Your search keyword '"Chun, Tae-Hwa"' showing total 11 results

1. Adipose extracellular matrix remodelling in obesity and insulin resistance.

Author

Lin, De, Chun, Tae-Hwa, and Kang, Li

Subjects

*ADIPOSE tissues, *EXTRACELLULAR matrix, *OBESITY, *INSULIN resistance, *CELL physiology

Abstract

The extracellular matrix (ECM) of adipose tissues undergoes constant remodelling to allow adipocytes and their precursor cells to change cell shape and function in adaptation to nutritional cues. Abnormal accumulation of ECM components and their modifiers in adipose tissues has been recently demonstrated to cause obesity-associated insulin resistance, a hallmark of type 2 diabetes. Integrins and other ECM receptors (e.g. CD44) that are expressed in adipose tissues have been shown to regulate insulin sensitivity. It is well understood that a hypoxic response is observed in adipose tissue expansion during obesity progression and that hypoxic response accelerates fibrosis and inflammation in white adipose tissues. The expansion of adipose tissues should require angiogenesis; however, the excess deposition of ECM limits the angiogenic response of white adipose tissues in obesity. While recent studies have focused on the metabolic consequences and the mechanisms of adipose tissue expansion and remodelling, little attention has been paid to the role played by the interaction between peri-adipocyte ECM and their cognate cell surface receptors. This review will address what is currently known about the roles played by adipose ECM, their modifiers, and ECM receptors in obesity and insulin resistance. Understanding how excess ECM deposition in the adipose tissue deteriorates insulin sensitivity would provide us hints to develop a new therapeutic strategy for the treatment of insulin resistance and type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2016

2. Peri-adipocyte ECM remodeling in obesity and adipose tissue fibrosis.

Author

Chun, Tae-Hwa

Subjects

*FAT cells, *EXTRACELLULAR matrix, *LABORATORY mice, *OBESITY, *METABOLISM, *ADIPOGENESIS, *CARDIOVASCULAR diseases, *ADIPOSE tissues

Abstract

Adipocytes differentiate and function in environments rich in extracellular matrix (ECM) proteins. The phenotypes of genetically modified mice have aided in recognizing the importance of ECM proteins and their modifiers, e.g., proteinases, in the regulation of obesity and metabolism. Most of the molecular mechanisms through which ECM proteins and modifiers regulate adipogenesis or adipocyte function have not been fully defined. Adipose tissue fibrosis may be a factor that links obesity to diabetes or cardiovascular disease risk in conjunction with tissue inflammation. Defining the molecular mechanisms through which the ECM environment regulates adipogenesis and adipocyte function should provide us with a better understanding of the disease link between obesity and diabetes or cardiovascular diseases. [ABSTRACT FROM AUTHOR]

Published

2012

3. A Pericellular Collagenase Directs the 3-Dimensional Development of White Adipose Tissue

Author

Chun, Tae-Hwa, Hotary, Kevin B., Sabeh, Farideh, Saltiel, Alan R., Allen, Edward D., and Weiss, Stephen J.

Subjects

*ADIPOSE tissues, *PROTEIN precursors, *COLLAGENASES, *METALLOPROTEINASES

Abstract

Summary: White adipose tissue (WAT) serves as the primary energy depot in the body by storing fat. During development, fat cell precursors (i.e., preadipocytes) undergo a hypertrophic response as they mature into lipid-laden adipocytes. However, the mechanisms that regulate adipocyte size and mass remain undefined. Herein, we demonstrate that the membrane-anchored metalloproteinase, MT1-MMP, coordinates adipocyte differentiation in vivo. In the absence of the protease, WAT development is aborted, leaving tissues populated by mini-adipocytes which render null mice lipodystrophic. While MT1-MMP preadipocytes display a cell autonomous defect in vivo, null progenitors retain the ability to differentiate into functional adipocytes during 2-dimensional (2-D) culture. By contrast, within the context of the 3-dimensional (3-D) ECM, normal adipocyte maturation requires a burst in MT1-MMP-mediated proteolysis that modulates pericellular collagen rigidity in a fashion that controls adipogenesis. Hence, MT1-MMP acts as a 3-D-specific adipogenic factor that directs the dynamic adipocyte-ECM interactions critical to WAT development. [Copyright &y& Elsevier]

Published

2006

4. 3D engineered scaffold for large-scale Vigil immunotherapy production.

Author

Kerneis, Fabienne, Bognar, Ernest, Stanbery, Laura, Moon, Seongjun, Kim, Do Hoon, Deng, Yuxuan, Hughes, Elliot, Chun, Tae-Hwa, Tharp, Darron, Zupanc, Heidi, Jay, Chris, Walter, Adam, Nemunaitis, John, and Lahann, Joerg

Subjects

*CORE needle biopsy, *COLORECTAL cancer, *TISSUE culture, *IMMUNOTHERAPY, *EXTRACELLULAR matrix, *TISSUE scaffolds

Abstract

Previously, we reported successful cellular expansion of a murine colorectal carcinoma cell line (CT-26) using a three-dimensional (3D) engineered extracellular matrix (EECM) fibrillar scaffold structure. CCL-247 were grown over a limited time period of 8 days on 3D EECM or tissue culture polystyrene (TCPS). Cells were then assayed for growth, electroporation efficiency and Vigil manufacturing release criteria. Using EECM scaffolds, we report an expansion of CCL-247 (HCT116), a colorectal carcinoma cell line, from a starting concentration of 2.45 × 105 cells to 1.9 × 106 cells per scaffold. Following expansion, 3D EECM-derived cells were assessed based on clinical release criteria of the Vigil manufacturing process utilized for Phase IIb trial operation with the FDA. 3D EECM-derived cells passed all Vigil manufacturing release criteria including cytokine expression. Here, we demonstrate successful Vigil product manufacture achieving the specifications necessary for the clinical trial product release of Vigil treatment. Our results confirm that 3D EECM can be utilized for the expansion of human cancer cell CCL-247, justifying further clinical development involving human tissue sample manufacturing including core needle biopsy and minimal ascites samples. [ABSTRACT FROM AUTHOR]

Published

2024

5. Significance and therapeutic potential of the natriuretic peptides/cGMP/cGMP-dependent protein kinase pathway in vascular regeneration.

Author

Yamahara, Kenichi, Itoh, Hiroshi, Chun, Tae-Hwa, Ogawa, Yoshihiro, Yamashita, Jun, Sawada, Naoki, Fukunaga, Yasutomo, Sone, Masakatsu, Yurugi-Kobayashi, Takami, Miyashita, Kazutoshi, Tsujimoto, Hirokazu, Kook, Hyun, Feil, Robert, Garbers, David L., Hofmann, Franz, and Nakao, Kazuwa

Subjects

*PEPTIDE hormones, *PROTEIN kinases

Abstract

Natriuretic peptides (NPs), which consist of atrial, brain, and C-type natriuretic peptides (ANP, BNP, and CNP, respectively), are characterized as cardiac or vascular hormones that elicit their biological effects by activation of the cGMP/cGMP-dependent protein kinase (cGK) pathway. We recently reported that adenoviral gene transfer of CNP into rabbit blood vessels not only suppressed neointimal formation but also accelerated reendothelialization, a required step for endothelium-dependent vasorelaxation and antithrombogenicity. Accordingly, we investigated the therapeutic potential of the NPs/cGMP/cGK pathway for vascular regeneration. In transgenic (Tg) mice that overexpress BNP in response to hindlimb ischemia, neovascularization with appropriate mural cell coating was accelerated without edema or bleeding, and impaired angiogenesis by the suppression of nitric oxide production was effectively rescued. Furthermore, in BNP-Tg mice, inflammatory cell infiltration in ischemic tissue and vascular superoxide production were suppressed compared with control mice. Ischemia-induced angiogenesis was also significantly potentiated in cGK type I Tg mice, but attenuated in cGK type I knockout mice. NPs significantly stimulated capillary network formation of cultured endothelial cells by cGK stimulation and subsequent Erk1/2 activation. Furthermore, gene transfer of CNP into ischemic muscles effectively accelerated angiogenesis. These findings reveal an action of the NPs/cGMP/cGK pathway to exert multiple vasculoprotective and regenerative actions in the absence of apparent adverse effects, and therefore suggest that NPs as the endogenous cardiovascular hormone can be used as a strategy of therapeutic angiogenesis in patients with tissue ischemia. [ABSTRACT FROM AUTHOR]

Published

2003

6. Coordinate regulation of endothelin and adrenomedullin secretion by oxidative stress in endothelial cells.

Author

Saito, Takatoshi, Itoh, Hiroshi, Chun, Tae-Hwa, Fukunaga, Yasutomo, Yamashita, Jun, Doi, Kentaro, Tanaka, Tokuji, Inoue, Mayumi, Masatsugu, Ken, Sawada, Naoki, Sakaguchi, Satsuki, Arai, Hiroshi, Mukoyama, Masashi, Tojo, Katsuyoshi, Hosoya, Tatsuo, and Nakao, Kazuwa

Subjects

*ENDOTHELIUM, *PEPTIDES, *ADRENOMEDULLIN, *PHYSIOLOGY

Abstract

Presents a study which examined the effects of H[sub2]O[sub2] on the expression of two endothelium derived vasoactive peptides, endothelin and adrenomedullin. Materials and methods; Results; Discussion.

Published

2001

7. Fibro-Adipogenic Remodeling of the Diaphragm in Obesity-Associated Respiratory Dysfunction.

Author

Buras, Eric D., Converso-Baran, Kimber, Davis, Carol S., Takeshi Akama, Fumihito Hikage, Michele, Daniel E., Brooks, Susan V., Tae-Hwa Chun, Akama, Takeshi, Hikage, Fumihito, and Chun, Tae-Hwa

Subjects

*OBESITY, *RESPIRATORY diseases, *DIAPHRAGM (Anatomy), *HIGH-fat diet, *HYPERCAPNIA, *THROMBOSPONDIN-1, *CELL proliferation, *ADIPOSE tissue physiology, *ADIPOSE tissues, *ANIMAL experimentation, *CELL culture, *CELL physiology, *COLLAGEN, *COMPARATIVE studies, *FAT cells, *IMMUNOHISTOCHEMISTRY, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *RESEARCH, *RESEARCH funding, *ULTRASONIC imaging, *WESTERN immunoblotting, *EVALUATION research, *METABOLISM

Abstract

Respiratory dysfunction is a common complication of obesity, conferring cardiovascular morbidity and increased mortality and often necessitating mechanical ventilatory support. While impaired lung expansion in the setting of increased adipose mass and reduced central response to hypercapnia have been implicated as pathophysiological drivers, the impact of obesity on respiratory muscles-in particular, the diaphragm-has not been investigated in detail. Here, we demonstrate that chronic high-fat diet (HFD) feeding impairs diaphragm muscle function, as assessed in vivo by ultrasonography and ex vivo by measurement of contractile force. During an HFD time course, progressive adipose tissue expansion and collagen deposition within the diaphragm parallel contractile deficits. Moreover, intradiaphragmatic fibro-adipogenic progenitors (FAPs) proliferate with long-term HFD feeding while giving rise to adipocytes and type I collagen-depositing fibroblasts. Thrombospondin 1 (THBS1), a circulating adipokine, increases with obesity and induces FAP proliferation. These findings suggest a novel role for FAP-mediated fibro-adipogenic diaphragm remodeling in obesity-associated respiratory dysfunction. [ABSTRACT FROM AUTHOR]

Published

2019

8. The Exocyst Complex Regulates Free Fatty Acid Uptake by Adipocytes.

Author

Inoue, Mayumi, Akama, Takeshi, Jiang, Yibin, and Chun, Tae-Hwa

Subjects

*FREE fatty acids, *FAT cells, *TYPE 1 diabetes, *PHOSPHATIDYLINOSITOL 3-kinases, *GENE silencing

Abstract

The exocyst is an octameric molecular complex that drives vesicle trafficking in adipocytes, a rate-limiting step in insulin-dependent glucose uptake. This study assessed the role of the exocyst complex in regulating free fatty acid (FFA) uptake by adipocytes. Upon differentiating into adipocytes, 3T3-L1 cells acquire the ability to incorporate extracellular FFAs in an insulin-dependent manner. A kinetic assay using fluoresceinated FFA (C12 dodecanoic acid) uptake allows the real-time monitoring of FFA internalization by adipocytes. The insulin-dependent uptake of C12 dodecanoic acid by 3T3-L1 adipocytes is mediated by Akt and phosphatidylinositol 3 (PI3)-kinase. Gene silencing of the exocyst components Exo70 and Sec8 significantly reduced insulin-dependent FFA uptake by adipocytes. Consistent with the roles played by Exo70 and Sec8 in FFA uptake, mCherry-tagged Exo70 and HA-tagged Sec8 partially colocalize with lipid droplets within adipocytes, suggesting their active roles in the development of lipid droplets. Tubulin polymerization was also found to regulate FFA uptake in collaboration with the exocyst complex. This study demonstrates a novel role played by the exocyst complex in the regulation of FFA uptake by adipocytes. [ABSTRACT FROM AUTHOR]

Published

2015

9. Fat depot-specific gene signature and ECM remodeling of Sca1high adipose-derived stem cells.

Author

Tokunaga, Masakuni, Inoue, Mayumi, Jiang, Yibin, Barnes, Richard H., Buchner, David A., and Chun, Tae-Hwa

Subjects

*FAT cells, *STEM cells, *CELL surface antigens, *GENE expression, *ADIPOSE tissues, *GLUCOSE transporters, *COLLAGENASES

Abstract

Stem cell antigen-1 (Sca1 or Ly6A/E) is a cell surface marker that is widely expressed in mesenchymal stem cells, including adipose-derived stem cells (ASCs). We hypothesized that the fat depot-specific gene signature of Sca1high ASCs may play the major role in defining adipose tissue function and extracellular matrix (ECM) remodeling in a depot-specific manner. Herein we aimed to characterize the unique gene signature and ECM remodeling of Sca1high ASCs isolated from subcutaneous (inguinal) and visceral (epididymal) adipose tissues. Sca1high ASCs are found in the adventitia and perivascular areas of adipose tissues. Sca1high ASCs purified with magnetic-activated cell sorting (MACS) demonstrate dendrite or round shape with the higher expression of cytokines and chemokines (e.g., Il6, Cxcl1) and the lower expression of a glucose transporter (Glut1). Subcutaneous and visceral fat-derived Sca1high ASCs particularly differ in the gene expressions of adhesion and ECM molecules. While the expression of the major membrane-type collagenase (MMP14) is comparable between the groups, the expressions of secreted collagenases (MMP8 and MMP13) are higher in visceral Sca1high ASCs than in subcutaneous ASCs. Consistently, slow but focal MMP-dependent collagenolysis was observed with subcutaneous adipose tissue-derived vascular stromal cells, whereas rapid and bulk collagenolysis was observed with visceral adipose tissue-derived cells in MMP-dependent and -independent manners. These results suggest that the fat depot-specific gene signatures of ASCs may contribute to the distinct patterns of ECM remodeling and adipose function in different fat depots. [ABSTRACT FROM AUTHOR]

Published

2014

10. Angiotensin II suppresses growth arrest specific homeobox (Gax) expression via redox-sensitive mitogen-activated protein kinase (MAPK)

Author

Saito, Takatoshi, Itoh, Hiroshi, Yamashita, Jun, Doi, Kentaro, Chun, Tae-Hwa, Tanaka, Tokuji, Inoue, Mayumi, Masatsugu, Ken, Fukunaga, Yasutomo, Sawada, Naoki, Sakaguchi, Satsuki, Arai, Hiroshi, Tojo, Katsuyoshi, Tajima, Naoko, Hosoya, Tatsuo, and Nakao, Kazuwa

Subjects

*OXIDATIVE stress, *ANGIOTENSINS, *PROTEIN kinases, *MITOGENS

Abstract

Abstract: Oxidative stress is known to be involved in growth control of vascular smooth muscle cells (VSMCs). We and others have demonstrated that angiotensin II (Ang II) has an important role in vascular remodeling. Several reports suggested that VSMC growth induced by Ang II was elicited by oxidative stress. Gax, growth arrest-specific homeobox is a homeobox gene expressed in the cardiovascular system. Over expression of Gax is demonstrated to inhibit VSMC growth. We previously reported that Ang II down-regulated Gax expression. To address the regulatory mechanism of Gax, we investigated the significance of oxidative stress in Ang II-induced suppression of Gax expression. We further examined the involvement of mitogen-activated protein kinases (MAPKs), which is crucial for cell growth and has shown to be activated by oxidative stress, on the regulation of Gax expression by Ang II. Ang II markedly augmented intracellular H2O2 production which was decreased by pretreatment with N-acetylcystein (NAC), an anti-oxidant. Ang II and H2O2 decreased Gax expression dose-dependently and these effects were blocked by administration of both NAC and pyrrolidine dithiocarbamate (PDTC), another anti-oxidant. Ang II and H2O2 induced marked activation of extracellular signal-responsive kinase1/2 (ERK1/2), which was blocked by NAC. Ang II and H2O2 also activated p38MAPK, and they were blocked by pre-treatment with NAC. However, the level of activated p38MAPK was quite low in comparison with ERK1/2. Ang II- or H2O2-induced Gax down-regulation was significantly inhibited by PD98059, an ERK1/2 inhibitor but not SB203580, a p38MAPK inhibitor. The present results demonstrated the significance of regulation of Gax expression by redox-sensitive ERK1/2 activation. [Copyright &y& Elsevier]

Published

2005

11. Therapeutic potential of thiazolidinediones in activation of peroxisome proliferator-activated receptor γ for monocyte recruitment and endothelial regeneration

Author

Tanaka, Tokuji, Fukunaga, Yasutomo, Itoh, Hiroshi, Doi, Kentaro, Yamashita, Jun, Chun, Tae-Hwa, Inoue, Mayumi, Masatsugu, Ken, Saito, Takatoshi, Sawada, Naoki, Sakaguchi, Satsuki, Arai, Hiroshi, and Nakao, Kazuwa

Subjects

*HYPOGLYCEMIC agents, *DIABETES complications, *INSULIN antibodies, *INSULIN resistance, *MACROPHAGES

Abstract

Abstract: Thiazolidinediones, a new class of antidiabetic drugs that increase insulin sensitivity, have been shown to be ligands for peroxisome proliferator-activated receptor γ (PPARγ). Recent studies demonstrating that PPARγ occurs in macrophages have focused attention on its role in macrophage functions. In this study, we investigated the effect of thiazolidinediones on monocyte proliferation and migration in vitro and the mechanisms involved. In addition, we examined the therapeutic potentials of thiazolidinediones for injured atherosclerotic lesions. Troglitazone and pioglitazone, the two thiazolidinediones, as well as 15-deoxy-Δ12,14-prostaglandin J2 inhibited in a dose-dependent manner the serum-induced proliferation of THP-1 (human monocytic leukemia cells) and of U937 (human monoblastic leukemia cells), which permanently express PPARγ. These ligands for PPARγ also significantly inhibited migration of THP-1 induced by monocyte chemoattractant protein-1 (MCP-1). Troglitazone and 15-deoxy-Δ12,14-prostaglandin J2 significantly suppressed the mRNA expression of the MCP family-specific receptor CCR2 (chemokine CCR2 receptor) in THP-1 at the transcriptional level. Furthermore, troglitazone significantly inhibited MCP-1 binding to THP-1. Oral administration of troglitazone to Watanabe heritable hyperlipidemic (WHHL) rabbits after balloon injury suppressed acute recruitment of monocytes/macrophages and accelerated re-endothelialization. These results suggest that thiazolidinediones have therapeutic potential for the treatment of diabetic vascular complications. [Copyright &y& Elsevier]

Published

2005