15 results on '"Iori ITAGAKI"'
Search Results
2. Experimental techniques for the development of a uterus transplantation model in cynomolgus macaques
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Yoko Saiki, Ikuo Kawamoto, Chizuru Iwatani, Takahiro Nakagawa, Hideaki Tsuchiya, Yojiro Kato, Yohei Masugi, Daisuke Aoki, Kenshi Nakagawa, Mitsuru Murase, Kouji Banno, Iori Kisu, Iori Itagaki, Yohei Yamada, Hirohito Ishigaki, Hideaki Obara, Yusuke Matoba, Takashi Shiina, Masataka Adachi, Kentaro Matsubara, and Katsura Emoto
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030219 obstetrics & reproductive medicine ,Non human primate ,business.industry ,Uterus ,Obstetrics and Gynecology ,Bioinformatics ,Cynomolgus macaque ,03 medical and health sciences ,Uterine transplantation ,0302 clinical medicine ,030220 oncology & carcinogenesis ,Uterus transplantation ,Animals ,Humans ,Macaca ,Medicine ,Female ,business ,Infertility, Female - Abstract
Uterus transplantation (UTx) is now a treatment for women with uterine factor infertility to have a child. However, UTx is still largely at the experimental stage, and many medical issues remain unsolved. Therefore, adequate studies in large animals including non-human primates are required for validation of these issues. UTx research, especially in non-human primates, can provide important information for its full establishment in humans due to the anatomical and physiological similarities between the two. We accumulated data from UTx studies using cynomolgus macaques since 2009 and established autologous and allogeneic UTx models which led to deliveries after performing the procedure. In this paper, we summarized key points to develop UTx models in cynomolgus macaques based on our experience. UTx models in non-human primates can surely contribute new and beneficial knowledge in this field and can be useful for the further development of UTx in humans.
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- 2020
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3. Paromomycin sulfate is an effective treatment for balantidiasis in captive cynomolgus monkeys
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Ikuo Kawamoto, Takahiro Nakagawa, Takahiro Asano, Hideaki Tsuchiya, Shinichiro Nakamura, Iori Itagaki, and Daichi Arakawa
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Male ,0301 basic medicine ,Original ,Balantidium coli ,Balantidium ,Paromomycin ,Antiprotozoal Agents ,Pharmacology ,General Biochemistry, Genetics and Molecular Biology ,Feces ,03 medical and health sciences ,0302 clinical medicine ,Oral administration ,medicine ,Animals ,Effective treatment ,Balantidiasis ,General Veterinary ,biology ,business.industry ,Monkey Diseases ,General Medicine ,biology.organism_classification ,Antimicrobial ,medicine.disease ,Macaca fascicularis ,Paromomycin Sulfate ,030104 developmental biology ,cynomolgus monkey ,paromomycin sulfate ,Female ,Animal Science and Zoology ,business ,Care staff ,030217 neurology & neurosurgery - Abstract
There are few effective antimicrobial agents against Balantidium coli infection. The effect of paromomycin sulfate (PS) against B. coli was confirmed in this study of 596 captive cynomolgus monkeys. In several trials, the minimum dose and duration of oral administration of PS were 25 mg/day for 5 + 5 days, with a 2-day withdrawal interval. To facilitate daily PS administration, pumpkin cakes supplemented with PS were made, which not only resulted in precise effects but also increased the efficiency of preparation and administration of PS by the animal care staff. No cysts or trophozoites were detected at 14 or 16 days after the last treatments. There were no obvious differences in blood and biochemical parameters between before and after administration of PS. These results indicate that PS is effective for elimination of B. coli without hematological side effects. These data could contribute to the control of microbiological pathogens during veterinary care and colony management in primate facilities.
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- 2019
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4. Clinical features of irreversible rejection after allogeneic uterus transplantation in cynomolgus macaques
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Hideaki Tsuchiya, Daisuke Aoki, Hideaki Obara, Yusuke Matoba, Masatsugu Ema, Takashi Shiina, Takahiro Nakagawa, Hirohito Ishigaki, Kouji Banno, Mitsuru Murase, Yohei Yamada, Iori Itagaki, Hiroyuki Urano, Ikuo Kawamoto, Iori Kisu, Yoko Saiki, Kentaro Matsubara, Kenshi Nakagawa, Yohei Masugi, Chizuru Iwatani, Katsura Emoto, Kazumasa Ogasawara, and Yojiro Kato
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0301 basic medicine ,Graft Rejection ,Indocyanine Green ,medicine.medical_specialty ,Pathology ,Time Factors ,Reproductive disorders ,medicine.medical_treatment ,Uterus ,lcsh:Medicine ,Article ,03 medical and health sciences ,chemistry.chemical_compound ,Leukocyte Count ,0302 clinical medicine ,Laparotomy ,Internal medicine ,Uterus transplantation ,medicine ,Animals ,Transplantation, Homologous ,lcsh:Science ,Ultrasonography ,Immunosuppression Therapy ,Multidisciplinary ,Hysterectomy ,Hematology ,L-Lactate Dehydrogenase ,business.industry ,lcsh:R ,Optical Imaging ,Immunosuppression ,Transplantation ,Experimental models of disease ,Macaca fascicularis ,030104 developmental biology ,medicine.anatomical_structure ,C-Reactive Protein ,chemistry ,Infertility ,lcsh:Q ,Female ,business ,Indocyanine green ,030217 neurology & neurosurgery - Abstract
Uterus transplantation (UTx) is a potential option for women with uterine factor infertility to have a child. The clinical features indicating irreversible rejection of the uterus are unknown. In our experimental series of allogeneic UTx in cynomolgus macaques, six female macaques were retrospectively examined, which were unresponsive to treatment with immunosuppressants (i.e. irreversible rejection). Clinical features including general condition, hematology, uterine size, indocyanine green (ICG) fluorescence imaging by laparotomy, and histopathological findings of the removed uterus were evaluated. In all cases, general condition was good at the time of diagnosis of irreversible rejection and thereafter. Laboratory evaluation showed temporary increases in white blood cells, lactate dehydrogenase and C-reactive protein, then these levels tended to decrease gradually. In transabdominal ultrasonography, the uterus showed time-dependent shrinkage after transient swelling at the time of diagnosis of irreversible rejection. In laparotomy, a whitish transplanted uterus was observed and enhancement of the transplanted uterus was absent in ICG fluorescence imaging. Histopathological findings in each removed uterus showed hyalinized fibrosis, endometrial deficit, lymphocytic infiltration and vasculitis. These findings suggest that uterine transplantation rejection is not fatal, in contrast to rejection of life-supporting organs. Since the transplanted uterus with irreversible rejection atrophies naturally, hysterectomy may be unnecessary.
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- 2020
5. Allowable warm ischemic time and morphological and biochemical changes in uterine ischemia/reperfusion injury in cynomolgus macaque: a basic study for uterus transplantation
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Hideaki Tsuchiya, Ikuo Kawamoto, Hayato Narita, Atsushi Yoshida, Daisuke Aoki, Iori Itagaki, Kazumasa Ogasawara, Yuya Nogami, Iori Kisu, Kouji Banno, Kiyoko Umene, Masataka Adachi, Takahiro Nakagawa, and Katsura Emoto
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Pathology ,medicine.medical_specialty ,Time Factors ,Ischemia ,Uterus ,030230 surgery ,Warm Ischemic Time ,Cynomolgus macaque ,03 medical and health sciences ,0302 clinical medicine ,Reperfusion therapy ,Uterus transplantation ,Hum ,medicine ,Animals ,Humans ,Lactic Acid ,Warm Ischemia ,Ultrasonography ,Acid-Base Equilibrium ,030219 obstetrics & reproductive medicine ,Warm Ischemia Time ,business.industry ,Optical Imaging ,Rehabilitation ,Obstetrics and Gynecology ,medicine.disease ,Menstruation ,Transplantation ,Macaca fascicularis ,medicine.anatomical_structure ,Reproductive Medicine ,Reperfusion Injury ,Anesthesia ,Models, Animal ,Potassium ,Female ,030211 gastroenterology & hepatology ,Blood Gas Analysis ,business ,Infertility, Female ,Reperfusion injury ,Blood sampling - Abstract
Study question How long is the allowable warm ischemic time of the uterus and what morphological and biochemical changes are caused by uterine ischemia/reperfusion injury in cynomolgus macaques? Summary answer Warm ischemia in the uterus of cynomolgus macaques is tolerated for up to 4 h and reperfusion after uterine ischemia caused no further morphological and biochemical changes. What is known already Uterus transplantation is a potential option for women with uterine factor infertility. The allowable warm ischemic time and ischemia/reperfusion injury of the uterus in humans and non-human primates is unknown. Study design, size, duration This experimental study included 18 female cynomolgus macaques with periodic menstruation. Participants/materials, setting, methods Animals were divided into six groups of three monkeys each: a control group and groups with uterine ischemia for 0.5, 1, 2, 4 and 8 h. Biopsies of uterine tissues were performed before blood flow blockage, after each blockage time, and after reperfusion for 3 h. Blood sampling was performed after each blockage time, and after reperfusion for 5, 15 and 30 min for measurement of biochemical data. Resumption of menstruation was monitored after the surgical procedure. Morphological, physiological and biochemical changes after ischemia and reperfusion were evaluated. Main results and the role of chance Mild muscle degeneration and zonal degeneration were observed in all animals subjected to warm ischemia for 4 or 8 h, but there were no marked differences in the appearance of specimens immediately after ischemia and after reperfusion for 3 h in animals subjected to 4 or 8 h of warm ischemia. There were no significant changes in any biochemical parameters at any time point in each group. Periodical menstruation resumed in all animals with warm ischemia up to 4 h, but did not recover in animals with warm ischemia for 8 h with atrophic uteri. Limitations, reason for caution Warm ischemia in actual transplantation was not exactly mimicked in this study because uteri were not perfused, cooled, transplanted or reanastomosed with vessels. Results in non-human primates cannot always be extrapolated to humans. Wider implications of the findings The findings suggest that the tolerable warm ischemia time in the uterus is expected to be longer than that in other vital organs. Study funding/competing interest(s) This study was supported by the Japan Society for the Promotion of Science (JSPS) KAKENHI Grant Number 26713050. None of the authors has a conflict of interest to declare.
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- 2017
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6. Hematological and pathological features of massive hepatic necrosis in two radiated tortoises (Astrochelys radiata)
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Daisuke Kiryu, Iori Itagaki, Nobuhide Kido, Tomoko Omiya, and Kaori Ono
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0301 basic medicine ,Pathology ,medicine.medical_specialty ,General Veterinary ,biology ,040301 veterinary sciences ,Radiated tortoise ,04 agricultural and veterinary sciences ,Anorexia ,030108 mycology & parasitology ,Severe fibrosis ,biology.organism_classification ,0403 veterinary science ,03 medical and health sciences ,medicine.anatomical_structure ,Hypokinesia ,Giant cell ,White blood cell ,Massive Hepatic Necrosis ,medicine ,medicine.symptom ,Pathological - Abstract
Two radiated tortoises (Astrochelys radiata) exhibited anorexia and hypokinesia. In both cases, hematological and serum biochemical examinations revealed high alkaline phosphatase levels, moderately high aspartate aminotransferase levels and white blood cell counts approximately within the normal range. Despite being treated, the tortoises died 9 and 43 days after the first clinical examination. Gross pathological examinations revealed that the livers of both animals were extremely swollen and contained pale yellow necrotic tissue. Histopathological assessment revealed that the livers contained a massive area of hepatic necrosis surrounded by migration of macrophages and multinucleated giant cells. In one of the cases, severe fibrosis was observed. The present study provides reference information for similar cases in the future.
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- 2017
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7. Evaluation of allowable time and histopathological changes in warm ischemia of the uterus in cynomolgus monkey as a model for uterus transplantation
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Ikuo Kawamoto, Daisuke Aoki, Takahiro Nakagawa, Toshihiro Nagai, Kazumasa Ogasawara, Yuya Nogami, Masataka Adachi, Hideaki Tsuchiya, Kouji Banno, Iori Itagaki, Iori Kisu, Katsura Emoto, and Kiyoko Umene
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0301 basic medicine ,Cytoplasm ,Pathology ,medicine.medical_specialty ,Biopsy ,Uterus ,Ischemia ,Endoplasmic Reticulum ,Menstruation ,03 medical and health sciences ,0302 clinical medicine ,Uterus transplantation ,Animals ,Medicine ,Warm Ischemia ,Amenorrhea ,Cell Nucleus ,Microscopy ,030219 obstetrics & reproductive medicine ,Smooth muscle tissue ,medicine.diagnostic_test ,business.industry ,Obstetrics and Gynecology ,Muscle, Smooth ,General Medicine ,medicine.disease ,Chromatin ,Mitochondria, Muscle ,Macaca fascicularis ,030104 developmental biology ,medicine.anatomical_structure ,Reperfusion Injury ,Models, Animal ,Reperfusion ,Female ,Atrophy ,business ,Reperfusion injury ,Corpus Uteri - Abstract
Introduction The objective of this study was to examine the allowable warm ischemic time and pathological changes due to ischemia and reperfusion injury in the uterus of the cynomolgus monkey as a model for uterus transplantation. Material and methods Six female cynomolgus monkeys were used in the study. The uterus was resected from the vaginal canal and connected through the bilateral ovarian and uterine arteries and veins only. One animal was used as a control. In the other five animals, the bilateral uterine and ovarian vessels were clamped for 0.5, 1, 2, 4 and 8 h, respectively. Biopsy of the smooth muscle tissue of corpus uteri was performed after each ischemic time and after subsequent reperfusion for 3 h. Biopsy samples were observed by light and electron microscopy. Menstruation recovery was monitored. Results There were no particular findings in both light and electron microscopy after ischemia for up to 2 h and after subsequent reperfusion. There were no marked changes after ischemia for 4 h, but dilated nuclear pores and rough endoplasmic reticulum swelling were found after reperfusion. These changes also occurred, along with mitochondrial swelling and cristae loss after ischemia for 8 h, and plasma membrane loss, nuclear fragmentation and chromatin condensation were found after reperfusion. Periodical menstruation restarted in all animals with ischemia up to 4 h, but the animal with ischemia for 8 h had amenorrhea and uterine atrophy. Conclusions The uterus of the cynomolgus monkey tolerates warm ischemia for up to 4 h.
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- 2016
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8. Surgical technique for allogeneic uterus transplantation in macaques
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Ikuo Kawamoto, Hirohito Ishigaki, Hideaki Obara, Shin Ichi Sato, Katsura Emoto, Masataka Adachi, Iori Itagaki, Yuko Kitagawa, Iori Kisu, Daisuke Aoki, Kentaro Matsubara, Hideaki Tsuchiya, Kazumasa Ogasawara, Takahiro Nakagawa, Yuya Nogami, Yojiro Kato, Kenshi Nakagawa, Yasushi Itoh, Takashi Shiina, Yusuke Matoba, Yoko Saiki, Yohei Yamada, Kouji Banno, and Kiyoko Umene
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Models, Anatomic ,medicine.medical_specialty ,Femoral artery ,Anastomosis ,Article ,Hemoglobins ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,medicine.artery ,Uterus transplantation ,Animals ,Transplantation, Homologous ,Medicine ,Immunosuppression Therapy ,030219 obstetrics & reproductive medicine ,Multidisciplinary ,medicine.diagnostic_test ,business.industry ,Uterus ,Abdominal aorta ,External iliac artery ,Tissue Donors ,Surgery ,Transplantation ,Macaca fascicularis ,chemistry ,030220 oncology & carcinogenesis ,Models, Animal ,Angiography ,cardiovascular system ,Female ,business ,Indocyanine green - Abstract
No study has reported an animal model of uterus transplantation (UTx) using cynomolgus macaques. We aimed to establish a surgical technique of allogeneic UTx assuming the recovery of a uterus from a deceased donor in cynomolgus macaques. Four allogeneic UTxs were performed in female cynomolgus macaques. Donor surgeries comprised en bloc recovery of organs with iliac vessels on both sides, and/or abdominal aorta/vena cava after sufficient perfusion from one femoral artery or external iliac artery. Before perfusion, 150 mL of whole blood was obtained from the donor for subsequent blood transfusion to the recipient. Four uterine grafts were orthotopically transplanted to recipients. End-to-side anastomosis was performed to the iliac vessels on one side in case 1 and iliac vessels on both sides in case 2; aorto-aorto/cavo-caval anastomosis was performed in cases 3 and 4. Arterial blood flow of the uterine grafts was determined by intraoperative indocyanine green (ICG) angiography. ICG angiography results showed sufficient blood flow to all uterine grafts, and anaemia did not progress. Under appropriate immune suppression, all recipients survived for more than 90 days post-transplantation, without any surgical complications. We describe a surgical technique for allogeneic UTx in cynomolgus macaques.
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- 2016
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9. Hematological and pathological features of massive hepatic necrosis in two radiated tortoises (Astrochelys radiata)
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Nobuhide, Kido, Iori, Itagaki, Daisuke, Kiryu, Tomoko, Omiya, and Kaori, Ono
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Liver Cirrhosis ,massive hepatic necrosis ,radiated tortoise ,Wildlife Science ,serum biochemical value ,Alkaline Phosphatase ,Note ,Turtles ,Fatal Outcome ,Leukocytes ,Animals ,Female ,Aspartate Aminotransferases ,Astrochelys radiate - Abstract
Two radiated tortoises (Astrochelys radiata) exhibited anorexia and hypokinesia. In both cases, hematological and serum biochemical examinations revealed high alkaline phosphatase levels, moderately high aspartate aminotransferase levels and white blood cell counts approximately within the normal range. Despite being treated, the tortoises died 9 and 43 days after the first clinical examination. Gross pathological examinations revealed that the livers of both animals were extremely swollen and contained pale yellow necrotic tissue. Histopathological assessment revealed that the livers contained a massive area of hepatic necrosis surrounded by migration of macrophages and multinucleated giant cells. In one of the cases, severe fibrosis was observed. The present study provides reference information for similar cases in the future.
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- 2016
10. Watershed infarcts in a multiple microembolic model of monkey
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Fumiko Ono, Kayo Adachi, Takakuni Maki, Hidefumi Ito, Masafumi Ihara, Hideaki Wakita, Mitsuhito Mase, Ryosuke Takahashi, Naoyuki Saito, Iori Itagaki, and Hidekazu Tomimoto
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Male ,Pathology ,medicine.medical_specialty ,education ,Hemodynamics ,Macaque monkey ,Fluid-attenuated inversion recovery ,Macaque ,Microcirculation ,Pathogenesis ,Embolic ,medicine.artery ,biology.animal ,Watershed infarct ,medicine ,Animals ,Hemodynamic ,cardiovascular diseases ,medicine.diagnostic_test ,biology ,Cerebral infarction ,business.industry ,General Neuroscience ,Magnetic resonance imaging ,Cerebral Infarction ,medicine.disease ,Magnetic Resonance Imaging ,Disease Models, Animal ,Macaca fascicularis ,Intracranial Embolism ,Acute Disease ,Chronic Disease ,cardiovascular system ,Internal carotid artery ,business - Abstract
It has long been debated whether watershed infarcts are caused by hemodynamic or embolic mechanisms. In the present study, we investigated microembolic roles in the pathogenesis of watershed infarcts by examining MRI in a macaque monkey model of multiple microinfarcts. 50 μm microbeads were injected into each internal carotid artery twice with a month interval. Monkeys (n=4) injected with 2250-2800 microbeads per unilateral side showed both cortical and internal watershed infarcts in the acute phase and atrophic changes with microbleeds in the chronic phase. These results suggest embolic pathogenesis can contribute to the genesis of both cortical and internal watershed infarcts in primates.
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- 2011
11. The effect of an aldose reductase inhibitor (Epalrestat) on diabetic nephropathy in rats
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Iori Itagaki, Kazuhiko Ebata, Yukio Shigeta, Yoshihisa Kamanaka, Masakazu Haneda, Kiyoshi Shimizu, and Ryuichi Kikkawa
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Blood Glucose ,Male ,medicine.medical_specialty ,Rhodanine ,Endocrinology, Diabetes and Metabolism ,Renal function ,Enzyme-Linked Immunosorbent Assay ,Kidney ,Diabetes Mellitus, Experimental ,Renal Circulation ,Diabetic nephropathy ,Rats, Sprague-Dawley ,chemistry.chemical_compound ,Endocrinology ,Polyol pathway ,Aldehyde Reductase ,Internal medicine ,Diabetes mellitus ,Internal Medicine ,medicine ,Albuminuria ,Animals ,Diabetic Nephropathies ,Epalrestat ,business.industry ,Body Weight ,General Medicine ,Organ Size ,medicine.disease ,Streptozotocin ,Aldose reductase inhibitor ,Glomerular Mesangium ,Rats ,chemistry ,Renal blood flow ,Thiazolidines ,business ,medicine.drug ,Glomerular Filtration Rate - Abstract
In order to clarify the possible contribution of the abnormal polyol pathway to the development of diabetic nephropathy, the effect of aldose reductase inhibitor on renal function and morphology was examined in streptozotocin (STZ)-induced diabetic rats. Six months after STZ injection, glomerular filtration rate and renal plasma flow showed marked decline with significant increase in nuclear-free mesangial area (MA) and relative mesangial area (RMA; MA per glomerular area) in diabetic rats. Oral administration of an aldose reductase inhibitor, Epalrestat, prevented renal hypofunction and mesangial expansion in diabetic rats without influencing the levels of blood glucose. These results suggest that the abnormal polyol pathway in diabetic rats is closely related to the development of mesangial expansion, a morphologic representative of diabetic glomerulopathy, and renal hypofunction.
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- 1994
12. Spontaneous histogenic tumors of epididymis observed in B6C3F1 mice
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Keisuke Shinomiya, Iori Itagaki, and Masaharu Tanaka
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Epididymis ,Male ,Pathology ,medicine.medical_specialty ,General Veterinary ,Uterus ,Mice, Inbred Strains ,Sarcoma ,Biology ,Histiocytic sarcoma ,medicine.disease ,Malignancy ,Mice ,medicine.anatomical_structure ,Sex Factors ,Testicular Neoplasms ,Xanthofibroma ,Uterine Neoplasms ,medicine ,Animals ,Female ,Carcinogen ,Histiocyte - Abstract
Four primary histiogenic tumors of the epididymis were discovered in 110 male B6C3F1 mice used in a carcinogenicity study in our laboratory. From the results, all these tumors were considered to be spontaneous. Histologically, the tumors were characterized by compact growth of spindle to oval shaped histiocytic cells with or without a cleaved nucleus. Focal hemorrhage was present in three cases, and erythrophagocytosis occurred in such lesions. The tumors had some similar histological features of histiocytic sarcomas, which had been observed with high malignancy in other male and female animals. However, systemic growth and atypism of neoplastic cells found in the histiocytic sarcomas were not observed in these epididymal tumors. On the other hand, four histiogenic tumors of the uterus, with features characteristic of epididymal tumors, were observed in 106 female mice. The uterine histiogenic tumors were regarded as benign or precursor lesions of histiocytic sarcoma. Furthermore, it is suspected that histiocytic sarcoma arises from the epididymis.
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- 1993
13. Chordoma with Osseous Element in a F344 Rat
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Tsuneo Fujita, Yoshiya Aze, Kouji Shimouchi, Iori Itagaki, Makiko Narita, and Masaharu Tanaka
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Male ,Pathology ,medicine.medical_specialty ,Spinal Neoplasms ,General Veterinary ,F344 rats ,Anatomy ,Biology ,Bone tissue ,medicine.disease ,Rats, Inbred F344 ,Rats ,Metastasis ,Fibrous stroma ,medicine.anatomical_structure ,Chordoma ,medicine ,Hepatic stellate cell ,Animals ,Sacrococcygeal Region ,Retroperitoneal Neoplasms ,Vertebral column - Abstract
Chordoma occurred in the sacrococcygeal region of the vertebral column of a 97-week old male control F344 rat. Macroscopically, it was a mass (20 mm in diameter) protruding into the retroperitoneum and the cut surface was white to dark-reddish and showed a gelatinous appearance. Histologically, the tumor was composed of physaliphorous and stellate cells growing in nests or cords and divided into lobules by a thin fibrous stroma. The tumor cells locally invaded adjacent tissues, but no metastasis to other organs was noted. Centrally, the tumor often had islands of bone that entrapped physaliphorous cells and the bone tissue consisted of well-differentiated osteocytes. Based on these findings, this tumor was diagnosed as chordoma with osseous element.
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- 1993
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14. Cellular injury and lipid peroxidation induced by hexavalent chromium in isolated rat hepatocytes
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Iori Itagaki, Yoshinori Furukawa, Shunji Ueno, Katuhiro Aikawa, and Nobuyuki Susa
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Chromium ,Male ,chemistry.chemical_classification ,biology ,Thiobarbituric acid ,Glutathione peroxidase ,Glutathione reductase ,Rats, Inbred Strains ,General Medicine ,Glutathione ,In Vitro Techniques ,Ascorbic acid ,Rats ,Lipid peroxidation ,chemistry.chemical_compound ,Liver ,chemistry ,Biochemistry ,Catalase ,biology.protein ,Animals ,Potassium Dichromate ,Lipid Peroxidation ,Peroxidase - Abstract
In order to elucidate the relationship between cellular injury and lipid peroxidation induced by hexavalent chromium (CrVI), isolated rat hepatocytes treated with any one of scavengers of active oxygen species, antioxidants or antichromium agent were incubated with K2Cr2O7 as CrVI (1 mM Cr). After the incubation, the development of lipid peroxidation was determined as thiobarbituric acid (TBA)-reacting materials in total lipid extracts from the incubated hepatocytes. Cellular injury was observed as a leakage of lactate dehydrogenase (LDH) from hepatocytes into incubation medium. The contents of reduced glutathione (GSH) in hepatocytes were also assessed. Results obtained were as follows: (1) CrVI facilitated lipid peroxidation in isolated hepatocytes after 20 min of incubation. On the other hand, the cellular injury induced by CrVI was barely observed even after 60 min of incubation. (2) The CrVI-induced lipid peroxidation was inhibited by catalase and mannitol as scavengers of active oxygen species, or N,N'-diphenyl-p-phenylenediamine and alpha-tocopherol as antioxidants. However the cytotoxicity of CrVI could not be prevented by these chemicals. (3) CrVI depleted the contents of intracellular GSH and diminished the activities of glutathione reductase (GR) and glutathione-S-transferase (GST) except glutathione peroxidase. (4) The scavengers of active oxygen species and the antioxidants could not prevent the depletion of intracellular GSH induced by CrVI. (6) Ascorbic acid, antichromium agent, prevented all of the lipid peroxidation, the cellular injury and intracellular GSH depletion induced by CrVI.(ABSTRACT TRUNCATED AT 250 WORDS)
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- 1989
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15. Effect of chromium on lipid peroxidation in isolated rat hepatocytes
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Yuka Takashima, Nobuyuki Susa, Iori Itagaki, Shunji Ueno, Katuhiro Aikawa, Yoshinori Furukawa, and Takeshi Komiyama
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Chromium ,Male ,Lipid Peroxides ,Chromium Compounds ,L-Lactate Dehydrogenase ,Thiobarbituric acid ,chemistry.chemical_element ,Rats, Inbred Strains ,General Medicine ,Glutathione ,Rats ,Lipid peroxidation ,chemistry.chemical_compound ,chemistry ,Biochemistry ,Liver ,Lactate dehydrogenase ,Animals ,Hexavalent chromium ,Incubation ,Cells, Cultured - Abstract
To study the effects of hexavalent and trivalent chromium on lipid peroxidation, isolated rat hepatocytes were incubated with different concentrations of chromium compounds at 37°C for 60min. Lipid peroxidation was determined as thiobarbituric acid (TBA)-reacting materials. Cellular injury was observed as a leakage of lactate dehydrogenase (LDH) from hepatocytes into incubation medium. The contents of reduced glutathione(GSH) in hepatocytes were also assessed. Results obtained were as follows: (1) Lipid peroxidation of isolated rat hepatocytes which was expressed as TBA-reactant formation was inhibited by trivalent chromium at the range of concentrations tested in this experiment (125∼1000μM). Hexavalent one inhibited lipid peroxidation at low concentration (125μM), but facilitated that at high concentration (1000μM). (2) LDH-leakage was facilitated by the addition of hexavalent chromium (K2Cr2O7, 125∼1000μM), on the other hand trivalent one (Cr(NO3)3) inhibited it significantly at concentrations more than 250μM. (3) The hexavalent chromium-induced lipid peroxidation was inhibited by antioxidants such as N, N'-dipheyl-p-phenylenediamine (DPPD), α-tocopherol and diethyl dithiocarbamate (DDTC). However, LDH-leakage from hepatocytes was not inhibited by these antioxidants. (4) After the pretreatment with GSH depleting agent such as diethyl maleate (DEM) on isolated hepatocytes, the lipid peroxidation induced by hexavalent chromium was significantly enhanced and was dependent on the chromium concentrations in the incubation medium. Furthermore this enhancement of lipid peroxidation was canceled by the addition of GSH (10mM). (5) The lipid peroxidation induced by ascorbate was significantly inhibited by the addition of hexavalent chromium as well as trivalent one. This effect of hexavalent chromium might be essentially due to the reduction of hexavalent chromium to trivalent one by ascorbate. These results suggest that chromium in trivalent form inhibits lipid peroxidation in isolated hepatocytes, while hexavalent one facilitates it but is not necessarily correlated to cellular injury.
- Published
- 1988
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