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81 results on '"Kayanuma, Hideki"'

1. Preclinical/clinical trials of thrice-weekly administration of a combination of tegafur/ gimeracil/oteracil (TS-1) and toceranib phosphate in dogs with intranasal tumors.

Author

NISHIYAMA, Yuta, MARUO, Takuya, FUKUYAMA, Yasuhiro, ODAKA, Yuka, KAWATA, Eiyu, UENO, Hirona, KAYANUMA, Hideki, NAKAYAMA, Tomohiro, and TAKAHASHI, Hiroki

Subjects
SQUAMOUS cell carcinoma, CARCINOMA, ORAL medication, CLINICAL trials, DOGS
Abstract

Intranasal tumors in dogs are malignant solid tumors that are primarily treated with radiotherapy and often recur post-treatment. Combination therapy is pivotal in cancer therapy. Effective drugs include fluoropyrimidine 5-fluorouracil (5-FU) and toceranib phosphate. TS-1, an oral formulation containing the 5-FU prodrug tegafur and enzyme modulators gimeracil and oteracil, is proven to be safe in dogs with solid tumors. While the oral drug toceranib phosphate (Palladia®) is safely administered, the combined toxicity with TS-1 is unknown. We aimed to determine the dosage of this combination in dogs. In the preclinical/clinical trials conducted here, we used a standard 3+3 cohort design with fixed doses of toceranib phosphate (2.4 mg/kg) administered thrice weekly. TS-1 administration was initiated at a dose of 0.5 mg/kg (upper limit 2.0 mg/kg) thrice weekly. Four cohorts were included to confirm the safety of TS-1 and toceranib phosphate. Each cohort was followed up for 1 month. The intranasal tumor types included in the clinical trial (n=13) were adenocarcinoma (n=7), squamous cell carcinoma (n=1), non-epithelial malignancy (n=2), undifferentiated carcinoma (n=1), and transitional carcinoma (n=2). The TS-1 dosage could be increased up to its dose limit in the preclinical/clinical trials. The TS-1 dose to combine with toceranib phosphate thrice weekly was 2.0 mg/kg. This regimen was well-tolerated in dogs. Thus, combined TS-1 and toceranib phosphate therapy is safe for dogs with intranasal tumors. [ABSTRACT FROM AUTHOR]

Published
2024
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2. Comparison of a new immobilization method using a reusable 3‐point fixation cylinder system and bite‐block type immobilization methods in veterinary radiotherapy.

Author

Yoda, Shinichiro, Maruo, Takuya, Arai, Haruka, Takahashi, Rihoko, Kusaka, Takuya, Nishiyama, Yuta, and Kayanuma, Hideki

Abstract

In veterinary radiotherapy, highly reproducible immobilization is important for accurate irradiation. Consequently, we developed a new reusable head‐immobilization method for dogs using cylinders. This study aimed to compare the accuracy of our novel immobilization method using cylinders with that of bite‐block type immobilization methods. Three immobilization methods were compared: bite‐block only, bite‐block combined with torso immobilization, and immobilization using cylinders. Five beagles with canine teeth underwent CT five times for each of the three immobilization methods. One beagle without canine teeth underwent CT 15 times using each method. Three maxillary landmarks (maxillary incisor, frontal sinus, and occipital bone) and one mandibular landmark (mandibular incisor) were established, and the errors in each immobilization method were measured. For all head landmarks, the error in the immobilization method using cylinders was the most reproducible, with the smallest errors. No significant differences were observed in the time required for immobilization. Although there were limitations (such as the use of dogs from a single breed, a single episode of anesthesia, no disassembly of the immobilization system between scans, and the same person performing the positioning on the same day), we found our new reusable immobilization method using cylinders was the most accurate among the three compared methods. This was a proof‐of‐principle study to evaluate head immobilization using cylinders, and further investigations are needed to confirm its clinical utility. [ABSTRACT FROM AUTHOR]

Published
2024
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4. Screening of bacterial DNA in bile sampled from healthy dogs and dogs suffering from liver- or gallbladder-associated disease

Author

NEO, Sakurako, TAKEMURA-UCHIYAMA, Iyo, UCHIYAMA, Jumpei, MURAKAMI, Hironobu, SHIMA, Ayaka, KAYANUMA, Hideki, YOKOYAMA, Taiki, TAKAGI, Satoshi, KANAI, Eiichi, HISASUE, Masaharu, NEO, Sakurako, TAKEMURA-UCHIYAMA, Iyo, UCHIYAMA, Jumpei, MURAKAMI, Hironobu, SHIMA, Ayaka, KAYANUMA, Hideki, YOKOYAMA, Taiki, TAKAGI, Satoshi, KANAI, Eiichi, and HISASUE, Masaharu

Abstract

Although the biliary system is generally aseptic, gallbladder microbiota has been reported in humans and some animals apart from dogs. We screened and analyzed the bacterial deoxyribonucleic acid in canine gallbladders using bile sampled from 7 healthy dogs and 52 dogs with liver- or gallbladder-associated disease. PCR screening detected bacteria in 17.3% of diseased dogs (9/52) and none in healthy dogs. Microbiota analysis of PCR-positive samples showed that the microbial diversity differed between liver- and gallbladder-associated disease groups. Thus, a specific bacterial community appears to occur at a certain frequency in the bile of diseased dogs.

Published
2022

11. Intraoperative acridine orange photodynamic therapy and cribriform electron-beam irradiation for canine intranasal carcinomas: 14 cases

Author

Maruo, Takuya, Fukuyama, Yasuhiro, Nagata, Koichi, Yoshioka, Chie, Nishiyama, Yuta, Shinpei Kawarai, Kayanuma, Hideki, Orito, Kensuke, and Nakayama, Tomohiro

Subjects
Dogs, Intraoperative Care, Photochemotherapy, Animals, Scientific, Electrons, Dog Diseases, Neoplasm Recurrence, Local, Combined Modality Therapy, Acridine Orange, Retrospective Studies
Abstract

Canine intranasal carcinomas are almost always malignant. Surgery alone often results in rapid tumor regrowth. Radiotherapy is the treatment of choice for dogs with intranasal tumors. Here, we retrospectively assessed treatment of intranasal carcinoma by marginal tumor resection followed by intraoperative acridine orange (AO) photodynamic therapy (PDT) and cribriform plate electron-beam intraoperative radiotherapy (IORT). Fourteen canine cases were assessed, 12 of which had stage I tumors, one with stage III, and one with stage IV. Recurrence was detected in 8, with a median recurrence from the time of treatment of 6 months (range: 3 to 16 months). The median progression-free survival time and overall survival time after treatment were 13 and 22 months, respectively. Adverse events were mild. Marginal tumor resection followed by intraoperative AO-PDT and cribriform plate electron-beam IORT may increase the tumor control time in dogs with marginally resectable intranasal malignant tumors beyond that incurred by surgery alone.

Published
2019

18. Suspected panosteitis in a crossbred calf

Author

Sato, Reiichiro, Ito, Tetsuo, Suganuma, Tsunenori, Une, Yumi, Kudo, Tomoo, Kayanuma, Hideki, Kanai, Eiichi, Suzuki, Takehito, Ochiai, Hideharu, Enomoto, Nahoko, Itoh, Seigo, Onda, Ken, and Wada, Yasunori

Subjects
body regions, Male, animal structures, Biopsy, Animals, Cattle Diseases, Scientific, Cattle, Osteitis
Abstract

A male crossbred calf developed a limp and pain upon deep pressure on the right hind limb and the right forelimb. The radiographic findings of affected limbs and pathological findings of bone biopsy were similar to those observed in canine panosteitis. This is the first case of suspected panosteitis reported in cattle.

Published
2015

24. Primary Lung Carcinoma with Paraneoplastic Leukocytosis in a Dog

Author

Sato, Toshihiko, primary, Shida, Takuo, additional, Maruo, Takuya, additional, Kawamura, Hiroko, additional, Yamada, Toru, additional, Ito, Tetsuro, additional, Takeda, Haruo, additional, Sugiyama, Hiroki, additional, Ishikawa, Takeshi, additional, Madarame, Hiroo, additional, Kayanuma, Hideki, additional, and Suganuma, Tsunenori, additional

Published
2012
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26. Low-dose chemotherapy for canine appendicular osteosarcoma

Author

Shida, Takuo, primary, Fujii, Takashi, additional, Kawamura, Hiroko, additional, Yamada, Toru, additional, Takeda, Haruo, additional, Maruo, Takuya, additional, Imai, Rie, additional, Ito, Tetsuro, additional, Madarame, Hiroo, additional, Kayanuma, Hideki, additional, and Suganuma, Tsunenori, additional

Published
2011
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29. Initial response to L-asparaginase and prednisolone induction chemotherapy in 107 cases of canine lymphoma

Author

Shida, Takuo, primary, Fukuoka, Rieko, additional, Maruo, Takuya, additional, Ito, Tetsuro, additional, Kawamura, Hiroko, additional, Takeda, Haruo, additional, Sugiyama, Hiroki, additional, Ishikawa, Takeshi, additional, Yamada, Tohru, additional, Madarame, Hiroo, additional, Kayanuma, Hideki, additional, and Suganuma, Tsunenori, additional

Published
2010
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30. A Retrospective Study in 1,070 Feline Tumor Cases of Japan.

Author

Shida, Takuo, primary, Yamada, Tohru, additional, Maruo, Takuya, additional, Ishida, Takuo, additional, Kawamura, Hiroko, additional, Takeda, Haruo, additional, Sugiyama, Hiroki, additional, Ishikawa, Takeshi, additional, Ito, Tetsuro, additional, Madarame, Hiroo, additional, Kayanuma, Hideki, additional, and Suganuma, Tsunenori, additional

Published
2010
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35. Adjuvant chemotherapy with low-dose cisplatin following surgery for malignant tumors in dogs: 16 cases

Author

Sato, Toshihiko, primary, Kawamura, Hiroko, additional, Yamada, Toru, additional, Maruo, Takuya, additional, Kanakubo, Kayo, additional, Ito, Tetsuro, additional, Takeda, Haruo, additional, Sugiyama, Hiroki, additional, Ishikawa, Takeshi, additional, Madarame, Hiroo, additional, Kayanuma, Hideki, additional, Suganuma, Tsunenori, additional, and Shida, Takuo, additional

Published
2010
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43. Rectal Mucosal Pull-Through Surgical Technique for Canine Rectal Multiple Tumor

Author

SHIDA, Takuo, primary, MARUO, Takuya, additional, SUGA, Keiichiro, additional, KAWAMURA, Hiroko, additional, TAKEDA, Haruo, additional, SUGIYAMA, Hiroki, additional, ISHIKAWA, Takeshi, additional, INOUE, Akira, additional, YAMADA, Toru, additional, ITO, Tetsuro, additional, MADARAME, Hiroo, additional, KAYANUMA, Hideki, additional, and SUGANUMA, Tsunenori, additional

Published
2008
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49. Evaluation of the Susceptibility Artifacts and Tissue Injury Caused by Implanted Microchips in Dogs on 1.5 T Magnetic Resonance Imaging.

Author

SAITO, Miyoko, ONO, Shin, KAYANUMA, Hideki, HONNAMI, Muneki, MUTO, Makoto, and UNE, Yumi

Subjects
TISSUE wounds, INTEGRATED circuits, LABORATORY dogs, MAGNETIC resonance imaging, DIAGNOSTIC imaging, MEDICAL imaging systems
Abstract

The article presents a study which examined the susceptibility artifacts and tissue injury caused by implanted microchips in dogs by evaluating magnetic resonance imaging (MRI) results and the histopathological changes after 1.5 Tesla MRI. It states that signal loss and image distortion were recorded over a wide range around the area where the microchip was implanted. The calculation as the actual visibly distorted area divided by the area of the cervical region and calculation by drawing round or oval that enclosed the visible artifact with the microchip as the central point are explained.

Published
2010
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50. Preclinical/clinical trials of thrice-weekly administration of a combination of tegafur/gimeracil/oteracil (TS-1) and toceranib phosphate in dogs with intranasal tumors.

Author

Nishiyama Y, Maruo T, Fukuyama Y, Odaka Y, Kawata E, Ueno H, Kayanuma H, Nakayama T, and Takahashi H

Subjects
Animals, Dogs, Male, Female, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Drug Administration Schedule, Dog Diseases drug therapy, Tegafur administration & dosage, Tegafur therapeutic use, Pyridines administration & dosage, Pyridines therapeutic use, Drug Combinations, Indoles administration & dosage, Indoles therapeutic use, Pyrroles administration & dosage, Pyrroles therapeutic use, Oxonic Acid administration & dosage, Oxonic Acid therapeutic use, Nose Neoplasms veterinary, Nose Neoplasms drug therapy
Abstract

Intranasal tumors in dogs are malignant solid tumors that are primarily treated with radiotherapy and often recur post-treatment. Combination therapy is pivotal in cancer therapy. Effective drugs include fluoropyrimidine 5-fluorouracil (5-FU) and toceranib phosphate. TS-1, an oral formulation containing the 5-FU prodrug tegafur and enzyme modulators gimeracil and oteracil, is proven to be safe in dogs with solid tumors. While the oral drug toceranib phosphate (Palladia ® ) is safely administered, the combined toxicity with TS-1 is unknown. We aimed to determine the dosage of this combination in dogs. In the preclinical/clinical trials conducted here, we used a standard 3+3 cohort design with fixed doses of toceranib phosphate (2.4 mg/kg) administered thrice weekly. TS-1 administration was initiated at a dose of 0.5 mg/kg (upper limit 2.0 mg/kg) thrice weekly. Four cohorts were included to confirm the safety of TS-1 and toceranib phosphate. Each cohort was followed up for 1 month. The intranasal tumor types included in the clinical trial (n=13) were adenocarcinoma (n=7), squamous cell carcinoma (n=1), non-epithelial malignancy (n=2), undifferentiated carcinoma (n=1), and transitional carcinoma (n=2). The TS-1 dosage could be increased up to its dose limit in the preclinical/clinical trials. The TS-1 dose to combine with toceranib phosphate thrice weekly was 2.0 mg/kg. This regimen was well-tolerated in dogs. Thus, combined TS-1 and toceranib phosphate therapy is safe for dogs with intranasal tumors.

Published
2024
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