101 results on '"Nishii, Naohito"'
Search Results
2. Effect of age, sex, and breed on serum cystatin C and creatinine concentrations in dogs
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Iwasa, Naoki, Takashima, Satoshi, Iwasa, Tatsuo, Kumazawa, Rie, Nomura, Saki, Asami, Sara, Shimizu, Mamu, Kobatake, Yui, and Nishii, Naohito
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- 2022
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3. PCR-based genotyping assays to detect germline APC variant associated with hereditary gastrointestinal polyposis in Jack Russell terriers
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Yoshizaki, Kyoko, Hirata, Akihiro, Matsushita, Hiroyuki, Nishii, Naohito, Kawabe, Mifumi, Mori, Takashi, and Sakai, Hiroki
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- 2021
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4. Evaluation of muscle mass and intramuscular fatty infiltration in dogs with hypercortisolism and their association with prognosis.
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Yoshida, Kei, Kobatake, Yui, Takashima, Satoshi, and Nishii, Naohito
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MUSCLE mass ,DOGS ,CUSHING'S syndrome ,MUSCULAR atrophy ,COMPUTED tomography - Abstract
Background: Muscle atrophy and intramuscular fatty infiltration, as well as their association with prognosis, have not been quantified in dogs with spontaneous hypercortisolism (HC). Objective: To quantitatively evaluate muscle atrophy and IM fatty infiltration in dogs with HC and determine their prognostic impact. Animals: Fifty‐three dogs with HC and 66 control dogs without HC. Methods: Retrospective cohort study. Medical records and computed tomography images obtained between 2014 and 2021 were evaluated. Kaplan‐Meier curves and log‐rank tests were used to analyze the effect of muscle atrophy and IM fatty infiltration on the prognosis of dogs with HC. Results: Dogs with HC showed lower visually measured cross‐sectional area (VCSA) and cross‐sectional area based on attenuation (HCSA) than control dogs (median [interquartile range {IQR}]: 50.3 mm2/mm [36.2‐67.8] vs 66.7 mm2/mm [48.0‐85.9]; P <.001; 30.4 mm2/mm [13.7‐57.2] vs 54.8 mm2/mm [39.7‐71.5]; P <.001, respectively). Dogs with HC had lower epaxial muscle attenuation (L3HU) than control dogs (median [IQR]: 21.2 Hounsfield [HU] [12.4‐28.2] vs 33.2 HU [22.6‐43.6]; P <.001). Dogs with HC with lower HCSA or L3HU had shorter survival (median [IQR]: 670 days [222‐673] vs 949 days [788‐1074], P <.01; 523 days [132‐670] vs 949 days [756‐1074], P <.01, respectively) but not lower VCSA (median [IQR]: 673 days [132‐788] vs 949 days [523 to not applicable]; P =.30). Conclusion and Clinical Importance: Hypercortisolism in dogs causes muscle atrophy and IM fatty infiltration and is associated with poor prognosis. [ABSTRACT FROM AUTHOR]
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- 2024
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5. Serum cystatin C concentration measured routinely is a prognostic marker for renal disease in dogs
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Iwasa, Naoki, Takashima, Satoshi, Iwasa, Tatsuo, Iwasa, Kazuko, Suzuki, Tomomi, Kobatake, Yui, Kitagawa, Hitoshi, and Nishii, Naohito
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- 2018
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6. Intravenous infusion of amino acids in dogs attenuates hypothermia during anaesthesia and stimulates insulin secretion
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Takashima, Satoshi, Shibata, Sanae, Yamada, Kazuto, Ogawa, Mizuho, Nishii, Naohito, and Kitagawa, Hitoshi
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- 2016
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7. Identification of a CD4 variant in Microminipigs not detectable with available anti-CD4 monoclonal antibodies
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Matsubara, Tatsuya, Nishii, Naohito, Takashima, Satoshi, Takasu, Masaki, Imaeda, Noriaki, Aiki-Oshimo, Kayo, Yamazoe, Kazuaki, Kametani, Yoshie, Ando, Asako, and Kitagawa, Hitoshi
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- 2015
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8. Natural anti-insulin autoantibodies in cats: Enzyme-linked immunosorbent assay for the determination of plasma anti-insulin IgG and its concentrations in domestic cats
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Takashima, Satoshi, Nishii, Naohito, Hachisu, Tatsuyuki, Kojima, Masaaki, Kigure-Hoshino, Megumi, Ogawa, Shizuko, Suzuki, Takafumi, Iwasawa, Atsushi, Ohba, Yasunori, and Kitagawa, Hitoshi
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- 2013
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9. Prognostic value of serum cystatin C concentration in dogs with myxomatous mitral valve disease.
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Iwasa, Naoki, Kumazawa, Rie, Nomura, Saki, Shimizu, Mamu, Iwata, Munetaka, Hara, Mayuka, Kawabe, Mifumi, Kobatake, Yui, Takashima, Satoshi, and Nishii, Naohito
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CYSTATIN C ,MITRAL valve ,DOGS ,PROGNOSIS ,LOG-rank test ,CREATININE - Abstract
Background: Impaired renal function is 1 of the poor prognostic factors in dogs with myxomatous mitral valve disease (MMVD). However, the value of cystatin C (Cys‐C), a marker of renal function, as a prognostic marker for MMVD in dogs has not yet been explored. Objective: This study aims to investigate the prognostic value of Cys‐C in dogs with MMVD. Animals: Fifty client‐owned small‐breed dogs with MMVD were included in this study. Methods: This is a retrospective, cross‐sectional study. The prognostic value of serum Cys‐C concentration was assessed using univariable and multivariable Cox hazard regression analyses. Kaplan‐Meier survival curves for MMVD‐specific survival in dogs stratified into high and low Cys‐C groups were generated and analyzed using the log‐rank test. Results: Serum Cys‐C concentrations were significantly associated with MMVD‐related death (P <.01) in both univariable (hazard ratio [HR], 5.086; 95% confidence interval [CI], 1.950‐13.270) and multivariable Cox hazard regression analysis (HR, 4.657; 95% CI, 1.767‐12.270). The high Cys‐C group (n = 14) had a significantly shorter MMVD‐specific survival time than the low Cys‐C group (n = 36; P <.01). In dogs with normal blood creatinine concentrations, the high Cys‐C group (n = 10) had a significantly shorter MMVD‐specific survival time than the low Cys‐C group (n = 36; P <.01). Conclusions and Clinical Importance: High serum Cys‐C concentrations were associated with a worse prognosis of MMVD. Furthermore, serum Cys‐C could be a predictor of MMVD prognosis even in dogs with normal blood creatinine concentration. [ABSTRACT FROM AUTHOR]
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- 2023
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10. Molecular Mechanisms of Aggregation of Canine SOD1 E40K Amyloidogenic Mutant Protein.
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Wakayama, Kento, Kimura, Shintaro, Kobatake, Yui, Kamishina, Hiroaki, Nishii, Naohito, Takashima, Satoshi, Honda, Ryo, and Kamatari, Yuji O.
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MUTANT proteins ,AMYOTROPHIC lateral sclerosis ,AMINO acid residues ,AMYLOID beta-protein ,SUPEROXIDE dismutase ,STRUCTURAL stability ,NEURODEGENERATION - Abstract
Canine degenerative myelopathy (DM) is a human amyotrophic lateral sclerosis (ALS)-like neurodegenerative disease. It is a unique, naturally occurring animal model of human ALS. Canine DM is associated with the aggregation of canine superoxide dismutase 1 (cSOD1), which is similar to human ALS. Almost 100% of cases in dogs are familial, and the E40K mutation in cSOD1 is a major causative mutation of DM. Therefore, it is important to understand the molecular mechanisms underlying cSOD1(E40K) aggregation. To address this, we first analyzed the structural model of wild type cSOD1. Interactions were evident between amino acid E40 and K91. Therefore, the mutation at residue E40 causes loss of the interaction and may destabilize the native structure of cSOD1. Differential scanning fluorimetry revealed that the E40K mutant was less stable than the wild type. Moreover, stability could be recovered by the E40K and K91E double mutation. Acceleration of amyloid fibril formation in vitro and aggregate formation in cells of cSOD1(E40K) was also suppressed by the introduction of this double mutation in thioflavin T fluorescence assay results and in transfectant cells, respectively. These results clearly show the importance of the interaction between amino acid residues E40 and K91 in cSOD1 for the stability of the native structure and aggregation. [ABSTRACT FROM AUTHOR]
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- 2023
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11. Assignment of the SLA alleles and reproductive potential of selective breeding Duroc pig lines
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Soe, Ok Kar, Ohba, Yasunori, Imaeda, Noriaki, Nishii, Naohito, Takasu, Masaki, Yoshioka, Gou, Kawata, Hisako, Shigenari, Atsuko, Uenishi, Hirohide, Inoko, Hidetoshi, Ando, Asako, and Kitagawa, Hitoshi
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- 2008
12. Relationship between anti-insulin antibody production and severe insulin resistance in a diabetic cat.
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KOMIYA, Takumi, MORI, Akihiro, NISHII, Naohito, ODA, Hitomi, ONOZAWA, Eri, SEKI, Seri, and SAKO, Toshinori
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INSULIN antibodies ,ANTIBODY formation ,INSULIN resistance ,DIABETIC acidosis ,GLYCEMIC control ,KETOACIDOSIS - Abstract
A 5-year-old castrated male domestic shorthair cat was diagnosed with diabetic ketoacidosis and severe insulin resistance. Although the conventional treatment for diabetic ketoacidosis was provided, the cat required frequent hospitalization because of severe dehydration and repeated diabetic ketoacidosis. We detected anti-insulin antibodies for human in this cat. Serum insulin-binding IgG levels were markedly elevated compared with those in healthy cats and other diabetic cats. We initiated prednisolone to suppress the effects of anti-insulin antibodies. After initiation of prednisolone, the cat was gradually recovered with increasing activity and appetite. Furthermore, satisfactory glycemic control was achieved with combined subcutaneous injection of insulin detemir and insulin degludec. [ABSTRACT FROM AUTHOR]
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- 2021
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13. Familial adenomatous polyposis in dogs: hereditary gastrointestinal polyposis in Jack Russell Terriers with germline APC mutations.
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Yoshizaki, Kyoko, Hirata, Akihiro, Nishii, Naohito, Kawabe, Mifumi, Goto, Minami, Mori, Takashi, and Sakai, Hiroki
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ADENOMATOUS polyposis coli ,DOGS ,GERM cells ,DOG diseases ,COLON polyps ,ADENOMATOUS polyps ,DESMOID tumors - Abstract
Many hereditary disorders in dogs have equivalents in humans and thus attract attention as natural animal models. Breed predisposition to certain diseases often provides promising clues to explore novel hereditary disorders in dogs. Recently, cases of gastrointestinal (GI) polyps in Jack Russell Terriers (JRTs) have increased in Japan. In 21 affected JRTs, polyps were found in either or both the stomach and colorectum, with a predilection for the gastric antrum and rectum. Multiple polyps were found in 13 of 21 examined dogs, including 5 dogs with both gastric and colorectal polyps. Some dogs were found to have GI polyps at an early age, with the youngest case being 2.3 years old. Histopathologically, 43 of 46 GI polyps (93.5%) were diagnosed as adenomas or adenocarcinomas. Immunohistochemical analysis revealed cytoplasmic and nuclear accumulation of β-catenin in the tumor cells. As in the case of human patients with familial adenomatous polyposis, all examined JRTs with GI polyps (n = 21) harbored the identical heterozygous germline APC mutations, represented by a 2-bp substitution (c.[462A>T; 463A>T]). The latter substitution was a non-sense mutation (p.K155X) resulting in a truncated APC protein, thus suggesting a strong association with this cancer-prone disorder. Somatic mutation and loss of the wild-type APC allele were detected in the GI tumors of JRTs, suggesting that biallelic APC inactivation was involved in tumor development. This study demonstrated that despite differences in the disease conditions between human and dog diseases, germline APC mutation confers a predisposition to GI neoplastic polyps in both dogs and humans. [ABSTRACT FROM AUTHOR]
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- 2021
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14. Evaluation of monitoring methods in asymptomatic dogs with high serum cystatin C concentrations.
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IWASA, Naoki, TAKASHIMA, Satoshi, IWASA, Tatsuo, IWASA, Kazuko, SUZUKI, Tomomi, KUMAZAWA, Rie, NOMURA, Saki, KOBATAKE, Yui, KITAGAWA, Hitoshi, and NISHII, Naohito
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CHRONIC kidney failure ,EVALUATION methodology ,DOGS ,VETERINARY hospitals ,SERUM - Abstract
This study evaluated the monitoring methods in asymptomatic dogs with high serum cystatin C (Cys-C) concentrations. Ten dogs with high serum Cys-C were divided into two groups based on the owner's choice; one receiving clinical pathology-based monitoring at an animal hospital specialised in chronic kidney disease, and the other receiving symptom-based monitoring at home, partly because they showed no clinical symptoms. The dogs that received the clinical pathology-based monitoring led to an early treatment intervention, resulted in a longer survival period than dogs received the symptom-based monitoring (P<0.05). It became clear that early treatment intervention by clinical pathology-based monitoring extends the renal survival period even in asymptomatic dogs with increased serum Cys-C concentrations. [ABSTRACT FROM AUTHOR]
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- 2019
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15. 黒毛和種牛の死産/周産期虚弱子牛症候群における胸腺形成不全(臨床繁殖学)
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TAKASU, Masaki, SHIROTA, Kinji, OHBA, Yasunori, NISHII, Naohito, MURASE, Tetsuma, MIYAZAWA, Kiyoshi, and KITAGAWA, Hitoshi
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- 2008
16. ガスクロマトグラフィー/マススペクトロメトリーによって診断されたオロット酸尿症の黒毛和種牛の1例(内科学)
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OHBA, Yasunori, TAKASU, Masaki, NISHII, Naohito, HOSODA, Iwai, KITOH, Katsuya, MATSUMOTO, Isamu, ZHANG, Chunhua, and KITAGAWA, Hitoshi
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- 2007
17. 家系の異なる発育不良の黒毛和種牛における内分泌機能(内科学)
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TAKASU, Masaki, HAGIWARA, Youko, OHBA, Yasunori, NISHII, Naohito, HOSODA, Iwai, KITOH, Katsuya, KATOH, Kazuo, and KITAGAWA, Hitoshi
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- 2005
18. 尿細管形成不全のウシにおける血清の成長ホルモンとインスリン様成長因子-1濃度(内科学)
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NISHII, Naohito, OHBA, Yasunori, TAKASU, Masaki, KATOH, Kazuo, KITOH, Katsuya, SASAKI, Yoshihide, and KITAGAWA, Hitoshi
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- 2005
19. グルコース負荷試験において低いインスリン分泌反応を示した発育不良の黒毛和種牛(内科学)
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TAKASU, Masaki, OHBA, Yasunori, HAGIWARA, Youko, HOSODA, Iwai, NISHII, Naohito, KITOH, Katsuya, MIYAZAWA, Kiyoshi, and KITAGAWA, Hitoshi
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- 2005
20. Body and major organ sizes of young mature microminipigs determined by computed tomography.
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Takasu, Masaki, Tsuji, Eriko, Imaeda, Noriaki, Matsubara, Tatsuya, Maeda, Masami, Ito, Yusuke, Shibata, Sanae, Ando, Asako, Nishii, Naohito, Yamazoe, Kazuaki, and Kitagawa, Hitoshi
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COMPUTED tomography ,BEAGLE (Dog breed) ,ANIMAL morphology ,MEDICAL research ,LABORATORY swine - Abstract
To understand the anatomical characteristics of microminipigs, one of the smallest miniature pigs, as a large animal model, we measured the body and organ sizes of four-, five-, six-, and seven-month-old microminipigs (n = 4, females) using computed tomography. In addition, the results were compared with those of young mature beagles (10 months old, two males and three females), which have been widely used as a large animal model. The microminipigs at 4–6 months of age were much smaller than the beagles. However, when the microminipigs reached seven months of age, their overall size was similar to that of the beagles. The thoracic cavity volume of the seven-month-old microminipigs was less than half that of the beagles, and the cavity was largely filled by the heart. The liver size of the seven-month-old microminipigs was approximately half of that of the beagles. Moreover, the spleen of the seven-month-old microminipigs was different in morphology, but not different in size from that of the beagles. In addition, although their volumes were the same, the kidneys of the seven-month-old microminipigs, unlike those of the beagles, were flattened in shape. Collectively, the major abdominal organs of the seven-month-old microminipigs were either the same size or smaller than those of the beagles, but the abdominal cavity volume of the seven-month-old microminipigs was larger than that of the beagles. Thus, the abdominal cavity of microminipigs is assumed to be filled with the gastrointestinal tract. The anatomical characteristics of the young mature microminipigs revealed in our study suggest that microminipigs could have great potential as a large animal model for biomedical research. [ABSTRACT FROM AUTHOR]
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- 2015
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21. Enterolithiasis in a cat
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Yuki, Masashi, Sugimoto, Noriko, Takahashi, Kuniaki, Ohtsuka, Hiromi, Nishii, Naohito, and Suzuki, Kiyomi
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- 2006
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22. Insulin Responses to Administrations of Amino Acids and Fatty Acids in Healthy Cats.
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Yasuda, Kyoji, Takashima, Satoshi, Takagi, Mitsuru, Nishii, Naohito, Ohba, Yasunori, and Kitagawa, Hitoshi
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CATS ,INSULIN ,LEUCINE ,ARGININE ,ALANINE ,FATTY acids - Abstract
The article presents a study which examines the changes in plasma glucose and insulin concentrations after intravenous administration of amino acids and fatty acids in healty cats to compare the stimulation ability of insulin secretion. The authors state that arginine had a strong insulinotropic effect while leucine, alanine, and fatty acids had weak ones. They conclude that intravenous arginine tolerance test may be useful for estimation of insulin response in cats.
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- 2011
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23. Cloning, expression and investigation for polymorphisms of canine peroxisome proliferator-activated receptors
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Nishii, Naohito, Takasu, Masaki, Soe, Ok Kar, Maeda, Sadatoshi, Ohba, Yasunori, Inoue-Murayama, Miho, and Kitagawa, Hitoshi
- Subjects
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GENETIC polymorphisms , *DOGS , *PEROXISOMES , *CLONING , *GENE expression , *LIPID metabolism - Abstract
Abstract: Peroxisome proliferator-activated receptors (PPARs) are ligand-activated transcription factors implicated in lipid metabolism. In this study, the full-length cDNA of canine PPARβ and γ were sequenced, and expression of PPARs was evaluated in normal tissues and primary cultures of adipocytes in dogs, followed by investigations for polymorphisms of canine PPARγ. Comparison of the deduced amino acid sequences of canine PPARβ and γ cDNA with that of human PPARβ and γ cDNA revealed 95.9% and 98.2% identity, respectively. PPARβ expression was ubiquitous and high PPARγ expression was detected in the subcutaneous and omental adipose tissues, spleen and large intestine. Canine PPARγ mRNA expression in cultured adipocytes began to increase from 4 days after induction of differentiation, and increased nearly ninefold within 10 days after induction of differentiation. Although expression level of PPARα was low in the cultured adipocytes, it slightly increased within 10 days. In contrast, expression of PPARβ showed only small variations during adipocyte differentiation, though expression levels were relatively high. These results suggest that PPARγ may play an important role in adipocyte differentiation in dogs. Investigations for polymorphisms of PPARγ revealed a silent polymorphism, C1362T, in 3 of 92 dogs. [Copyright &y& Elsevier]
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- 2007
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24. Postprandial changes in leptin concentrations of cerebrospinal fluid in dogs during development of obesity.
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Nishii, Naohito, Nodake, Hiroyuki, Takasu, Masaki, Soe, Okkar, Ohba, Yasunori, Maeda, Sadatoshi, Ohtsuka, Yoshihiko, Honjo, Tsutomu, Saito, Masayuki, and Kitagawa, Hitoshi
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BEAGLE (Dog breed) , *DOGS , *OBESITY , *ANIMAL diseases , *LEPTIN - Abstract
Objective--To evaluate postprandial changes in the leptin concentration of CSF in dogs during development of obesity. Animals--male Beagles. Procedures--Weight gain was induced and assessments were made when the dogs were in thin, optimal, and obese body conditions (BCs). The fat area at the level of the L3 vertebra was measured via computed tomography to assess the degree of obesity. Dogs were evaluated in fed and unfed states. Dogs in the fed state received food at 9 AM. Blood and CSF samples were collected at 8 AM, 4 PM, and 10 PM. Results--Baseline CSF leptin concentrations in the thin, optimal, and obese dogs were 24.3 ± 2.7 pg/mL, 86.1 ± 14.7 pg/mL, and 116.2 ± 47.3 pg/mL, respectively. In the thin BC, CSF leptin concentration transiently increased at 4 PM. In the optimal BC, baseline CSF leptin concentration was maintained until 10 PM. In the obese BC, CSF leptin concentration increased from baseline value at 4 PM and 10 PM. Correlation between CSF leptin concentration and fat area was good at all time points. There was a significant negative correlation between the CSF leptin concentration- to-serum leptin concentration ratio and fat area at 4 PM; this correlation was not significant at 8 AM and 10 PM. Conclusions and Clinical Relevance--Decreased transport of leptin at the blood-brain barrier may be 1 mechanism of leptin resistance in dogs. However, leptin resistance at the blood-brain barrier may not be important in development of obesity in dogs. [ABSTRACT FROM AUTHOR]
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- 2006
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25. Effects of administration of glucocorticoids and feeding status on plasma leptin concentrations in dogs.
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Nishii, Naohito, Takasu, Masaki, Ohba, Yasunori, Maeda, Sadatoshi, Kitoh, Katsuya, Ohtsuka, Yoshihiko, Honjo, Tsutomu, Saito, Masayuki, and Kitagawa, Hitoshi
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GLUCOCORTICOIDS , *SERUM , *LEPTIN , *INSULIN , *CORTISONE , *LABORATORY dogs , *VETERINARY endocrinology , *VETERINARY medicine - Abstract
Objective--To investigate effects of short- and long-term administration of glucocorticoids, feeding status, and serum concentrations of insulin and cortisol on plasma leptin concentrations in dogs. Animals--20 nonobese dogs Procedure--For experiment 1, plasma leptin concentrations and serum concentrations of insulin and cortisol were monitored for 24 hours in 4 dogs administered dexamethasone (0.1 mg/kg, IV) or saline (0.9% NaCl) solution for fed and nonfed conditions. For experiment 2, 11 dogs were administered prednisolone (1 mg/kg, PO, q 24 h for 56 days [7 dogs] and 2 mg/kg, PC, q 24 h for 28 days [4 dogs]) and 5 dogs served as control dogs. Plasma leptin and serum insulin concentrations were monitored weekly. Results--For experiment 1, dexamethasone injection with the fed condition drastically increased plasma leptin concentrations. Furthermore, injection of saline solution with the fed condition increased plasma leptin concentrations. These increases in plasma leptin concentrations correlated with increases in serum insulin concentrations. Dexamethasone injection with the nonfed condition increased plasma leptin concentrations slightly but continuously. Injection of saline solution with the nonfed condition did not alter plasma leptin concentrations. For experiment 2, prednisolone administration at either dosage and duration did not alter plasma leptin concentrations in any dogs. Conclusions and Clinical Relevance--Dexamethasone injection and feeding increased plasma leptin concentrations in dogs. In addition, dexamethasone administration enhanced the effect of feeding on increases in plasma leptin concentrations. Daily oral administration of prednisolone (1 or 2 mg/kg) did not affect plasma leptin concentrations in dogs. [ABSTRACT FROM AUTHOR]
- Published
- 2006
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26. Plasma Leptin Concentration in Dogs with Diabetes Mellitus.
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NISHII, Naohito, YAMASAKI, Miho, TAKASU, Masaki, HONJOH, Tsutomu, SHIBATA, Haruki, OTSUKA, Yoshihiko, TAKASHIMA, Satoshi, OHBA, Yasunori, and KITAGAWA, Hitoshi
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LEPTIN ,DOGS ,DIABETES ,PEOPLE with diabetes ,OBESITY in animals ,LABORATORY dogs - Abstract
The article provides information on a study which evaluated the plasma leptin concentration in dogs with diabetes mellitus. A total of 36 dogs, normal and diabetic, were divided into non-obese and obese groups based on body condition score. Plasma leptin concentrations in obese normal dogs were significantly higher than that of the non-obese normal dogs. There was no significant difference between the plasma leptin concentrations of non-obese and obese diabetic dogs. Furthermore, the obese diabetic dogs had significantly lower plasma leptin concentration than that in the obese normal dogs. The results indicate that the plasma leptin concentrations in the diabetic dogs were influenced by factors other than adiposity.
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- 2010
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27. Genetic Association between Swine Leukocyte antigen Class II Haplotypes and Reproduction Traits in Microminipigs.
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Ando, Asako, Imaeda, Noriaki, Matsubara, Tatsuya, Takasu, Masaki, Miyamoto, Asuka, Oshima, Shino, Nishii, Naohito, Kametani, Yoshie, Shiina, Takashi, Kulski, Jerzy K., and Kitagawa, Hitoshi
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ANIMAL litters ,HAPLOTYPES ,BREEDING ,REPRODUCTION ,SWINE ,LEUCOCYTES - Abstract
The effects of swine leukocyte antigen (SLA) molecules on numerous production and reproduction performance traits have been mainly reported as associations with specific SLA haplotypes that were assigned using serological typing methods. In this study, we intended to clarify the association between SLA class II genes and reproductive traits in a highly inbred population of 187 Microminipigs (MMP), that have eight different types of SLA class II haplotypes. In doing so, we compared the reproductive performances, such as fertility index, gestation period, litter size, and number of stillbirth among SLA class II low resolution haplotypes (Lrs) that were assigned by a polymerase chain reaction-sequence specific primers (PCR-SSP) typing method. Only low resolution haplotypes were used in this study because the eight SLA class II high-resolution haplotypes had been assigned to the 14 parents or the progenitors of the highly inbred MMP herd in a previous publication. The fertility index of dams with Lr-0.13 was significantly lower than that of dams with Lr-0.16, Lr-0.17, Lr-0.18, or Lr-0.37. Dams with Lr-0.23 had significantly smaller litter size at birth than those with Lr-0.17, Lr-0.18, or Lr-0.37. Furthermore, litter size at weaning of dams with Lr-0.23 was also significantly smaller than those dams with Lr-0.16, Lr-0.17, Lr-0.18, or Lr-0.37. The small litter size of dams with Lr-0.23 correlated with the smaller body sizes of these MMPs. These results suggest that SLA class II haplotypes are useful differential genetic markers for further haplotypic and epistatic studies of reproductive traits, selective breeding programs, and improvements in the production and reproduction performances of MMPs. [ABSTRACT FROM AUTHOR]
- Published
- 2019
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28. Long-term management of high-grade atrioventricular block using cilostazol in a cat.
- Author
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Iwasa, Naoki, Nishii, Naohito, Takashima, Satoshi, Kobatake, Yui, Nomura, Saki, Iwasa, Kazuko, Iwasa, Tatsuo, Suzuki, Tomomi, Machida, Noboru, and Kitagawa, Hitoshi
- Published
- 2019
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29. Trismus due to myotonia associated with hyperadrenocorticism in a dog.
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Yokota S, Kobatake Y, Maekawa M, Takashima S, and Nishii N
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- Dogs, Female, Animals, Trismus veterinary, Trismus complications, Adrenocorticotropic Hormone, Myotonia complications, Myotonia veterinary, Dog Diseases diagnosis, Dog Diseases drug therapy, Dog Diseases etiology, Adrenocortical Hyperfunction complications, Adrenocortical Hyperfunction veterinary
- Abstract
We present the report of trismus due to hyperadrenocorticism-associated myotonia diagnosed by electromyography in a dog. An intact female Miniature Dachshund, 13 years and 9 months old, presented with stiff gait and trismus as well as polyuria and polydipsia. Abdominal ultrasonography showed enlarged adrenal glands. An adrenocorticotropic hormone stimulation test revealed an exaggerated response. Based on these findings, this case was diagnosed with hyperadrenocorticism. Electromyography revealed myotonic discharge in the temporalis muscle and limbs. Therefore, trismus was considered to be caused by hyperadrenocorticism-associated myotonia, and the case was treated with oral trilostane (1.3 mg/kg, once daily). During the 4-month follow-up period, despite the partial improvement in stiff gait, trismus did not recover. Long-term data on more cases are warranted to assess the prognosis and clinical characteristics of trismus due to hyperadrenocorticism-associated myotonia.
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- 2023
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30. Molecular Mechanisms of Aggregation of Canine SOD1 E40K Amyloidogenic Mutant Protein.
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Wakayama K, Kimura S, Kobatake Y, Kamishina H, Nishii N, Takashima S, Honda R, and Kamatari YO
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- Dogs, Animals, Humans, Superoxide Dismutase-1 genetics, Mutation, Amino Acids genetics, Mutant Proteins genetics, Superoxide Dismutase metabolism, Amyotrophic Lateral Sclerosis genetics, Amyotrophic Lateral Sclerosis metabolism, Neurodegenerative Diseases metabolism
- Abstract
Canine degenerative myelopathy (DM) is a human amyotrophic lateral sclerosis (ALS)-like neurodegenerative disease. It is a unique, naturally occurring animal model of human ALS. Canine DM is associated with the aggregation of canine superoxide dismutase 1 (cSOD1), which is similar to human ALS. Almost 100% of cases in dogs are familial, and the E40K mutation in cSOD1 is a major causative mutation of DM. Therefore, it is important to understand the molecular mechanisms underlying cSOD1(E40K) aggregation. To address this, we first analyzed the structural model of wild type cSOD1. Interactions were evident between amino acid E40 and K91. Therefore, the mutation at residue E40 causes loss of the interaction and may destabilize the native structure of cSOD1. Differential scanning fluorimetry revealed that the E40K mutant was less stable than the wild type. Moreover, stability could be recovered by the E40K and K91E double mutation. Acceleration of amyloid fibril formation in vitro and aggregate formation in cells of cSOD1(E40K) was also suppressed by the introduction of this double mutation in thioflavin T fluorescence assay results and in transfectant cells, respectively. These results clearly show the importance of the interaction between amino acid residues E40 and K91 in cSOD1 for the stability of the native structure and aggregation.
- Published
- 2022
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31. Urinary liver-type fatty acid-binding protein in two dogs with acquired Fanconi syndrome: A case report.
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Takashima S, Nasu T, Ohata K, Oikawa T, Sugaya T, Kobatake Y, Shibata S, and Nishii N
- Subjects
- Dogs, Animals, Fatty Acid-Binding Proteins urine, Chickens, Liver, Fanconi Syndrome diagnosis, Fanconi Syndrome veterinary, Fanconi Syndrome complications, Glycosuria complications, Glycosuria veterinary, Dog Diseases diagnosis, Dog Diseases etiology
- Abstract
Background: Fanconi syndrome (FS) is defined as multiple defects of the proximal tubules and is diagnosed by clinical symptoms. However, in dogs with FS, the damage in the proximal tubules that is responsible for the clinical symptoms has not been evaluated. Among FS cases, tubular damage in acquired FS is reversible following the elimination of a causative factor. Liver-type fatty acid-binding protein (L-FABP) is a biomarker of tubular damage in various animals including dogs. Urinary L-FABP measurement may be useful for the diagnosis and follow-up evaluation in canine FS., Case Description: At the first visit, two Toy Poodles that had no remarkable findings on physical examination presented with glycosuria without hyperglycemia, hypokalemia, hyperchloremia, increased levels of plasma alkaline phosphatase, and metabolic acidosis. Considering all the factors involved, the dogs were clinically diagnosed with acquired FS. The owner reported that they routinely fed the dog with chicken jerky, a recently considered cause of acquired FS. Following the withdrawal of the jerky, abnormalities including glycosuria improved in both dogs. Moreover, urinary L-FABP levels, which were high at diagnosis, presented a decreasing trend during the follow-up. However, in one dog, the elevated urinary L-FABP level did not return to normal., Conclusion: Although the clinical symptoms of acquired FS in dogs could be improved by the elimination of a causative factor, the severity of tubular damage described by urinary L-FABP may not be necessarily linked to the degree of functional deterioration. Therefore, the evaluation of proximal tubular damage by L-FABP may be of clinical value during the follow-up of acquired FS in canines., Competing Interests: Keiichi Ohata and Tsuyoshi Oikawa are the senior scientists of CMIC Holdings Co., Ltd. (Tokyo, Japan), a company that produces ELISA kits with high sensitivity for L-FABP analysis. They were responsible for validation analyses and measurement of an ELISA. No other potential conflicts of interest relevant to this article are reported.
- Published
- 2022
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32. Quantitative assessment of muscle mass and gene expression analysis in dogs with glucocorticoid-induced muscle atrophy.
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Yoshida K, Matsuoka T, Kobatake Y, Takashima S, and Nishii N
- Subjects
- Animals, Dogs, Gene Expression, Muscle, Skeletal pathology, Muscles pathology, Muscular Atrophy chemically induced, Muscular Atrophy genetics, Muscular Atrophy veterinary, Prednisolone, Dog Diseases chemically induced, Dog Diseases genetics, Dog Diseases metabolism, Glucocorticoids adverse effects
- Abstract
The present study aimed to quantitatively evaluate muscle mass and gene expression in dogs with glucocorticoid-induced muscle atrophy. Five healthy beagles received oral prednisolone for 4 weeks (1 mg/kg/day), and muscle mass was then evaluated via computed tomography. Histological and gene expression analyses were performed using biopsy samples from the biceps femoris before and after prednisolone administration. The cross-sectional area of the third lumbar paraspinal and mid-femoral muscles significantly decreased after glucocorticoid administration (from 27.5 ± 1.9 to 22.6 ± 2.0 cm
2 and from 55.1 ± 4.7 to 50.7 ± 4.1 cm2 , respectively; P<0.01). The fast- and slow-twitch muscle fibers were both atrophied (from 2,779 ± 369 to 1,581 ± 207 μm2 and from 2,871 ± 211 to 1,971 ± 169 μm2 , respectively; P<0.05). The expression of the growth factor receptor-bound protein 10 (GRB10) significantly increased after prednisolone administration (P<0.05). Because GRB10 suppresses insulin signaling and the subsequent mammalian target of rapamycin complex 1 activity, increased expression of GRB10 may have resulted in a decrease in protein anabolism. Taken together, 1 mg/kg/day oral prednisolone for 4 weeks induced significant muscle atrophy in dogs, and GRB10 might participate in the pathology of glucocorticoid-induced muscle atrophy in canines.- Published
- 2022
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33. Stillbirth rates and their association with swine leucocyte antigen class II haplotypes in Microminipigs.
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Imaeda N, Ando A, Matsubara T, Takasu M, Nishii N, Miyamoto A, Ohshima S, Kametani Y, Suzuki S, Shiina T, Ono T, Kulski JK, and Kitagawa H
- Abstract
Objective: Microminipig (MMP) is a miniature pig with an extra small body size for experimental use. In the present study, the occurrence of stillbirths and their genetic association with swine leukocyte antigen (SLA) class II haplotypes were evaluated in a population of MMPs., Methods: The occurrences of stillbirth and genetic association with SLA class II haplotypes using 483 stillborn and 2,246 live piglets, and their parents were compared among the three groups of newborn piglet litters; an all stillborn (AS) group consisting of only stillborn piglet litters, a partial stillborn (PS) group consisting of stillborn and live piglet litters, and an all alive (AA) group consisting of only live piglet litters., Results: The incidence of stillborn piglets was 483/2,729 (17.7%). Distributions of litter sizes, numbers of stillborn piglets in a litter, parities, and gestation periods were distinct among the three groups. The frequencies of low resolution haplotype (Lr)-0.7 or Lr-0.23 were higher in the AS group than in the PS or AA groups. In sires, the frequency of Lr-0.7 associated with the AS group was significantly higher in the AS group than with the AA group. In dams, the frequency of Lr-0.23 was significantly higher in the AS group than in the PS or AA groups, whereas the frequency of Lr-0.7 was not significantly different., Conclusion: The incidence of stillborn piglets in MMPs appears to be higher than those in other pig breeds. Several traits related with stillbirths such as the number of stillborn piglets and parities of the AS group were different from those of the PS and AA groups. Specific SLA class II haplotypes were associated significantly with a high incidence of stillbirths and could be used as genetic markers to adopt breeding strategies to lower the rate of stillbirth in MMPs.
- Published
- 2021
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34. Clinical evaluation of urinary liver-type fatty acid-binding protein for the diagnosis of renal diseases in dogs.
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Takashima S, Nagamori Y, Ohata K, Oikawa T, Sugaya T, Kobatake Y, and Nishii N
- Subjects
- Animals, Biomarkers, Creatinine, Dogs, Fatty Acid-Binding Proteins genetics, Liver, Dog Diseases diagnosis, Kidney Diseases diagnosis, Kidney Diseases veterinary
- Abstract
Liver-type fatty acid-binding protein (L-FABP) is a biomarker for the early detection of renal diseases in humans. L-FABP is a cytotoxic oxidation product secreted from the proximal tubules under ischemic and oxidative stress conditions. First, L-FABP gene expression in the kidney and liver was evaluated. Next, the urinary L-FABP concentrations in dogs with or without renal diseases were measured using a novel enzyme-linked immunosorbent assay kit. Urinary L-FABP was normalized relative to urinary creatinine (uCre) concentrations (µg/g uCre). Finally, the relationships between urinary L-FABP and renal biomarkers used in canine medicine or serum alanine transaminase (ALT) as an indicator of liver damage were examined. Serum and urine samples from 94 client-owned dogs including 23 dogs with renal diseases and 71 dogs without renal diseases were used for analysis. Relative L-FABP gene expression was confirmed both in the liver and kidney. Dogs with renal diseases had a significantly higher urinary L-FABP than those without, and its predictive cutoff value was 26 µg/g uCre. Urinary L-FABP was significantly correlated with serum creatinine (r=0.4674, P<0.01), urea nitrogen (r=0.4907, P<0.01), urine specific gravity (r=-0.5100, P<0.01), and urine protein/creatinine ratio (r=0.7216, P<0.01), but not with serum ALT. Hence, dogs with a high urinary L-FABP value were more likely to have renal diseases.
- Published
- 2021
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35. The Long-Term Clinical Course of Canine Degenerative Myelopathy and Therapeutic Potential of Curcumin.
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Kobatake Y, Nakata K, Sakai H, Sasaki J, Yamato O, Takashima S, Nishii N, Maeda S, Islam MS, and Kamishina H
- Abstract
Canine degenerative myelopathy (DM), recognized as a spontaneous model of amyotrophic lateral sclerosis, is known as a late-onset progressive degenerative disease of the spinal cord. Because of the progressive nature of DM, many dogs are elected to be euthanized, resulting in limited information on the end-stage clinical presentation. We investigated the long-term clinical course from diagnosis to natural death to further deepen our understanding of the entire clinical picture of this disease. Because curcumin was administered in some cases, the therapeutic effect of curcumin on DM was also examined. Forty dogs included in this study were client-owned Pembroke Welsh Corgis with a definitive diagnosis of DM by necropsy and histopathology. Dogs were excluded from this study if they died from another disease or were elected to be euthanized. Information on the long-term clinical symptoms of DM was investigated based on a questionnaire, which was collected from the dog owners. Urinary incontinence and respiratory disorder were observed in most dogs, as was respiratory impairment-correlated death. In contrast, signs consistent with brainstem dysfunction were noticed at the terminal stage in a small portion of dogs. Although further studies with more cases are needed, the results of this study suggest that administration of curcumin is effective in slowing the progression of DM.
- Published
- 2021
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36. Long-term survival of a dog with Alexander disease.
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Kobatake Y, Nishimura N, Sakai H, Iwana S, Yamato O, Nishii N, and Kamishina H
- Subjects
- Animals, Dogs, Female, Magnetic Resonance Imaging veterinary, Spinal Cord, Alexander Disease veterinary, Dog Diseases diagnosis, Nervous System Diseases veterinary
- Abstract
A 1-year- and 11-month-old spayed female toy poodle had showed progressive ataxia and paresis in the hindlimbs since 11 months old. Magnetic resonance imaging revealed high signal intensity on T2-weighted and fluid-attenuated inversion recovery images at the thoracic and lumbar spinal cord. The dog's neurological condition slowly deteriorated and flaccid tetraparesis was exhibited. At 4 years and 11 months old, the dog died of respiratory failure. On postmortem examination, eosinophilic corkscrew bundles (Rosenthal fibers) were observed mainly in the thoracic and lumbar spinal cord. Histological features were comparable to previously reported cases with Alexander disease. This is a first case report to describe the clinical course and long-term prognosis of a dog with Alexander disease.
- Published
- 2020
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37. Long-term management of high-grade atrioventricular block using cilostazol in a cat.
- Author
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Iwasa N, Nishii N, Takashima S, Kobatake Y, Nomura S, Iwasa K, Iwasa T, Suzuki T, Machida N, and Kitagawa H
- Abstract
Case Summary: A 12-year-old neutered female domestic shorthair cat was admitted for syncope. Clinical signs and electrocardiography revealed high-grade atrioventricular (AV) block. Treatment with cilostazol ameliorated the clinical signs and arrhythmia. However, the high-grade AV block recurred on several occasions. After 640 days, the cat presented again with clinical deterioration owing to reoccurrence of the arrhythmia and it died 11 days later. Histopathological examination revealed a loss of conduction cells within the His bundle., Relevance and Novel Information: To our knowledge, this is the first report of high-grade AV block treated with cilostazol in a cat. Treatment with cilostazol prolonged survival for 650 days without pacemaker implantation. Histological findings suggested that the AV block was related to fibrosis of the impulse conduction system., Competing Interests: Conflict of interest: The authors declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article., (© The Author(s) 2019.)
- Published
- 2019
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38. Effect of cyclooxygenase-2 inhibitors at therapeutic doses on body temperature during anesthesia in healthy dogs administered with amino acids.
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Takashima S, Takitani SI, Kitamura M, Nishii N, Kitagawa H, and Shibata S
- Subjects
- Amino Acids administration & dosage, Anesthesia adverse effects, Animals, Body Temperature drug effects, Cyclooxygenase 2 Inhibitors administration & dosage, Diphenylamine administration & dosage, Diphenylamine pharmacology, Dogs, Female, Glucose Tolerance Test veterinary, Heart Rate drug effects, Infusions, Intravenous veterinary, Insulin Secretion drug effects, Male, Meloxicam administration & dosage, Phenylacetates administration & dosage, Anesthesia veterinary, Cyclooxygenase 2 Inhibitors pharmacology, Diphenylamine analogs & derivatives, Meloxicam pharmacology, Phenylacetates pharmacology
- Abstract
In healthy dogs, amino acid infusion significantly attenuates the decrease in body temperature during anesthesia by facilitating insulin secretion, suggesting that such an increase in insulin secretion is related to increased heat production. In dogs, selective cyclooxygenase-2 (COX-2) inhibitors, which are used for pain relief in veterinary medicine, possess anti-pyretic action. And, in mice and humans, selective COX-2 inhibitors increase insulin secretion and sensitivity. Therefore, treatment with COX-2 inhibitors may negate or accelerate the attenuating effect on decreased body temperature during anesthesia by amino acid infusion. In the present study, influences on insulin secretion and body temperature by treatment with meloxicam or robenacoxib at therapeutic dose were evaluated in healthy dogs. Treatment with meloxicam or robenacoxib did not affect insulin secretion in the unanesthetized and anesthetized dogs, and did not affect body temperature and heart rate under the anesthetized condition with amino acid infusion. In conclusion, COX-2 inhibitors at therapeutic doses did not affect body temperature during anesthesia in dogs administered amino acids.
- Published
- 2019
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39. Concentrations of leptin, adiponectin, and resistin in the serum of obese cats during weight loss.
- Author
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Takashima S, Nishii N, Kobatake Y, Kiyosue M, Kimura S, and Kitagawa H
- Subjects
- Adiponectin blood, Animals, Cat Diseases diet therapy, Cats, Diet veterinary, Female, Leptin blood, Obesity diet therapy, Resistin blood, Cat Diseases blood, Obesity blood, Weight Loss physiology
- Abstract
We monitored changes in serum leptin, adiponectin, and resistin concentrations in obese cats during weight loss. Six naturally developed obese cats were fed low-fat, high-fiber dry food during a 9-week experimental period. Serum leptin, adiponectin, and resistin concentrations were measured at week 0, 4, 8, and 9. Body weight became significantly lower week 4 onward than that at week 0 (P<0.05 or 0.01). At week 9, serum leptin concentrations were significantly lower than those at week 0 (P<0.05). Contrarily, serum adiponectin and resistin concentrations did not significantly differ within the 9 weeks. While serum leptin levels were strongly positively correlated with body weight (r=0.923, P<0.001), serum adiponectin levels were moderately negatively correlated with it (r=-0.529, P<0.01), with serum resistin having a no correlation with body weight. Serum leptin levels might be more closely related with pathogenesis of adiposity than serum adiponectin or resistin in cats.
- Published
- 2019
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40. Risk factors for low plasma thyroxine and high plasma thyroid-stimulating hormone concentrations in dogs with non-thyroidal diseases.
- Author
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Nishii N, Okada R, Matsuba M, Takashima S, Kobatake Y, and Kitagawa H
- Subjects
- Animals, Cross-Sectional Studies, Dogs, Female, Male, Retrospective Studies, Risk Factors, Dog Diseases blood, Thyrotropin blood, Thyroxine blood
- Abstract
The aim of the current study was to identify independent risk factors for thyroid axis alterations in dogs with non-thyroidal diseases. In this retrospective cross-sectional study, data and plasma samples from 207 dogs with non-thyroidal diseases was used. The involvement of various factors (disease severity, sex, age, breed, category and duration of disease, and medication) in the alteration of plasma thyroxine (T4) or thyroid-stimulation hormone (TSH) concentrations was analyzed using multivariate logistic regression. Among the 207 dogs analyzed, 99 (47.8%) had low plasma T4 concentrations, while 45 (21.7%) had high TSH concentrations. Intact male sex [odds ratio (OR), 3.25; 1.67-6.35; P<0.001], Labrador Retrievers (OR, 18.70; 2.32-151.00; P=0.006), moderate (OR, 2.39; 1.21-4.74; P=0.012) and severe diseases (OR, 6.84; 2.27-20.70; P<0.001) were associated with increased risk for low plasma T4 concentrations. Meanwhile, intact male (OR, 3.93; 1.51-10.30; P=0.005), spayed female (OR, 4.22; 1.59-11.20; P=0.004), older age (OR, 2.73; 1.28-5.84; P=0.009), and Miniature Dachshunds (OR, 5.39; 2.38-12.20; P<0.001) had increased risk for high plasma TSH concentrations. Disease severity had been determined as an independent risk factor for canine NTIS. In addition, sex, age and breed were also associated with thyroid axis alterations in dogs with non-thyroidal diseases.
- Published
- 2019
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41. Influence of swine leukocyte antigen haplotype on serum antibody titers against swine erysipelas vaccine and reproductive and meat production traits of SLA-defined selectively bred Duroc pigs.
- Author
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Imaeda N, Ando A, Takasu M, Matsubara T, Nishii N, Takashima S, Shigenari A, Shiina T, and Kitagawa H
- Subjects
- Agriculture, Animals, Antibodies, Bacterial immunology, Breeding, Female, Male, Red Meat, Reproduction, Swine, Antibodies, Bacterial blood, Bacterial Vaccines immunology, Haplotypes, Histocompatibility Antigens Class I immunology, Swine Erysipelas immunology
- Abstract
We investigated possible associations of SLA class II haplotypes with serum antibody titers against a swine erysipelas vaccine, reproductive and meat production traits using a population of selective breeding Duroc pigs. In the selective breeding Duroc pigs, four SLA class II-DRB1 and -DQB1 alleles were assigned by using PCR-sequence specific primer technique. Low-resolution haplotype (Lr)-0.30 and/or Lr-0.13 were deduced from the SLA class II alleles in the population of SLA-defined Duroc pigs. SLA-homozygous piglets with the Lr-0.30 haplotype had relatively lower serum antibody titers against the vaccine compared to those with Lr-0.13. In contrast, there were no statistically significant differences in reproductive performance between the SLA-defined pigs with two SLA class II haplotypes. Weaning and rearing rates until the body weight of 105 kg was reached in homozygous piglets with Lr-0.30 were significantly lower than those in homozygous piglets with Lr-0.13. The SLA-defined pigs had lower birth and weaning weights, body weights at 60 days of age, and daily weight gains than non-selective breeding Duroc pigs. Furthermore, the SLA-defined pigs had slightly lower back fat thickness compared to the non-selective breeding pigs. The rib eye areas of homozygous or heterozygous pigs with Lr-0.13 were larger than those of homozygous pigs with Lr-0.30 and non-selective breeding pigs. These data suggested that SLA haplotypes had the potential as useful genetic markers for selective breeding in the population of SLA-defined Duroc pigs.
- Published
- 2018
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42. Genetic association of swine leukocyte antigen class II haplotypes and body weight in Microminipigs.
- Author
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Matsubara T, Takasu M, Imaeda N, Nishii N, Takashima S, Nishimura T, Nishimura T, Shiina T, Ando A, and Kitagawa H
- Abstract
Objective: Microminipigs are a novel animal model with extensive applications in laboratory studies owing, in part, to their extremely small body sizes. In this study, the relationship between swine leukocyte antigen (SLA) class II haplotype and body weight was evaluated in the Microminipig population., Methods: A total of 1,900 haplotypes, covering SLA class II haplotypes Lr-0.7, Lr-0.23, Lr-0.17, Lr-0.37, Lr-0.16, Lr-0.11, Lr-0.13, and Lr-0.18, were analyzed in 950 piglets. Birth weights and weights on postnatal day 50 were examined in piglets with eight different SLA class II haplotypes., Results: The mean birth weight of piglets with the Lr-0.23 haplotype (0.415 kg, n = 702) was significantly lower than that of piglets with Lr-0.17 (0.445 kg, n = 328) and Lr-0.37 (0.438 kg, n = 383) haplotypes. At postnatal day 50, the mean body weight of piglets with the Lr-0.23 haplotype (3.14 kg) was significantly lower than that of piglets with the Lr-0.13 haplotype (3.46 kg, p<0.01). There were no significant differences in daily gains (DGs) among the eight haplotypes. However, piglets with the Lr-0.11 and -0.18 haplotype combination or any heterozygous haplotype combinations containing Lr-0.23 had significantly lower DGs than those of piglets with the Lr-0.18, 0.37 haplotype combination., Conclusion: Piglets with the Lr-0.23 haplotype had relatively low body weights at birth and on postnatal day 50 and slightly lower DGs than those of piglets with other haplotypes. Therefore, the Lr-0.23 SLA class II haplotype may be a suitable marker for the selective breeding of Microminipigs with small body sizes.
- Published
- 2018
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43. The long-term safety of D-allulose administration in healthy dogs.
- Author
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Nishii N, Takashima S, Kobatake Y, Tokuda M, and Kitagawa H
- Subjects
- Animals, Blood Glucose analysis, Blood Glucose drug effects, Cholesterol blood, Dogs, Female, Fructose adverse effects, Glucose Tolerance Test veterinary, Hypoglycemic Agents adverse effects, Insulin blood, Lipids blood, Male, Fructose pharmacology, Hypoglycemic Agents pharmacology
- Abstract
The safety and biological effects of a long-term dose of D-allulose were evaluated in healthy dogs. For 12 weeks, the dogs were administered D-allulose (0.2 g/kg) or placebo daily. Plasma total cholesterol concentrations in the D-allulose group were significantly lower than those in the control group at and after week 2 (P<0.05). D-Allulose administration did not cause clinical signs or changes in hematological and biochemical levels, except for lipids. D-Allulose administration also did not influence body weight. Plasma glucose and insulin concentrations in the glucose tolerance test, performed one day after the termination of D-allulose administration, were not different between groups, suggesting no cumulative effects of D-allulose on glucose metabolism in healthy dogs. In conclusion, long-term administration of D-allulose caused no harmful effects in dogs.
- Published
- 2017
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44. Effects of D-allulose on glucose metabolism after the administration of sugar or food in healthy dogs.
- Author
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Nishii N, Nomizo T, Takashima S, Matsubara T, Tokuda M, and Kitagawa H
- Subjects
- Animals, Blood Glucose metabolism, Food, Glucose administration & dosage, Insulin blood, Maltose administration & dosage, Postprandial Period, Dogs metabolism, Fructose pharmacology, Glucose metabolism, Hypoglycemic Agents pharmacology
- Abstract
D-allulose is a C-3 epimer of D-fructose and has recently been investigated for its hypoglycemic effects. In the present study, the effects of D-allulose on glucose metabolism were evaluated in healthy dogs administrated sugar or food. The oral administrations of D-allulose decreased plasma glucose concentrations after oral glucose or maltose administration, with a diminished plasma insulin rise. The glucose suppressive effect of D-allulose was also observed after intravenous glucose administrations without increase in plasma insulin concentration. In contrast, D-allulose showed no effect on plasma glucose and insulin concentrations after feeding. The present results suggest that D-allulose administration may be beneficial in dogs with impaired glucose tolerance. Further studies investigating the therapeutic efficacy of D-allulose in diabetic dogs are required.
- Published
- 2016
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45. Identification and characterization of two CD4 alleles in Microminipigs.
- Author
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Matsubara T, Nishii N, Takashima S, Takasu M, Imaeda N, Aiki-Oshimo K, Yamazoe K, Kakisaka M, Takeshima SN, Aida Y, Kametani Y, Kulski JK, Ando A, and Kitagawa H
- Subjects
- Amino Acid Sequence, Animals, Base Sequence, CD4 Antigens genetics, Gene Expression Regulation physiology, Genotype, Polymerase Chain Reaction methods, Polymorphism, Restriction Fragment Length, RNA, Messenger genetics, RNA, Messenger metabolism, Swine genetics, Swine, Miniature genetics, Alleles, CD4 Antigens metabolism, Genetic Variation, Swine metabolism, Swine, Miniature metabolism
- Abstract
Background: We previously identified two phenotypes of CD4+ cells with and without reactions to anti-pig CD4 monoclonal antibodies by flow cytometry in a herd of Microminipigs. In this study, we analyzed the coding sequences of CD4 and certified the expression of CD4 molecules in order to identify the genetic sequence variants responsible for the positive and negative PBMCs reactivity to anti-pig CD4 monoclonal antibodies., Results: We identified two CD4 alleles, CD4.A and CD4.B, corresponding to antibody positive and negative, respectively, by nucleotide sequencing of PCR products using CD4 specific primer pairs. In comparison with the swine CD4 amino-acid sequence [GenBank: NP_001001908], CD4.A had seven amino-acid substitutions and CD4.B had 15 amino-acid substitutions. The amino-acid sequences within domain 1 of CD4.B were identical to the swine CD4.2 [GenBank: CAA46584] sequence that had been reported previously to be a modified CD4 molecule that had lost reactivity with an anti-pig CD4 antibody in NIH miniature pigs. Homozygous and heterozygous CD4.A and CD4.B alleles in the Microminipigs herd were characterised by using the RFLP technique with the restriction endonuclease, BseRI. The anti-pig CD4 antibody recognized pig PBMCs with CD4.AA and CD4.AB, but did not recognized those with CD4.BB. We transfected HeLa cells with the FLAG-tagged CD4.A or CD4.B vectors, and certified that transfected HeLa cells expressed FLAG in both vectors. The failure of cells to react with anti-CD4 antibodies in CD4.B pigs was associated to ten amino-acid substitutions in domain 1 and/or one amino-acid substitution in joining region 3 of CD4.B. We also found exon 8 was defective in some CD4.A and CD4.B resulting in the loss of the transmembrane domain, which implies that these CD4 proteins are secreted from helper T cells into the circulation., Conclusions: We identified that amino-acids substitutions of domain 1 in CD4.B gave rise to the failure of some CD4 expressing cells to react with particular anti-pig CD4 monoclonal antibodies. In addition, we developed a PCR-RFLP method that enabled us to simply identify the CD4 sequence variant and the positive and negative PBMCs reactivity to our anti-pig CD4 monoclonal antibodies without the need to use flow cytometric analysis.
- Published
- 2016
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46. Single oral dose safety of D-allulose in dogs.
- Author
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Nishii N, Nomizo T, Takashima S, Matsubara T, Tokuda M, and Kitagawa H
- Subjects
- Administration, Oral, Animals, Blood Glucose analysis, Diarrhea chemically induced, Diarrhea veterinary, Dog Diseases chemically induced, Dogs, Female, Fructose administration & dosage, Insulin blood, Male, Sweetening Agents administration & dosage, Vomiting chemically induced, Vomiting veterinary, Fructose adverse effects, Sweetening Agents adverse effects
- Abstract
Healthy dogs were administered acute oral doses of D-allulose (also called D-psicose) to evaluate its toxicity. Six dogs received oral doses of either a placebo or D-allulose solution (1 and 4 g/kg) on three different study days. One dog experienced vomiting, and five dogs showed transient diarrhea when 4 g/kg of D-allulose was administered. All dogs were active and had a good appetite throughout the study period. Blood glucose concentration slightly decreased without a rise in plasma insulin concentration 2 hr after D-allulose administration. Plasma alkaline phosphatase activities showed a mild increase between 12 and 48 hr after D-allulose administration. These data suggested that a single oral dose of D-allulose does not show severe toxicity in dogs.
- Published
- 2016
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47. Molecular cloning of feline resistin and the expression of resistin, leptin and adiponectin in the adipose tissue of normal and obese cats.
- Author
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Takashima S, Nishii N, Kato A, Matsubara T, Shibata S, and Kitagawa H
- Subjects
- Animals, Cat Diseases genetics, Cats, Cattle, Cloning, Molecular, Female, Humans, Male, Mice, Obesity genetics, Obesity metabolism, Rats, Resistin metabolism, Sequence Homology, Nucleic Acid, Adiponectin metabolism, Adipose Tissue metabolism, Cat Diseases metabolism, Leptin metabolism, Obesity veterinary, Resistin genetics
- Abstract
Resistin, one of the adipokines that has a cycteine-rich C-terminus, is considered to relate to the development of insulin resistance in rats. However, in cats, there is little knowledge regarding resistin. In this study, we cloned the feline resistin cDNA from adipose tissue by RT-PCR. The feline resistin clone contained an entire open reading frame encoding 107 amino acids that had 72.8%, 75.4%, 50.9% and 51.8% homology with bovine, human, mouse and rat homologues, respectively. In both subcutaneous and visceral adipose tissues, the transcription levels of feline resistin mRNA were significantly higher in obese cats than normal cats, and those of feline adiponectin mRNA were significantly lower in obese cats than normal cats. However, there was no difference in the expression of feline leptin between normal and obese cats. On the other hand, in both normal and obese cats, there were no significant differences in resistin, leptin and adiponectin mRNA levels between subcutaneous and visceral adipose tissues. In cats, the altered expression of resistin and adiponectin mRNA with obesity may contribute to the pathogenesis of insulin resistance and subsequent diabetes mellitus. In addition to feline adiponectin, the feline resistin cDNA clone obtained in this study will be useful for further investigation of the pathogenesis of obesity in cats.
- Published
- 2016
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48. Ligand-binding characteristics of feline insulin-binding immunoglobulin G.
- Author
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Suzuki T, Nishii N, Takashima S, Matsubara T, Iwasawa A, Takeuchi H, Tahara K, Hachisu T, and Kitagawa H
- Subjects
- Animals, Chromatography, Affinity, Female, Insulin genetics, Ligands, Male, Protein Binding, Antibody Affinity, Cats, Immunoglobulin G immunology, Insulin metabolism
- Abstract
Polyclonal immunoglobulin (Ig) G autoantibodies against insulin have been identified in sera of healthy cats. We purified and fractionated insulin-binding IgGs from cat sera by affinity chromatography and analyzed affinity of insulin-binding IgGs for insulin and their epitopes. Following the passing of fraction A, which did not bind to insulin, insulin-binding IgGs were eluted into two fractions, B and C, by affinity chromatography using a column fixed with bovine insulin. Dissociation constant (KD) values between insulin-binding IgGs and insulin, determined by surface plasmon resonance analysis (Biacore™system), were 1.64e(-4) M for fraction B (low affinity IgGs) and 2e(-5) M for fraction C (high affinity IgGs). Epitope analysis was conducted using 16 peptide fragments synthesized in concord with the amino acid sequence of feline insulin by an enzyme-linked immunosorbent assay. Fractions B and C showed higher absorbance (affinity) of the peptide fragment of 10 amino acid residues at the carboxyl-terminal of the B chain (peptide No. 19), followed by peptide fragments of 6 to 15 amino acid residues of the B chain (peptide No. 8). Fraction C showed a higher absorbance to 7 to 16 amino acid residues of the B chain (peptide No. 5) compared with the absorbance of fraction B. Polyclonal insulin-binding IgGs may form a macromolecule complex with insulin through the multiple affinity sites of IgG molecules. Feline insulin-binding IgGs are multifocal and may be composed of multiple IgG components and insulin.
- Published
- 2015
- Full Text
- View/download PDF
49. GH-producing mammary tumors in two dogs with acromegaly.
- Author
-
Murai A, Nishii N, Morita T, and Yuki M
- Subjects
- Acromegaly etiology, Acromegaly pathology, Animals, Dog Diseases metabolism, Dogs, Female, Hysterectomy veterinary, Immunohistochemistry veterinary, Insulin blood, Insulin-Like Growth Factor I metabolism, Mammary Neoplasms, Animal complications, Mammary Neoplasms, Animal surgery, Ovariectomy veterinary, Treatment Outcome, Acromegaly veterinary, Dog Diseases pathology, Growth Hormone blood, Mammary Neoplasms, Animal metabolism
- Abstract
Two intact female dogs were admitted for growing mammary tumors. They had symptoms of acromegaly including weight gain, enlargement of the head, excessive skin folds, and inspiratory stridor. Serum concentrations of growth hormone (GH), insulin-like growth factor-I (IGF-I), and insulin were elevated in the two cases. From these findings, both dogs were diagnosed with acromegaly. In case 1, the GH, IGF-I, and insulin levels subsided after removal of the focal benign mammary tumors and ovariohysterectomy. In case 2, those levels subsided after removal of only focal mammary carcinoma. In both cases, immunohistochemical investigations for GH were positive in the mammary tumor cells but not in the normal mammary glands. We concluded that GH-producing mammary tumors caused the present acromegaly.
- Published
- 2012
- Full Text
- View/download PDF
50. Experimental hyperlipemia induces insulin resistance in cats.
- Author
-
Nishii N, Maeda H, Murahata Y, Matsuu A, and Hikasa Y
- Subjects
- Animals, Cats, Fatty Acids, Nonesterified blood, Female, Male, Triglycerides blood, Blood Glucose metabolism, Hyperlipidemias blood, Insulin Resistance physiology
- Abstract
The effect of experimental hyperlipemia on insulin sensitivity was evaluated in seven healthy cats. Serum triglyceride and free fatty acid concentrations were significantly (P<0.05) higher when lipid-heparin was administered (2,894 ± 1,526 mg/dl and 4.54 ± 0.70 mEq/l, respectively) than when saline was administered (70 ± 42 mg/dl and 0.22 ± 0.08 mEq/l, respectively). A glucose clamp test revealed that the mean glucose infusion rate when lipid-heparin was administered (5.80 ± 0.67 mg/kg/min) was significantly (P<0.05) lower than when saline was administered (8.52 ± 1.83 mg/kg/min). These results suggest that experimental hyperlipemia induced insulin resistance in the healthy cats.
- Published
- 2012
- Full Text
- View/download PDF
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