Your search keyword '"Gil-Bernabe, Paloma"' showing total 9 results

1. Amelioration of Diabetes by Protein S.

Author

Taro Yasuma, Yutaka Yano, D'Alessandro-Gabazza, Corina N., Masaaki Toda, Gil-Bernabe, Paloma, Tetsu Kobayashi, Kota Nishihama, Hinneh, Josephine A., Rumi Mifuji-Moroka, Roeen, Ziaurahman, Morser, John, Cann, Isaac, Iwasa Motoh, Yoshiyuki Takei, Gabazza, Esteban C., Yasuma, Taro, Yano, Yutaka, Toda, Masaaki, Kobayashi, Tetsu, and Nishihama, Kota

Subjects

PROTEIN S, INFLAMMATION, APOPTOSIS, GENE expression, DIABETIC nephropathies, ANIMAL experimentation, ANIMALS, BLOOD proteins, BLOOD sugar, CELL lines, DIABETES, FAT cells, GLUCOSE tolerance tests, INSULIN resistance, TYPE 1 diabetes, ISLANDS of Langerhans, LIVER, MICE, TYPE 2 diabetes, SKELETAL muscle

Abstract

Protein S is an anticoagulant factor that also regulates inflammation and cell apoptosis. The effect of protein S on diabetes and its complications is unknown. This study compared the development of diabetes between wild-type and transgenic mice overexpressing human protein S and the development of diabetic glomerulosclerosis between mice treated with and without human protein S and between wild-type and protein S transgenic mice. Mice overexpressing protein S showed significant improvements in blood glucose level, glucose tolerance, insulin sensitivity, and insulin secretion compared with wild-type counterparts. Exogenous protein S improved insulin sensitivity in adipocytes, skeletal muscle, and liver cell lines in db/db mice compared with controls. Significant inhibition of apoptosis with increased expression of BIRC3 and Bcl-2 and enhanced activation of Akt/PKB was induced by protein S in islet β-cells compared with controls. Diabetic wild-type mice treated with protein S and diabetic protein S transgenic mice developed significantly less severe diabetic glomerulosclerosis than controls. Patients with type 2 diabetes had significantly lower circulating free protein S than healthy control subjects. This study shows that protein S attenuates diabetes by inhibiting apoptosis of β-cells and the development of diabetic nephropathy. [ABSTRACT FROM AUTHOR]

Published

2016

2. Thrombin-Activatable Fibrinolysis Inhibitor Protects against Acute Lung Injury by Inhibiting the Complement System.

Author

Naito, Masahiro, Taguchi, Osamu, Kobayashi, Tetsu, Takagi, Takehiro, D'Alessandro-Gabazza, Corina N., Matsushima, Yuki, Boveda-Ruiz, Daniel, Gil-Bernabe, Paloma, Matsumoto, Takahiro, Chelakkot-Govindalayathil, Ayshwarya-Lakshmi, Toda, Masaaki, Yasukawa, Atsushi, Hataji, Osamu, Morser, John, and Yoshiyuki Takei

Published

2013

3. Eosinophils Promote Epithelial to Mesenchymal Transition of Bronchial Epithelial Cells

Author

Yasukawa, Atsushi, Hosoki, Koa, Toda, Masaaki, Miyake, Yasushi, Matsushima, Yuki, Matsumoto, Takahiro, Boveda-Ruiz, Daniel, Gil-Bernabe, Paloma, Nagao, Mizuho, Sugimoto, Mayumi, Hiraguchi, Yukiko, Tokuda, Reiko, Naito, Masahiro, Takagi, Takehiro, D'Alessandro-Gabazza, Corina N., Suga, Shigeru, Kobayashi, Tetsu, Fujisawa, Takao, Taguchi, Osamu, and Gabazza, Esteban C.

Subjects

EOSINOPHILS, EPITHELIAL cells, MESENCHYMAL stem cells, TRANSFORMING growth factors, LABORATORY mice, MOLECULAR biology

Abstract

Eosinophilic inflammation and remodeling of the airways including subepithelial fibrosis and myofibroblast hyperplasia are characteristic pathological findings of bronchial asthma. Epithelial to mesenchymal transition (EMT) plays a critical role in airway remodelling. In this study, we hypothesized that infiltrating eosinophils promote airway remodelling in bronchial asthma. To demonstrate this hypothesis we evaluated the effect of eosinophils on EMT by in vitro and in vivo studies. EMT was assessed in mice that received intra-tracheal instillation of mouse bone marrow derived eosinophils and in human bronchial epithelial cells co-cultured with eosinophils freshly purified from healthy individuals or with eosinophilic leukemia cell lines. Intra-tracheal instillation of eosinophils was associated with enhanced bronchial inflammation and fibrosis and increased lung concentration of growth factors. Mice instilled with eosinophils pre-treated with transforming growth factor(TGF)-β1 siRNA had decreased bronchial wall fibrosis compared to controls. EMT was induced in bronchial epithelial cells co-cultured with human eosinophils and it was associated with increased expression of TGF-β1 and Smad3 phosphorylation in the bronchial epithelial cells. Treatment with anti-TGF-β1 antibody blocked EMT in bronchial epithelial cells. Eosinophils induced EMT in bronchial epithelial cells, suggesting their contribution to the pathogenesis of airway remodelling. [ABSTRACT FROM AUTHOR]

Published

2013

4. Efficacy of a Novel Class of RNA Interference Therapeutic Agents.

Author

Hamasaki, Tomohiro, Suzuki, Hiroshi, Shirohzu, Hisao, Matsumoto, Takahiro, D'Alessandro-Gabazza, Corina N., Gil-Bernabe, Paloma, Boveda-Ruiz, Daniel, Naito, Masahiro, Kobayashi, Tetsu, Toda, Masaaki, Mizutani, Takayuki, Taguchi, Osamu, Morser, John, Eguchi, Yutaka, Kuroda, Masahiko, Ochiya, Takahiro, Hayashi, Hirotake, Gabazza, Esteban C., Ohgi, Tadaaki, and Xiaolin Zi

Subjects

RNA interference, GENES, DOUBLE-stranded RNA, LABORATORY mice, LUNG injuries, LUNG diseases

Abstract

RNA interference (RNAi) is being widely used in functional gene research and is an important tool for drug discovery. However, canonical double-stranded short interfering RNAs are unstable and induce undesirable adverse effects, and thus there is no currently RNAi-based therapy in the clinic. We have developed a novel class of RNAi agents, and evaluated their effectiveness in vitro and in mouse models of acute lung injury (ALI) and pulmonary fibrosis. The novel class of RNAi agents (nkRNAH, PnkRNATM) were synthesized on solid phase as single- stranded RNAs that, following synthesis, self-anneal into a unique helical structure containing a central stem and two loops. They are resistant to degradation and suppress their target genes. nkRNA and PnkRNA directed against TGF-b1mRNA ameliorate outcomes and induce no off-target effects in three animal models of lung disease. The results of this study support the pathological relevance of TGF-b1 in lung diseases, and suggest the potential usefulness of these novel RNAi agents for therapeutic application. [ABSTRACT FROM AUTHOR]

Published

2012

5. TNF-α is associated with loss of lean body mass only in already cachectic COPD patients.

Author

Eagan, Tomas M. L., Gabazza, Esteban C., D'Alessandro-Gabazza, Corina, Gil-Bernabe, Paloma, Aoki, Shinya, Hardie, Jon A., Bakke, Per S., and Wagner, Peter D.

Subjects

TUMOR necrosis factors, LEAN body mass, OBSTRUCTIVE lung diseases patients, CACHEXIA, C-reactive protein, ENZYME-linked immunosorbent assay

Abstract

Background: Systemic inflammation may contribute to cachexia in patients with chronic obstructive pulmonary disease (COPD). In this longitudinal study we assessed the association between circulating C-reactive protein (CRP), tumor necrosis factor (TNF)-α, interleukin (IL)-1ß, and IL-6 levels and subsequent loss of fat free mass and fat mass in more than 400 COPD patients over three years. Methods: The patients, aged 40-76, GOLD stage II-IV, were enrolled in 2006/07, and followed annually. Fat free mass and fat mass indexes (FFMI & FMI) were calculated using bioelectrical impedance, and CRP, TNF-α, IL-1ß, and IL-6 were measured using enzyme immunoassays. Associations with mean change in FFMI and FMI of the four inflammatory plasma markers, sex, age, smoking, FEV1, inhaled steroids, arterial hypoxemia, and Charlson comorbidity score were analyzed with linear mixed models. Results: At baseline, only CRP was significantly (but weakly) associated with FFMI (r = 0.18, p<0.01) and FMI (r = 0.27, p<0.01). Univariately, higher age, lower FEV1, and use of beta2-agonists were the only significant predictors of decline in FFMI, whereas smoking, hypoxemia, Charlson score, and use of inhaled steroids predicted increased loss in FMI. Multivariately, high levels of TNF-α (but not CRP, IL-1ß or IL-6) significantly predicted loss of FFMI, however only in patients with established cachexia at entry. Conclusion: This study does not support the hypothesis that systemic inflammation is the cause of accelerated loss of fat free mass in COPD patients, but suggests a role for TNF-α in already cachectic COPD patients. [ABSTRACT FROM AUTHOR]

Published

2012

6. Role of Thrombin-Activatable Fibrinolysis Inhibitor in Allergic Bronchial Asthma.

Author

Fujiwara, Atsushi, Taguchi, Osamu, Takagi, Takehiro, D'Alessandro-Gabazza, Corina, Boveda-Ruiz, Daniel, Toda, Masaaki, Yasukawa, Atsushi, Matsushima, Yuki, Miyake, Yasushi, Kobayashi, Hiroyasu, Kobayashi, Tetsu, Gil-Bernabe, Paloma, Naito, Masahiro, Yoshida, Masamichi, Morser, John, Takei, Yoshiyuki, and Gabazza, Esteban

Subjects

ASTHMA, THROMBIN, FIBRINOLYSIS, CARBOXYPEPTIDASES, MICE, ANIMAL experimentation

Abstract

Background: Bronchial asthma is an inflammatory disease of the airways. Thrombin-activatable fibrinolysis inhibitor (TAFI) is a carboxypeptidase that besides inhibiting fibrinolysis, also regulates inflammatory processes. The only validated substrate known for TAFI is fibrin. In the present study we evaluated the role of TAFI in bronchial asthma by comparing the development of allergic bronchial asthma between wild-type (WT) and TAFI-deficient mice (KO). Methods: Asthmatic inflammation was induced by sensitization and challenge with ovalbumin in WT (WT/OVA) and TAFI KO (KO/OVA) mice. WT mice (WT/SAL) and TAFI KO (KO/SAL) were used as controls. Cytokines, markers of inflammation, and coagulation were measured in bronchoalveolar lavage fluid (BALF). Results: Airway hyperresponsiveness was worse in KO/OVA mice than in WT/OVA mice or control mice. Markers of lung injury were significantly increased in BALF from KO/OVA mice compared to WT/OVA mice. Airway hyperresponsiveness and the BALF concentrations of IL-5 and osteopontin were significantly increased in KO/OVA mice compared to WT/OVA mice. Treatment of WT/OVA and KO/OVA mice with a C5a receptor antagonist significantly decreased hyperresponsiveness along with the BALF concentrations of total protein and C5a compared to untreated asthmatic mice. Conclusion: The results of this study suggest that TAFI plays a protective role in the pathogenesis of allergic inflammation probably by inhibiting the complement system. [ABSTRACT FROM AUTHOR]

Published

2012

7. Development and Preclinical Efficacy of Novel Transforming Growth Factor-β1 Short Interfering RNAs for Pulmonary Fibrosis.

Author

D'Alessandro-Gabazza, Corina N., Tetsu Kobayashi, Boveda-Ruiz, Daniel, Takehiro Takagi, Masaaki Toda, Gil-Bernabe, Paloma, Yasushi Miyake, Atsushi Yasukawa, Yoshikazu Matsuda, Noboru Suzuki, Hiromitsu Saito, Yutaka Yano, Ayako Fukuda, Tetsuya Hasegawa, Hidekazu Toyobuku, Rennard, Stephen I., Wagner, Peter D., Morser, John, Yoshiyuki Takei, and Osamu Taguchi

Published

2012

8. Erratum. Amelioration of Diabetes by Protein S. Diabetes 2016;65:1940-1951.

Author

Yasuma, Taro, Yano, Yutaka, D'Alessandro-Gabazza, Corina N, Toda, Masaaki, Gil-Bernabe, Paloma, Kobayashi, Tetsu, Nishihama, Kota, Hinneh, Josephine A, Mifuji-Moroka, Rumi, Roeen, Ziaurahman, Morser, John, Cann, Isaac, Motoh, Iwasa, Takei, Yoshiyuki, and Gabazza, Esteban C

Published

2016

9. TNF-α is associated with loss of lean body mass only in already cachectic COPD patients.

Author

Eagan, Tomas Ml, Gabazza, Esteban C, D'Alessandro-Gabazza, Corina, Gil-Bernabe, Paloma, Aoki, Shinya, Hardie, Jon A, Bakke, Per S, Wagner, Peter D, and Eagan, Tomas M L

Abstract

Background: Systemic inflammation may contribute to cachexia in patients with chronic obstructive pulmonary disease (COPD). In this longitudinal study we assessed the association between circulating C-reactive protein (CRP), tumor necrosis factor (TNF)-α, interleukin (IL)-1ß, and IL-6 levels and subsequent loss of fat free mass and fat mass in more than 400 COPD patients over three years.Methods: The patients, aged 40-76, GOLD stage II-IV, were enrolled in 2006/07, and followed annually. Fat free mass and fat mass indexes (FFMI & FMI) were calculated using bioelectrical impedance, and CRP, TNF-α, IL-1ß, and IL-6 were measured using enzyme immunoassays. Associations with mean change in FFMI and FMI of the four inflammatory plasma markers, sex, age, smoking, FEV1, inhaled steroids, arterial hypoxemia, and Charlson comorbidity score were analyzed with linear mixed models.Results: At baseline, only CRP was significantly (but weakly) associated with FFMI (r = 0.18, p < 0.01) and FMI (r = 0.27, p < 0.01). Univariately, higher age, lower FEV1, and use of beta2-agonists were the only significant predictors of decline in FFMI, whereas smoking, hypoxemia, Charlson score, and use of inhaled steroids predicted increased loss in FMI. Multivariately, high levels of TNF-α (but not CRP, IL-1ß or IL-6) significantly predicted loss of FFMI, however only in patients with established cachexia at entry.Conclusion: This study does not support the hypothesis that systemic inflammation is the cause of accelerated loss of fat free mass in COPD patients, but suggests a role for TNF-α in already cachectic COPD patients. [ABSTRACT FROM AUTHOR]

Published

2012