37.7] kg/m(2). Ibuprofen plasma levels were higher under fasted conditions and remained detectable for 28 h under both conditions. The AUC(0–24) and C(max) were lower in fed subjects vs fasted subjects, and T(max) was delayed in fed subjects vs fasted subjects. Ibuprofen was detected immediately after ingestion in the stomach under fasting and fed conditions until 7 h after dosing. Higher levels of ibuprofen were detected in the small intestine soon after dosing in fasted subjects compared to fed. In contrast to plasma drug concentration, overall gastric concentrations remained higher under fed conditions due to increased gastric pH vs fasting condition. The gastric pH increased to near neutrality after feeding before decreasing to acidic levels after 7 h. Induction of the fed state reduced systemic levels but increased gastric levels of ibuprofen, which suggest that slow gastric emptying and transit dominate the effect for plasma drug concentration. The finding of high levels of ibuprofen in stomach and small intestine 7 h post dosing was unexpected. Future work is needed to better understand the role of various GI parameters, such as motility and gastric emptying, on systemic ibuprofen levels in order to improve in vitro predictive models.

Published

2017

31. In Vitro Dissolution of Fluconazole and Dipyridamole in Gastrointestinal Simulator (GIS), Predicting in Vivo Dissolution and Drug–Drug Interaction Caused by Acid-Reducing Agents

Author

Kazuki Matsui, Gordon L. Amidon, Gregory E. Amidon, and Yasuhiro Tsume

Subjects

Reducing agent, Administration, Oral, Pharmaceutical Science, Pharmacology, Mice, IVIVC, In vivo, Drug Discovery, medicine, Animals, Drug Interactions, Solubility, Fluconazole, Dissolution, Simulation, Gastrointestinal tract, Chemistry, Dipyridamole, Hydrogen-Ion Concentration, Gastrointestinal Tract, Solutions, Intestinal Absorption, Molecular Medicine, medicine.drug

Abstract

Weakly basic drugs typically exhibit pH-dependent solubility in the physiological pH range, displaying supersaturation or precipitation along the gastrointestinal tract. Additionally, their oral bioavailabilities may be affected by coadministration of acid-reducing agents that elevate gastric pH. The purpose of this study was to assess the feasibility of a multicompartmental in vitro dissolution apparatus, Gastrointestinal Simulator (GIS), in predicting in vivo dissolution of certain oral medications. In vitro dissolution studies of fluconazole, a BCS class I, and dipyridamole, a BCS class II weak bases (class IIb), were performed in the GIS as well as United States Pharmacopeia (USP) apparatus II and compared with the results of clinical drug-drug interaction (DDI) studies. In both USP apparatus II and GIS, fluconazole completely dissolved within 60 min regardless of pH, reflecting no DDI between fluconazole and acid-reducing agents in a clinical study. On the other hand, seven-fold and 15-fold higher concentrations of dipyridamole than saturation solubility were observed in the intestinal compartments in GIS with gastric pH 2.0. Precipitation of dipyridamole was also observed in the GIS, and the percentage of dipyridamole in solution was 45.2 ± 7.0%. In GIS with gastric pH 6.0, mimicking the coadministration of acid-reducing agents, the concentration of dipyridamole was equal to its saturation solubility, and the percentage of drug in solution was 9.3 ± 2.7%. These results are consistent with the clinical DDI study of dipyridamole with famotidine, which significantly reduced the Cmax and area under the curve. An In situ mouse infusion study combined with GIS revealed that high concentration of dipyridamole in the GIS enhanced oral drug absorption, which confirmed the supersaturation of dipyridamole. In conclusion, GIS was shown to be a useful apparatus to predict in vivo dissolution for BCS class IIb drugs.

Published

2015

32. Potential Development of Tumor-Targeted Oral Anti-Cancer Prodrugs: Amino Acid and Dipeptide Monoester Prodrugs of Gemcitabine

Author

David Smith, Yasuhiro Tsume, Adam J. Drelich, and Gordon L. Amidon

Subjects

pancreatic cancer, Pharmaceutical Science, gemcitabine prodrugs, Pharmacology, 030226 pharmacology & pharmacy, Deoxycytidine, Analytical Chemistry, 0302 clinical medicine, Drug Delivery Systems, Drug Stability, Drug Discovery, stroma cells, Prodrugs, Amino Acids, Chemistry, Cytosine deaminase, Esters, Cytidine deaminase, Dipeptides, Prodrug, 3. Good health, Chemistry (miscellaneous), 030220 oncology & carcinogenesis, Drug delivery, Molecular Medicine, medicine.drug, Antineoplastic Agents, Permeability, Article, lcsh:QD241-441, 03 medical and health sciences, lcsh:Organic chemistry, Pancreatic cancer, Cell Line, Tumor, Cytidine Deaminase, medicine, Humans, cytosine deaminase, Physical and Theoretical Chemistry, Thymidine phosphorylase, metabolism, Cell Proliferation, Thymidine Phosphorylase, Organic Chemistry, medicine.disease, Gemcitabine, Enzyme Activation, Pancreatic Neoplasms, Drug Liberation, Cancer cell

Abstract

One of the main obstacles for cancer therapies is to deliver medicines effectively to target sites. Since stroma cells are developed around tumors, chemotherapeutic agents have to go through stroma cells in order to reach tumors. As a method to improve drug delivery to the tumor site, a prodrug approach for gemcitabine was adopted. Amino acid and dipeptide monoester prodrugs of gemcitabine were synthesized and their chemical stability in buffers, resistance to thymidine phosphorylase and cytidine deaminase, antiproliferative activity, and uptake/permeability in HFF cells as a surrogate to stroma cells were determined and compared to their parent drug, gemcitabine. The activation of all gemcitabine prodrugs was faster in pancreatic cell homogenates than their hydrolysis in buffer, suggesting enzymatic action. All prodrugs exhibited great stability in HFF cell homogenate, enhanced resistance to glycosidic bond metabolism by thymidine phosphorylase, and deamination by cytidine deaminase compared to their parent drug. All gemcitabine prodrugs exhibited higher uptake in HFF cells and better permeability across HFF monolayers than gemcitabine, suggesting a better delivery to tumor sites. Cell antiproliferative assays in Panc-1 and Capan-2 pancreatic ductal cell lines indicated that the gemcitabine prodrugs were more potent than their parent drug gemcitabine. The transport and enzymatic profiles of gemcitabine prodrugs suggest their potential for delayed enzymatic bioconversion and enhanced resistance to metabolic enzymes, as well as for enhanced drug delivery to tumor sites, and cytotoxic activity in cancer cells. These attributes would facilitate the prolonged systemic circulation and improved therapeutic efficacy of gemcitabine prodrugs.

Published

2017

33. Low Buffer Capacity and Alternating Motility along the Human Gastrointestinal Tract: Implications for in Vivo Dissolution and Absorption of Ionizable Drugs

Author

Gordon L. Amidon, Bart Hens, William L. Hasler, Bo Wen, Gail Benninghoff, Robert Lionberger, Raimar Loebenberg, Greg E. Amidon, Jason Baker, Kerby Shedden, Jeffrey Wysocki, Mark J. Koenigsknecht, Duxin Sun, Niloufar Salehi, Yasuhiro Tsume, Jianghong Fan, Allen Lee, Marival Bermejo, Joseph Dickens, Paulo Paixão, Arjang Talattof, Alex Yu, and Ann Frances

Subjects

Absorption (pharmacology), Adult, Time Factors, Manometry, Pharmaceutical Science, Administration, Oral, Ibuprofen, 02 engineering and technology, Bioequivalence, Pharmacology, Buffers, 030226 pharmacology & pharmacy, Jejunum, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Oral administration, Drug Discovery, medicine, Ingestion, Humans, Intestinal Mucosa, Chemistry, Hydrogen-Ion Concentration, Middle Aged, 021001 nanoscience & nanotechnology, Healthy Volunteers, Bioavailability, Absorption, Physiological, Body Fluids, Gastrointestinal Tract, Drug Liberation, medicine.anatomical_structure, Intestinal Absorption, Solubility, Therapeutic Equivalency, Duodenum, Molecular Medicine, 0210 nano-technology, Gastrointestinal Motility, medicine.drug, Tablets

Abstract

In this study, we determined the pH and buffer capacity of human gastrointestinal (GI) fluids (aspirated from the stomach, duodenum, proximal jejunum, and mid/distal jejunum) as a function of time, from 37 healthy subjects after oral administration of an 800 mg immediate-release tablet of ibuprofen (reference listed drug; RLD) under typical prescribed bioequivalence (BE) study protocol conditions in both fasted and fed states (simulated by ingestion of a liquid meal). Simultaneously, motility was continuously monitored using water-perfused manometry. The time to appearance of phase III contractions (i.e., housekeeper wave) was monitored following administration of the ibuprofen tablet. Our results clearly demonstrated the dynamic change in pH as a function of time and, most significantly, the extremely low buffer capacity along the GI tract. The buffer capacity on average was 2.26 μmol/mL/ΔpH in fasted state (range: 0.26 and 6.32 μmol/mL/ΔpH) and 2.66 μmol/mL/ΔpH in fed state (range: 0.78 and 5.98 μmol/mL/ΔpH) throughout the entire upper GI tract (stomach, duodenum, and proximal and mid/distal jejunum). The implication of this very low buffer capacity of the human GI tract is profound for the oral delivery of both acidic and basic active pharmaceutical ingredients (APIs). An in vivo predictive dissolution method would require not only a bicarbonate buffer but also, more significantly, a low buffer capacity of dissolution media to reflect in vivo dissolution conditions.

Published

2017

34. Mechanistic Fluid Transport Model to Estimate Gastrointestinal Fluid Volume and Its Dynamic Change Over Time

Author

Gordon L. Amidon, Amit Pai, Trachette L. Jackson, Duxin Sun, Ann Frances, Bo Wen, Mark J. Koenigsknecht, Alex Yu, Jeffrey Wysocki, William L. Hasler, Luca Marciani, Yasuhiro Tsume, and Jason Baker

Subjects

medicine.medical_specialty, Pharmaceutical Science, Administration, Oral, 030226 pharmacology & pharmacy, Gastroenterology, Phenolsulfonphthalein, Jejunum, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, medicine, Humans, Compartment (pharmacokinetics), Gastrointestinal Transit, Phenol red, Chemistry, Stomach, Fluid compartments, Fluid transport, Magnetic Resonance Imaging, Small intestine, Drug Liberation, medicine.anatomical_structure, Gastric Emptying, Intestinal Absorption, 030220 oncology & carcinogenesis, Duodenum, Biomedical engineering

Abstract

Gastrointestinal (GI) fluid volume and its dynamic change are integral to study drug disintegration, dissolution, transit, and absorption. However, key questions regarding the local volume and its absorption, secretion, and transit remain unanswered. The dynamic fluid compartment absorption and transit (DFCAT) model is proposed to estimate in vivo GI volume and GI fluid transport based on magnetic resonance imaging (MRI) quantified fluid volume. The model was validated using GI local concentration of phenol red in human GI tract, which was directly measured by human GI intubation study after oral dosing of non-absorbable phenol red. The measured local GI concentration of phenol red ranged from 0.05 to 168 μg/mL (stomach), to 563 μg/mL (duodenum), to 202 μg/mL (proximal jejunum), and to 478 μg/mL (distal jejunum). The DFCAT model characterized observed MRI fluid volume and its dynamic changes from 275 to 46.5 mL in stomach (from 0 to 30 min) with mucus layer volume of 40 mL. The volumes of the 30 small intestine compartments were characterized by a max of 14.98 mL to a min of 0.26 mL (0–120 min) and a mucus layer volume of 5 mL per compartment. Regional fluid volumes over 0 to 120 min ranged from 5.6 to 20.38 mL in the proximal small intestine, 36.4 to 44.08 mL in distal small intestine, and from 42 to 64.46 mL in total small intestine. The DFCAT model can be applied to predict drug dissolution and absorption in the human GI tract with future improvements.

Published

2017

35. Unpredictable Performance of pH-Dependent Coatings Accentuates the Need for Improved Predictive in Vitro Test Systems

Author

Jozef Al-Gousous, Peter Langguth, Maoqi Fu, Isam I. Salem, and Yasuhiro Tsume

Subjects

medicine.medical_specialty, Drug Liberation, In vitro test, Chemistry, Pharmaceutical, Pharmaceutical Science, Ph dependent, Biological Availability, 02 engineering and technology, Pharmacology, In Vitro Techniques, 030226 pharmacology & pharmacy, Dosage form, Biopharmaceutics, Excipients, 03 medical and health sciences, 0302 clinical medicine, Drug Discovery, Intestine, Small, medicine, Intensive care medicine, Gastric emptying, business.industry, Hydrogen-Ion Concentration, 021001 nanoscience & nanotechnology, Enteric coating, Bioavailability, Solubility, Drug delivery, Molecular Medicine, Tablets, Enteric-Coated, 0210 nano-technology, business, medicine.drug

Abstract

First introduced in the second half of the 19th century, enteric coatings are commonly used to protect acid-labile drugs, reduce the risk of gastric side effects due to irritating drugs, or for local drug delivery to the lower gastrointestinal (GI) tract. The currently available enteric-coatings are based on pH-sensitive weakly acidic polymers. Despite the long history of their use, the causes behind their performance often being unpredictable have not been properly investigated with most of the attention being focused only on the gastric emptying. However, little attention has been given to the postgastric emptying disintegration and dissolution of these dosage forms. This lack of attention has contributed to the difficulty in predicting the in vivo behavior of these dosage forms and to cases of bioavailability problems with some enteric-coated products. Therefore, increased attention needs to be given to this issue.

Published

2017

36. The Biopharmaceutics Classification System: Subclasses for in vivo predictive dissolution (IPD) methodology and IVIVC

Author

Yasuhiro Tsume, Greg E. Amidon, Gordon L. Amidon, Deanna M. Mudie, and Peter Langguth

Subjects

Drug, media_common.quotation_subject, Administration, Oral, Pharmaceutical Science, Computational biology, Pharmacology, Models, Biological, Permeability, Article, Intestinal absorption, Quality by Design, Dosage form, Biopharmaceutics, IVIVC, In vivo, Terminology as Topic, Animals, Humans, Technology, Pharmaceutical, Computer Simulation, Pharmacokinetics, Intestinal Mucosa, media_common, Chemistry, Reproducibility of Results, Hydrogen-Ion Concentration, Biopharmaceutics Classification System, Intestinal Absorption, Pharmaceutical Preparations, Solubility

Abstract

The Biopharmaceutics Classification System (BCS) has found widespread utility in drug discovery, product development and drug product regulatory sciences. The classification scheme captures the two most significant factors influencing oral drug absorption; solubility and intestinal permeability and it has proven to be a very useful and a widely accepted starting point for drug product development and drug product regulation. The mechanistic base of the BCS approach has, no doubt, contributed to its wide spread acceptance and utility. Nevertheless, underneath the simplicity of BCS are many detailed complexities, both in vitro and in vivo which must be evaluated and investigated for any given drug and drug product. In this manuscript we propose a simple extension of the BCS classes to include sub-specification of acid (a), base (b) and neutral (c) for classes II and IV. Sub-classification for Classes I and III (high solubility drugs as currently defined) is generally not needed except perhaps in border line solubility cases. It is well known that the , pKa physical property of a drug (API) has a significant impact on the aqueous solubility dissolution of drug from the drug product both in vitro and in vivo for BCS Class II and IV acids and bases, and is the basis, we propose for a sub-classification extension of the original BCS classification. This BCS sub-classification is particularly important for in vivo predictive dissolution methodology development due to the complex and variable in vivo environment in the gastrointestinal tract, with its changing pH, buffer capacity, luminal volume, surfactant luminal conditions, permeability profile along the gastrointestinal tract and variable transit and fasted and fed states. We believe this sub-classification is a step toward developing a more science-based mechanistic in vivo predictive dissolution (IPD) methodology. Such a dissolution methodology can be used by development scientists to assess the likelihood of a formulation and dosage form functioning as desired in humans, can be optimized along with parallel human pharmacokinetic studies to set a dissolution methodology for Quality by Design (QbD) and in vitro-in vivo correlations (IVIVC) and ultimately can be used as a basis for a dissolution standard that will ensure continued in vivo product performance.

Published

2014

37. The development of orally administrable gemcitabine prodrugs with d-enantiomer amino acids: Enhanced membrane permeability and enzymatic stability

Author

Xueqin Song, Gordon L. Amidon, Yasuhiro Tsume, Tuba Incecayir, and John M. Hilfinger

Subjects

Antimetabolites, Antineoplastic, Cell Membrane Permeability, Membrane permeability, Administration, Oral, Pharmaceutical Science, Deoxycytidine, Article, Mice, Enzyme Stability, medicine, Animals, Humans, Prodrugs, Amino Acids, Thymidine phosphorylase, chemistry.chemical_classification, Mice, Inbred BALB C, Chemistry, Stereoisomerism, General Medicine, Metabolism, Prodrug, Gemcitabine, Amino acid, Enzyme, Biochemistry, Caco-2, Female, Caco-2 Cells, Biotechnology, medicine.drug

Abstract

Gemcitabine prodrugs with D- and L-configuration amino acids were synthesized and their chemical stability in buffers, resistance to glycosidic bond metabolism, enzymatic activation, permeability in Caco-2 cells and mouse intestinal membrane, anti-proliferation activity in cancer cell were determined and compared to that of parent drug, gemcitabine. Prodrugs containing D-configuration amino acids were enzymatically more stable than ones with c-configuration amino acids. The activation of all gemcitabine prodrugs was 1.3-17.6-fold faster in cancer cell homogenate than their hydrolysis in buffer, suggesting enzymatic action. The enzymatic activation of amino acid monoester prodrugs containing D-configuration amino acids in cell homogenates was 2.2-10.9-fold slower than one of amino acid monoester prodrugs with L-configuration amino acids. All prodrugs exhibited enhanced resistance to glycosidic bond metabolism by thymidine phosphorylase compared to parent gemcitabine. Gemcitabine prodrugs showed superior the effective permeability in mouse jejunum to gemcitabine. More importantly, the high plasma concentration of D-amino acid gemcitabine prodrugs was observed more than one of L-amino acid gemcitabine prodrugs. In general, the 5'-mono-amino acid monoester gemcitabine prodrugs exhibited higher permeability and uptake than their parent drug, gemcitabine. Cell proliferation assays in AsPC-1 pancreatic ductal cell line indicated that gemcitabine prodrugs were more potent than their parent drug, gemcitabine. The transport and enzymatic profiles of 5'-D-valyl-gemcitabine and 5'-D-phenylalanyl-gemcitabine suggest their potential for increased oral uptake and delayed enzymatic bioconversion as well as enhanced uptake and cytotoxic activity in cancer cells, would facilitate the development of oral dosage form for anti-cancer agents and, hence, improve the quality of life for the cancer patients. (C) 2014 Published by Elsevier B.V.

Published

2014

38. Measurement of in vivo Gastrointestinal Release and Dissolution of Three Locally Acting Mesalamine Formulations in Regions of the Human Gastrointestinal Tract

Author

Siwei Li, Mark J. Koenigsknecht, Jason Baker, Gordon L. Amidon, Duxin Sun, Ruijuan Luo, Ying Wang, William L. Hasler, Yasuhiro Tsume, Bo Wen, Xinyuan Zhang, Robert Lionberger, Michael J. Bly, Ann F. Fioritto, and Alex Yu

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Chemistry, Pharmaceutical, Pharmaceutical Science, Administration, Oral, digestive system, 030226 pharmacology & pharmacy, Gastroenterology, Jejunum, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Pharmacokinetics, In vivo, Internal medicine, Drug Discovery, medicine, Humans, Dissolution testing, Mesalamine, business.industry, Stomach, digestive, oral, and skin physiology, Human gastrointestinal tract, Middle Aged, medicine.disease, Ulcerative colitis, Gastrointestinal Tract, Drug Liberation, medicine.anatomical_structure, Solubility, Duodenum, Molecular Medicine, 030211 gastroenterology & hepatology, Female, business

Abstract

As an orally administered, locally acting gastrointestinal drug, mesalamine products are designed to achieve high local drug concentration in the gastrointestinal (GI) tract for the treatment of ulcerative colitis. The aim of this study was to directly measure and compare drug dissolution of three mesalamine formulations in human GI tract and to correlate their GI concentration with drug concentration in plasma. Healthy human subjects were orally administered Pentasa, Apriso, or Lialda. GI fluids were aspirated from stomach, duodenum, proximal jejunum, mid jejunum, and distal jejunum regions. Mesalamine (5-ASA) and its primary metabolite acetyl-5-mesalamine (Ac-5-ASA) were measured using LC-MS/MS. GI tract pH was measured from each GI fluid sample, which averaged 1.82, 4.97, 5.67, 6.17, and 6.62 in the stomach, duodenum, proximal jejunum, middle jejunum, and distal jejunum, respectively. For Pentasa, high levels of 5-ASA in solution were observed in the stomach, duodenum, proximal jejunum, mid jejunum, and distal jejunum from 1 to 7 h. Apriso had minimal 5-ASA levels in stomach, low to medium levels of 5-ASA in duodenum and proximal jejunum from 4 to 7 h, and high levels of 5-ASA in distal jejunum from 3 to 7 h. In contrast, Lialda had minimal 5-ASA levels from stomach and early small intestine. A composite appearance rate (CAR) was calculated from the deconvolution of individual plasma concentration to reflect drug release, dissolution, transit, and absorption in the GI tract. Individuals dosed with Pentasa had high levels of CAR from 1 to 10 h; individuals dosed with Apriso had low levels of CAR from 1 to 4 h and high levels of CAR from 5 to 10 h; Lialda showed minimal levels of CAR from 0 to 5 h, then increased to medium levels from 5 to 12 h, and then decreased to further lower levels after 12 h. In the colon region, Pentasa and Apriso showed similar levels of accumulated 5-ASA excreted in the feces, while Lialda showed slightly higher 5-ASA accumulation in feces. However, all three formulations showed similar levels of metabolite Ac-5-ASA in the feces. These results provide direct measurement of drug dissolution in the GI tract, which can serve as a basis for investigation of bioequivalence for locally acting drug products.

Published

2016

39. Sulforaphane enhances the anticancer activity of taxanes against triple negative breast cancer by killing cancer stem cells

Author

Lichao Sun, Shuhua Bai, Gi Lim, Joseph Burnett, Yasuhiro Tsume, Hayley J. Paholak, Ronak B. Shah, Duxin Sun, Rebekah Lim, Yanyan Li, Tao Zhang, Sean P. McDermott, and Max S. Wicha

Subjects

0301 basic medicine, Cancer Research, Time Factors, Transcription, Genetic, Aldehyde dehydrogenase, Triple Negative Breast Neoplasms, Docetaxel, Mice, SCID, Pharmacology, chemistry.chemical_compound, 0302 clinical medicine, Isothiocyanates, Mice, Inbred NOD, Antineoplastic Combined Chemotherapy Protocols, Triple-negative breast cancer, biology, Cell Death, Chemistry, Primary tumor, Tubulin Modulators, Tumor Burden, Gene Expression Regulation, Neoplastic, Phenotype, Oncology, Paclitaxel, 030220 oncology & carcinogenesis, Sulfoxides, Neoplastic Stem Cells, Female, Taxoids, Inflammation Mediators, medicine.drug, Signal Transduction, Transfection, Article, 03 medical and health sciences, Breast cancer, NF-kappa B p52 Subunit, Cancer stem cell, Cell Line, Tumor, medicine, Animals, Humans, Cell Proliferation, Dose-Response Relationship, Drug, Interleukin-6, Interleukin-8, Transcription Factor RelA, medicine.disease, Xenograft Model Antitumor Assays, 030104 developmental biology, biology.protein, Cancer research, Sulforaphane

Abstract

Triple negative breast cancer (TNBC) typically exhibits rapid progression, high mortality and faster relapse rates relative to other breast cancer subtypes. In this report we examine the combination of taxanes (paclitaxel or docetaxel) with a breast cancer stem cell (CSC)-targeting agent sulforaphane for use against TNBC. We demonstrate that paclitaxel or docetaxel treatment induces IL-6 secretion and results in expansion of CSCs in TNBC cell lines. Conversely, sulforaphane is capable of preferentially eliminating CSCs, by inhibiting NF-κB p65 subunit translocation, downregulating p52 and consequent downstream transcriptional activity. Sulforaphane also reverses taxane-induced aldehyde dehydrogenase-positive (ALDH+) cell enrichment, and dramatically reduces the size and number of primary and secondary mammospheres formed. In vivo in an advanced treatment orthotopic mouse xenograft model together with extreme limiting dilution analysis (ELDA), the combination of docetaxel and sulforaphane exhibits a greater reduction in primary tumor volume and significantly reduces secondary tumor formation relative to either treatment alone. These results suggest that treatment of TNBCs with cytotoxic chemotherapy would be greatly benefited by the addition of sulforaphane to prevent expansion of and eliminate breast CSCs.

Published

2016

40. Exploring Bioequivalence of Dexketoprofen Trometamol Drug Products with the Gastrointestinal Simulator (GIS) and Precipitation Pathways Analyses

Author

Gregory E. Amidon, Alfredo García-Arieta, Naír Rodríguez-Hornedo, Marival Bermejo, Alejandro Ruiz-Picazo, Yasuhiro Tsume, Jozef Al-Gousous, Deanna M. Mudie, Bart Hens, Gordon L. Amidon, Isabel González-Álvarez, and Gislaine Kuminek

Subjects

liquid–liquid phase separation, SALT DISPROPORTIONATION, gastrointestinal absorption, Sodium, lcsh:RS1-441, Pharmaceutical Science, Excipient, chemistry.chemical_element, Salt (chemistry), Hydrochloric acid, SOLUBILITY, Calcium, Bioequivalence, Article, lcsh:Pharmacy and materia medica, chemistry.chemical_compound, FLUIDS, EMA, oral absorption, ABSORPTION, medicine, Pharmacology & Pharmacy, SUPERSATURATED SOLUTIONS, dexketoprofen, Simulation, chemistry.chemical_classification, Science & Technology, Chemistry, liquid-liquid phase separation, Phosphate, Dexketoprofen, SIMILARITIES, gastrointestinal simulator, in vitro dissolution, IN-VITRO DISSOLUTION, Life Sciences & Biomedicine, VIVO DISSOLUTION, METHODOLOGY, microscopy imaging, medicine.drug

Abstract

The present work aimed to explain the differences in oral performance in fasted humans who were categorized into groups based on the three different drug product formulations of dexketoprofen trometamol (DKT) salt&mdash, Using a combination of in vitro techniques and pharmacokinetic analysis. The non-bioequivalence (non-BE) tablet group achieved higher plasma Cmax and area under the curve (AUC) than the reference and BE tablets groups, with only one difference in tablet composition, which was the presence of calcium monohydrogen phosphate, an alkalinizing excipient, in the tablet core of the non-BE formulation. Concentration profiles determined using a gastrointestinal simulator (GIS) apparatus designed with 0.01 N hydrochloric acid and 34 mM sodium chloride as the gastric medium and fasted state simulated intestinal fluids (FaSSIF-v1) as the intestinal medium showed a faster rate and a higher extent of dissolution of the non-BE product compared to the BE and reference products. These in vitro profiles mirrored the fraction doses absorbed in vivo obtained from deconvoluted plasma concentration&ndash, time profiles. However, when sodium chloride was not included in the gastric medium and phosphate buffer without bile salts and phospholipids were used as the intestinal medium, the three products exhibited nearly identical concentration profiles. Microscopic examination of DKT salt dissolution in the gastric medium containing sodium chloride identified that when calcium phosphate was present, the DKT dissolved without conversion to the less soluble free acid, which was consistent with the higher drug exposure of the non-BE formulation. In the absence of calcium phosphate, however, dexketoprofen trometamol salt dissolution began with a nano-phase formation that grew to a liquid&ndash, liquid phase separation (LLPS) and formed the less soluble free acid crystals. This phenomenon was dependent on the salt/excipient concentrations and the presence of free acid crystals in the salt phase. This work demonstrated the importance of excipients and purity of salt phase on the evolution and rate of salt disproportionation pathways. Moreover, the presented data clearly showed the usefulness of the GIS apparatus as a discriminating tool that could highlight the differences in formulation behavior when utilizing physiologically-relevant media and experimental conditions in combination with microscopy imaging.

Published

2019

41. The Extracellular Microenvironment Explains Variations in Passive Drug Transport Across Different Airway Epithelial Cell Types

Author

Kyoung Ah Min, Kathleen A. Stringer, Arjang Talattof, Jing Yu Yu, Gus R. Rosania, Yasuhiro Tsume, and Dong Hyun Lim

Subjects

Passive transport, Pharmaceutical Science, Respiratory Mucosa, Biology, Permeability, Article, Cell Line, Tumor, Extracellular, medicine, Animals, Humans, Pharmacokinetics, Pharmacology (medical), Cells, Cultured, Drug transport, Pharmacology, Cellular architecture, Organic Chemistry, Water, Biological Transport, Epithelial Cells, Propranolol, Small molecule, Coculture Techniques, Epithelium, Cell biology, medicine.anatomical_structure, Immunology, Molecular Medicine, Coculture Technique, Airway, Biotechnology

Abstract

We sought to identify key variables in cellular architecture and physiology that might explain observed differences in the passive transport properties of small molecule drugs across different airway epithelial cell types.Propranolol (PR) was selected as a weakly basic, model compound to compare the transport properties of primary (NHBE) vs. tumor-derived (Calu-3) cells. Differentiated on Transwell™ inserts, the architecture of pure vs. mixed cell co-cultures was studied with confocal microscopy followed by quantitative morphometric analysis. Cellular pharmacokinetic modeling was used to identify parameters that differentially affect PR uptake and transport across these two cell types.Pure Calu-3 and NHBE cells possessed different structural and functional properties. Nevertheless, mixed Calu-3 and NHBE cell co-cultures differentiated as stable cell monolayers. After measuring the total mass of PR, the fractional areas covered by Calu-3 and NHBE cells allowed deconvoluting the transport properties of each cell type. Based on the apparent thickness of the unstirred, cell surface aqueous layer, local differences in the extracellular microenvironment explained the measured variations in passive PR uptake and permeation between Calu-3 and NHBE cells.Mixed cell co-cultures can be used to compare the local effects of the extracellular microenvironment on drug uptake and transport across two epithelial cell types.

Published

2013

42. Novel inhibitors of bacterial virulence: Development of 5,6-dihydrobenzo[h]quinazolin-4(3H)-ones for the inhibition of group A streptococcal streptokinase expression

Author

Yuanxi Xu, Xiaoqin Li, Yasuhiro Tsume, Wenpeng Zhang, Bryan D. Yestrepsky, Jenny G. Ryu, Scott D. Larsen, Meghan E. Breen, Hongmin Sun, Roderick Joseph Sorenson, Walajapet Rajeswaran, Duxin Sun, and Michael W. Wilson

Subjects

Cell Survival, medicine.drug_class, Clinical Biochemistry, Antibiotics, Pharmaceutical Science, medicine.disease_cause, Biochemistry, Article, Virulence factor, Microbiology, Mice, Structure-Activity Relationship, Antibiotic resistance, Streptococcal Infections, Drug Discovery, medicine, Animals, Humans, Structure–activity relationship, Potency, Streptokinase, Mode of action, Molecular Biology, Chemistry, Streptococcus, Organic Chemistry, Gene Expression Regulation, Bacterial, Anti-Bacterial Agents, Solubility, Staphylococcus aureus, Biofilms, Microsomes, Liver, Quinazolines, Molecular Medicine, HeLa Cells

Abstract

Resistance to antibiotics is an increasingly dire threat to human health that warrants the development of new modes of treating infection. We recently identified 1 (CCG-2979) as an inhibitor of the expression of streptokinase, a critical virulence factor in Group A Streptococcus that endows blood-borne bacteria with fibrinolytic capabilities. In this report, we describe the synthesis and biological evaluation of a series of novel 5,6-dihydrobenzo[h]quinazolin-4(3H)-one analogs of 1 undertaken with the goal of improving the modest potency of the lead. In addition to achieving an over 35-fold increase in potency, we identified structural modifications that improve the solubility and metabolic stability of the scaffold. The efficacy of two new compounds 12c (CCG-203592) and 12k (CCG-205363) against biofilm formation in Staphylococcus aureus represents a promising additional mode of action for this novel class of compounds.

Published

2013

43. Carrier-Mediated Prodrug Uptake to Improve the Oral Bioavailability of Polar Drugs: An Application to an Oseltamivir Analogue

Author

Elke Lipka, Tuba Incecayir, Gordon L. Amidon, Yasuhiro Tsume, Tomoka Gose, Hao Xu, John M. Hilfinger, Jing Sun, Takeo Nakanishi, and Ikumi Tamai

Subjects

Male, 0301 basic medicine, Cell Membrane Permeability, Membrane permeability, medicine.drug_class, Administration, Oral, Biological Availability, Pharmaceutical Science, Pharmacology, Antiviral Agents, 030226 pharmacology & pharmacy, Article, Mice, Xenopus laevis, 03 medical and health sciences, Oseltamivir, 0302 clinical medicine, medicine, Animals, Humans, Prodrugs, Mice, Knockout, chemistry.chemical_classification, Drug Carriers, Oligopeptide, Neuraminidase inhibitor, Chemistry, Diastereomer, Hep G2 Cells, Prodrug, Amino acid, Bioavailability, 030104 developmental biology, Biochemistry, Caco-2, Female, Caco-2 Cells

Abstract

The goal of this study was to improve the intestinal mucosal cell membrane permeability of the poorly absorbed guanidino analogue of a neuraminidase inhibitor, oseltamivir carboxylate (GOC) using a carrier-mediated strategy. Valyl amino acid prodrug of GOC with isopropyl-methylene-dioxy linker (GOC-ISP-Val) was evaluated as the potential substrate for intestinal oligopeptide transporter, hPEPT1 in Xenopus laevis oocytes heterologously expressing hPEPT1, and an intestinal mouse perfusion system. The diastereomers of GOC-ISP-Val were assessed for chemical and metabolic stability. Permeability of GOC-ISP-Val was determined in Caco-2 cells and mice. Diastereomer 2 was about 2 times more stable than diastereomer 1 in simulated intestinal fluid and rapidly hydrolyzed to the parent drug in cell homogenates. The prodrug had a 9 times-enhanced apparent permeability (P-app) in Caco-2 cells compared with the parent drug. Both diastereomer exhibited high effective permeability (P-eff) in mice, 6.32 +/- 3.12 and 5.20 +/- 2.81 x 10(-5) cm/s for diastereomer 1 and 2, respectively. GOC-ISP-Val was found to be a substrate of hPEPT1. Overall, this study indicates that the prodrug, GOC-ISP-Val, seems to be a promising oral anti-influenza agent that has sufficient stability at physiologically relevant pHs before absorption, significantly improved permeability via hPEPT1 and potentially rapid activation in the intestinal cells. (C) 2016 American Pharmacists Association (R). Published by Elsevier Inc. All rights reserved.

Published

2016

44. In silicoprediction of drug dissolution and absorption with variation in intestinal pH for BCS class II weak acid drugs: ibuprofen and ketoprofen

Author

Yasuhiro Tsume, Alfredo García-Arieta, Peter Langguth, and Gordon L. Amidon

Subjects

Pharmacology, Ketoprofen, Chromatography, Chemistry, Pharmaceutical Science, General Medicine, Bioequivalence, Ibuprofen, Dosage form, Bioavailability, medicine, Pharmacology (medical), Dissolution testing, Solubility, Dissolution, medicine.drug

Abstract

The FDA Biopharmaceutical Classification System guidance allows waivers for in vivo bioavailability and bioequivalence studies for immediate-release solid oral dosage forms only for BCS class I. Extensions of the in vivo biowaiver for a number of drugs in BCS class III and BCS class II have been proposed, in particular, BCS class II weak acids. However, a discrepancy between the in vivo BE results and in vitro dissolution results for BCS class II acids was recently observed. The objectives of this study were to determine the oral absorption of BCS class II weak acids via simulation software and to determine if the in vitro dissolution test with various dissolution media could be sufficient for in vitro bioequivalence studies of ibuprofen and ketoprofen as models of carboxylic acid drugs. The oral absorption of these BCS class II acids from the gastrointestinal tract was predicted by GastroPlus ™ . Ibuprofen did not satisfy the bioequivalence criteria at lower settings of intestinal pH of 6.0. Further the experimental dissolution of ibuprofen tablets in a low concentration phosphate buffer at pH 6.0 (the average buffercapacity 2.2mmoll -1 /pH) was dramatically reduced compared with the dissolution in SIF (the average buffer capacity 12.6mmoll -1 /pH). Thus these predictions for the oral absorption of BCS class II acids indicate that the absorption patterns depend largely on the intestinal pH and buffer strength and must be considered carefully for a bioequivalence test. Simulation software may be a very useful tool to aid the selection of dissolution media that may be useful in setting an in vitro bioequivalence dissolution standard. Copyright © 2012 John Wiley & Sons, Ltd.

Published

2012

45. Enhancing the Intestinal Membrane Permeability of Zanamivir: A Carrier Mediated Prodrug Approach

Author

Deepak Gupta, John M. Hilfinger, Jing Sun, Gordon L. Amidon, Arik Dahan, Sheeba Varghese Gupta, Kyung Dall Lee, and Yasuhiro Tsume

Subjects

Cell Membrane Permeability, Membrane permeability, viruses, Pharmaceutical Science, Article, HeLa, Zanamivir, Drug Stability, Drug Discovery, medicine, Animals, Humans, Prodrugs, Intestinal Mucosa, Chromatography, High Pressure Liquid, chemistry.chemical_classification, Drug Carriers, Molecular Structure, biology, Membrane transport protein, virus diseases, biochemical phenomena, metabolism, and nutrition, Prodrug, biology.organism_classification, Combinatorial chemistry, Rats, respiratory tract diseases, Amino acid, Intestines, chemistry, Biochemistry, Caco-2, biology.protein, Molecular Medicine, Caco-2 Cells, Drug carrier, HeLa Cells, medicine.drug

Abstract

The purpose of this study was to improve the membrane permeability and oral absorption of the poorly permeable anti-influenza agent, zanamivir. The poor oral bioavailability is attributed to the high polarity (cLogP ∼ -5) resulting from the polar and zwitterionic nature of zanamivir. In order to improve the permeability of zanamivir, prodrugs with amino acids were developed to target the intestinal membrane transporter, hPepT1. Several acyloxy ester prodrugs of zanamivir conjugated with amino acids were synthesized and characterized. The prodrugs were evaluated for their chemical stability in buffers at various pHs and for their transport and tissue activation by enzymes. The acyloxy ester prodrugs of zanamivir were shown to competitively inhibit [(3)H]Gly-Sar uptake in Caco-2 cells (IC(50): 1.19 ± 0.33 mM for L-valyl prodrug of zanamivir). The L-valyl prodrug of zanamivir exhibited ∼3-fold higher uptake in transfected HeLa/hPepT1 cells compared to wild type HeLa cells, suggesting, at least in part, carrier mediated transport by the hPepT1 transporter. Further, enhanced transcellular permeability of prodrugs across Caco-2 monolayer compared to the parent drug (P(app) = 2.24 × 10(-6) ± 1.33 × 10(-7) cm/s for L-valyl prodrug of zanamivir), with only parent zanamivir appearing in the receiver compartment, indicates that the prodrugs exhibited both enhanced transport and activation in intestinal mucosal cells. Most significantly, several of these prodrugs exhibited high intestinal jejunal membrane permeability, similar to metoprolol, in the in situ rat intestinal perfusion system, a system highly correlated with human jejunal permeability. In summary, this mechanistic targeted prodrug strategy, to enhance oral absorption via intestinal membrane carriers such as hPepT1, followed by activation to parent drug (active pharmaceutical ingredient or API) in the mucosal cell, significantly improves the intestinal epithelial cell permeability of zanamivir and has the potential to provide the high oral bioavailability necessary for oral zanamivir therapy.

Published

2011

46. Potential of Amino Acid/Dipeptide Monoester Prodrugs of Floxuridine in Facilitating Enhanced Delivery of Active Drug to Interior Sites of Tumors: A Two-Tier Monolayer In Vitro Study

Author

Gordon L. Amidon, Yasuhiro Tsume, and John M. Hilfinger

Subjects

Drug, media_common.quotation_subject, Cell, Pharmaceutical Science, Permeability, chemistry.chemical_compound, Drug Delivery Systems, Drug Stability, Floxuridine, Cell Line, Tumor, Neoplasms, Enzyme Stability, Monolayer, medicine, Humans, Prodrugs, Pharmacology (medical), Amino Acids, Cell Proliferation, media_common, Pharmacology, chemistry.chemical_classification, Dipeptide, Chemistry, Organic Chemistry, Cancer, Dipeptides, Prodrug, medicine.disease, Amino acid, medicine.anatomical_structure, Biochemistry, Delayed-Action Preparations, Molecular Medicine, Biotechnology, medicine.drug

Abstract

To evaluate the advantages of amino acid/dipeptide monoester prodrugs for cancer treatments by assessing the uptake and cytotoxic effects of floxuridine prodrugs in a secondary cancer cell monolayer following permeation across a primary cancer cell monolayer.The first Capan-2 monolayer was grown on membrane transwell inserts; the second monolayer was grown at the bottom of a plate. The permeation of floxuridine and its prodrugs across the first monolayer and the uptake and cell proliferation assay on secondary layer were sequentially determined.All floxuridine prodrugs exhibited greater permeation across the first Capan-2 monolayer than the parent drug. The correlation between uptake and growth inhibition in the second monolayer with intact prodrug permeating the first monolayer suggests that permeability and enzymatic stability are essential for sustained action of prodrugs in deeper layers of tumors. The correlation of uptake and growth inhibition were vastly superior for dipeptide prodrugs to those obtained with mono amino acid prodrugs.Although a tentative general overall correlation between intact prodrug and uptake or cytotoxic action was obtained, it appears that a mixture of floxuridine prodrugs with varying beneficial characteristics may be more effective in treating tumors.

Published

2011

47. Oral Bioavailability of Peptide and Peptidomimetic Drugs

Author

Jing Sun, Yasuhiro Tsume, Arik Dahan, Jonathan M. Miller, and Gordon L. Amidon

Subjects

chemistry.chemical_classification, Peptidomimetic, Chemistry, Peptide, Pharmacology, Dosage form, Bioavailability

Published

2011

48. The Biowaiver Extension for BCS Class III Drugs: The Effect of Dissolution Rate on the Bioequivalence of BCS Class III Immediate-Release Drugs Predicted by Computer Simulation

Author

Yasuhiro Tsume and Gordon L. Amidon

Subjects

Cell Membrane Permeability, Pharmaceutical Science, Pharmacology, Bioequivalence, Dosage form, Intestinal absorption, Pharmacokinetics, In vivo, Drug Discovery, medicine, Humans, Computer Simulation, Cimetidine, Chemistry, Amoxicillin, Atenolol, Propranolol, Bioavailability, Gastrointestinal Tract, Gastric Emptying, Pharmaceutical Preparations, Molecular Medicine, Software, Metoprolol, medicine.drug

Abstract

The Biopharmaceutical Classification System (BCS) guidance issued by the FDA allows waivers for in vivo bioavailability and bioequivalence studies for immediate-release (IR) solid oral dosage forms only for BCS class I drugs. However, a number of drugs within BCS class III have been proposed to be eligible for biowaivers. The World Health Organization (WHO) has shortened the requisite dissolution time of BCS class III drugs on their Essential Medicine List (EML) from 30 to 15 min for extended biowaivers; however, the impact of the shorter dissolution time on AUC(0-inf) and C(max) is unknown. The objectives of this investigation were to assess the ability of gastrointestinal simulation software to predict the oral absorption of the BCS class I drugs propranolol and metoprolol and the BCS class III drugs cimetidine, atenolol, and amoxicillin, and to perform in silico bioequivalence studies to assess the feasibility of extending biowaivers to BCS class III drugs. The drug absorption from the gastrointestinal tract was predicted using physicochemical and pharmacokinetic properties of test drugs provided by GastroPlus (version 6.0). Virtual trials with a 200 mL dose volume at different drug release rates (T(85%) = 15 to 180 min) were performed to predict the oral absorption (C(max) and AUC(0-inf)) of the above drugs. Both BCS class I drugs satisfied bioequivalence with regard to the release rates up to 120 min. The results with BCS class III drugs demonstrated bioequivalence using the prolonged release rate, T(85%) = 45 or 60 min, indicating that the dissolution standard for bioequivalence is dependent on the intestinal membrane permeability and permeability profile throughout the gastrointestinal tract. The results of GastroPlus simulations indicate that the dissolution rate of BCS class III drugs could be prolonged to the point where dissolution, rather than permeability, would control the overall absorption. For BCS class III drugs with intestinal absorption patterns similar to those of cimetidine, atenolol or amoxicillin, the dissolution criteria for extension of biowaivers to BCS class III drugs warrants further investigation.

Published

2010

49. Oral absorption of phytosterols and emulsified phytosterols by Sprague-Dawley rats

Author

David Kritchevsky, Yasuhiro Tsume, Bryan Delaney, Wade N. Schmelzer, Steve McCurry, Luke A. Stevens, Jae Seung Kim, John M. Hilfinger, Gordon L. Amidon, and James Haworth

Subjects

food.ingredient, Endocrinology, Diabetes and Metabolism, Campesterol, Clinical Biochemistry, Biochemistry, Soybean oil, Absorption, Rats, Sprague-Dawley, chemistry.chemical_compound, food, Blood serum, Animals, Molecular Biology, Chromatography, High Pressure Liquid, Micelles, Mouth, Nutrition and Dietetics, Chromatography, Stigmasterol, beta-Sitosterol, Esterification, Cholesterol, Phytosterol, Phytosterols, Water, Sitosterols, Diet, Rats, Bioavailability, Kinetics, Solubility, chemistry, Phosphatidylcholines, Emulsions

Abstract

Clinical studies have demonstrated that consumption of phytosterol esters in lipid-based foods decreases serum concentrations of total and LDL cholesterol. These substances represent minimal potential for adverse effects when consumed orally because of their low bioavailability. However, some studies have reported estrogenic and other effects in laboratory animals treated parenterally with phytosterols, demonstrating that these substances may have the potential to cause adverse effects if absorbed. Water-soluble phytosterols have been prepared by formulation with emulsifiers to expand delivery options to include non-lipid-based foods. However, emulsifiers are used as excipients in the formulation of lipophilic pharmaceuticals to increase solubility, thereby increasing their absorption. Therefore, oral consumption of emulsified water-soluble phytosterols could potentially increase their absorption. In the current study, absorption of phytosterols prepared as water-soluble emulsified micelles with two different food-grade emulsifiers was evaluated in Sprague-Dawley rats and compared with absorption of non-micellar free phytosterols and esterified phytosterol mixtures dissolved in a lipophilic vehicle (soybean oil). Rats were dosed via gavage with 42 mg/kg of formulated phytosterol preparations. Blood was collected at 8, 16, 24, and 32 hours, extracted with hexane, derivatized with benzoyl chloride, and analyzed by high-performance liquid chromatography to determine concentrations of beta-sitosterol, and campesterol. Plasma concentrations and AUC(0-32 hours) [microg/mL/h] of beta-sitosterol and campesterol were lower in plasma obtained from rats treated with emulsified phytosterol preparations than in animals treated with free phytosterols dissolved in soybean oil. Because the pharmacokinetic profile of water-soluble phytosterols is similar to that of phytosterols administered in a lipid vehicle, the safety profile is likely to be the same as that of phytosterols and phytosterol esters in currently used applications.

Published

2004

50. Gastrointestinal Motility and Luminal pH Influence in Vivo Dissolution and Systemic Absorption of Drug Product in Human Gastrointestinal Tract Under Fed and Fasted Conditions

Author

Duxin Sun, Bo Wen, Barry E. Bleske, Ann F. Fioritto, Yasuhiro Tsume, Jeffery Wysocki, William L. Hasler, Allen Lee, Alex Yu, Joseph Dickens, Kerby Shedden, Jason Baker, Gordon L. Amidon, and Mark J. Koenigsknecht

Subjects

medicine.anatomical_structure, Hepatology, In vivo, Chemistry, Human gastrointestinal tract, Gastroenterology, medicine, Drug product, Systemic absorption, Motility, Pharmacology, Dissolution

Published

2017