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101. Antipsychotics-Associated Serious Adverse Events in Children: An Analysis of the FAERS Database

Author

20283666, Kimura, Goji, Kadoyama, Kaori, Brown, J.B., Nakamura, Tsutomu, Miki, Ikuya, Nisiguchi, Kohshi, Sakaeda, Toshiyuki, Okuno, Yasushi, 20283666, Kimura, Goji, Kadoyama, Kaori, Brown, J.B., Nakamura, Tsutomu, Miki, Ikuya, Nisiguchi, Kohshi, Sakaeda, Toshiyuki, and Okuno, Yasushi

Abstract

Objective: The reports submitted to the US Food and Drug Administration (FDA) Adverse Event Reporting System (FAERS) from 1997 to 2011 were reviewed to assess serious adverse events induced by the administration of antipsychotics to children. Methods: Following pre-processing of FAERS data by elimination of duplicated records as well as adjustments to standardize drug names, reports involving haloperidol, olanzapine, quetiapine, clozapine, ziprasidone, risperidone, and aripiprazole were analyzed in children (age 0-12). Signals in the data that signified a drug-associated adverse event were detected via quantitative data mining algorithms. The algorithms applied to this study include the empirical Bayes geometric mean, the reporting odds ratio, the proportional reporting ratio, and the information component of a Bayesian confidence propagation neural network. Neuroleptic malignant syndrome (NMS), QT prolongation, leukopenia, and suicide attempt were focused on as serious adverse events. Results: In regard to NMS, the signal scores for haloperidol and aripiprazole were greater than for other antipsychotics. Significant signals of the QT prolongation adverse event were detected only for ziprasidone and risperidone. With respect to leukopenia, the association with clozapine was noteworthy. In the case of suicide attempt, signals for haloperidol, olanzapine, quetiapine, risperidone, and aripiprazole were detected. Conclusions: It was suggested that there is a level of diversity in the strength of the association between various first- and second-generation antipsychotics with associated serious adverse events, which possibly lead to fatal outcomes. We recommend that research be continued in order to gather a large variety and quantity of related information, and that both available and newly reported data be placed in the context of multiple medical viewpoints in order to lead to improved levels of care.

Published
2015

104. Oxaliplatin up-regulated the function and expression of P-glycoprotein/MDR1 in porcine kidney epithelial LLC-PK cells

Author

Kishi, Hisato, Kitada, Noriaki, Ohnishi, Noriaki, Sakaeda, Toshiyuki, Takara, Kohji, and Yokoyama, Teruyoshi

Subjects
urogenital system, oxaliplatin, polycyclic compounds, up-regulation, MDR1, LLC-PK, P-glycoprotein, physiological processes, neoplasms
Abstract

The purpose of this study was to clarify the effects of oxaliplatin on the function and expression of the multidrug efflux transporter P-glycoprotein/MDR1 in a porcine kidney epithelial cell line, LLC-PK, as a renal tubular epithelial model. LLC-PK cells were pretreated with or without oxaliplatin for 48 h, and the growth inhibitory effects of a MDR1 substrate, paclitaxel, and the transport of a MDR1 substrate, Rhodamine123, were assessed. The level of MDR1 mRNA and protein was also examined in the cells treated with or without oxaliplatin for 48 h using RT-PCR and immunoblotting. In the present study, the pretreatment with oxaliplatin tended to suppress the growth inhibitory effects of paclitaxel in LLC-PK cells, presumably by accelerating the functions of MDR1. In addition, the uptake of Rhodamine123 was reduced significantly by pretreatment with oxaliplatin, and the efflux of Rhodamine123 from LLC-PK cells was enhanced significantly. These accelerated functions were supported by the suppression of Rhodamine123 s transport by a representative MDR1 substrate/inhibitor, ciclosporin, at 10 µM. The exposure to oxaliplatin for 48 h resulted in an increase in the expression of MDR1 in LLC-PK cells. These findings were similar to those obtained with cisplatin, a nephrotoxic drug. In conclusion, the present findings suggested that transient exposure for 48 h to oxaliplatin caused the up-regulation of MDR1 function and expression in LLC-PK cells, as was the case for cisplatin., EXCLI Journal ; Vol. 5, 2006

Published
2006

105. Dissolving microneedles for enhanced local delivery of capsaicin to rat skin tissue.

Author

Ito, Yukako, Kobuchi, Shinji, Inoue, Genta, Kakumu, Eisaku, Aoki, Miki, Sakaeda, Toshiyuki, and Takada, Kanji

Subjects
THERAPEUTIC use of capsaicin, ANIMAL models in research, ANALGESICS, PHARMACOKINETICS, DRUG administration
Abstract

Capsaicin-loaded dissolving microneedles (DMNs) were prepared to investigate the analgesic effect of capsaicin on the skin. The dimensions of each microneedle (MN) were as follows: diameter of the basement, 17 mm; length, 500 μm; and width, 300 μm. The average capsaicin content in the DMNs loaded with a low and high dose of capsaicin was 8.8 ± 0.5 mg and 12.5 ± 0.4 mg. Almost all the capsaicin, 99.3 ± 4.1% and 99.7 ± 2.2% for low-dose and high-dose DMNs were released within 20 min. High amounts of capsaicin were recovered with 102.8 ± 0.1% of capsaicin after storage at 23 °C for 90 days. The pharmacological activity of capsaicin DMNs was compared to that of capsaicin cream as a positive control, by measuring the idiospasm of depilated rat skin. The time required to achieve 50% idiospasm suppression was 26.3 ± 1.9 min and 53.0 ± 2.3 min for low-dose and high-dose DMNs. A pharmacokinetic study showed high tissue capsaicin levels of 660.2 ± 120.6 and 1805.3 ± 218.1 μg/g wet weight for low-dose and high-dose DMNs at 5 min after administration. The results suggest that DMNs could exert a rapid local analgesic action on the skin. [ABSTRACT FROM PUBLISHER]

Published
2017
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109. Serum Lactate Dehydrogenase Levels as a Predictive Marker of Oxaliplatin-Induced Hypersensitivity Reactions in Japanese Patients with Advanced Colorectal Cancer

Author

Seki, Kyoko, primary, Tsuduki, Yasuo, additional, Ioroi, Takeshi, additional, Yamane, Michiko, additional, Yamauchi, Hiroko, additional, Shiraishi, Yukinari, additional, Ogawa, Tadaaki, additional, Nakata, Izumi, additional, Nishiguchi, Kohshi, additional, Matsubayashi, Teruhisa, additional, Takakubo, Yoshihide, additional, Yamamori, Motohiro, additional, Kuwahara, Akiko, additional, Okamura, Noboru, additional, and Sakaeda, Toshiyuki, additional

Published
2014
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111. Genetic Polymorphisms in SLC23A2 as Predictive Biomarkers of Severe Acute Toxicities after Treatment with a Definitive 5-Fluorouracil/Cisplatin-Based Chemoradiotherapy in Japanese Patients with Esophageal Squamous Cell Carcinoma

Author

Minegaki, Tetsuya, primary, Kuwahara, Akiko, additional, Yamamori, Motohiro, additional, Nakamura, Tsutomu, additional, Okuno, Tatsuya, additional, Miki, Ikuya, additional, Omatsu, Hideaki, additional, Tamura, Takao, additional, Hirai, Midori, additional, Azuma, Takeshi, additional, Sakaeda, Toshiyuki, additional, and Nishiguchi, Kohshi, additional

Published
2014
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112. Effects of S-2474, a novel nonsteroidal anti-inflammatory drug, on amyloid β protein-induced neuronal cell death

Author

Yagami, Tatsurou, Ueda, Keiichi, Asakura, Kenji, Sakaeda, Toshiyuki, Kuroda, Takayuki, Hata, Satoshi, Kambayashi, Yoshikazu, and Fujimoto, Masafumi

Subjects
Cerebral Cortex, Neurons, Amyloid beta-Peptides, Cell Death, Dose-Response Relationship, Drug, Anti-Inflammatory Agents, Non-Steroidal, Embryo, Mammalian, Cyclic S-Oxides, Rats, Rats, Sprague-Dawley, Thiazoles, Pregnancy, Papers, Animals, Female, Cells, Cultured
Abstract

1. The accumulation of amyloid beta protein (Abeta) in the brain is a characteristic feature of Alzheimer's disease (AD). Clinical trials of AD patients with nonsteroidal anti-inflammatory drugs (NSAIDs) indicate a clinical benefit. NSAIDs are presumed to act by suppressing inhibiting chronic inflammation in the brain of AD patients. 2. In the present study, we investigated effects of S-2474 on Abeta-induced cell death in primary cultures of rat cortical neurons. 3. S-2474 is a novel NSAID, which inhibits cyclo-oxygenase-2 (COX-2) and contains the di-tert-butylphenol antioxidant moiety. S-2474 significantly prevented neurons from Abeta(25 - 35)- and Abeta(1 - 40)-induced cell death. S-2474 ameliorated Abeta-induced apoptotic features such as the condensation of chromatin and the fragmentation of DNA completely. 4. Prior to cell death, Abeta(25 - 35) generated prostaglandin D(2) (PGD(2)) and free radicals from neurons. PGD(2) is a product of cyclo-oxygenase (COX), and caused neuronal cell death. 5. S-2474 significantly inhibited the Abeta(25 - 35)-induced generation of PGD(2) and free radicals. 6. The present cortical cultures contained little non-neuronal cells, indicating that S-2474 affected neuronal survival directly, but not indirectly via non-neuronal cells. Both an inhibitory effect of COX-2 and an antioxidant effect might contribute to the neuroprotective effects of S-2474. 7. In conclusion, S-2474 exhibits protective effects against neurotoxicity of Abeta. Furthermore, the present study suggests that S-2474 may possess therapeutic potential for AD via ameliorating degeneration in neurons as well as suppressing chronic inflammation in non-neuronal cells.

Published
2001

113. VEGF 936C>T is predictive of threshold retinopathy of prematurity in Japanese infants with a 30-week gestational age or less

Author

Yagi,Mariko, Yamamori,Motohiro, Morioka,Ichiro, Yokoyama,Naoki, Honda,Shigeru, Negi,Akira, Nakamura,Tsutomu, Okamura,Noboru, Okumura,Katsuhiko, Sakaeda,Toshiyuki, Matsuo,Masafumi, Yagi,Mariko, Yamamori,Motohiro, Morioka,Ichiro, Yokoyama,Naoki, Honda,Shigeru, Negi,Akira, Nakamura,Tsutomu, Okamura,Noboru, Okumura,Katsuhiko, Sakaeda,Toshiyuki, and Matsuo,Masafumi

Abstract

Mariko Yagi1, Motohiro Yamamori4, Ichiro Morioka2, Naoki Yokoyama2, Shigeru Honda3, Akira Negi3, Tsutomu Nakamura1, Noboru Okamura4, Katsuhiko Okumura1, Toshiyuki Sakaeda5, Masafumi Matsuo21Department of Clinical Evaluation of Pharmacotherapy, 2Department of Pediatrics, 3Department of Surgery, Division of Ophthalmology, Kobe University Graduate School of Medicine, Kobe, Japan; 4Department of Clinical Pharmacy, School of Pharmaceutical Sciences, Mukogawa Women's University, Nishinomiya, Japan; 5Center for Integrative Education of Pharmacy Frontier, Graduate School of Pharmaceutical Sciences, Kyoto University, Kyoto, JapanAbstract: Vascular endothelial growth factor (VEGF) contributes to the development of retinopathy of prematurity (ROP). We investigated the association of ROP with VEGF genetic polymorphisms and its clinical parameters in Japanese people. Sixty-seven infants with a gestational age of 30 weeks or less were enrolled and classified into the threshold ROP group (infants with Stage 3 ROP in zone I or II, five continuous or eight total clock hours of the retina and the presence of plus disease, n = 30) and the nonthreshold ROP group (n = 37). The VEGF genotypes of −1498T>C, −1154G>A, −634C>G, −7C>T, 936C>T, and 1612G>A were determined. VEGF 936C>T polymorphism and 11 clinical parameters were significantly different between the two ROP groups by univariate analysis. A logistic regression analysis with adjustments for gestational age and birth weight showed that the heterozygous or homozygous carrier state of the T alleles of VEGF 936C>T polymorphism (odds ratio 5.12; 95% confidence interval: 1.25–20.92; P = 0.023) and duration of oxygen administration (odds ratio 1.05; 95% confidence interval: 1.00–1.10; P = 0.042) were independent risk factors of threshold ROP. VEGF 936C>T polymorphism may predict threshold ROP in Japanese infa

Published
2011

114. Ligand orientation governs conjugation capacity of UDP-glucuronosyltransferase 1A1

Author

1000020332281, Takaoka, Yutaka, Ohta, Mika, Takeuchi, Atsuko, Miura, Kenji, Matsuo, Masafumi, Sakaeda, Toshiyuki, Sugano, Aki, 1000080189258, Nishio, Hisahide, 1000020332281, Takaoka, Yutaka, Ohta, Mika, Takeuchi, Atsuko, Miura, Kenji, Matsuo, Masafumi, Sakaeda, Toshiyuki, Sugano, Aki, 1000080189258, and Nishio, Hisahide

Published
2010

115. Replacement of cisplatin with nedaplatin in a definitive 5-fluorouracil/cisplatin-based chemoradiotherapy in Japanese patients with esophageal squamous cell carcinoma

Author

20227060, Kuwahara, Akiko, Yamamori, Motohiro, Nishiguchi, Kohshi, Okuno, Tatsuya, Chayahara, Naoko, Miki, Ikuya, Tamura, Takao, Inokuma, Tsubasa, Takemoto, Yoshiji, Nakamura, Tsutomu, Kataoka, Kazusaburo, Sakaeda, Toshiyuki, 20227060, Kuwahara, Akiko, Yamamori, Motohiro, Nishiguchi, Kohshi, Okuno, Tatsuya, Chayahara, Naoko, Miki, Ikuya, Tamura, Takao, Inokuma, Tsubasa, Takemoto, Yoshiji, Nakamura, Tsutomu, Kataoka, Kazusaburo, and Sakaeda, Toshiyuki

Abstract

Objective: The effects of replacing cisplatin (CDDP) with cis-diammineglycolatoplatinum (nedaplatin, NDP), a second-generation platinum complex, on the pharmacokinetics of 5-fluorouracil (5-FU) were investigated in Japanese patients with esophageal squamous cell carcinoma, who were treated with a definitive 5-FU/CDDP-based chemoradiotherapy. Methods: Fifty-six patients were enrolled, 49 treated with CDDP and 7 treated with NDP. A course consisted of continuous infusion of 5-FU at 400 mg/m2/day for days 1-5 and 8-12, infusion of CDDP or NDP at 40 mg/m2/day on days 1 and 8, and radiation at 2 Gy/day on days 1 to 5, 8 to 12, and 15 to 19, with a second course repeated after a 2-week interval. Plasma concentrations of 5-FU were determined by high performance liquid chromatography at 5 PM on days 3, 10, 38 and45, and at 5 AM on days 4, 11, 39 and 46. Results and conclusions: The circadian rhythm in plasma concentrations of 5-FU observed in the case of CDDP was altered when NDP was used instead. The clinical response can be predicted by monitoring plasma concentrations of 5-FU in the CDDP group, but not in the NDP group.

Published
2009

116. Molecular pathology of Sandhoff disease with p.Arg505Gln in HEXB: application of simulation analysis

Author

Yasui, Naoko, primary, Takaoka, Yutaka, additional, Nishio, Hisahide, additional, Nurputra, Dian K, additional, Sekiguchi, Kenji, additional, Hamaguchi, Hirotoshi, additional, Kowa, Hisatomo, additional, Maeda, Eiichi, additional, Sugano, Aki, additional, Miura, Kenji, additional, Sakaeda, Toshiyuki, additional, Kanda, Fumio, additional, and Toda, Tatsushi, additional

Published
2013
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120. Change in Pharmacokinetics of Model Compounds with Different Elimination Processes in Rats during Hypothermia

Author

Nishida, Koyo, Okazaki, Madoka, Sakamoto, Ryuichi, Inaoka, Natsuko, Miyake, Hideaki, Fumoto, Shintaro, Nakamura, Junzo, Nakashima, Mikiro, Sasaki, Hitoshi, Kakumoto, Mikio, Sakaeda, Toshiyuki, Nishida, Koyo, Okazaki, Madoka, Sakamoto, Ryuichi, Inaoka, Natsuko, Miyake, Hideaki, Fumoto, Shintaro, Nakamura, Junzo, Nakashima, Mikiro, Sasaki, Hitoshi, Kakumoto, Mikio, and Sakaeda, Toshiyuki

Abstract

We compared the pharmacokinetics of model compounds with different elimination processes between hypothermic and normothermic rats, to obtain basic information concerning drug therapy during hypothermia. Male Wistar rats were anesthetized with sodium pentobarbital and kept at temperatures of 37 °C (normothermic group) by heat lamp, and 32 °C or 28 °C (hypothermic group) by external cooling. We chose phenolsulfonphthalein (PSP), indocyanine green (ICG) and fluorescein isothiocyanate (FITC)-dextran (FD-4, Mw 4400) as model compounds to determine changes in clearance pathways during hypothermia therapy. The plasma concentrations of PSP as biliary, urinary and metabolic elimination type were increased significantly in the hypothermic group (32 °C, 28 °C) after i.v. administration at a dose of 1 mg, compared to the normothermic group (37 °C). Each PSP clearance (bile, urine and metabolites) in the hypothermic group was decreased, suggesting an influence of hypothermia on the active elimination process. The decreasing tendency was marked at a temperature of 28 °C. Moreover, the plasma concentrations of ICG as the biliary excretion type after i.v. administration to the hypothermic rats at a dose of 1 mg were higher with more than 50% decrease in the total body clearance compared to normothermic rats. On the other hand, there was almost no difference in the i.v. pharmacokinetics of FD-4 as the urinary excretion type between 37 °C and 32 °C. However, renal clearance of FD-4 was significantly decreased at a temperature of 28 °C. Accordingly, the change in pharmacokinetics of a drug in the hypothermic group could differ with the elimination processes., Biological & Pharmaceutical Bulletin v.30(9) p.1763-1767, 2007

Published
2007

121. Population pharmacokinetic modelling and simulation of 5-fluorouracil incorporating a circadian rhythm in rats.

Author

Kobuchi, Shinji, Ito, Yukako, Nakano, Yuya, and Sakaeda, Toshiyuki

Subjects
FLUOROURACIL, PHARMACOKINETICS, CIRCADIAN rhythms, LABORATORY rats, COMPUTER simulation
Abstract

1. The aim of this study was to develop a population pharmacokinetic (PK) model for 5-fluorouracil (5-FU) and perform simulations to identify the circadian rhythm of the PK of 5-FU and the degree of circadian effects on the 5-FU plasma concentrations. 2. 5-FU plasma concentrations in rats following administration of 5-FU at varying time points throughout the day were obtained and used to develop the population PK model incorporating a circadian rhythm. The Cosinor method was used to describe the circadian variation of 5-FU clearance. 3. Our population PK model could successfully characterize the 5-FU disposition and provide reliable PK parameter estimates. The mesor, amplitude and acrophase of Cosinor model were estimated as 1.93 L/h/kg, 0.10 L/h/kg and 2.02 h, respectively. The peak clearance levels were estimated at ∼2 Hours After Light Onset (HALO) and the trough levels at ∼14 HALO. The plasma concentration–time profile of 5-FU after continuous infusion of 5-FU in rats successfully simulated the circadian variation of steady-state plasma concentrations. 4. The population PK model with individual 5-FU plasma concentrations, dose levels and sampling time points could be valuable for estimating area under the curve (AUC) levels and determining individual 5-FU dose management. [ABSTRACT FROM PUBLISHER]

Published
2016
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125. THRB Genetic Polymorphisms Can Predict Severe Myelotoxicity after Definitive Chemoradiotherapy in Patients with Esophageal Squamous Cell Carcinoma

Author

Miki, Ikuya, primary, Nakamura, Tsutomu, additional, Kuwahara, Akiko, additional, Yamamori, Motohiro, additional, Nishiguchi, Kohshi, additional, Tamura, Takao, additional, Okuno, Tatsuya, additional, Omatsu, Hideaki, additional, Mizuno, Shigeto, additional, Hirai, Midori, additional, Azuma, Takeshi, additional, and Sakaeda, Toshiyuki, additional

Published
2012
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127. VEGF -634C/G Genotype is Predictive of Long-term Survival after Treatment with a Definitive 5-Fluorouracil/cisplatin-based Chemoradiotherapy in Japanese Patients with Esophageal Squamous Cell Carcinoma

Author

Tamura, Takao, primary, Kuwahara, Akiko, additional, Yamamori, Motohiro, additional, Nishiguchi, Kohshi, additional, Nakamura, Tsutomu, additional, Okuno, Tatsuya, additional, Miki, Ikuya, additional, Manabe, Yuki, additional, and Sakaeda, Toshiyuki, additional

Published
2012
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131. Effects of plasma concentrations of 5-fluorouracil on long-term survival after treatment with a definitive 5-fluorouracil/cisplatin-based chemoradiotherapy in Japanese patients with esophageal squamous cell carcinoma

Author

Kuwahara, Akiko, primary, Yamamori, Motohiro, additional, Kadoyama, Kaori, additional, Nishiguchi, Kohshi, additional, Nakamura, Tsutomu, additional, Miki, Ikuya, additional, Tamura, Takao, additional, Okuno, Tatsuya, additional, Omatsu, Hideaki, additional, and Sakaeda, Toshiyuki, additional

Published
2011
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137. Risk Factors for Oxaliplatin-Induced Hypersensitivity Reactions in Japanese Patients with Advanced Colorectal Cancer

Author

Seki, Kyoko, primary, Senzaki, Kenzou, additional, Tsuduki, Yasuo, additional, Ioroi, Takeshi, additional, Fujii, Michiko, additional, Yamauchi, Hiroko, additional, Shiraishi, Yukinari, additional, Nakata, Izumi, additional, Nishiguchi, Kohshi, additional, Matsubayashi, Teruhisa, additional, Takakubo, Yoshihide, additional, Okamura, Noboru, additional, Yamamori, Motohiro, additional, Tamura, Takao, additional, and Sakaeda, Toshiyuki, additional

Published
2011
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139. Effects of Bolus Injection of 5-Fluorouracil on Steady-State Plasma Concentrations of 5-Fluorouracil in Japanese Patients with Advanced Colorectal Cancer

Author

Tamura, Takao, primary, Kuwahara, Akiko, additional, Kadoyama, Kaori, additional, Yamamori, Motohiro, additional, Nishiguchi, Kohshi, additional, Inokuma, Tsubasa, additional, Takemoto, Yoshiji, additional, Chayahara, Naoko, additional, Okuno, Tatsuya, additional, Miki, Ikuya, additional, Fujishima, Yoshimi, additional, and Sakaeda, Toshiyuki, additional

Published
2011
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141. ASSOCIATION OF GENETIC POLYMORPHISMS WITH HEPATOTOXICITY IN PATIENTS WITH CHILDHOOD ACUTE LYMPHOBLASTIC LEUKEMIA OR LYMPHOMA

Author

Horinouchi, Masanori, primary, Yagi, Mariko, additional, Imanishi, Hiroyuki, additional, Mori, Takeshi, additional, Yanai, Tomoko, additional, Hayakawa, Akira, additional, Takeshima, Yasuhiro, additional, Hijioka, Michiyo, additional, Okamura, Noboru, additional, Sakaeda, Toshiyuki, additional, Matsuo, Masafumi, additional, Okumura, Katsuhiko, additional, and Nakamura, Tsutomu, additional

Published
2010
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142. TNFRSF1B A1466G genotype is predictive of clinical efficacy after treatment with a definitive 5-fluorouracil/cisplatin-based chemoradiotherapy in Japanese patients with esophageal squamous cell carcinoma

Author

Kuwahara, Akiko, primary, Yamamori, Motohiro, additional, Fujita, Megumi, additional, Okuno, Tatsuya, additional, Tamura, Takao, additional, Kadoyama, Kaori, additional, Okamura, Noboru, additional, Nakamura, Tsutomu, additional, and Sakaeda, Toshiyuki, additional

Published
2010
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144. Effect of dose-escalation of 5-fluorouracil on circadian variability of its pharmacokinetics in Japanese patients with Stage III/IVa esophageal squamous cell carcinoma

Author

Kuwahara, Akiko, primary, Yamamori, Motohiro, additional, Nishiguchi, Kohshi, additional, Okuno, Tatsuya, additional, Chayahara, Naoko, additional, Miki, Ikuya, additional, Tamura, Takao, additional, Kadoyama, Kaori, additional, Inokuma, Tsubasa, additional, Takemoto, Yoshiji, additional, Nakamura, Tsutomu, additional, Kataoka, Kazusaburo, additional, and Sakaeda, Toshiyuki, additional

Published
2010
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145. A Novel Method for Preparation of Animal Models of Liver Damage: Liver Targeting of Carbon Tetrachloride in Rats

Author

Mukai, Takahiro, Mera, Kunihiro, Nishida, Koyo, Nakashima, Mikiro, Sasaki, Hitoshi, Sakaeda, Toshiyuki, Nakamura, Junzo, Mukai, Takahiro, Mera, Kunihiro, Nishida, Koyo, Nakashima, Mikiro, Sasaki, Hitoshi, Sakaeda, Toshiyuki, and Nakamura, Junzo

Abstract

Animal models prepared by treatment with toxic compounds such as a carbon tetrachloride have been used to examine drug disposition in hepatic diseases. However, it is possible that these compounds accumulate and cause damage to other organs as they are administered systemically. In this study, we used the liver surface application technique to deliver a toxic compound to the liver to prepare an appropriate animal model in which only the liver is significantly damaged. To restrict the absorption area in the liver, a cylindrical diffusion cell was attached to the liver surface of male Wistar rats. Twenty-four hours after direct addition of carbon tetrachloride to the diffusion cell, plasma levels of glutamic-oxaloacetic transaminase (GOT) and glutamic-pyruvic transaminase (GPT), and hepatic malondialdehyde (MDA) concentration were increased, while there were no changes in plasma creatinine or renal MDA level. On the other hand, not only GOT, GPT and hepatic MDA, but also creatinine and renal MDA levels were markedly increased by p.o. and i.p. administration of carbon tetrachloride, suggesting renal damage. These results indicated that the animal models of liver damage prepared by utilizing drug delivery techniques to accumulate toxic compounds in the liver would enable us to investigate the precise effects of hepatic disorder on drug disposition., Biological & Pharmaceutical Bulletin v.25(11) p.1494-1497, 2002

Published
2002

148. Phase I and Pharmacokinetic Study of Tegafur-Uracil/Leucovorin Combined With 5-Fluorouracil/Leucovorin and Irinotecan in Patients With Advanced Colorectal Cancer

Author

Chayahara, Naoko, primary, Tamura, Takao, additional, Yamamori, Motohiro, additional, Kadowaki, Yuko, additional, Okuno, Tatsuya, additional, Miki, Ikuya, additional, Tsuda, Masahiro, additional, Nishisaki, Hogara, additional, Maeda, Tetsuo, additional, Inoue, Yoshifumi, additional, Okumura, Katsuhiko, additional, Azuma, Takeshi, additional, Kasuga, Masato, additional, Sakaeda, Toshiyuki, additional, and Hirai, Midori, additional

Published
2009
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149. Replacement of cisplatin with nedaplatin in a definitive 5-fluorouracil/cisplatin-based chemoradiotherapy in Japanese patients with esophageal squamous cell carcinoma

Author

Kuwahara, Akiko, primary, Yamamori, Motohiro, additional, Nishiguchi, Kohshi, additional, Okuno, Tatsuya, additional, Chayahara, Naoko, additional, Miki, Ikuya, additional, Tamura, Takao, additional, Inokuma, Tsubasa, additional, Takemoto, Yoshiji, additional, Nakamura, Tsutomu, additional, Kataoka, Kazusaburo, additional, and Sakaeda, Toshiyuki, additional

Published
2009
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150. VEGF G-1154A is Predictive of Severe Acute Toxicities during Chemoradiotherapy for Esophageal Squamous Cell Carcinoma in Japanese Patients

Author

Sakaeda, Toshiyuki, primary, Yamamori, Motohiro, additional, Kuwahara, Akiko, additional, Hiroe, Satoko, additional, Nakamura, Tsutomu, additional, Okumura, Katsuhiko, additional, Okuno, Tatsuya, additional, Miki, Ikuya, additional, Chayahara, Naoko, additional, Okamura, Noboru, additional, and Tamura, Takao, additional

Published
2008
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