Your search keyword '"Nao, Nakano"' showing total 7 results

1. Historical control data on developmental toxicity studies in rats

Author

Shimpei Kajita, Kanata Ibi, Hiromasa Takashima, Toshiki Matsuoka, Yumi Sakai, Yoji Miwa, Mika Senuma, Tohru Uesugi, Masao Horimoto, Tatsuya Shimizu, Michio Fujiwara, Ken-ichi Noritake, Shino Nishizawa, Takayuki Hirano, Makiko Kuwagata, Masayuki Ube, Akihito Yamashita, Yuka Kirihata, Taishi Tateishi, Satoshi Kudo, Ryu-ichi Katagiri, Kaoru Yabe, Sho Tanaka, Takafumi Oota, Hitoshi Hojo, Nao Nakano, Terumasa Taniguchi, Yuko Sakai, Makoto Ema, and Hiroshi Mineshima

Subjects

0301 basic medicine, Male, Embryology, Pathology, medicine.medical_specialty, Skeletal anomalies, Developmental Disabilities, Developmental toxicity, Physiology, 030105 genetics & heredity, Biology, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, medicine, Animals, Rats, Wistar, Fetus, 030219 obstetrics & reproductive medicine, Reproducibility of Results, General Medicine, Immunohistochemistry, Rats, Disease Models, Animal, Phenotype, Pediatrics, Perinatology and Child Health, Female, Historical control, Reproductive toxicity, Fetal malformation, Developmental Biology

Abstract

Historical control data from prenatal developmental toxicity studies in rats have been used to evaluate whether toxicology outcomes were induced by exposure to a chemical or were within the range of spontaneous variation. These data are also important for monitoring animal characteristics. As a follow-up to historical control data from 1998 to 2010, this study analyzed control data from prenatal developmental studies performed in rats from 2011 to 2015. Data were collected from studies performed by 24 Japanese laboratories, including 15 pharmaceutical and chemical companies and nine contract research organizations, in Sprague-Dawley and two-sub-strains of Wistar Hannover rats. The data included maternal reproductive findings at terminal cesarean section and fetal findings, including incidences of spontaneous external, visceral, and skeletal anomalies. No noticeable differences in maternal reproductive data were observed among laboratories. The inter-laboratory variations in the incidences of fetal anomalies seemed to be due to differences in the selection of observation parameters, observation criteria, and classification of the findings, as well as to differences in terminology of fetal alterations. These historical control data may be helpful for adequate interpretation of experimental results and for evaluating the reproductive and developmental toxicities of various chemicals.

Published

2018

2. Historical control data on developmental toxicity studies in rodents

Author

Akihiko Hirose, Seiki Matsuo, Hiroaki Hara, Ryota Tanaka, Ryou Fukushima, Ikuo Matsuura, Akihito Yamashita, Makoto Ema, Nao Nakano, Sakiko Fujii, Harutaka Oku, Kunifumi Inawaka, Hiroshi Mineshima, Taishi Tateishi, Ryohei Yokoi, Katsumi Endoh, Mutsuko Hirata-Koizumi, Masato Naya, Nobuhito Hoshino, Yoji Miwa, Hiroko Noyori, Yukari Imai, Kiyoshi Matsumoto, Ikuro Takakura, Yoshihiro Katsumata, Yuko Tominaga, Atsushi Ono, Yoshinori Hosokawa, Kazuhiro Shimomura, Maki Maeda, Toshiki Matsuoka, Hitoshi Hojo, Toshiaki Yamauchi, Tohru Uesugi, Hirohito Kato, Keiichi Itoh, Hiroyuki Izumi, Kaoru Yabe, Hiroshi Inada, Masao Horimoto, Tatsuya Shimizu, Takafumi Ohta, and Chizuru Urakawa

Subjects

Embryology, Rodent, Evolutionary biology, biology.animal, Pediatrics, Perinatology and Child Health, Developmental toxicity, General Medicine, Historical control, Biology, Developmental Biology

Published

2014

3. Effect of PPARβ/δ Agonist on the Placentation and Embryo-Fetal Development in Rats

Author

Masa-aki Hattori, Nobuhiko Yamauchi, Mikinori Torii, Motoyuki Kawai, Nao Nakano, Vishwajit S. Chowdhury, Masako Kaneto, and Kyohei Nishimura

Subjects

Embryology, medicine.medical_specialty, Pregnancy, Fetus, business.industry, Health, Toxicology and Mutagenesis, Developmental toxicity, Toxicology, Endometrium, medicine.disease, Placental Malformation, medicine.anatomical_structure, Endocrinology, Oral administration, Internal medicine, Placenta, medicine, Gestation, business, Developmental Biology

Abstract

BACKGROUND The present study was conducted to evaluate the developmental toxicity in the endometrium and placenta due to GW501516 administration by gavage to pregnant rats. METHODS GW501516 was orally administered repeatedly to pregnant rats from gestation day (GD) 6 to 17 at a dose of 0, 30, and 100 mg/kg/day. In next study, GW501516 was also orally administered to pregnant rats on GD 7, 8, 9, 10, or 11 at a single dose of 275 or 350 mg/kg. In these studies, caesarean section was performed to examine the pregnancy outcome on GD21. Additionally, GW501516 was orally administered to pregnant rats on GD 10 at a single dose of 275 mg/kg. Placentae were subjected for temporal histological examinations on GD 11, 13, 15, or 17. RESULTS Placental malformation was induced by repeated administration of GW501516 at a dose of 100 mg/kg/day. Single oral administration of GW501516 at a dose of 275 and/or 350 mg/kg on GD 8, 9, 10, or 11 induced placental malformation, whereas GW501516 administered on GD 10 was the most effective for increasing placental malformation. Histopathologically, single oral administration of GW501516 on GD 10 induced cystic degeneration associated with cellular lysis of glycogen cells started from GD 15 in the basal zone. CONCLUSIONS High frequency of placental malformation was observed by the administration of GW501516. From GD 8 to 11, especially GD 10, is more sensitive period to induce the placental malformation.

Published

2013

4. Historical control data on prenatal developmental toxicity studies in rabbits

Author

Ikuo Matsuura, Keiichi Itoh, Hiroyuki Izumi, Harutaka Oku, Ryota Tanaka, Nao Nakano, Nobuhito Hoshino, Masato Naya, Tohru Uesugi, Kei Shiozawa, Katsumi Endoh, Hitoshi Hojo, Sakiko Fujii, Ken-ichi Noritake, Atsuko Hishikawa, Seiki Matsuo, Kaoru Yabe, Kazuhiro Chihara, Kiyoshi Matsumoto, Akihiro Arima, Yoji Miwa, Makoto Ema, Ayumi Inoue, Hanako Nishizawa, Hiroshi Mineshima, Ikuro Takakura, Hiroshi Inada, Yasumoto Mizoguchi, Maki Maeda, Yoshinori Hosokawa, Yuzo Asano, Hiroaki Aoyama, Masao Horimoto, Hidenori Miyata, Tatsuya Shimizu, Ryohei Yokoi, Kazuhiro Shimomura, Hiroko Noyori, Hiroaki Hara, Hashihiro Higuchi, Toshiaki Yamauchi, and Takafumi Ohta

Subjects

Embryology, Fetus, Pregnancy, Pathology, medicine.medical_specialty, business.industry, Background data, Developmental toxicity, Physiology, General Medicine, medicine.disease, Pediatrics, Perinatology and Child Health, medicine, JAPANESE WHITE, New zealand white, Historical control, business, Fetal malformation, Developmental Biology

Abstract

Historical control data on rabbit prenatal developmental toxicity studies, performed between 1994-2010, were obtained from 20 laboratories, including 11 pharmaceutical and chemical companies and nine contract laboratories, in Japan. In this paper, data were incorporated from a laboratory if the information was based on 10 studies or more. Japanese White rabbits and New Zealand White rabbits were used for prenatal developmental toxicity studies. The data included maternal reproductive findings at terminal cesarean sections and fetal findings including spontaneous incidences of morphological alterations. No noticeable differences between strains or laboratories were observed in the maternal reproductive and fetal developmental data. The inter-laboratory variations in the incidences of fetal external, visceral, and skeletal alterations seem to be due to differences in the selection of observation parameters, observation criteria, and classification of the findings, and terminology of fetal alterations.

Published

2012

5. Historical control data on developmental toxicity studies in rodents

Author

Makoto, Ema, Katsumi, Endoh, Ryou, Fukushima, Sakiko, Fujii, Hiroaki, Hara, Mutsuko, Hirata-Koizumi, Akihiko, Hirose, Hitoshi, Hojo, Masao, Horimoto, Nobuhito, Hoshino, Yoshinori, Hosokawa, Yukari, Imai, Hiroshi, Inada, Kunifumi, Inawaka, Keiichi, Itoh, Yoshihiro, Katsumata, Hiroyuki, Izumi, Hirohito, Kato, Maki, Maeda, Kiyoshi, Matsumoto, Seiki, Matsuo, Toshiki, Matsuoka, Ikuo, Matsuura, Hiroshi, Mineshima, Yoji, Miwa, Nao, Nakano, Masato, Naya, Hiroko, Noyori, Takafumi, Ohta, Harutaka, Oku, Atsushi, Ono, Tatsuya, Shimizu, Kazuhiro, Shimomura, Ikuro, Takakura, Ryota, Tanaka, Taishi, Tateishi, Yuko, Tominaga, Tohru, Uesugi, Chizuru, Urakawa, Kaoru, Yabe, Akihito, Yamashita, Toshiaki, Yamauchi, and Ryohei, Yokoi

Subjects

Male, Drug Evaluation, Preclinical, Reproducibility of Results, History, 20th Century, Control Groups, History, 21st Century, Rats, Mice, Pregnancy, Research Design, Cricetinae, Animals, Female, Growth and Development

Abstract

Historical control data on rodent developmental toxicity studies, performed between 1994 and 2010, were obtained from 19 laboratories in Japan, including 10 pharmaceutical and chemical companies and nine contract research organizations. Rats, mice, and hamsters were used for developmental toxicity studies. Data included maternal reproductive findings at terminal cesarean sections and fetal findings including the spontaneous incidences of external, visceral, and skeletal anomalies. No noticeable differences were observed in maternal reproductive data between laboratories. Inter-laboratory variations in the incidences of fetuses with anomalies appeared to be due to differences in the selection of observation parameters, observation criteria, classification of the findings, and terminology of fetal alterations. Historical control data are useful for the appropriate interpretation of experimental results and evaluation of the effects of chemical on reproductive and developmental toxicities.

Published

2013

6. Effect of PPARβ/δ agonist on the placentation and embryo-fetal development in rats

Author

Kyohei, Nishimura, Nao, Nakano, Vishwajit Sur, Chowdhury, Masako, Kaneto, Mikinori, Torii, Masa-aki, Hattori, Nobuhiko, Yamauchi, and Motoyuki, Kawai

Subjects

Male, Dose-Response Relationship, Drug, Placenta, Administration, Oral, Organ Size, Placentation, Rats, Fetal Development, Rats, Sprague-Dawley, Endometrium, Thiazoles, Maternal Exposure, Pregnancy, Animals, Female, PPAR delta, PPAR-beta

Abstract

The present study was conducted to evaluate the developmental toxicity in the endometrium and placenta due to GW501516 administration by gavage to pregnant rats.GW501516 was orally administered repeatedly to pregnant rats from gestation day (GD) 6 to 17 at a dose of 0, 30, and 100 mg/kg/day. In next study, GW501516 was also orally administered to pregnant rats on GD 7, 8, 9, 10, or 11 at a single dose of 275 or 350 mg/kg. In these studies, caesarean section was performed to examine the pregnancy outcome on GD21. Additionally, GW501516 was orally administered to pregnant rats on GD 10 at a single dose of 275 mg/kg. Placentae were subjected for temporal histological examinations on GD 11, 13, 15, or 17.Placental malformation was induced by repeated administration of GW501516 at a dose of 100 mg/kg/day. Single oral administration of GW501516 at a dose of 275 and/or 350 mg/kg on GD 8, 9, 10, or 11 induced placental malformation, whereas GW501516 administered on GD 10 was the most effective for increasing placental malformation. Histopathologically, single oral administration of GW501516 on GD 10 induced cystic degeneration associated with cellular lysis of glycogen cells started from GD 15 in the basal zone.High frequency of placental malformation was observed by the administration of GW501516. From GD 8 to 11, especially GD 10, is more sensitive period to induce the placental malformation.

Published

2012

7. Historical control data on prenatal developmental toxicity studies in rabbits

Author

Makoto, Ema, Hiroaki, Aoyama, Akihiro, Arima, Yuzo, Asano, Kazuhiro, Chihara, Katsumi, Endoh, Sakiko, Fujii, Hiroaki, Hara, Hashihiro, Higuchi, Atsuko, Hishikawa, Hitoshi, Hojo, Masao, Horimoto, Nobuhito, Hoshino, Yoshinori, Hosokawa, Hiroshi, Inada, Ayumi, Inoue, Keiichi, Itoh, Hiroyuki, Izumi, Maki, Maeda, Kiyoshi, Matsumoto, Seiki, Matsuo, Ikuo, Matsuura, Hiroshi, Mineshima, Yoji, Miwa, Hidenori, Miyata, Yasumoto, Mizoguchi, Nao, Nakano, Masato, Naya, Hanako, Nishizawa, Ken-Ichi, Noritake, Hiroko, Noyori, Takafumi, Ohta, Harutaka, Oku, Tatsuya, Shimizu, Kazuhiro, Shimomura, Kei, Shiozawa, Ikuro, Takakura, Ryota, Tanaka, Tohru, Uesugi, Kaoru, Yabe, Toshiaki, Yamauchi, and Ryohei, Yokoi

Subjects

Disease Models, Animal, Fetus, Teratogens, Pregnancy, Abnormalities, Drug-Induced, Animals, Female, Rabbits

Abstract

Historical control data on rabbit prenatal developmental toxicity studies, performed between 1994-2010, were obtained from 20 laboratories, including 11 pharmaceutical and chemical companies and nine contract laboratories, in Japan. In this paper, data were incorporated from a laboratory if the information was based on 10 studies or more. Japanese White rabbits and New Zealand White rabbits were used for prenatal developmental toxicity studies. The data included maternal reproductive findings at terminal cesarean sections and fetal findings including spontaneous incidences of morphological alterations. No noticeable differences between strains or laboratories were observed in the maternal reproductive and fetal developmental data. The inter-laboratory variations in the incidences of fetal external, visceral, and skeletal alterations seem to be due to differences in the selection of observation parameters, observation criteria, and classification of the findings, and terminology of fetal alterations.

Published

2012