715 results on '"Masahiro, Kimura"'
Search Results
152. ATR inhibitor AZD6738 increases the sensitivity of colorectal cancer cells to 5‑fluorouracil by inhibiting repair of DNA damage
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Takuya, Suzuki, Takahisa, Hirokawa, Anri, Maeda, Shinnosuke, Harata, Kaori, Watanabe, Takeshi, Yanagita, Hajime, Ushigome, Nozomi, Nakai, Yuzo, Maeda, Kazuyoshi, Shiga, Ryo, Ogawa, Akira, Mitsui, Masahiro, Kimura, Yoichi, Matsuo, Hiroki, Takahashi, and Shuji, Takiguchi
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Sulfonamides ,Cancer Research ,Indoles ,Morpholines ,Ataxia Telangiectasia Mutated Proteins ,General Medicine ,Pyrimidines ,Oncology ,Cell Line, Tumor ,Colonic Neoplasms ,Animals ,Humans ,Fluorouracil ,Colorectal Neoplasms ,DNA Damage - Abstract
The repair of DNA damage caused by chemotherapy in cancer cells occurs mainly at two cell cycle checkpoints (G
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- 2022
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153. Functional Properties of Mouse Chitotriosidase Expressed in the Periplasmic Space of Escherichia coli.
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Masahiro Kimura, Satoshi Wakita, Kotarou Ishikawa, Kazutaka Sekine, Satoshi Yoshikawa, Akira Sato, Kazuaki Okawa, Akinori Kashimura, Masayoshi Sakaguchi, Yasusato Sugahara, Daisuke Yamanaka, Naohito Ohno, Peter O Bauer, and Fumitaka Oyama
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Medicine ,Science - Abstract
Chitotriosidase (Chit1) is an enzyme associated with various diseases, including Gaucher disease, chronic obstructive pulmonary disease, Alzheimer disease and cystic fibrosis. In this study, we first expressed mouse mature Chit1 fused with V5 and (His)6 tags at the C-terminus (Chit1-V5-His) in the cytoplasm of Escherichia coli and found that most of the expressed protein was insoluble. In contrast, Chit1 tagged with Protein A at the N-terminus and V5-His at the C-terminus, was expressed in the periplasmic space of E. coli as a soluble protein and successfully purified. We evaluated the chitinolytic properties of the recombinant enzyme using 4-nitrophenyl N,N'-diacetyl-β-D-chitobioside [4NP-chitobioside, 4NP-(GlcNAc)2] and found that its activity was comparable to CHO cells-expressed Chit1-V5-His. Optimal conditions for the E. coli-produced Chit1 were pH ~5.0 at 50°C. Chit1 was stable after 1 h incubation at pH 5.0~11.0 on ice and its chitinolytic activity was lost at pH 2.0, although the affinity to chitin remained unchanged. Chit1 efficiently cleaved crystalline and colloidal chitin substrates as well as oligomers of N-acetyl-D-glucosamine (GlcNAc) releasing primarily (GlcNAc)2 fragments at pH 5.0. On the other hand, (GlcNAc)3 was relatively resistant to digestion by Chit1. The degradation of 4NP-(GlcNAc)2 and (GlcNAc)3 was less evident at pH 7.0~8.0, while (GlcNAc)2 production from colloidal chitin and (GlcNAc)6 at these pH conditions remained strong at the neutral conditions. Our results indicate that Chit1 degrades chitin substrates under physiological conditions and suggest its important pathophysiological roles in vivo.
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- 2016
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154. Modeling network growth with directional attachment and communities.
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Masahiro Kimura, Kazumi Saito, and Naonori Ueda
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- 2004
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155. Modeling of growing networks with directional attachment and communities.
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Masahiro Kimura, Kazumi Saito, and Naonori Ueda
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- 2004
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156. On Unique Representations of Certain Dynamical Systems Produced by Continuous-Time Recurrent Neural Networks.
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Masahiro Kimura
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- 2002
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157. The Interaction Between Cancer-associated Fibroblasts and Cancer Cells Enhances Bcl-xL and Mcl-1 in Colorectal Cancer
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ANRI MAEDA, HIROKI TAKAHASHI, SHINNOSUKE HARATA, KAORI WATANABE, TAKESHI YANAGITA, TAKUYA SUZUKI, HAJIME USHIGOME, NOZOMU NAKAI, YUZO MAEDA, TAKAHISA HIROKAWA, KAZUYOSHI SHIGA, RYO OGAWA, MASAYASU HARA, YOICHI MATSUO, AKIRA MITSUI, MASAHIRO KIMURA, and SHUJI TAKIGUCHI
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STAT3 Transcription Factor ,Cancer Research ,Interleukin-6 ,bcl-X Protein ,Apoptosis ,General Medicine ,Cell Communication ,HCT116 Cells ,Coculture Techniques ,Oncology ,Cancer-Associated Fibroblasts ,Humans ,Myeloid Cell Leukemia Sequence 1 Protein ,Phosphorylation ,Colorectal Neoplasms ,Janus Kinases ,Signal Transduction - Abstract
The acquisition of resistance to apoptosis is one of the biggest problems in colorectal cancer (CRC) treatment. This study aimed to elucidate the mechanisms of resistance to apoptosis with a focus on interleukin (IL)-6 produced by the interaction between cancer cells and cancer-associated fibroblasts (CAFs).DLD-1 and HCT116 cell lines were treated with IL-6 and furthermore co-cultured with CAFs. The expression levels of Bcl-xL, Mcl-1 and phosphorylation of STAT3 were evaluated by western blotting. We also performed immunostaining for CRC specimens and evaluated the correlation between CAFs invasion and Bcl-xL/Mcl-1 expression.Both IL-6 and co-culturing enhanced Bcl-xL, Mcl-1 and the phosphorylation of STAT3. Immunohistochemistry showed a positive correlation between CAFs and Bcl-xL/Mcl-1. These results showed that the interaction between CAFs and cancer cells enhances Bcl-xL and Mcl-1 through the IL-6/STAT3 signaling pathway.Our findings provide new potential therapeutic targets and strategies for CRC treatment.
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- 2021
158. Mouse Acidic Chitinase Effectively Degrades Random-Type Chitosan to Chitooligosaccharides of Variable Lengths under Stomach and Lung Tissue pH Conditions
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Fumitaka Oyama, Chinatsu Takasaki, Shiro Seki, Masayuki Nakamura, Satoshi Wakita, Yasusato Sugahara, Peter Bauer, Yuta Kida, Masahiro Kimura, Kazuhisa Matsuda, Eri Tabata, Koji Hiraoka, Syunsuke Kobayashi, Maiko Uehara, and Vaclav Matoska
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chitooligosaccharides ,Oligosaccharides ,Pharmaceutical Science ,Organic chemistry ,macromolecular substances ,chitin ,Article ,Substrate Specificity ,Analytical Chemistry ,Chitosan ,Mice ,chemistry.chemical_compound ,QD241-441 ,X-Ray Diffraction ,Chitin ,In vivo ,Drug Discovery ,medicine ,FACE method ,Animals ,Physical and Theoretical Chemistry ,Lung ,biology ,Chemistry ,Hydrolysis ,Stomach ,Chitinases ,Hydrogen-Ion Concentration ,block-type chitosan ,In vitro ,carbohydrates (lipids) ,medicine.anatomical_structure ,Biochemistry ,Organ Specificity ,Chemistry (miscellaneous) ,Acetylation ,Chitinase ,biology.protein ,Molecular Medicine ,Degradation (geology) ,acidic chitinase ,random-type chitosan - Abstract
Chitooligosaccharides exhibit several biomedical activities, such as inflammation and tumorigenesis reduction in mammals. The mechanism of the chitooligosaccharides’ formation in vivo has been, however, poorly understood. Here we report that mouse acidic chitinase (Chia), which is widely expressed in mouse tissues, can produce chitooligosaccharides from deacetylated chitin (chitosan) at pH levels corresponding to stomach and lung tissues. Chia degraded chitin to produce N-acetyl-d-glucosamine (GlcNAc) dimers. The block-type chitosan (heterogenous deacetylation) is soluble at pH 2.0 (optimal condition for mouse Chia) and was degraded into chitooligosaccharides with various sizes ranging from di- to nonamers. The random-type chitosan (homogenous deacetylation) is soluble in water that enables us to examine its degradation at pH 2.0, 5.0, and 7.0. Incubation of these substrates with Chia resulted in the more efficient production of chitooligosaccharides with more variable sizes was from random-type chitosan than from the block-type form of the molecule. The data presented here indicate that Chia digests chitosan acquired by homogenous deacetylation of chitin in vitro and in vivo. The degradation products may then influence different physiological or pathological processes. Our results also suggest that bioactive chitooligosaccharides can be obtained conveniently using homogenously deacetylated chitosan and Chia for various biomedical applications.
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- 2021
159. Chitinase 3-like 1 secreted from cancer-associated fibroblasts promotes tumor angiogenesis via interleukin-8 secretion in colorectal cancer
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Kaori Watanabe, Kazuyoshi Shiga, Anri Maeda, Shinnosuke Harata, Takeshi Yanagita, Takuya Suzuki, Hajime Ushigome, Yuzo Maeda, Takahisa Hirokawa, Ryo Ogawa, Masayasu Hara, Hiroki Takahashi, Yoichi Matsuo, Akira Mitsui, Masahiro Kimura, and Shuji Takiguchi
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Male ,Cancer Research ,IL-8 ,Blotting, Western ,Interleukin-8 ,Enzyme-Linked Immunosorbent Assay ,colorectal cancer ,Articles ,Cell Line ,angiogenesis ,Oncology ,Cancer-Associated Fibroblasts ,Japan ,Humans ,Angiogenesis Inducing Agents ,CHI3L1 ,Chitinase-3-Like Protein 1 ,CAF ,Colorectal Neoplasms ,Aged ,Cell Proliferation - Abstract
The cancer-stromal interaction has been demonstrated to promote tumor progression, and cancer-associated fibroblasts (CAFs), which are the main components of stromal cells, have attracted attention as novel treatment targets. Chitinase 3-like 1 (CHI3L1) is a chitinase-like protein, which affects cell proliferation and angiogenesis. However, the mechanisms through which cells secrete CHI3L1 and through which CHI3L1 mediates tumor progression in the cancer microenvironment are still unclear. Accordingly, the present study assessed the secretion of CHI3L1 in the microenvironment of colorectal cancer and evaluated how CHI3L1 affects tumor angiogenesis. CAFs and normal fibroblasts (NFs) established from colorectal cancer tissue, and human colon cancer cell lines were evaluated using immunostaining, cytokine antibody array, RNA interference, reverse transcription-quantitative PCR (RT-qPCR), ELISA, western blotting and angiogenesis assays. The expression and secretion of CHI3L1 in CAFs were stronger than those in NFs and colorectal cancer cell lines. In addition, interleukin-13 receptor α2 (IL-13Rα2), a receptor for CHI3L1, was not expressed in colorectal cancer cell lines, but was expressed in fibroblasts, particularly CAFs. Furthermore, the expression and secretion of IL-8 in CAFs was stronger than that in NFs and cancer cell lines, and recombinant CHI3L1 addition increased IL-8 expression in CAFs, whereas knockdown of CHI3L1 suppressed IL-8 expression. Furthermore, IL-13Rα2 knockdown suppressed the enhancement of IL-8 expression induced by CHI3L1 treatment in CAFs. For vascular endothelial growth factor-A (VEGFA), similar results to IL-8 were observed in an ELISA for comparison of secretion between CAFs and NFs and for changes in secretion after CHI3L1 treatment in CAFs; however, no significant differences were observed for changes in expression after CHI3L1 treatment or IL-13Rα2 knockdown in CAFs assessed using RT-qPCR assays. Angiogenesis assays revealed that tube formation in vascular endothelial cells was suppressed by conditioned medium from CAFs with the addition of human CHI3L1 neutralizing antibodies compared with control IgG, and also suppressed by conditioned medium from CAFs transfected with CHI3L1, IL-8 or VEGFA small interfering RNA compared with negative control small interfering RNA. Overall, the present findings indicated that CHI3L1 secreted from CAFs acted on CAFs to increase the secretion of IL-8, thereby affecting tumor angiogenesis in colorectal cancer.
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- 2021
160. Dynamic integration of height maps into a 3-D world representation from range image sequences.
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Minoru Asada, Masahiro Kimura, and Yoshiaki Shirai
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- 1990
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161. Dynamical systems produced by recurrent neural networks.
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Masahiro Kimura and Ryohei Nakano
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- 2000
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162. A Case of Aorto-duodenal Fistula Treated by Omental Plugging
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Takaya Nagasaki, Hiroyuki Asai, Masahiro Kimura, Toru Imagami, Satoshi Taniwaki, and Yuki Eguchi
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medicine.medical_specialty ,business.industry ,Fistula ,medicine ,Aorto-duodenal ,medicine.disease ,business ,Surgery - Published
- 2020
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163. Concurrent Use of Biphasic Cuirass Ventilation and Low-intensity Noninvasive Positive Pressure Ventilation
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Toshikazu Ikeda, Kanako Kobayashi, Yusuke Tsubouchi, Shuichi Yano, Emiko Nishikawa, Masahiro Kimura, Shinichi Iwamoto, Mitsuhiro Tada, and Toru Kadowaki
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Pulmonary and Respiratory Medicine ,business.industry ,Anesthesia ,Biphasic cuirass ventilation ,Medicine ,Critical Care and Intensive Care Medicine ,business ,Positive pressure ventilation ,Intensity (physics) - Published
- 2020
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164. Transport mechanisms of water molecules and ions in sub-nano channels of nanostructured water treatment liquid-crystalline membranes: a molecular dynamics simulation study
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Takeshi Sakamoto, Takafumi Ogawa, Hiroki Nada, Masahiro Kimura, Takashi Kato, and Masahiro Henmi
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Environmental Engineering ,Chemistry ,Metadynamics ,Ionic bonding ,02 engineering and technology ,010402 general chemistry ,021001 nanoscience & nanotechnology ,01 natural sciences ,0104 chemical sciences ,Ion ,Molecular dynamics ,Membrane ,Permeability (electromagnetism) ,Chemical physics ,Molecule ,Water treatment ,0210 nano-technology ,Water Science and Technology - Abstract
Membranes with sub-nano channels formed by self-organization of ionic liquid-crystalline (LC) compounds have great potential as water treatment membranes. In this study, the transport mechanisms of water molecules and ions in the sub-nano channels of the LC membranes are investigated by molecular dynamics simulations for NaCl and NaNO3 solutions. The simulation results suggest that there are different transport mechanisms for water molecules and ions; the transport of water molecules occurs by Brownian diffusion, whereas that of ions occurs by jump diffusion between particular sites in the sub-nano channel. A free-energy landscape of an ion in the channel is analyzed using a metadynamics method, which indicates distinct local minima at particular sites and supports the jump diffusion mechanism. The effects of the LC compounds' structural flexibility and the electrostatic interaction with the wall of the sub-nano channels on the permeability of water molecules and ions are also investigated by molecular dynamics simulations. Simulation results suggest both the structural flexibility and the electrostatic interaction, which are characteristics of the LC membranes, are important factors in determining the water treatment performance. The structural flexibility affects the permeability of the membrane to water molecules and the electrostatic interaction reduces the permeability to ions.
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- 2020
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165. A Case of Primary Peritonitis due to Group A Streptococcus
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Saburo Sugita, Masahiro Kimura, Takaya Nagasaki, Toru Imagami, Misato Sawai, and Yuki Eguchi
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Primary Peritonitis ,medicine.medical_specialty ,Streptococcus ,business.industry ,Internal medicine ,General Engineering ,medicine ,General Earth and Planetary Sciences ,medicine.disease_cause ,business ,Group A ,Gastroenterology ,General Environmental Science - Published
- 2020
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166. Sporadic neurofibroma of transverse colon in a patient without neurofibromatosis type 1: A case report
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Keisuke Ito, Toru Imagami, Masahiro Kimura, Saburo Sugita, Takaya Nagasaki, and Shingo Inaguma
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Laparoscopic surgery ,medicine.medical_specialty ,Colon ,Colorectal cancer ,medicine.medical_treatment ,Colonoscopy ,Article ,NF1, neurofibromatosis type 1 ,03 medical and health sciences ,0302 clinical medicine ,Biopsy ,medicine ,Neurofibroma ,Neurofibromatosis ,MPNSTs, malignant peripheral nerve sheath tumors ,medicine.diagnostic_test ,business.industry ,Fecal occult blood ,Transverse colon ,Endoscopy ,CME, complete mesocolic excision ,medicine.disease ,CT, computed tomography ,030220 oncology & carcinogenesis ,030211 gastroenterology & hepatology ,Surgery ,Radiology ,business - Abstract
Introduction The occurrence of sporadic colonic neurofibroma particularly in a patient without neurofibromatosis type 1 has been rarely reported. Therefore, the clinical significance of this disease has not been fully elucidated. Presentation of case An 81-year-old woman with a positive fecal occult blood test result was referred to our institution for the evaluation of anemia. On colonoscopy, a 50-mm submucosal tumor-like mass was found in the hepatic flexure of the colon. Superficial biopsy and boring biopsy showed unspecific granulation tissues, and immunostaining revealed that the mesenchymal tumor was negative for CD34, c-kit, desmin, and S100 protein. The patient underwent laparoscopic right colectomy with complete mesocolic excision (CME). Pathologically, the tumor was diagnosed as neurofibroma. Discussion Gastrointestinal neurofibromas are known to cause clinical symptoms. No colonic neurofibroma has been diagnosed before resection. Moreover, neurofibromas, particularly large lesions, reportedly undergo malignant transformation. Surgical extirpation with clear margins is the primary treatment, and laparoscopic surgery is considered acceptable for colonic neurofibroma and colon cancer. Conclusion Based on our experience, a preoperative diagnosis was impossible for colonic neurofibroma. Laparoscopic surgery with CME is considered feasible for sporadic colonic neurofibroma.
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- 2020
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167. Cardioprotective Effects of VCP Modulator KUS121 in Murine and Porcine Models of Myocardial Infarction
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Randolph Ruiz Rodriguez, Fumiko Nakazeki, Takeshi Kimura, Chiharu Otani, Yuya Ide, Sijia Xu, Takahiro Horie, Akira Kakizuka, Toshimitsu Watanabe, Koh Ono, Yui Miyasaka, Satoshi Koyama, Yasuhide Kuwabara, Naritatsu Saito, Masamichi Yamamoto, Tomohiro Nishino, Shin Watanabe, Yasuhiro Nakashima, Tomohiro Yamasaki, Masahiro Kimura, Hitoo Nishi, Motoko Yanagita, Masataka Nishiga, Shuhei Tsuji, and Tetsushi Nakao
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0301 basic medicine ,lcsh:Diseases of the circulatory (Cardiovascular) system ,medicine.medical_treatment ,030204 cardiovascular system & hematology ,HF, heart failure ,PRECLINICAL RESEARCH ,0302 clinical medicine ,CMR, cardiac magnetic resonance ,Medicine ,LV, left ventricular/ventricle ,TTC, triphenyltetrazolium chloride ,Myocardial infarction ,I/R, ischemia and reperfusion ,FS, fractional shortening ,IHD, ischemic heart disease ,myocardial infarction ,H2O2, hydrogen peroxide ,MI, myocardial infarction ,Cardiology ,cardiovascular system ,AAR, area at risk ,ATPase, adenosine triphosphatase ,ER stress ,KUS121, Kyoto University Substance 121 ,Cardiology and Cardiovascular Medicine ,IBMPFD, inclusion body myopathy associated with Paget's disease of bone and frontotemporal dementia ,medicine.medical_specialty ,ATP, adenosine triphosphate ,Ischemia ,CHOP, C/EBP homologous protein ,FRET, fluorescence resonance energy transfer ,ER, endoplasmic reticulum ,03 medical and health sciences ,Reperfusion therapy ,Internal medicine ,KUS121 ,EF, ejection fraction ,cardiovascular diseases ,PCI, percutaneous coronary intervention ,business.industry ,Endoplasmic reticulum ,TUNEL, terminal deoxynucleotidyl transferase dUTP nick-end labeling ,BiP, immunoglobulin heavy chain-binding protein ,Percutaneous coronary intervention ,medicine.disease ,Infarct size ,ATP ,VCP, valosin-containing protein ,030104 developmental biology ,LAD, left anterior descending artery ,lcsh:RC666-701 ,Unfolded protein response ,business ,Reperfusion injury - Abstract
Visual Abstract, Highlights • KUS121 was developed to selectively inhibit the adenosine triphosphatase activity of valosin-containing protein without affecting other cellular functions of valosin-containing protein. • KUS121 preserved adenosine triphosphate levels, reduced endoplasmic reticulum stress, and suppressed cell death in H9C2 rat cardiomyoblast cells, treated with tunicamycin or hydrogen peroxide, or cultured in glucose-free medium. • In murine ischemia and reperfusion injury models, KUS121 treatment after reperfusion attenuated the infarcted size and preserves cardiac function by maintaining adenosine triphosphate levels and reducing ER stress. • In porcine ischemia and reperfusion injury models, intracoronary administration of KUS121 also attenuated the infarcted area in a dose-dependent manner. • These results indicated that KUS121 is a promising novel therapeutic agent for myocardial infarction., Summary No effective treatment is yet available to reduce infarct size and improve clinical outcomes after acute myocardial infarction by enhancing early reperfusion therapy using primary percutaneous coronary intervention. The study showed that Kyoto University Substance 121 (KUS121) reduced endoplasmic reticulum stress, maintained adenosine triphosphate levels, and ameliorated the infarct size in a murine cardiac ischemia and reperfusion injury model. The study confirmed the cardioprotective effect of KUS121 in a porcine ischemia and reperfusion injury model. These findings confirmed that KUS121 is a promising novel therapeutic agent for myocardial infarction in conjunction with primary percutaneous coronary intervention.
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- 2019
168. Direct comparison of chitinolytic properties and determination of combinatory effects of mouse chitotriosidase and acidic mammalian chitinase
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Takatoshi Umeyama, Kazuaki Okawa, Fumitaka Oyama, Vaclav Matoska, Masayoshi Sakaguchi, Peter Bauer, Masahiro Kimura, and Satoshi Wakita
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Chitin ,02 engineering and technology ,ACIDIC MAMMALIAN CHITINASE ,Biochemistry ,Substrate Specificity ,Mice ,03 medical and health sciences ,chemistry.chemical_compound ,Bacterial Proteins ,Structural Biology ,Animals ,Molecular Biology ,030304 developmental biology ,chemistry.chemical_classification ,0303 health sciences ,biology ,Hydrolysis ,Chitinases ,General Medicine ,Hydrogen-Ion Concentration ,Carbohydrate ,021001 nanoscience & nanotechnology ,biology.organism_classification ,Recombinant Proteins ,Molecular Weight ,Hexosaminidases ,Enzyme ,chemistry ,Serratia marcescens ,Chitinase ,biology.protein ,Colorimetry ,0210 nano-technology ,Bacteria - Abstract
Chitotriosidase (Chit1) and acidic mammalian chitinase (AMCase) have been implicated in food processing and various pathophysiological conditions such as chronic inflammatory diseases. By combination of the colorimetric analysis and fluorophore-assisted carbohydrate electrophoresis (FACE) method, we directly compared the chitinolytic properties of mouse Chit1 and AMCase and determined their combinatory effects in artificial and natural chitin substrates processing. Chit1 and AMCase display different dynamics of chitinolytic properties through acidic to neutral conditions. At pH2.0, the activity of AMCase was higher than that of Chit1 and stronger or comparable with that of Serratia marcescens chitinase B, a well-characterized bacterium chitinase. Changes of degradation products using different substrates indicate that AMCase and Chit1 have diverse properties under various pH conditions. Exposure of the chitin substrates to both Chit1 and AMCase did not indicate any mutual interference of these enzymes and showed no synergistic effect, in contrast to observations regarding some bacterial chitinases. Our results suggest that Chit1 and AMCase have no synergistic effect under physiological conditions.
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- 2019
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169. Application of High-Precision Assembly Technology for Large Structures by Laser Beam Welding
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Takashi Kagawa, Tomoyuki Nishiyama, Masahiro Kimura, and Shuho Tsubota
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Optics ,Materials science ,business.industry ,Laser beam welding ,business - Abstract
Toroidal Field coils (TF coils), which produce strong magnetic field in ITER, are used in order to confine the high temperature and high density plasmas stably for fusion reaction. The conductor made of Nb3Sn strands transform a superconducting conductor by heat treatment. The superconducting conductor is inserted into the D-shaped Radial Plate (RP), which have the structure with spiral grooves on both side for it, and then, insulating tapes are wound step by step around the superconducting conductor in RP as taking up the superconducting conductor. After insertion of the insulation-treated conductor into RP, Cover Plates (CPs) are put on RP spiral grooves and seal welded. After welding of CPs on RP of both sides, that the D-shaped Double Pancake (DP) is completed. The accuracy affects the TF coil performance and the deviation from ideal shapes and locations of the coils generates so called ‘error field’. In order to start up and confine the plasma stably, the allowable amount of the error field is about a few Gauss (Gauss : 1 × 10-4 T)[1]. Therefore, the dimensional accuracy of the 1/10000 order such as the profile within ±3mm for the circumference length and the flatness within ±3mm in the whole area of the D-shaped DP (14m × 9m) of approx. 37 m is required by ITER design. In addition, the TF coil is a huge component (with a weigh of about 300 ton) to withstand the high electromagnetic force of hundreds of MN. It is an essential requirement for ITER design to achieve the accuracy of more than 1/10000 even though machining after welding is not allowed. Laser beam welding technology for large structure with thick plate of Mitsubishi Heavy Industries was applied the TF coils to minimize and avoid large welding deformation in the conventional welding process such as TIG welding to meet the ITER requirements.
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- 2021
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170. Learning dynamical systems by recurrent neural networks from orbits.
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Masahiro Kimura and Ryohei Nakano
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- 1998
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171. Surface deformation with differential geometric structures.
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Masahiro Kimura, Takafumi Saito, and Mikio Shinya
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- 1996
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172. Development of Clinical Database System Specialized for Heavy Particle Therapy.
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Masami Mukai, Yutaka Ando, Yuki Yokooka, Yasuo Okuda, Masayoshi Seki, Masahiro Kimura, Hiroshi Tsuji, and Tadashi Kamada
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- 2015
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173. Learning Asynchronous-Time Information Diffusion Models and its Application to Behavioral Data Analysis over Social Networks
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Kazumi Saito, Masahiro Kimura, Kouzou Ohara, and Hiroshi Motoda
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- 2012
174. A Rare Case of Hypertrophic Cardiomyopathy with Subendocardial Late Gadolinium Enhancement in an Apical Aneurysm with Thrombus
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Yusuke Morita, Takao Kato, Mitsumasa Okano, Kanae Su, Masahiro Kimura, Eri Minamino, Eisaku Nakane, Toshiaki Izumi, Shoichi Miyamoto, Tetsuya Haruna, and Moriaki Inoko
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Medical physics. Medical radiology. Nuclear medicine ,R895-920 - Abstract
The mechanisms responsible for the development of apical aneurysms in cases of hypertrophic cardiomyopathy (HCM) are currently unclear but likely involve multiple factors. Here, we present a case of HCM with marked subendocardial fibrosis involving the apical and proximal portions of the left ventricle. A 71-year-old man with left ventricular hypertrophy presented with signs and symptoms of heart failure. The presence of asymmetrical left ventricular hypertrophy and bilateral, thickened ventricular walls with an apical aneurysm on transthoracic echocardiography suggested a diagnosis of HCM with ventricular dysfunction. No intraventricular pressure gradients with obstruction were identified. Late gadolinium enhancement (LGE) with cardiac magnetic resonance imaging and endomyocardial biopsies showed subendocardial fibrosis involving the apical aneurysm and proximal portion. Whereas LGE in a transmural pattern is commonly observed in HCM apical aneurysms, subendocardial LGE, as noted in the present case, is a relatively rare occurrence. Thus, the present case may provide unique insights into the adverse remodeling process and formation of apical aneurysms in cases of HCM.
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- 2014
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175. Tracheoesophageal Fistula due to a Damaged Tracheal Stent
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Masahiro Kimura, Yoshiyuki Kuwabara, Hideyuki Ishiguro, Tatsuya Tanaka, and Hiromitsu Takeyama
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Surgery ,RD1-811 - Abstract
We describe the management of a tracheoesophageal fistula due to a damaged tracheal stent, which was first inserted to treat tracheal stenosis. A 29-year-old woman with a history of treated epilepsy had a seizure and suffered from smoke inhalation during a fire. Breathing difficulties appeared and gradually worsened; consultation was obtained two years afterward. After undergoing a thorough examination, the patient was diagnosed with tracheal strangulation. A noncovered, metallic stent was inserted. When the patient was 37 years old, she was admitted to our hospital for the treatment of a tracheoesophageal fistula. We diagnosed it as a tracheoesophageal fistula due to the collapse of the damaged tracheal stent toward the esophageal side, and we decided to perform a mediastinal tracheostomy. Granulation may be formed in the circumference of a stent that has been present for a prolonged period, and removal of the stent may become difficult. This case suggests that insertion of a noncovered, metallic stent is contraindicated for a benign disease.
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- 2014
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176. Efficient Detection of Hot Span in Information Diffusion from Observation
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Kouzou Ohara, Kazumi Saito, Masahiro Kimura, and Hiroshi Motoda
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- 2011
177. Overview of the 84
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Koh, Ono, Satoshi, Shizuta, Erika, Yamamoto, Naritatsu, Saito, Neiko, Ozasa, Takao, Kato, Eri, Kato, Takahiro, Horie, Junichi, Tazaki, Hiroki, Shiomi, Shin, Watanabe, Hirotoshi, Watanabe, Yugo, Yamashita, Yusuke, Yoshikawa, Hideyuki, Kinoshita, Takeru, Makiyama, Yoshinori, Yoshida, Noboru, Ashida, Yasuaki, Nakagawa, Yasuhiro, Nakashima, Osamu, Baba, Hirohiko, Kohjitani, Masahiro, Kimura, Hideaki, Inazumi, Takashi, Yoshizawa, Akihiro, Komasa, and Takeshi, Kimura
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Societies, Scientific ,Japan ,Cardiovascular Diseases ,Research ,Surveys and Questionnaires ,Cardiology ,Telecommunications ,Humans ,Congresses as Topic - Abstract
Due to the COVID-19 pandemic, the 84
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- 2021
178. A simple and reliable procedure for laparoscopic port-site closure
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Takaya Nagasaki, Akira Mitsui, Yoshiyuki Kuwabara, Masahiro Kimura, Satomi Sawai, Seiji Nakaya, Saburo Sugita, and Yuki Eguchi
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Laparoscopic surgery ,medicine.medical_specialty ,medicine.medical_treatment ,Operative Time ,Closure (topology) ,Port site ,03 medical and health sciences ,0302 clinical medicine ,Postoperative Complications ,medicine ,Operation time ,Humans ,Hernia ,Laparoscopy ,medicine.diagnostic_test ,Sutures ,business.industry ,medicine.disease ,Port (computer networking) ,Surgery ,030220 oncology & carcinogenesis ,030211 gastroenterology & hepatology ,Laparoscopic Port ,business - Abstract
One of the complications in laparoscopic surgery is port-site hernia. It is a rare but potentially dangerous complication. Especially when using ports with a size 10 mm or more, it is required to securely close the port site. However, this procedure is often difficult especially for obese patients. We herein devised a new closure method by using a device developed for port site. These techniques are methods that can close the port site by a combination of putting in and out of thread and port rotation without removing a port. The port-site closure with these techniques was done for 53 port sites of 41 patients. The port site was closed horizontally or vertically, depending on the shape of the port site for two patients. Modified Z-suture was done for other 37 patients. To date, we have not noted any complications from this new method, including port-site hernia. With our technique, we could save operation time and reduce stress of us especially for obese patients. We would like to increase the number of patients and verify the safety and usefulness in further study.
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- 2021
179. Dynamic integration of height maps into a 3D world representation from range image sequences.
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Minoru Asada, Masahiro Kimura, Yasuhiro Taniguchi, and Yoshiaki Shirai
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- 1992
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180. Efficient Computing of PageRank Scores on Exact Expected Transition Matrix of Large Uncertain Graph
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Hiroshi Motoda, Kouzou Ohara, Takayasu Fushimi, Kazumi Saito, and Masahiro Kimura
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Computer science ,Computation ,Stochastic matrix ,02 engineering and technology ,Measure (mathematics) ,law.invention ,PageRank ,Ranking ,law ,020204 information systems ,0202 electrical engineering, electronic engineering, information engineering ,Rank (graph theory) ,020201 artificial intelligence & image processing ,Focus (optics) ,Centrality ,Algorithm ,Computer Science::Databases - Abstract
Ranking nodes in uncertain graph is computationally expensive when the graph is huge due to the extremely large number of possible worlds. Some approximation is needed in general. We focus on PageRank centrality measure to rank and propose a method that does not use any approximation for uncertain graph in which all the links can be uncertain. We first compute the expected transition matrix over all the possible graphs accurately and then run PageRank algorithm only once to rank the nodes (p-avg approach). This is not the same as computing the scores for each individual graph first and then rank the nodes by taking their average (s-avg approach). Exact computation of the latter is not possible because of the heavy computational load and only the approximate scores are obtained by limiting the number of graphs by sampling. We have tested the performance from various angles using three real world networks. We show that the proposed method (p-avg approach) gives very high precision to the s-avg approach for highly ranked nodes and can be a good alternative to it. Pactically, the p-avg approach runs orders of magnitude, i.e., sample size, faster than the s-avg approach.
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- 2020
- Full Text
- View/download PDF
181. Port site hernia repair using the VersaOne™ Fascial Closure System: a case report
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Takeyasu Katada, Seiichi Nakaya, Yoshiyuki Kuwabara, Yuki Eguchi, Misato Sawai, Saburo Sugita, Emi Hagui, Takaya Nagasaki, Akira Mitsui, and Masahiro Kimura
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Laparoscopic surgery ,medicine.medical_specialty ,AcademicSubjects/MED00910 ,Umbilicus (mollusc) ,medicine.medical_treatment ,Case Report ,laparoscopic herniorrhaphy ,Abdominal wall ,03 medical and health sciences ,0302 clinical medicine ,Suture (anatomy) ,medicine ,Laparoscopy ,jscrep/040 ,medicine.diagnostic_test ,business.industry ,Fascia ,Hernia repair ,abdominal incisional hernia ,port site hernia ,Surgery ,body regions ,medicine.anatomical_structure ,030220 oncology & carcinogenesis ,Abdomen ,030211 gastroenterology & hepatology ,port site closure ,business - Abstract
The use of laparoscopic surgery has become widespread in recent years. One of its complications is port site hernia (PHS). It can be difficult to close the fascia at the time of laparoscopy, especially in obese patients, and there is a risk of herniation through a fascial defect with incomplete closure. It is important to ascertain closure of the defect when repairing PHS to prevent recurrence. We report a 47-year-old woman who developed a PHS at the superior aspect of the umbilicus. We repaired the defect using the VersaOneTM Fascial Closure System with laparoscopic guidance. This system allows the port site to be reliably closed while observing the suture from the abdominal cavity. The incision is the same size as a port site. If the abdominal wall is thick and the PHS has a diameter of ~10 mm, this method is considered to be indicated, regardless of the site.
- Published
- 2020
182. Functional non-coding RNAs in vascular diseases
- Author
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Koh Ono, Masahiro Kimura, Randolph Ruiz Rodriguez, Takahiro Horie, Osamu Baba, Takeshi Kimura, Sawa Miyagawa, and Shuhei Tsuji
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0301 basic medicine ,RNA, Untranslated ,RNA ,Cell Biology ,Disease ,Computational biology ,Biology ,Biochemistry ,03 medical and health sciences ,030104 developmental biology ,0302 clinical medicine ,030220 oncology & carcinogenesis ,Genomic technology ,microRNA ,Humans ,Vascular Diseases ,Molecular Biology - Abstract
Recently, advances in genomic technology such as RNA sequencing and genome-wide profiling have enabled the identification of considerable numbers of non-coding RNAs (ncRNAs). MicroRNAs (miRNAs) have been studied for decades, leading to the identification of those with disease causing and/or protective effects in vascular disease. Although other ncRNAs such as long non-coding RNAs (lncRNAs) have not been fully described yet, recent studies have indicated their important functions in the development of vascular diseases. Here, we summarize the current understanding of the mechanisms and functions of ncRNAs, focusing on miRNAs, circular RNAs, and lncRNAs in vascular diseases.
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- 2020
183. Characterization of mouse di
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Misa, Ohno, Masao, Miyazaki, Masahiro, Kimura, Yusaku, Minowa, Masayoshi, Sakaguchi, Fumitaka, Oyama, and Tetsuro, Yamashita
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Kinetics ,Mice ,Acetylglucosaminidase ,Animals ,Oligosaccharides ,Chitin ,Substrate Specificity - Abstract
Di
- Published
- 2020
184. Lionheart LincRNA alleviates cardiac systolic dysfunction under pressure overload
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Masahiro Kimura, Tetsushi Nakao, Shin Watanabe, Yoshinori Yoshida, Osamu Baba, Masataka Nishiga, Takeshi Hatani, Tsukasa Inada, Yui Miyasaka, Naoya Sowa, Shinji Ito, Yasuhiro Nakashima, Yasuhide Kuwabara, Shuhei Tsuji, Hisanori Kiryu, Masayasu Izuhara, Koh Ono, Satoshi Koyama, Kazuya Nagao, Yuya Ide, Tomohiro Nishino, Takahiro Horie, Fumiko Nakazeki, and Takeshi Kimura
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0301 basic medicine ,Systole ,Biopsy ,Heart Ventricles ,Medicine (miscellaneous) ,030204 cardiovascular system & hematology ,Biology ,Contractile protein ,General Biochemistry, Genetics and Molecular Biology ,Article ,03 medical and health sciences ,0302 clinical medicine ,Downregulation and upregulation ,Myosin ,medicine ,Pressure ,Animals ,Humans ,Promoter Regions, Genetic ,lcsh:QH301-705.5 ,Pressure overload ,Mice, Knockout ,Heart ,Dependovirus ,medicine.disease ,Long non-coding RNA ,Cell biology ,Rats ,Up-Regulation ,Mice, Inbred C57BL ,Cardiac hypertrophy ,030104 developmental biology ,Phenotype ,lcsh:Biology (General) ,Heart failure ,biology.protein ,Long non-coding RNAs ,RNA, Long Noncoding ,MYH6 ,General Agricultural and Biological Sciences ,Protein A - Abstract
Recent high-throughput approaches have revealed a vast number of transcripts with unknown functions. Many of these transcripts are long noncoding RNAs (lncRNAs), and intergenic region-derived lncRNAs are classified as long intergenic noncoding RNAs (lincRNAs). Although Myosin heavy chain 6 (Myh6) encoding primary contractile protein is down-regulated in stressed hearts, the underlying mechanisms are not fully clarified especially in terms of lincRNAs. Here, we screen upregulated lincRNAs in pressure overloaded hearts and identify a muscle-abundant lincRNA termed Lionheart. Compared with controls, deletion of the Lionheart in mice leads to decreased systolic function and a reduction in MYH6 protein levels following pressure overload. We reveal decreased MYH6 results from an interaction between Lionheart and Purine-rich element-binding protein A after pressure overload. Furthermore, human LIONHEART levels in left ventricular biopsy specimens positively correlate with cardiac systolic function. Our results demonstrate Lionheart plays a pivotal role in cardiac remodeling via regulation of MYH6., Kuwabara et al. identify a novel long intergenic noncoding RNA (lincRNA), termed Lionheart, upregulated in pressure overloaded hearts in mice. Deleting this gene results in decreased systolic function and reduction in MYH6 protein levels following pressure overload. They demonstrate that Lionheart interacts with PURA, preventing its binding to the promoter region of Myh6 locus, leading to reduced MYH6 protein expression.
- Published
- 2020
185. MiR-33a is a therapeutic target in SPG4-related hereditary spastic paraplegia human neurons
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Masahiro Kimura, Keiko Imamura, Kayoko Tsukita, Yasuhide Kuwabara, Koh Ono, Yuya Ide, Yasuhiro Nakashima, Shigehiko Suzuki, Akitsu Hotta, Takahiro Horie, Tetsushi Nakao, Osamu Baba, Yuishin Izumi, Motoko Naitoh, Tomohiro Nishino, Haruhisa Inoue, Ryuji Kaji, Masataka Nishiga, Hitoo Nishi, Fumiko Nakazeki, Takeshi Kimura, Toshitaka Kawarai, Shuhei Tsuji, Satoshi Koyama, and Itaru Tsuge
- Subjects
0301 basic medicine ,Hereditary spastic paraplegia ,Intron ,General Medicine ,Biology ,medicine.disease ,Spastin ,Phenotype ,Sterol regulatory element-binding protein ,Cell biology ,03 medical and health sciences ,030104 developmental biology ,0302 clinical medicine ,microRNA ,medicine ,Binding site ,Induced pluripotent stem cell ,030217 neurology & neurosurgery - Abstract
Recent reports, including ours, have indicated that microRNA (miR)-33 located within the intron of sterol regulatory element binding protein (SREBP) 2 controls cholesterol homeostasis and can be a potential therapeutic target for the treatment of atherosclerosis. Here, we show that SPAST, which encodes a microtubule-severing protein called SPASTIN, was a novel target gene of miR-33 in human. Actually, the miR-33 binding site in the SPAST 3′-UTR is conserved not in mice but in mid to large mammals, and it is impossible to clarify the role of miR-33 on SPAST in mice. We demonstrated that inhibition of miR-33a, a major form of miR-33 in human neurons, via locked nucleic acid (LNA)-anti-miR ameliorated the pathological phenotype in hereditary spastic paraplegia (HSP)-SPG4 patient induced pluripotent stem cell (iPSC)-derived cortical neurons. Thus, miR-33a can be a potential therapeutic target for the treatment of HSP-SPG4.
- Published
- 2019
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- View/download PDF
186. Comparative functional analysis between human and mouse chitotriosidase: Substitution at amino acid 218 modulates the chitinolytic and transglycosylation activity
- Author
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Peter Bauer, Fumitaka Oyama, Vaclav Matoska, Kazutaka Sekine, Takashi Watanabe, Daisuke Yamanaka, Aoi Ikejiri, Minori Kamaya, Hitomi Ishizuka, Masahiro Kimura, and Masayoshi Sakaguchi
- Subjects
Glycosylation ,Chitin ,02 engineering and technology ,Biochemistry ,Gene Expression Regulation, Enzymologic ,law.invention ,03 medical and health sciences ,chemistry.chemical_compound ,Mice ,Structural Biology ,law ,Escherichia coli ,Animals ,Humans ,Molecular Biology ,030304 developmental biology ,chemistry.chemical_classification ,0303 health sciences ,Messenger RNA ,Functional analysis ,Chitinases ,Tryptophan ,General Medicine ,021001 nanoscience & nanotechnology ,Recombinant Proteins ,Amino acid ,Enzyme ,Hexosaminidases ,chemistry ,Amino Acid Substitution ,Recombinant DNA ,Leucine ,0210 nano-technology - Abstract
Chitotriosidase (Chit1) and acidic mammalian chitinase (AMCase) have been attracting research interest due to their involvement in various pathological conditions such as Gaucher's disease and asthma, respectively. Both enzymes are highly expressed in mice, while the level of AMCase mRNA was low in human tissues. In addition, the chitinolytic activity of the recombinant human AMCase was significantly lower than that of the mouse counterpart. Here, we revealed a substantially higher chitinolytic and transglycosylation activity of human Chit1 against artificial and natural chitin substrates as compared to the mouse enzyme. We found that the substitution of leucine (L) by tryptophan (W) at position 218 markedly reduced both activities in human Chit1. Conversely, the L218W substitution in mouse Chit1 increased the activity of the enzyme. These results suggest that Chit1 may compensate for the low of AMCase activity in humans, while in mice, highly active AMCase may supplements low Chit1 activity.
- Published
- 2020
187. The Listeria innocua chitinase LinChi78 has a unique region that is necessary for hydrolytic activity
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Yuji Oka, Fumitaka Oyama, Masahiro Kimura, Shotaro Honda, Satoshi Wakita, Masao Kawakita, and Masayoshi Sakaguchi
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Listeria ,Conserved Domain Database ,DNA Mutational Analysis ,Mutant ,Applied Microbiology and Biotechnology ,03 medical and health sciences ,Hydrolysis ,Protein Domains ,Sequence Deletion ,030304 developmental biology ,chemistry.chemical_classification ,0303 health sciences ,biology ,Functional analysis ,030306 microbiology ,Chitinases ,Substrate (chemistry) ,General Medicine ,Fibronectin ,Enzyme ,chemistry ,Biochemistry ,Chitinase ,biology.protein ,Biotechnology - Abstract
Chitinases are generally composed of multiple domains; a catalytic domain and one or more additional domains that are not absolutely required but may modify the chitinolytic activity. The LinChi78 chitinase from Listeria innocua has a catalytic domain (CatD), a fibronectin type III-like (FnIII) domain, a chitin-binding domain (ChBD), and an unknown-function region (UFR) located between the CatD and FnIII domains. The UFR is 146 amino acid residues in length and does not have a homologous domain in the Conserved Domain Database. We performed a functional analysis of these domains and the UFR using several C-terminally and internally deleted mutants of LinChi78. Hydrolysis of an artificial substrate was almost unaffected by deletion of the ChBD and/or the FnIII domain, although the ChBD-deleted enzymes were approximately 30% less active toward colloidal chitin than LinChi78. On the other hand, deletion of the UFR led to an extensive loss of chitinase activity toward an artificial substrate as well as polymeric substrates. Upon further analysis, we found that the GKQTI stretch, between the 567th (G) and 571th (I) amino acid residues, in the UFR is critical for LinChi78 activity and demonstrated that Gln569 and Ile571 play central roles in eliciting this activity. Taken together, these results indicated that LinChi78 has a unique catalytic region composed of a typical CatD and an additional region that is essential for activity. Characterization of the unique catalytic region of LinChi78 will improve our understanding of GH18 chitinases.
- Published
- 2019
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188. High Virus Removal by Self-Organized Nanostructured 2D Liquid-Crystalline Smectic Membranes for Water Treatment
- Author
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Hiroki Nada, K. R. Sunil Kumar, Daniel Kuo, Masahiro Henmi, Nobuyoshi Miyamoto, Kazuma Hamaguchi, Riki Kato, Miaomiao Liu, Takeshi Sakamoto, Hiroyuki Katayama, Takashi Kato, Takafumi Ogawa, Kian Ping Gan, and Masahiro Kimura
- Subjects
Materials science ,02 engineering and technology ,010402 general chemistry ,01 natural sciences ,Water Purification ,Biomaterials ,chemistry.chemical_compound ,Liquid crystal ,General Materials Science ,In situ polymerization ,Mesogen ,Membranes, Artificial ,General Chemistry ,Permeation ,021001 nanoscience & nanotechnology ,0104 chemical sciences ,Liquid Crystals ,Nanostructures ,Monomer ,Membrane ,chemistry ,Chemical engineering ,Viruses ,Water treatment ,Self-assembly ,0210 nano-technology ,Biotechnology - Abstract
To obtain high quality of drinking water free from biocontaminants is especially important issue. A new strategy employing smectic liquid-crystalline ionic membranes exhibiting 2D structures of layered nanochannels for water treatment is proposed for efficient virus removal and sufficient water flux. The smectic A (SmA) liquid-crystalline membranes obtained by in situ polymerization of an ionic mesogenic monomer are examined for removal of three distinct viruses with small size: Qβ bacteriophage, MS2 bacteriophage, and Aichi virus. The semi-bilayer structure of the SmA significantly obstructs the virus penetration with an average log reduction value of 7.3 log10 or the equivalent of reducing 18 million viruses down to 1. Furthermore, the layered nanochannels of the SmA liquid crystal allow efficient water permeation compared to other types of liquid-crystalline membrane consisting of nanopores.
- Published
- 2020
189. Homeobox A4 suppresses vascular remodeling by repressing <scp>YAP</scp> / <scp>TEAD</scp> transcriptional activity
- Author
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Koh Ono, Toshimitsu Watanabe, Yuya Ide, Masahiro Kimura, Chiharu Otani, Takeshi Kimura, Tomohiro Yamasaki, Sijia Xu, Takahiro Horie, Randolph Ruiz Rodriguez, Osamu Baba, Shuhei Tsuji, Yasuhiro Nakashima, and Yui Miyasaka
- Subjects
Vascular Biology & Angiogenesis ,HOXA4 ,vascular remodeling ,Myocytes, Smooth Muscle ,Phenotypic switching ,Repressor ,Biology ,Biochemistry ,Article ,Mice ,03 medical and health sciences ,0302 clinical medicine ,Genetics ,Animals ,Enhancer ,Molecular Biology ,Transcription factor ,030304 developmental biology ,Homeodomain Proteins ,0303 health sciences ,Hippo signaling pathway ,Activator (genetics) ,Hippo signaling ,phenotypic switching ,Genes, Homeobox ,Articles ,homeobox genes ,Cell biology ,Development & Differentiation ,030217 neurology & neurosurgery ,Signal Transduction ,Transcription Factors - Abstract
The Hippo signaling pathway is involved in the pathophysiology of various cardiovascular diseases. Yes‐associated protein (YAP) and transcriptional enhancer activator domain (TEAD) transcriptional factors, the main transcriptional complex of the Hippo pathway, were recently identified as modulators of phenotypic switching of vascular smooth muscle cells (VSMCs). However, the intrinsic regulator of YAP/TEAD‐mediated gene expressions involved in vascular pathophysiology remains to be elucidated. Here, we identified Homeobox A4 (HOXA4) as a potent repressor of YAP/TEAD transcriptional activity using lentiviral shRNA screen. Mechanistically, HOXA4 interacts with TEADs and attenuates YAP/TEAD‐mediated transcription by competing with YAP for TEAD binding. We also clarified that the expression of HOXA4 is relatively abundant in the vasculature, especially in VSMCs. In vitro experiments in human VSMCs showed HOXA4 maintains the differentiation state of VSMCs via inhibition of YAP/TEAD‐induced phenotypic switching. We generated Hoxa4‐deficient mice and confirmed the downregulation of smooth muscle‐specific contractile genes and the exacerbation of vascular remodeling after carotid artery ligation in vivo. Our results demonstrate that HOXA4 is a repressor of VSMC phenotypic switching by inhibiting YAP/TEAD‐mediated transcription., HOXA4 suppresses vascular smooth muscle cell phenotypic switching and vascular remodeling by inhibiting YAP/TEAD‐mediated transcription.
- Published
- 2020
- Full Text
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190. Functionally modified chitotriosidase catalytic domain for chitin detection based on split-luciferase complementation
- Author
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Daisuke Yamanaka, Kento Suzuki, Masahiro Kimura, Fumitaka Oyama, and Yoshiyuki Adachi
- Subjects
Dermatophagoides farinae ,Polymers and Plastics ,Dermatophagoides pteronyssinus ,Organic Chemistry ,Carbohydrates ,Chitin ,Cockroaches ,Enzyme-Linked Immunosorbent Assay ,Biosensing Techniques ,Hexosaminidases ,Catalytic Domain ,Candida albicans ,Mutation ,Materials Chemistry ,Animals ,Luciferases - Abstract
In this study, we applied a luciferase-fragment complementation assay for chitin detection. When luciferase-fragment fused chitin-binding proteins were mixed with chitin, the reconstituted luciferase became active. The recombinant chitin-binding domain (CBD) and a functionally modified catalytic domain (CatD) of human chitotriosidase were employed for this method. We designed the CatD mutant as a chitin-binding protein with diminished chitinolytic activity. The non-wash assay using the CatD mutant had higher sensitivity than CBD for chitin detection and proved to be a structure-specific biosensor for chitin, including crude biomolecules (from fungi, mites, and cockroaches). The CatD mutant recognized a chitin-tetramer as the minimal binding unit and bound chitin at K
- Published
- 2022
- Full Text
- View/download PDF
191. Validation of the vulnerable crotch on a side-to-side anastomosis: Observation of the burst process
- Author
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Takaya Nagasaki, Yasuyuki Shibata, Yuki Eguchi, Shuhei Ueno, Masahiro Kimura, Nobuo Ochi, Satoshi Taniwaki, and Hiroyuki Asai
- Subjects
Stapled anastomosis ,medicine.medical_specialty ,Leak ,business.industry ,Crotch ,Lumen (anatomy) ,Anastomosis ,Surgery ,03 medical and health sciences ,0302 clinical medicine ,medicine.anatomical_structure ,030220 oncology & carcinogenesis ,Staple line ,Medicine ,030211 gastroenterology & hepatology ,business ,Side to side anastomosis ,Burst pressure - Abstract
The vulnerability of the crotch on a side-to-side anastomosis to leak has been widely recognized. However, countermeasures to prevent leaks from the crotch have not proven to be sufficient. A side-to-side anastomosis was performed between two intestinal specimens using a linear stapler. We analyzed the burst pressures of anastomoses. Comparison was made in five groups, with different staple heights, presence of Neoveil® (Gunze, Japan), with or without crotch buttressed with nylon. Using an endoscope inserted into the intestinal lumen, we observed the burst process. We observed a significant difference in the resistance of the crotch to leak between the two types of reinforcement. In all experimental groups, the leak was observed not only on the serosal surface but also from within the lumen. Neoveil® significantly increased the burst pressure (41.4 ± 3.6 vs. 88.8 ± 14.6 mm Hg; p
- Published
- 2018
- Full Text
- View/download PDF
192. SREBF1 /MicroRNA-33b Axis Exhibits Potent Effect on Unstable Atherosclerotic Plaque Formation In Vivo
- Author
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Fumiko Nakazeki, Takeshi Kimura, Susumu Miyamoto, Koji Hasegawa, Kazumichi Yoshida, Yuya Ide, Koh Ono, Yasuhide Kuwabara, Masataka Nishiga, Yasushi Takagi, Satoshi Koyama, Takahiro Horie, Osamu Baba, Tomohiro Nishino, Yasuhiro Nakashima, Hitoo Nishi, Naoya Sowa, Masahiro Kimura, Ritsuko Hanada, Tomoyuki Nakamura, Manabu Nagata, and Tetsushi Nakao
- Subjects
Male ,0301 basic medicine ,Bone marrow transplantation ,Mice, Knockout, ApoE ,Common disease ,Apoptosis ,030204 cardiovascular system & hematology ,Article ,03 medical and health sciences ,Membrane Microdomains ,0302 clinical medicine ,In vivo ,microRNA ,Animals ,Humans ,Triglycerides ,Aged ,Bone Marrow Transplantation ,Aged, 80 and over ,Chemistry ,Macrophages ,Cholesterol, HDL ,Cholesterol hdl ,Lipid metabolism ,Middle Aged ,Atherosclerosis ,Plaque, Atherosclerotic ,Sterol ,Mice, Inbred C57BL ,Disease Models, Animal ,MicroRNAs ,Phenotype ,030104 developmental biology ,Gene Expression Regulation ,Intestinal Absorption ,Case-Control Studies ,Cancer research ,Female ,Sterol Regulatory Element Binding Protein 1 ,Cardiology and Cardiovascular Medicine ,Signal Transduction - Abstract
Objective— Atherosclerosis is a common disease caused by a variety of metabolic and inflammatory disturbances. MicroRNA (miR)-33a within SREBF2 (sterol regulatory element-binding factor 2) is a potent target for treatment of atherosclerosis through regulating both aspects; however, the involvement of miR-33b within SREBF1 remains largely unknown. Although their host genes difference could lead to functional divergence of miR-33a/b, we cannot dissect the roles of miR-33a/b in vivo because of lack of miR-33b sequences in mice, unlike human. Approach and Results— Here, we analyzed the development of atherosclerosis using miR-33b knock-in humanized mice under apolipoprotein E–deficient background. MiR-33b is prominent both in human and mice on atheroprone condition. MiR-33b reduced serum high-density lipoprotein cholesterol levels and systemic reverse cholesterol transport. MiR-33b knock-in macrophages showed less cholesterol efflux capacity and higher inflammatory state via regulating lipid rafts. Thus, miR-33b promotes vulnerable atherosclerotic plaque formation. Furthermore, bone marrow transplantation experiments strengthen proatherogenic roles of macrophage miR-33b. Conclusions— Our data demonstrated critical roles of SREBF1 -miR-33b axis on both lipid profiles and macrophage phenotype remodeling and indicate that miR-33b is a promising target for treating atherosclerosis.
- Published
- 2018
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- View/download PDF
193. A Simple and Reliable Procedure Modification for Inverting Stripping Resection of the Esophagus
- Author
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Satoshi Taniwaki, Yuki Eguchi, Hiroyuki Asai, Kotaro Mizuno, Takaya Nagasaki, Yasuyuki Shibata, Masahiro Kimura, Nobuo Ochi, and Shuhei Ueno
- Subjects
Materials science ,medicine.anatomical_structure ,Simple (abstract algebra) ,medicine ,General Medicine ,Esophagus ,Stripping (fiber) ,Resection ,Biomedical engineering - Published
- 2018
- Full Text
- View/download PDF
194. Loss of periostin ameliorates adipose tissue inflammation and fibrosis in vivo
- Author
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Koh Ono, Fumiko Nakazeki, Takeshi Kimura, Satoshi Koyama, Masataka Nishiga, Naoya Sowa, Simon J. Conway, Masahiro Kimura, Shuhei Tsuji, Hitoo Nishi, Yasuhide Kuwabara, Shigeo Yoshida, Takahiro Horie, Motoko Yanagita, Yasuhiro Nakashima, Tetsushi Nakao, Yuya Ide, Tomohiro Nishino, and Osamu Baba
- Subjects
0301 basic medicine ,medicine.medical_specialty ,Adipose tissue ,lcsh:Medicine ,Inflammation ,Intra-Abdominal Fat ,Periostin ,Article ,Mice ,03 medical and health sciences ,Insulin resistance ,In vivo ,Fibrosis ,Internal medicine ,medicine ,Animals ,Obesity ,lcsh:Science ,Mice, Knockout ,Multidisciplinary ,business.industry ,lcsh:R ,Cellulitis ,Hypoxia (medical) ,medicine.disease ,Dietary Fats ,Haematopoiesis ,030104 developmental biology ,Endocrinology ,lcsh:Q ,Insulin Resistance ,medicine.symptom ,business ,Cell Adhesion Molecules - Abstract
Recent evidence suggests that the accumulation of macrophages as a result of obesity-induced adipose tissue hypoxia is crucial for the regulation of tissue fibrosis, but the molecular mechanisms underlying adipose tissue fibrosis are still unknown. In this study, we revealed that periostin (Postn) is produced at extraordinary levels by adipose tissue after feeding with a high-fat diet (HFD). Postn was secreted at least from macrophages in visceral adipose tissue during the development of obesity, possibly due to hypoxia. Postn−/− mice had lower levels of crown-like structure formation and fibrosis in adipose tissue and were protected from liver steatosis. These mice also showed amelioration in systemic insulin resistance compared with HFD-fed WT littermates. Mice deficient in Postn in their hematopoietic compartment also had lower levels of inflammation in adipose tissue, in parallel with a reduction in ectopic lipid accumulation compared with the controls. Our data indicated that the regulation of Postn in visceral fat could be beneficial for the maintenance of healthy adipose tissue in obesity.
- Published
- 2018
- Full Text
- View/download PDF
195. Which is more influential, 'Who' or 'When' for a user to rate in online review site?
- Author
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Masahiro Kimura, Kouzou Ohara, Kazumi Saito, and Hiroshi Motoda
- Subjects
Artificial Intelligence ,Computer science ,020204 information systems ,0202 electrical engineering, electronic engineering, information engineering ,020201 artificial intelligence & image processing ,02 engineering and technology ,Computer Vision and Pattern Recognition ,Theoretical Computer Science - Published
- 2018
- Full Text
- View/download PDF
196. Modification of the Postlethwait Method in Improvement of Esophageal Bypass: An Essential Treating Method
- Author
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Akira Mitsui, Yasuyuki Shibata, Yoshiyuki Kuwabara, and Masahiro Kimura
- Subjects
General Medicine - Published
- 2018
- Full Text
- View/download PDF
197. Digest Visualization of Photo Spots in Terms of Seasonal Uniqueness
- Author
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Masahito Kumano, Kazuya Hashimoto, and Masahiro Kimura
- Subjects
General Medicine - Published
- 2018
- Full Text
- View/download PDF
198. Askin’s tumor in an elderly patient
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Emiko Nishikawa, Shuichi Yano, Mitsuhiro Tada, Masahiro Kimura, Saburo Nagaoka, Fumihito Tajima, Takeshi Minamizaki, Shinichi Iwamoto, Toru Kadowaki, Toshikazu Ikeda, and Kanako Kobayashi
- Subjects
medicine.medical_specialty ,Palliative care ,business.industry ,MEDLINE ,Mediastinum ,medicine.disease ,Text mining ,medicine.anatomical_structure ,Medicine ,Radiology ,Sarcoma ,business ,Elderly patient ,Biopsy methods - Published
- 2019
- Full Text
- View/download PDF
199. Visualizing attractive periods of popular photo spots using Flickr data.
- Author
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Satoshi Iwabuchi, Masahito Kumano, Motonori Koseki, Keiko Ono, and Masahiro Kimura
- Published
- 2013
- Full Text
- View/download PDF
200. Age-hardening structure and mechanism of Cu–3at%Ni–1.5 at%Si Corson alloy
- Author
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Kazuhiko Fukamachi and Masahiro Kimura
- Subjects
Ostwald ripening ,Materials science ,Mechanical Engineering ,Alloy ,engineering.material ,Condensed Matter Physics ,symbols.namesake ,Crystallography ,Precipitation hardening ,Mechanics of Materials ,Transmission electron microscopy ,Scanning transmission electron microscopy ,Hardening (metallurgy) ,symbols ,engineering ,General Materials Science ,Crystal habit ,Spectroscopy - Abstract
The age-hardening structure and mechanism of a Cu–3at%Ni–1.5 at%Si Corson alloy were elucidated using high-resolution scanning transmission electron microscopy. The alloy samples were solution-treated at 850 °C and reached peak strength after 6 h of aging at 450 °C. The hardening structure is composed of δ′-Ni2Si precipitates, which are slightly distorted from δ-Ni2Si (oP12, Pnma, C23, Prototype: Co2Si) by the Cu matrix to increase coherence. After identifying the structure using atomic-resolution energy dispersive X-ray spectroscopy, the electron diffraction pattern could be completely indexed. The δ′-Ni2Si precipitates have stacking faults on the (004)δ'-Ni2Si planes, which result in dark bands in the transmission electron microscopy image of the precipitates and streaks in the electron diffraction pattern. No interface-like crystal habit plane or rigid boundary was observed between the δ′-Ni2Si precipitates and the Cu matrix, indicating a diffuse boundary. The δ′-Ni2Si lattice had corresponding planes that were almost parallel and approximately equal to all the planes in a particular slip system: {111}Cu Cu. From their orientation relationships, the precipitates were to be coherent with the matrix. Under the conditions of this study, the precipitates grew via Ostwald ripening and supported the peak strength via precipitation hardening with the cutting mechanism.
- Published
- 2022
- Full Text
- View/download PDF
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