Your search keyword '"Fujisaka, Shiho"' showing total 9 results

1. Increased Number of Mucosal-Associated Invariant T Cells Is Associated with the Inhibition of Nonalcoholic Fatty Liver Disease in High Fat Diet–Fed Mice.

Author

Kishi, Haruka, Usui, Isao, Jojima, Teruo, Fujisaka, Shiho, Wakamatsu, Sho, Mizunuma-Inoue, Yuiko, Niitani, Takafumi, Sakurai, Shintaro, Iijima, Toshie, Tomaru, Takuya, Tobe, Kazuyuki, and Aso, Yoshimasa

Subjects

NON-alcoholic fatty liver disease, LIVER cells, LIPID metabolism, ADIPOSE tissues, T cells, MICE, ADIPOSE tissue physiology

Abstract

Nonalcoholic fatty liver disease (NAFLD) is an emerging worldwide health concern. The disease may involve immune cells including T cells, but little is known about the role(s) of the innate-like T cells in the liver. Furthermore, the most abundant innate-like T cells in the human liver are mucosal-associated invariant T (MAIT) cells, but the involvement of MAIT cells in NAFLD remains largely unexplored because of their paucity in mice. In this study, we used a novel mouse line, Vα19, in which the number of MAIT cells is equivalent to or greater than that in humans. Compared with the control mice, Vα19 mice fed a high-fat diet (HFD) exhibited a reduction in lipid accumulation, NAFLD activity score, and transcripts relevant to lipogenesis. In addition, serum triglyceride and non-esterified fatty acids were lower in Vα19 mice fed normal chow or HFD. In contrast, the Vα19 mice showed little or no change in glucose tolerance, insulin sensitivity, inflammation in adipose tissues, or intestinal permeability compared with the controls, irrespective of diet. These results suggest that the presence of MAIT cells is associated with reduced lipogenesis and lipid accumulation in the liver; however, further studies are needed to clarify the role of MAIT cells in hepatic lipid metabolism. [ABSTRACT FROM AUTHOR]

Published

2022

2. Generation and characterization of a Meflin-CreERT2 transgenic line for lineage tracing in white adipose tissue.

Author

Kuwano, Takahide, Izumi, Hironori, Aslam, Muhammad Rahil, Igarashi, Yoshiko, Bilal, Muhammad, Nishimura, Ayumi, Watanabe, Yoshiyuki, Nawaz, Allah, Kado, Tomonobu, Ikuta, Koichi, Yamamoto, Seiji, Sasahara, Masakiyo, Fujisaka, Shiho, Yagi, Kunimasa, Mori, Hisashi, and Tobe, Kazuyuki

Subjects

WHITE adipose tissue, FAT cells, MESENCHYMAL stem cells, ADIPOSE tissues, HIGH-fat diet, GENES

Abstract

Meflin (Islr) expression has gained attention as a marker for mesenchymal stem cells, but its function remains largely unexplored. Here, we report the generation of Meflin-CreERT2 mice with CreERT2 inserted under the Meflin gene promoter to label Meflin-expressing cells genetically, thereby enabling their lineages to be traced. We found that in adult mice, Meflin-expressing lineage cells were present in adipose tissue stroma and had differentiated into mature adipocytes. These cells constituted Crown-like structures in the adipose tissue of mice after high-fat diet loading. Cold stimulation led to the differentiation of Meflin-expressing lineage cells into beige adipocytes. Thus, the Meflin-CreERT2 mouse line is a useful new tool for visualizing and tracking the lineage of Meflin-expressing cells. [ABSTRACT FROM AUTHOR]

Published

2021

3. Astaxanthin stimulates mitochondrial biogenesis in insulin resistant muscle via activation of AMPK pathway.

Author

Nishida, Yasuhiro, Nawaz, Allah, Kado, Tomonobu, Takikawa, Akiko, Igarashi, Yoshiko, Onogi, Yasuhiro, Wada, Tsutomu, Sasaoka, Toshiyasu, Yamamoto, Seiji, Sasahara, Masakiyo, Imura, Johji, Tokuyama, Kumpei, Usui, Isao, Nakagawa, Takashi, Fujisaka, Shiho, Kunimasa, Yagi, and Tobe, Kazuyuki

Subjects

ASTAXANTHIN, SKELETAL muscle, ADIPOSE tissues, MITOCHONDRIA formation, FREE fatty acids, GLUCOSE intolerance, MUSCLE metabolism, MUSCLES

Abstract

Background: Skeletal muscle is mainly responsible for insulin‐stimulated glucose disposal. Dysfunction in skeletal muscle metabolism especially during obesity contributes to the insulin resistance. Astaxanthin (AX), a natural antioxidant, has been shown to ameliorate hepatic insulin resistance in obese mice. However, its effects in skeletal muscle are poorly understood. The current study aimed to investigate the molecular target of AX in ameliorating skeletal muscle insulin resistance. Methods: We fed 6‐week‐old male C57BL/6J mice with normal chow (NC) or NC supplemented with AX (NC+AX) and high‐fat‐diet (HFD) or HFD supplemented with AX for 24 weeks. We determined the effect of AX on various parameters including insulin sensitivity, glucose uptake, inflammation, kinase signaling, gene expression, and mitochondrial function in muscle. We also determined energy metabolism in intact C2C12 cells treated with AX using the Seahorse XFe96 Extracellular Flux Analyzer and assessed the effect of AX on mitochondrial oxidative phosphorylation and mitochondrial biogenesis. Results: AX‐treated HFD mice showed improved metabolic status with significant reduction in blood glucose, serum total triglycerides, and cholesterol (p< 0.05). AX‐treated HFD mice also showed improved glucose metabolism by enhancing glucose incorporation into peripheral target tissues, such as the skeletal muscle, rather than by suppressing gluconeogenesis in the liver as shown by hyperinsulinemic–euglycemic clamp study. AX activated AMPK in the skeletal muscle of the HFD mice and upregulated the expressions of transcriptional factors and coactivator, thereby inducing mitochondrial remodeling, including increased mitochondrial oxidative phosphorylation component and free fatty acid metabolism. We also assessed the effects of AX on mitochondrial biogenesis in the siRNA‐mediated AMPK‐depleted C2C12 cells and showed that the effect of AX was lost in the genetically AMPK‐depleted C2C12 cells. Collectively, AX treatment (i) significantly ameliorated insulin resistance and glucose intolerance through regulation of AMPK activation in the muscle, (ii) stimulated mitochondrial biogenesis in the muscle, (iii) enhanced exercise tolerance and exercise‐induced fatty acid metabolism, and (iv) exerted antiinflammatory effects via its antioxidant activity in adipose tissue. Conclusions: We concluded that AX treatment stimulated mitochondrial biogenesis and significantly ameliorated insulin resistance through activation of AMPK pathway in the skeletal muscle. [ABSTRACT FROM AUTHOR]

Published

2020

4. Lipodystrophy Due to Adipose Tissue-Specific Insulin Receptor Knockout Results in Progressive NAFLD.

Author

Softic, Samir, Boucher, Jeremie, Solheim, Marie H., Shiho Fujisaka, Haering, Max-Felix, Homan, Erica P., Winnay, Jonathon, Perez-Atayde, Antonio R., Kahn, C. Ronald, and Fujisaka, Shiho

Subjects

LIPIDS, ECTOPIC tissue, LIPODYSTROPHY, METABOLIC syndrome, OBESITY, ADIPOSE tissues, ANIMAL experimentation, BIOLOGICAL models, BLOOD sugar, CELL receptors, DIET, FATTY liver, GLUCOSE tolerance tests, GLYCOGEN, GROWTH factors, IMMUNOBLOTTING, IMMUNOHISTOCHEMISTRY, LIVER, MICE, RESEARCH funding, SOMATOMEDIN, ALANINE aminotransferase

Abstract

Ectopic lipid accumulation in the liver is an almost universal feature of human and rodent models of generalized lipodystrophy and is also a common feature of type 2 diabetes, obesity, and metabolic syndrome. Here we explore the progression of fatty liver disease using a mouse model of lipodystrophy created by a fat-specific knockout of the insulin receptor (F-IRKO) or both IR and insulin-like growth factor 1 receptor (F-IR/IGFRKO). These mice develop severe lipodystrophy, diabetes, hyperlipidemia, and fatty liver disease within the first weeks of life. By 12 weeks of age, liver demonstrated increased reactive oxygen species, lipid peroxidation, histological evidence of balloon degeneration, and elevated serum alanine aminotransferase and aspartate aminotransferase levels. In these lipodystrophic mice, stored liver lipids can be used for energy production, as indicated by a marked decrease in liver weight with fasting and increased liver fibroblast growth factor 21 expression and intact ketogenesis. By 52 weeks of age, liver accounted for 25% of body weight and showed continued balloon degeneration in addition to inflammation, fibrosis, and highly dysplastic liver nodules. Progression of liver disease was associated with improvement in blood glucose levels, with evidence of altered expression of gluconeogenic and glycolytic enzymes. However, these mice were able to mobilize stored glycogen in response to glucagon. Feeding F-IRKO and F-IR/IGFRKO mice a high-fat diet for 12 weeks accelerated the liver injury and normalization of blood glucose levels. Thus, severe fatty liver disease develops early in lipodystrophic mice and progresses to advanced nonalcoholic steatohepatitis with highly dysplastic liver nodules. The liver injury is propagated by lipotoxicity and is associated with improved blood glucose levels. [ABSTRACT FROM AUTHOR]

Published

2016

5. Loss of Pdk1-Foxo1 Signaling in Myeloid Cells Predisposes to Adipose Tissue Inflammation and Insulin Resistance.

Author

Kawano, Yoshinaga, Nakae, Jun, Watanabe, Nobuyuki, Fujisaka, Shiho, Iskandar, Kristy, Sekioka, Risa, Hayashi, Yoshitake, Tobe, Kazuyuki, Kasuga, Masato, Noda, Tetsuo, Yoshimura, Akihiko, Onodera, Masafumi, and Itoh, Hiroshi

Subjects

INFLAMMATION, ADIPOSE tissues, OBESITY, INSULIN resistance, GENE expression, INTERLEUKIN-4

Abstract

Chronic inflammation in adipose tissue contributes to obesity-related insulin resistance. The 3-phosphoinositide-dependent protein kinase 1 (Pdk1)/forkhead transcription factor (Foxo1) pathway is important in regulating glucose and energy homeostasis, but little is known about this pathway in adipose tissue macrophages (ATMs). To investigate this, we generated transgenic mice that carried macrophage/granulocyte-specific mutations, including a Pdk1 knockout (LysMPdk1-/-), a Pdk1 knockout with transactivation-defective Foxo1 (Δ256LysMPdk1-/-), a constitutively active nuclear (CN) Foxo1 (CNFoxo1LysM), or a transactivation-defective Foxo1 (D256Foxo1LysM). We analyzed glucose metabolism and gene expression in ATM populations isolated with fluorescence-activated cell sorting. The LysMPdk1-/- mice exhibited elevated M1 macrophages in adipose tissue and insulin resistance. Overexpression of transactivation-defective Foxo1 rescued these phenotypes. CNFoxo1LysM promoted transcription of the C-C motif chemokine receptor 2 (Ccr2) in ATMs and increased M1 macrophages in adipose tissue. On a high-fat diet, CNFoxo1LysM mice exhibited insulin resistance. Pdk1 deletion or Foxo1 activation in bone marrow-derived macrophages abolished insulin and interleukin-4 induction of genes involved in alternative macrophage activation. Thus, Pdk1 regulated macrophage in filtration by inhibiting Foxo1-induced Ccr2 expression. This shows that the macrophage Pdk1/Foxo1 pathway is important in regulating insulin sensitivity in vivo. [ABSTRACT FROM AUTHOR]

Published

2012

6. The Radioprotective 105/MD-1 Complex Contributes to Diet-Induced Obesity and Adipose Tissue Inflammation.

Author

Watanabe, Yasuharu, Nakamura, Tomoya, Ishikawa, Sho, Fujisaka, Shiho, Usui, Isao, Tsuneyama, Koichi, Ichihara, Yoshinori, Wada, Tsutomu, Hirata, Yoichiro, Suganami, Takayoshi, Izaki, Hirofumi, Akira, Shizuo, Miyake, Kensuke, Kanayama, Hiro-omi, Shimabukuro, Michio, Sata, Masataka, Sasaoka, Toshiyasu, Ogawa, Yoshihiro, Tobe, Kazuyuki, and Takatsu, Kiyoshi

Subjects

IMMUNITY, RADIATION-protective agents, METABOLIC disorders, OBESITY, DIET in disease, ADIPOSE tissues, MICE

Abstract

Recent accumulating evidence suggests that innate immunity is associated with obesity-induced chronic inflammation and metabolic disorders. Here, we show that a Toll-like receptor (TLR) protein, radioprotective 105 (RP105)/myeloid differentiation protein (MD)-1 complex, contributes to high-fat diet (HFD)-induced obesity, adipose tissue inflammation, and insulin resistance. An HFD dramatically increased RP105 mRNA and protein expression in stromal vascular fraction of epididymal white adipose tissue (eWAT) in wild-type (WT) mice. RP105 mRNA expression also was significantly increased in the visceral adipose tissue of obese human subjects relative to nonobese subjects. The RP105/MD-1 complex was expressed by most adipose tissue macrophages (ATMs). An HFD increased RP105/MD-1 expression on the M1 subset of ATMs that accumulate in eWAT. Macrophages also acquired this characteristic in coculture with 3T3-L1 adipocytes. RP105 knockout (KO) and MD-1 KO mice had less HFD-induced adipose tissue inflammation, hepatic steatosis, and insulin resistance compared with wild-type (WT) and TLR4 KO mice. Finally, the saturated fatty acids, palmitic and stearic acids, are endogenous ligands for TLR4, but they did not activate RP105/MD-1. Thus, the RP105/MD-1 complex is a major mediator of adipose tissue inflammation independent of TLR4 signaling and may represent a novel therapeutic target for obesity-associated metabolic disorders. [ABSTRACT FROM AUTHOR]

Published

2012

7. Regulatory Mechanisms for Adipose Tissue M1 and M2 Macrophages in Diet-Induced Obese Mice.

Author

Fujisaka, Shiho, Usui, Isao, Bukhari, Agussalim, Ikutani, Masashi, Oya, Takeshi, Kanatani, Yukiko, Tsuneyama, Koichi, Nagai, Yoshinori, Takatsu, Kiyoshi, Urakaze, Masaharu, Kobayashi, Masashi, and Tobe, Kazuyuki

Subjects

*ADIPOSE tissues, *MACROPHAGES, *INSULIN, *LABORATORY mice, *GENE expression, *TUMOR necrosis factors, *PROTEINS, *INTERLEUKIN-10

Abstract

OBJECTIVE--To characterize the phenotypic changes of adipose tissue macrophages (ATMs) under different conditions of insulin sensitivity. RESEARCH DESIGN AND METHODS--The number and the expressions of marker genes for M1 and M2 macrophages from mouse epididymal fat tissue were analyzed using flow cytometry after the mice had been subjected to a high-fat diet (HFD) and pioglitazone treatment. RESULTS--Most of the CD11c-positive M1 macrophages and the CD206-positive M2 macrophages in the epididymal fat tissue were clearly separated using flow cytometry. The M1 and M2 macrophages exhibited completely different gene expression patterns. Not only the numbers of M1 ATMs and the expression of M1 marker genes, such as tumor necrosis factor-α and monocyte chemoattractant protein-1, but also the M1-to-M2 ratio were increased by an HFD and decreased by subsequent pioglitazone treatment, suggesting the correlation with whole-body insulin sensitivity. We also found that the increased number of M2 ATMs after an HFD was associated with the upregulated expression of interleukin (IL)-10, an anti-inflammatory Th2 cytokine, in the adipocyte fraction as well as in adipose tissue. The systemic overexpression of IL-10 by an adenovirus vector increased the expression of M2 markers in adipose tissue. CONCLUSIONS--M1 and M2 ATMs constitute different subsets of macrophages. Insulin resistance is associated with both the number of M1 macrophages and the M1-to-M2 ratio. The increased expression of IL-10 after an HFD might be involved in the increased recruitment of M2 macrophages. Diabetes 58:2574-2582, 2009 [ABSTRACT FROM AUTHOR]

Published

2009

8. Effects of pioglitazone on suppressor of cytokine signaling 3 expression: potential mechanisms for its effects on insulin sensitivity and adiponectin expression.

Author

Kanatani Y, Usui I, Ishizuka K, Bukhari A, Fujisaka S, Urakaze M, Haruta T, Kishimoto T, Naka T, Kobayashi M, Kanatani, Yukiko, Usui, Isao, Ishizuka, Ken, Bukhari, Agussalim, Fujisaka, Shiho, Urakaze, Masaharu, Haruta, Tetsuro, Kishimoto, Tadamitsu, Naka, Tetsuji, and Kobayashi, Masashi

Subjects

PROTEIN metabolism, TYROSINE metabolism, ADIPOSE tissues, ANIMAL experimentation, CARRIER proteins, CELLS, DIABETES, EPIDIDYMIS, FAT cells, FAT content of food, GENES, HYPOGLYCEMIC agents, INSULIN resistance, METABOLISM, MICE, PEPTIDE hormones, THIAZOLIDINEDIONES, PHARMACODYNAMICS

Abstract

Pioglitazone is widely used for the treatment of diabetic patients with insulin resistance. The mechanism of pioglitazone to improve insulin sensitivity is not fully understood. Recent studies have shown that the induction of suppressor of cytokine signaling 3 (SOCS3) is related to the development of insulin resistance. Here, we examined whether the insulin-sensitizing effect of pioglitazone affects the SOCS induction. In db/db mice and high-fat-fed mice, expression of SOCS3 mRNA in fat tissue was increased compared with that in lean control mice, and pioglitazone suppressed SOCS3 levels. In 3T3-L1 adipocytes, mediators of insulin resistance such as tumor necrosis factor-alpha (TNF-alpha), interleukin-6, growth hormone, and insulin increased SOCS3 expression, which was partially inhibited by pioglitazone. The ability of pioglitazone to suppress SOCS3 induction by TNF-alpha was greatly augmented by peroxisome proliferator-activated receptor gamma overexpression. SOCS3 overexpression and tyrphostin AG490, a Janus kinase 2 inhibitor, or dominant-negative STAT3 expression partially inhibited adiponectin secretion and was accompanied by decreased STAT3 phosphorylation. Conversely, pioglitazone increased adiponectin secretion and STAT3 phosphorylation in fat tissue of db/db mice and in 3T3-L1 adipocytes. These results suggest that pioglitazone exerts its effect to improve whole-body insulin sensitivity in part through the suppression of SOCS3, which is associated with the increase in STAT3 phosphorylation and adiponectin production in fat tissue. [ABSTRACT FROM AUTHOR]

Published

2007

9. Telmisartan Improves Insulin Resistance by Increasing Apoptosis of Fat Cells and Decreasing Macrophage Infiltration in High Fat-fed Mice.

Author

Fujisaka, Shiho, Usui, Isao, Yamazaki, Yu, Bukhari, Agussalim, Kanatani, Yukiko, Suzuki, Hikari, He, Jianying, Ishiki, Manabu, Iwata, Minoru, Hiratani, Kazuyuki, Urakaze, Masaharu, and Kobayashi, Masashi

Subjects

*ANGIOTENSIN II, *INSULIN resistance, *FAT cells, *MACROPHAGES, *APOPTOSIS, *ADIPOSE tissues, *LABORATORY mice

Abstract

AngiotensinII receptor blocker (ARB), a class of anti-hypertensive drug, is known to have beneficial effects on insulin resistance. Telmisartan, a new ARB, has another function as a partial agonist of PPARγ, which may be associated to its stronger effect to improve insulin sensitivity than the other ARBs. We have also reported that Telmisartsn improves insulin sensitivity with reduced body weight and adipoeyte size in high fat-fed mice. To further clarify the underlying mechanisms, we investigated the effects of Telmisartan on apoptosis, macrophage infiltration and cytokine production in adipose tissues of obese insulin resistant mice. C57BL mice were fed normal diet (ND) or high fat diet (HFD) for 24 weeks and then Telmisartan was orally administered for 5 weeks. Pioglitazone Or Candesartan were also administered as controls. Intraperitoneal insulin tolerance test (ITT), glucose tolerance test (GTT), HOMA-IR, weight of adipose tissue, adipocyte size, macrophage infiltration and apoptosis in adipose tissue were measured by standard technique. In HFD mice, glucose profiles were improved by either Telmisartan or Pioglitazone. HOMA-IR was reduced by Telmisartan by 19%. The average of adipocyte size in HFD mice was decreased by Telmisartan and Candesartan by 36% and 7%, respectively. The number of macrophages in adipose tissue was 5 times more in HFD mice, which was decreased by 65% and 20% by Telmisartan and Candesartan, respectively. TNFα mRNA in adipose tissue was reduced by 70% by Telmisartan in HFD mice. The number of apoptotic cells was less in HFD mice, and Telmisartan increased it. Telmisartan improved insulin resistance of HFD mice with reduced adipocyte size, infiltration of macrophages and TNFα level in adipose tissue. Enhancement of apoptosis in adipose tissue may be a part of the mechanisms for decreased adipocyte size and improvement of insulin resistance by Telmisartan. [ABSTRACT FROM AUTHOR]

Published

2007