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8. Synthesis of C labeled C with higher specific radioactivity.

Author

Tadai, T., Akiyama, K., Aoshima, H., Ibuki, R., and Kubuki, S.

Subjects
CARBON isotopes, RADIOACTIVITY, QUENCHING (Chemistry), LIQUID scintillation counting, ELECTRIC furnaces
Abstract

In this paper, we report the production of C[C] with the highest specific radioactivity to date by improving of previously reported method. To avoid the loss of C, the porous carbon after adsorbing C labeled furan resin was sintered by 'Baking' method instead of heating at 1,000 °C in the electric furnace. As a result of this improvement, the specific radioactivity of the produced C[C] was found to be 0.958 MBq/mg (18.7 mCi/mmol). This is the highest specific radioactivity among those reported to date. [ABSTRACT FROM AUTHOR]

Published
2015
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14. Effect of Lipid Composition on the Interaction of Liposomes with THP-1-Derived Macrophages.

Author

Ibuki R, Tokui T, Kuriyama M, Hosoda K, Tomoda H, and Sakai-Kato K

Subjects
Membrane Fluidity, Macrophages metabolism, Liposomes, Cholesterol
Abstract

Recently, liposomal formulations that target macrophages have been used to treat lung diseases. However, the detailed mechanism of the cellular uptake must be elucidated to identify a formulation with excellent cellular uptake efficiency to treat non-tuberculous mycobacterial lung disease. We studied the effect of lipid composition on the cellular uptake of 1,2-dipalmitoyl-sn-glycero-3-phosphocholine (DPPC)/cholesterol (Chol) liposomes with a size of approximately 200 nm into THP-1-derived macrophages. The amount of DPPC/Chol liposomes (80/20 mol%) was greater than that of DPPC/Chol (60/40 mol%) and DPPC/Chol (67/33 mol%) liposomes. The anisotropy of 1,6-diphenyl-1,3,5-hexatriene indicated that the membrane fluidity of the DPPC/Chol (80/20 mol%) liposomes was higher than that of the other two liposomes. DPPC/Chol (80/20 mol%) and DPPC/Chol (67/33 mol%) liposomes were taken up via clathrin- and caveolae-mediated endocytosis and phagocytosis. However, proteins involved in cellular uptake through ligand-receptor interactions were adsorbed to a greater extent on DPPC/Chol (80/20 mol%) liposomes than on DPPC/Chol (67/33 mol%) liposomes. Pretreatment of cells with antibodies against the low-density lipoprotein receptor and scavenger receptor type B1 largely inhibited the uptake efficiency of DPPC/Chol (80/20 mol%) liposomes. Our results indicate that the membrane fluidity of DPPC/Chol liposomes, which is controlled by the Chol ratio, is an important factor in controlling protein adsorption and the subsequent uptake efficiency of liposomes.

Published
2024
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15. Potential of Fairy Chemicals as Functional Cosmetic Ingredients: Effect of 2-Aza-8-Oxohypoxanthine on Skin Lightness.

Author

Aoshima H, Ito S, Ibuki R, and Kawagishi H

Subjects
Cyclooxygenase 2 genetics, Humans, Hypoxanthines metabolism, Skin metabolism, Cosmetics
Abstract

Among the "fairy chemicals" involved in forming the natural phenomenon of "fairy rings," we focused on 2-aza-8-oxohypoxanthine (AOH) as a candidate functional cosmetic ingredient. In previous studies, AOH was confirmed to be safe for use on human skin, and no adverse reactions were observed in any of the safety studies. In this study, we report the results of a clinical trial using a lotion containing AOH. Our analysis using the L* value for indices of skin lightness indicated that the AOH application significantly increased the L* value after 8 weeks. Since a previous DNA microarray study using normal human epidermal cells showed that AOH suppressed the expression of a group of genes that induce inflammatory cytokines (prostaglandin E synthase, prostaglandin-endoperoxide synthase 2 [cyclooxygenase-2], and interleukin-18), our results suggest that the AOH-induced suppression of inflammatory factors results in skin lightening.

Published
2022
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16. Development of novel sustained-release system, disintegration-controlled matrix tablet (DCMT) with solid dispersion granules of nilvadipine (II): in vivo evaluation.

Author

Tanaka N, Imai K, Okimoto K, Ueda S, Tokunaga Y, Ibuki R, Higaki K, and Kimura T

Subjects
Administration, Oral, Animals, Biological Availability, Calcium Channel Blockers chemistry, Calcium Channel Blockers pharmacokinetics, Chemistry, Pharmaceutical, Dogs, Hypromellose Derivatives, Intestinal Absorption, Male, Methylcellulose analogs & derivatives, Methylcellulose chemistry, Nifedipine administration & dosage, Nifedipine chemistry, Nifedipine pharmacokinetics, Solubility, Soybean Oil chemistry, Tablets, Enteric-Coated, Water chemistry, Calcium Channel Blockers administration & dosage, Delayed-Action Preparations, Nifedipine analogs & derivatives
Abstract

A novel sustained-release (SR) system, disintegration-controlled matrix tablet (DCMT), was developed for poorly water-soluble drugs. DCMT, consisting of wax and solid dispersion (SD) granules containing a disintegrant, could control the release of nilvadipine (NiD), a model compound, by its disintegration. In the present study, two DCMTs (DCMT-1 and DCMT-2) with different release rates of NiD were orally administered to beagle dogs, and in vivo absorption of NiD from DCMTs was compared with that from immediate-release (IR) tablets. DCMTs successfully sustained the absorption of NiD longer than IR tablets, while they did not decrease the bioavailability of NiD. DCMT-2, providing the slower release of NiD than DCMT-1, prolonged the absorption longer than DCMT-1. In vivo absorption profiles of NiD from DCMTs were significantly correlated with in vitro release profiles, suggesting that the release property from DCMTs would maintain regardless of the change in physiological condition through the gastrointestinal tract. Furthermore, the food intake did not affect the absorption of NiD after oral administration of DCMT-2. The present results strongly indicate that the DCMT system would be a promising SR system, which could improve the solubility and sustain the absorption of poorly water-soluble drugs.

Published
2006
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17. Development of novel sustained-release system, disintegration-controlled matrix tablet (DCMT) with solid dispersion granules of nilvadipine.

Author

Tanaka N, Imai K, Okimoto K, Ueda S, Tokunaga Y, Ohike A, Ibuki R, Higaki K, and Kimura T

Subjects
Calcium Channel Blockers pharmacokinetics, Chemistry, Pharmaceutical, Delayed-Action Preparations, Drug Compounding, Excipients, Hydrogen-Ion Concentration, Kinetics, Nifedipine administration & dosage, Nifedipine pharmacokinetics, Particle Size, Powders, Solubility, Soybean Oil, Tablets, Waxes, Calcium Channel Blockers administration & dosage, Nifedipine analogs & derivatives
Abstract

The goal of this study is to develop a novel sustained-release (SR) system for poorly water-soluble drugs by applying solid dispersion (SD) technique for improving the solubility. The developed SR system, disintegration-controlled matrix tablet (DCMT), consists of hydrogenated soybean oil (HSO) as wax and SD granules containing low-substituted hydroxypropylcellulose (L-HPC) as a disintegrant. In this study, nilvadipine (NiD) was chosen as a model compound. Sustained-release profiles of NiD from DCMT were identically controlled in several dissolution mediums in spite of varying pH and agitation speed. The release of NiD from DCMT was sustained more effectively by increasing the amount of wax or by decreasing the amount of disintegrant, and supersaturation of NiD was achieved without any re-crystallization in dissolution medium. The release rate of NiD from DCMT was controlled by the disintegration rate of tablet. The release profile of NiD was described by the Hixson-Crowell's model better than zero-order kinetics, first-order kinetics and Higuchi's model, which supports that the release of NiD from DCMT is regulated by the disintegration of the tablet. From this study, it was clarified that DCMT was one of the promising SR systems applying SD for the poorly water-soluble drugs.

Published
2005
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18. Formulation development of inhalation powders for FK888 using the E-haler to improve the inhalation performance at a high dose, and its absorption in healthy volunteers.

Author

Nakate T, Yoshida H, Ohike A, Tokunaga Y, Ibuki R, and Kawashima Y

Subjects
Absorption drug effects, Absorption physiology, Administration, Inhalation, Adult, Chemistry, Pharmaceutical, Humans, Lung drug effects, Lung metabolism, Male, Powders, Dipeptides administration & dosage, Dipeptides chemistry, Indoles administration & dosage, Indoles chemistry, Metered Dose Inhalers standards
Abstract

FK888 is a candidate selective NK1 receptor antagonist, and it exhibits poor absorption from the gastrointestinal tract in healthy volunteers. In a previous study, the optimized dry powder inhaler (DPI) formulation with carrier lactose using the Spinhaler was developed, although the maximum dose per capsule was only 5mg because the fine particle fraction (FPF) was reduced at doses over 5mg. The objective of this study was to develop an optimized DPI formulation for higher doses, such as 40 mg, with proportional systemic absorption. The Spinhaler and E-haler were used as the inhalation devices, and the in vitro deposition was evaluated using a multistage cascade impactor at different flow rates (28.3 and 60 l/min). When hydroxypropyl methylcellulose (HPMC) capsules were used as the container, and spherical soft agglomerates of fine FK888 particles (soft pellets) and the E-haler were used, the fraction of particles emitted from the inhalation system (Em) was significantly improved, to over 80% of the nominal dose, and no significant difference was found between the airflow rates (84.3+/-2.3% for 28.3 l/min, 88.1+/-3.6% for 60 l/min). It was also found that the E-haler was an extremely suitable device for obtaining the higher respirable particle percentage of emitted particles (RP) in the 40 mg formulation with the soft pellets contained in HPMC capsules (35.0+/-1.8% for 28.3 l/min and 42.5+/-3.5% for 60 l/min), compared with the Spinhaler (13.8+/-3.0% for 28.3 l/min and 28.9+/-1.0% for 60 l/min). Using the formulations with the E-haler, proportional systemic absorption was achieved up to 40 mg FK888 in healthy volunteers (62.91+/-27.58, 103.70+/-40.19 and 254.79+/-85.01 ngh/ml as AUCs for 10, 20 and 40 mg FK888, respectively; R(2)=0.9641). It is also expected that the E-haler will act as an efficient device when a higher dose, such as 40 mg, is required in clinical situations.

Published
2005
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19. Applicability of (SBE)7m-beta-CD in controlled-porosity osmotic pump tablets (OPTs).

Author

Okimoto K, Tokunaga Y, Ibuki R, Irie T, Uekama K, Rajewski RA, and Stella VJ

Subjects
Adjuvants, Pharmaceutic chemistry, Chemistry, Pharmaceutical methods, Delayed-Action Preparations chemistry, Solubility, beta-Cyclodextrins chemistry, Delayed-Action Preparations pharmacokinetics, Osmosis, Porosity, Tablets, beta-Cyclodextrins pharmacokinetics
Abstract

The purpose of this study was to investigate the general application of a controlled-porosity osmotic pump tablet (OPT) utilizing (SBE)7m-beta-CD as both a solubilizer and an osmotic agent for drugs with varying physical properties. OPTs utilizing (SBE)7m-beta-CD were prepared for five poorly soluble and two highly water-soluble drugs. The Japanese Pharmacopoeia dissolution method was used to study the drug and (SBE)7m-beta-CD release from the OPTs. The drug concentration in the OPT core after the OPT was placed in the release medium for two hours was assayed gravimetrically and by HPLC. An appropriate composition ratio (ACR) of (SBE)7m-beta-CD to drug at which drug release from the OPT was complete and pH-independent within the physiological pH range of the GI tract was determined for each drug. The ACR values correlate to the drug concentration in the OPT core when the OPTs were placed in the release medium for two hours. The release profiles of prednisolone (a poorly water-soluble drug) and sodium chloride (a water-soluble compound) from the OPTs were almost the same as that of (SBE)7m-beta-CD. Also, the release rate of each drug per unit membrane surface area from the OPTs was similar, regardless of the differences in drug solubility. The present results confirmed that (SBE)7m-beta-CD serves as both a solubility modulator and as an osmotic pumping agent for OPTs, from which the release rate of both water-soluble and poorly water-soluble drugs can be controlled., (copyright 2004 Elsevier B.V.)

Published
2004
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20. Effect of experimental acute renal and hepatic failure on absorption of tacrolimus in rat small intestine.

Author

Tamura S, Ohike A, Tokunaga Y, Ibuki R, Amidon GL, Sezaki H, and Yamashita S

Subjects
Animals, Male, Rats, Rats, Wistar, Acute Kidney Injury metabolism, Intestinal Absorption physiology, Intestine, Small metabolism, Liver Failure, Acute metabolism, Tacrolimus metabolism
Abstract

The objective of this study is to evaluate the effect of acute renal or hepatic failure on the intestinal absorption of tacrolimus. Simultaneous perfusion study in rat small intestine revealed that the extent of absorption into blood vessels was decreased in the jejunum and the ileum of rat of acute renal failure due to the decrease in the uptake of tacrolimus into enterocytes. In contrast, there observed no significant changes in tacrolimus absorption in rat of acute hepatic failure. Since it has been reported that tacrolimus absorption is regulated mainly by Cytochrome P-450 (CYP) mediated metabolism in the jejunum, but by P-glycoprotein (P-gp) mediated efflux in the ileum, these factors might contribute to the changes in intestinal absorption of tacrolimus in rat of acute renal failure. Enzyme inhibitor, ketoconazole, was co-perfused with tacrolimus to specify the effect of CYP and P-gp. However, since ketoconazole failed to recover the permeability in the jejunum and ileum of rat of acute renal failure, it is considered that the changes in CYP or P-gp functions might not be involved in the decreased uptake of tacrolimus. This type of kinetic study in rats should be valuable to identify the precise mechanisms of drug absorption and the effects of various diseases on it, such as acute renal or hepatic failure.

Published
2004
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21. Formulation development of inhalation powders for FK888 with carrier lactose using Spinhaler and its absorption in healthy volunteers.

Author

Nakate T, Yoshida H, Ohike A, Tokunaga Y, Ibuki R, and Kawashima Y

Subjects
Absorption drug effects, Absorption physiology, Administration, Inhalation, Adult, Chemistry, Pharmaceutical, Dipeptides pharmacokinetics, Dose-Response Relationship, Drug, Drug Carriers pharmacokinetics, Humans, Indoles pharmacokinetics, Lactose pharmacokinetics, Male, Powders, Dipeptides administration & dosage, Drug Carriers administration & dosage, Indoles administration & dosage, Lactose administration & dosage, Metered Dose Inhalers statistics & numerical data
Abstract

(4R)-4-Hydroxy-l-[(l-methyl-lH-indol-3-yl)carbonyl]-L-prolyl-N-benzyl-N-methyl-3-(2-naphthyl)-L-alaninamide (FK888) is a candidate selective NK1 receptor antagonist, and it exhibits poor absorption from the gastrointestinal (GI) tract in healthy volunteers. The objective of this study was to develop an optimized DPI formulation with carrier lactose using a Spinhaler, and thereby improve the systemic absorption of FK888. The fine particles of FK888 were blended with various carrier lactoses, and in vitro deposition properties were investigated using a twin impinger. The mixture using 100 M and 325 M lactoses [Sieved lactoses (SLs)] exhibited a higher emitted dose (Em) than 200 M, 450 M and micronized lactoses [Milled lactoses (MLs)]. The flowability of carrier lactose had an influence on the Em. On the other hand, the respirable particle (RP) fraction in the formulations with MLs was much higher than that of SLs, in spite of the blended ratios of lactose. It was also observed that the mixture of 325 M with the micronized lactose particles had the same RP as 200 M, although the 325 M alone had a low RP. Considering the Em and RP obtained, we chose 200 M for FK888 dry powder inhaler (DPI). The proportional absorption was found up to the 12.5% of the FK888 ratio (5 mg as unit dose) for the Cmax and AUC in healthy volunteers. In conclusion, 200 M, which has fine lactose particles and a better flowability than other MLs, is an extremely suitable carrier for maximizing the fine particle dose as far as FK888 is concerned. Furthermore, an improvement in the systemic absorption of FK888 was achieved using the dry powder formulations., (Coyright 2004 Elsevier B.V.)

Published
2004
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22. Establishment of new preparation method for solid dispersion formulation of tacrolimus.

Author

Yamashita K, Nakate T, Okimoto K, Ohike A, Tokunaga Y, Ibuki R, Higaki K, and Kimura T

Subjects
Administration, Oral, Analysis of Variance, Animals, Area Under Curve, Calorimetry, Differential Scanning instrumentation, Calorimetry, Differential Scanning methods, Chemistry, Pharmaceutical, Chromatography, High Pressure Liquid methods, Delayed-Action Preparations pharmacokinetics, Dogs, Drug Carriers chemistry, Drug Carriers pharmacology, Hemostatics chemistry, Hemostatics pharmacology, Hypromellose Derivatives, Immunosuppressive Agents pharmacokinetics, Macaca fascicularis, Male, Methylcellulose analogs & derivatives, Methylcellulose chemistry, Methylcellulose pharmacology, Methylene Chloride chemistry, Methylene Chloride pharmacology, Microscopy, Electron, Scanning, Polymers chemistry, Polymers pharmacology, Solubility, Tacrolimus blood, Tacrolimus pharmacokinetics, Temperature, Time Factors, X-Ray Diffraction instrumentation, X-Ray Diffraction methods, Delayed-Action Preparations chemistry, Immunosuppressive Agents chemistry, Tacrolimus chemistry
Abstract

The aim of this study was to establish a new preparation method for solid dispersion formulation (SDF) of tacrolimus, a poorly water-soluble drug, without dichloromethane, because no use of dichloromethane is recommended by ICH harmonized tripartite guideline. To select the appropriate carrier, three different SDFs with polyethylene glycol 6000 (PEG 6000), polyvinylpyrrolidone (PVP) and hydroxypropylmethylcellulose (HPMC) were prepared by the conventional solvent method, in which tacrolimus and the carrier were completely dissolved in the mixture of dichloromethane and ethanol. Powder X-ray diffraction (XRD) and differential scanning calorimetry (DSC) patterns indicated that tacrolimus exists in an amorphous state in all three SDFs. The supersaturated dissolution profiles of tacrolimus were observed in all SDFs, and the highest level of supersaturation for tacrolimus was obtained and maintained for 24h from SDF with HPMC. On the other hand, the supersaturated level from SDF with PEG 6000 or PVP decreased rapidly. The in vivo oral absorption study in dogs showed that bioavailability of tacrolimus from SDF with HPMC was remarkably improved compared with the crystalline powder. It was clarified that HPMC is the most appropriate carrier for SDF of tacrolimus. Then, SDF of tacrolimus was prepared by the new method, which allows us to make SDF of tacrolimus by swelling HPMC with ethanol, in which tacrolimus was completely dissolved. This new method does not need dichloromethane. The physicochemical properties of SDF with HPMC prepared by the new method were the same as those of SDF prepared by the conventional solvent method. Furthermore, SDF with HPMC prepared by the new method was still stable after stored at 40 degrees C for 3 months. The pharmacokinetic parameters after oral administration in monkeys showed no significant difference (P>0.01) between SDFs with HPMC prepared by the two methods. In conclusion, we have established the new preparation method for SDF of tacrolimus with HPMC and the new method makes it possible to prepare SDF of tacroliumus without dichloromethane.

Published
2003
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23. Comparison of the lung absorption of FK224 inhaled from a pressurized metered dose inhaler and a dry powder inhaler by healthy volunteers.

Author

Nakate T, Yoshida H, Ohike A, Tokunaga Y, Ibuki R, and Kawashima Y

Subjects
Administration, Inhalation, Adult, Dose-Response Relationship, Drug, Humans, Lung drug effects, Male, Metered Dose Inhalers, Middle Aged, Particle Size, Powders, Lung metabolism, Peptides, Cyclic administration & dosage, Peptides, Cyclic pharmacokinetics
Abstract

FK224 is a cyclopeptide drug with poor oral absorption due to proteolysis in the gastrointestinal tract. The objectives of this study were to investigate the absorption of FK224 from the lung in healthy volunteers, and compare the pharmacokinetic profiles of FK224 after inhalation from a pressurized metered dose inhaler (pMDI) and dry powder inhaler (DPI). The pMDI (Suspension type, 1 mg as FK224/puff) and DPI (4 mg and 10 mg as FK224/capsule, using Spinhaler as the device) were developed by formulating the same micronized particles of FK224 which were premixed with beta-cyclodextrin (beta-CyD) to improve the solubility of FK224. In the case of pMDI, 1, 4 or 8 mg was inhaled by the corresponding number of puffs with the pMDI. In addition, the in vitro drug delivery characteristics of the inhalers were evaluated using a multistage liquid impinger. In both inhalers, it was observed that FK224 could be absorbed into the systemic circulation from the lungs of the healthy volunteers, and the AUC and C(max) were proportionally increased depending on the emitted dose after inhalation. However, the pharmacokinetic (PK) parameters for DPI were significantly higher than that of pMDI, in spite of usage of the same fine particles for the formulations in both inhalers. Based on the distribution from the in vitro examination, the fine particle dose, which is defined as the dose region delivered as particles <3.8 microm, was calculated from the emitted dose inhaled by the healthy volunteers. It was found that the PK parameters for both inhalers were proportionally increased depending on the predicted fine particle dose regardless of the type of inhaler. This suggests that the absorption from the lung is influenced by the fine particle dose. We concluded that DPI is a suitable inhaler for FK224, and the alveolus, which is generally known as the site of action of the fine particles, is a possible absorptive site for FK224.

Published
2003
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24. The site-specific transport and metabolism of tacrolimus in rat small intestine.

Author

Tamura S, Tokunaga Y, Ibuki R, Amidon GL, Sezaki H, and Yamashita S

Subjects
ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism, Animals, Biological Transport, Caco-2 Cells, Humans, Intestinal Absorption, Male, Rats, Immunosuppressive Agents pharmacokinetics, Intestine, Small metabolism, Tacrolimus pharmacokinetics
Abstract

The objective of this study was to evaluate the absorption of tacrolimus by means of simultaneous perfusion of intestinal lumen and blood vessels in rats. In our previous report, the permeability of tacrolimus was found to be higher in the jejunum than in the ileum or colon, suggesting the site-dependent absorption after oral administration. However, in this article, simultaneous perfusion technique revealed that the extent of absorption into blood vessels was similar in the jejunum and the ileum regardless of the site difference in permeability as the absorption rate. In addition to the multidrug resistance-associated protein-mediated efflux, cytochrome P450 (P450)-mediated metabolism could be a possible mechanism to explain the inconsistencies in the site dependence of tacrolimus absorption. Two enzyme inhibitors, ketoconazole and midazolam, were coperfused in rat intestinal lumen with tacrolimus to specify the effect of P-gp and P450. In the jejunum, both inhibitors significantly enhanced the absorbed amount of tacrolimus, whereas the permeability was not affected. It was suggested that both inhibitors mainly suppress P450-mediated metabolism in the upper region of the intestine. In contrast, in the ileum, ketoconazole significantly enhanced both the absorbed amount and the permeability of tacrolimus. However, midazolam failed to enhance the absorption of tacrolimus, indicating the dominant role of P-glycoprotein (P-gp)-mediated efflux in the lower region. From these findings, it is concluded that the site-dependent differences in P-gp and/or P450 activity could be the prime cause of large intra- and interindividual variability in the oral absorption of tacrolimus.

Published
2003
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25. Improvement of pulmonary absorption of cyclopeptide FK224 in rats by co-formulating with beta-cyclodextrin.

Author

Nakate T, Yoshida H, Ohike A, Tokunaga Y, Ibuki R, and Kawashima Y

Subjects
Absorption, Administration, Intranasal, Administration, Oral, Animals, Area Under Curve, Biological Availability, Chemistry, Pharmaceutical, Injections, Subcutaneous, Kinins antagonists & inhibitors, Male, Particle Size, Peptides, Cyclic administration & dosage, Peptides, Cyclic chemistry, Pharmaceutical Solutions, Rats, Rats, Sprague-Dawley, Solubility, Substance P agonists, Suspensions, Time Factors, Cyclodextrins chemistry, Excipients chemistry, Lung metabolism, Peptides, Cyclic pharmacokinetics, beta-Cyclodextrins
Abstract

FK224 is a cyclopeptide drug with a low aqueous solubility. Following oral administration to rats, poor absorption was observed due to proteolysis in the gastrointestinal tract. The objective of this study was to investigate the effect of the pulmonary route on the systemic absorption of FK224 in comparison with other administration routes, and to determine the bioavailability (BA) of FK224 following pulmonary administration in rats using various dosage forms. From absorption studies on the Polyethylene Glycol 400 solution given by various routes (intranasal, subcutaneous, intratracheal and intravenous as reference), it was shown that pulmonary administration was a potentially attractive route for FK224. In the pulmonary absorption studies, after administration of the aqueous suspension, the BA was reduced to 2.7% compared with 16.8% for the solution. However, beta-cyclodextrin (beta-CyD) was found to be an effective additive as far as improving the solubility of FK224 was concerned. The BA of the aqueous suspension containing beta-CyD was increased to 19.2%. Pressurized metered dose inhalers were prepared by formulating beta-CyD with various molar ratios of 1:0, 1:1 and 1:7 (FK224/beta-CyD), and the resulting BAs were 4.3%, 29.0% and 91.2%, respectively. It was observed that both the C(max) and AUC of FK224 were increased as the amount of beta-CyD increased. The plasma profiles showed sustained absorption. In conclusion, we have seen that the lung is a suitable route for absorption of FK224, and beta-CyD is an extremely effective additive as far as improving the pulmonary absorption of FK224 is concerned. beta-CyD or derivatives with various degrees of aqueous solubility are potential drug carriers for controlling pulmonary absorption., (Copyright 2002 Elsevier Science B.V.)

Published
2003
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26. Tacrolimus is a class II low-solubility high-permeability drug: the effect of P-glycoprotein efflux on regional permeability of tacrolimus in rats.

Author

Tamura S, Ohike A, Ibuki R, Amidon GL, and Yamashita S

Subjects
ATP Binding Cassette Transporter, Subfamily B, Member 1 chemistry, Animals, Biological Availability, Caco-2 Cells, Chromatography, High Pressure Liquid, Humans, Immunosuppressive Agents pharmacokinetics, Intestinal Absorption, Jejunum drug effects, Jejunum metabolism, Male, Models, Biological, Perfusion, Rats, Solubility, Surface-Active Agents chemistry, Surface-Active Agents pharmacology, Tacrolimus pharmacokinetics, Water metabolism, Immunosuppressive Agents chemistry, Tacrolimus chemistry
Abstract

The objective of this study is to investigate the role of P-glycoprotein (P-gp), a membrane efflux pump associated with multidrug resistance (MDR) and a known substrate for tacrolimus, in determining the regional intestinal permeability of tacrolimus in rats. Thus, isolated segments of rat jejunum, ileum, or colon were perfused with tacrolimus solutions containing polyethoxylated hydrogenated castor oil 60 surfactant, and with or without verapamil, a P-gp substrate used to reverse the MDR phenotype. The results indicated that the intrinsic permeability of tacrolimus in the jejunum, calculated on the basis of the concentration of non-micellized free tacrolimus, was quite high ( approximately 1.4 x 10(-4) cm/s). The apparent permeability (P(app)) in the jejunum was unaffected by the presence of verapamil; however, the P(app) in the ileum and the colon increased significantly in the presence of verapamil and were similar to the values observed in the jejunum. The results suggest that systemic absorption of tacrolimus from the gastrointestinal tract could be significantly affected by P-gp efflux mechanisms. It is also possible that differences in P-gp function at various intestinal sites in a subject or at a given intestinal site in various subjects could lead to large intra- and interindividual variability in bioavailability of tacrolimus following oral administration., (Copyright 2002 Wiley-Liss, Inc. and the American Pharmaceutical Association .)

Published
2002
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27. [Labial adhesion in a reproductive woman with difficulties of sexual intercourse and urination: a case report].

Author

Uei T, Katou Y, Shimizu N, Yamanaka H, Seki M, and Ibuki R

Subjects
Adult, Female, Humans, Inflammation complications, Time Factors, Tissue Adhesions etiology, Tissue Adhesions surgery, Treatment Outcome, Vulvar Diseases surgery, Coitus, Sexual Dysfunction, Physiological etiology, Urination Disorders etiology, Vulvar Diseases etiology
Abstract

A 27-year-old female patient consulted us with chief complaints of difficulties of sexual intercourse and urination. On examination, the labia was found to be extensively fused at the midline, with a pinhole opening. We diagnosed it as labial adhesion. We operated on it under lumbar anesthesia. Four months after the operation, there were no symptoms of recurrence. Labial adhesion is thought to be caused by inflammation, lack of sexual activity and estrogen deficiency. It is not uncommon in children and post-menopausal women, but is extremely rare in reproductive women.

Published
2000

28. Effect of truncal vagotomy on gallbladder bile kinetics in conscious dogs.

Author

Muramatsu S, Sonobe K, Tohara K, Tanaka T, Mizumoto A, Ibuki R, Suzuki H, and Itoh Z

Subjects
Animals, Consciousness, Dogs, Fasting, Kinetics, Postprandial Period, Pylorus surgery, Vagus Nerve physiology, Vagus Nerve surgery, Bile metabolism, Gallbladder innervation, Gallbladder metabolism, Gallbladder Emptying physiology, Vagotomy
Abstract

Previous studies on the effects of vagotomy on gallbladder (GB) motility have yielded conflicting results. The aim of this study was to evaluate the effects of vagotomy on GB motility and bile kinetics using a new method. Twelve dogs were divided into two groups of six (control and pyloroplasty) and, 4 weeks later, underwent truncal vagotomy. A catheter secured in the GB fundus was used to monitor GB volume. After injecting polyethylene glycol (PEG) into the GB, combined measurements of GB volume and PEG concentration enabled GB emptying and bile kinetics to be estimated. Seven and five of the 12 vagotomized dogs were classified as having large and normal fasting GB volumes, respectively. Postprandial GB emptying was impaired when the fasting GB volume was enlarged. In the fasting state, bile kinetics of vagotomized dogs were significantly smaller than the control values. The emptying ability of the GB of vagotomized dogs with large fasting GB volumes was reduced considerably both in the postprandial and the fasting states. Such retention of bile in the GB after vagotomy may facilitate cholesterol crystal nucleation and stone growth.

Published
1999
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29. Design and evaluation of an osmotic pump tablet (OPT) for chlorpromazine using (SBE)7m-beta-CD.

Author

Okimoto K, Ohike A, Ibuki R, Aoki O, Ohnishi N, Irie T, Uekama K, Rajewski RA, and Stella VJ

Subjects
2-Hydroxypropyl-beta-cyclodextrin, Absorption, Animals, Chlorpromazine administration & dosage, Cyclodextrins administration & dosage, Delayed-Action Preparations, Dogs, Dopamine Antagonists administration & dosage, Drug Design, Fructose administration & dosage, Fructose chemistry, Fructose pharmacokinetics, Hydrogen-Ion Concentration, Lactose administration & dosage, Lactose chemistry, Lactose pharmacokinetics, Male, Osmotic Pressure, Solubility, Tablets, Chlorpromazine chemistry, Chlorpromazine pharmacokinetics, Cyclodextrins chemistry, Cyclodextrins pharmacokinetics, Dopamine Antagonists chemistry, Dopamine Antagonists pharmacokinetics, beta-Cyclodextrins
Abstract

Purpose: The purpose of this study was to develop a controlled-porosity osmotic pump tablet (OPT) which exhibits pH-independent release profiles for a basic drug using a sulfobutyl ether-beta-cyclodextrin, (SBE)7m-beta-CD, which acts as both a solubilizer and as an osmotic agent., Methods: Chlorpromazine free base (CLP) was chosen as a model drug for this study. The release of CLP from osmotic pump tablets was studied in vitro. In vivo absorption of CLP from the OPT was evaluated in male beagle dogs., Results: The CLP release profile from an OPT prepared from a core tablet composed of a 1:10 molar ratio of CLP to (SBE)7m-beta-CD was pH-independent, and was controlled by modulating the membrane thickness of the OPT. Another cyclodextrin, hydroxypropyl-beta-cyclodextrin (HP-beta-CD), and a sugar mixture of lactose and fructose resulted in pH-dependent release at the same molar ratio. An in vivo absorption study in dogs with an OPT containing (SBE)7m-beta-CD correlated very well with the in vitro release profiles using the Japanese Pharmacopoeia dissolution method., Conclusions: In addition to serving as a solubilizer and osmotic agent, (SBE)7m-beta-CD can also serve as the controlling agent for pH independent release of CLP from OPTs. This system successfully modified the in vivo input rate of CLP without compromising oral bioavailability.

Published
1999
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30. Long-term observations of uterine contractions in nonpregnant dogs.

Author

Ibuki R, Haga N, Muramatsu S, Mizumoto A, and Itoh Z

Subjects
Adrenergic Agonists pharmacology, Animals, Cholinergic Antagonists pharmacology, Dinoprost pharmacology, Dogs, Estrogens blood, Estrus drug effects, Estrus physiology, Female, Oxytocin pharmacology, Progesterone blood, Stomach physiology, Transducers, Pressure, Vagina cytology, Vagina physiology, Uterine Contraction physiology
Abstract

Uterine contractile activity in nonpregnant conscious dogs was investigated based on 2- to 6-mo-long continuous recording by means of a chronically implanted force transducer. We found that nonpregnant uterine contractile activity could be classified into six major patterns: sporadic contractions, weak and strong tonic contractions, weak and strong phasic contractions, and phasic contraction bursts. The contractile patterns during proestrus and estrus were the most active, with strong phasic and tonic contractions and phasic contraction bursts. The phasic and tonic contractions were inhibited dose-dependently by a beta 2 adrenergic agonist, ritodrine, and reproduced by an alpha 2 adrenergic agonist, clonidine. In contrast, the cholinergic inhibitors atropine and hexamethonium did not affect the spontaneous occurrence of these contractions, although bethanechol evoked uterine contractions. Oxytocin and prostaglandin F2 alpha-induced contractions were phasic during estrus, whereas they showed tonic increases with phasic contractions during proestrus, diestrus, and anestrus, and these contractions did not resemble the spontaneous contractions. In conclusion, the nonpregnant uterus contracts continuously in harmony with the estrous cycle phases, and its contractile activity is enhanced by alpha adrenergic receptors and inhibited by beta 2 adrenergic receptors.

Published
1997
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32. Development of a novel drug delivery system, time-controlled explosion system (TES). IV. In vivo drug release behavior.

Author

Ueda S, Ibuki R, Kawamura A, Murata S, Takahashi T, Kimura S, and Hata T

Subjects
Animals, Cellulose analogs & derivatives, Dogs, Excipients, Intestinal Absorption, Liver metabolism, Male, Membranes, Artificial, Metoprolol administration & dosage, Metoprolol pharmacokinetics, Delayed-Action Preparations
Abstract

Time-Controlled Explosion System (TES) has the time-controlled drug release property with a pre-designed lag time. The drug release from the system is initiated by destruction of the membrane. In this study, metoprolol tartrate was used as a model drug. After five types of TES with different in vitro lag times were orally administrated to dogs, plasma metoprolol concentration was monitored. There existed a good correlation between in vitro and in vivo lag time, while the extent of absorbed metoprolol decreased with prolongation of lag time. Next, the in vivo drug release behavior was directly investigated using five different colored TES with a lag time of two hours. Each TES was consecutively administrated to the fasted dogs at predetermined intervals. The amount of metoprolol released was monitored by recovering the administered TES from the gastrointestinal trace. The in vivo release profile corresponded with the in vitro one. It is demonstrated that TES can release the drug in in vivo conditions similarly to in vitro. Based on these results, the decrease of the absorption is suggested to be caused by increased hepatic first-pass metabolism of the drug due to the retarded release rate with longer lag time.

Published
1994
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33. Nuclear factor I stimulates transcription of the adenovirus 12 E1A gene in a cell-free system.

Author

Koikeda S, Ibuki R, Sawada Y, Nagata K, Shibata H, Masamune Y, and Nakanishi Y

Subjects
Adenovirus Early Proteins, Animals, Base Sequence, Carcinoma, Ehrlich Tumor metabolism, Cell-Free System, DNA genetics, DNA-Binding Proteins metabolism, HeLa Cells, Molecular Sequence Data, NFI Transcription Factors, Nuclear Proteins, Oncogene Proteins, Viral metabolism, RNA analysis, Y-Box-Binding Protein 1, Adenoviridae genetics, CCAAT-Enhancer-Binding Proteins, DNA-Binding Proteins genetics, Genes, Viral, Oncogene Proteins, Viral genetics, Transcription Factors, Transcription, Genetic
Abstract

Binding to the cis-acting region of NF-I-like protein and/or NF-III-like protein was previously suggested to be responsible for the preferential stimulation of transcription from distal start-site of the adenovirus 12 E1A gene in a cell-free system. In this study, nuclear extracts of Ehrlich ascites tumor cells depleted of NF-I-like protein were found to lose activity to stimulate the E1A gene transcription. This activity was recovered when NF-I purified from HeLa cells with no contamination of NF-III was supplemented. It is thus evident that NF-I is involved in stimulating distal transcription of the adenovirus 12 E1A gene. Moreover, activities for both stimulating the E1A gene transcription and binding to a region recognized by NF-I did not apparently exist in nuclear extracts of a cell line expressing the adenovirus 12 E1A gene. These results suggest that transcription of the adenovirus 12 E1A gene may possibly be autoregulated at least in part through modulation of the activity of NF-I.

Published
1990
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