Your search keyword '"Sugiyama, Kanako"' showing total 12 results

1. Structure-based analysis of domain function of chitin oligosaccharide deacetylase from Vibrio parahaemolyticus.

Author

Hirano, Takako, Sugiyama, Kanako, Sakaki, Yuta, Hakamata, Wataru, Park, Sam-Yong, and Nishio, Toshiyuki

Subjects

*CHITIN deacetylase, *OLIGOSACCHARIDES, *VIBRIO parahaemolyticus, *CRYSTAL structure, *CARBOHYDRATES, *MATHEMATICAL domains

Abstract

The X-ray crystal structure of chitin oligosaccharide deacetylase from Vibrio parahaemolyticus ( Vp -COD) was determined at an 1.35 Å resolution. The amino acid sequence and structure of Vp -COD show that the enzyme comprises one polysaccharide deacetylase domain (PDD) and two carbohydrate-binding domains (CBDs). On the basis of a chitin-binding assay with Vp -COD and its CBDs-deleted mutant, it was confirmed that CBDs can adhere to chitin. The catalytic activity of the CBDs-deleted mutant was only mildly depressed compared with that of Vp -COD, indicating that CBDs are unlikely to affect the configuration of the active center residues in active site of PDD. [ABSTRACT FROM AUTHOR]

Published

2015

2. Capturing the Hemoglobin Allosteric Transition in a Single Crystal Form.

Author

Shibayama, Naoya, Sugiyama, Kanako, Tame, Jeremy R. H., and Sam-Yong Park

Subjects

*HEMOGLOBINS, *SINGLE crystals, *ALLOSTERIC regulation, *PROTEINS, *X-ray diffraction

Abstract

Allostery in many oligomeric proteins has been postulated to occur via a ligand-binding-driven conformational transition from the tense (T) to relaxed (R) state, largely on the basis of the knowledge of the structure and function of hemoglobin, the most thoroughly studied of all allosteric proteins. However, a growing body of evidence suggests that hemoglobin possesses a variety of intermediates between the two end states. As such intermediate forms coexist with the end states in dynamic equilibrium and cannot be individually characterized by conventional techniques, very little is known about their properties and functions. Here we present complete structural and functional snapshots of nine equilibrium conformers of human hemoglobin in the half-liganded and fully liganded states by using a novel combination of X-ray diffraction analysis and microspectrophotometric O2 equilibrium measurements on three isomorphous crystals, each capturing three distinct equilibrium conformers. Notably, the conformational set of this crystal form varies according to shifts in the allosteric equilibrium, reflecting the differences in hemoglobin ligation state and crystallization solution conditions. We find that nine snapshot structures cover the complete conformational space of hemoglobin, ranging from T to R2 (the second relaxed quaternary structure) through R, with various relaxed intermediate forms between R and R2. Moreover, we find a previously unidentified intermediate conformer, between T and R, with an intermediate O2 affinity, sought by many research groups over a period of decades. These findings reveal a comprehensive picture of the equilibrium conformers and transition pathway for human hemoglobin. [ABSTRACT FROM AUTHOR]

Published

2014

3. Structures and Oxygen Affinities of Crystalline Human Hemoglobin C(β6 Glu → Lys) in the Rand R2 Quaternary Structu res*.

Author

Shibayama, Naoya, Sugiyama, Kanako, and Sam-Yong Park

Abstract

Recent crystallographic studies suggested that fully liganded human hemoglobin can adopt multiple quaternary conformations that include the two previously solved relaxed conformations, R and R2, whereas fully unliganded deoxyhemoglobin may adopt only one T (tense) quaternary conformation. An important unanswered question is whether R, R2, and other relaxed quaternary conformations represent different physiological states with different oxygen affinities. Here, we answer this question by showing the oxygen equilibrium curves of single crystals of human hemoglobin in the R and R2 state. In this study, we have used a naturally occurring mutant hemoglobin C (j36 GIu-~Lys) to stabilize the R and R2 crystals. Additionally, we have refined the x-ray crystal structure of carbonmonoxyhemoglobin C, in the R and R2 state, to 1.4 and 1.8 A resolution, respectively, to compare precisely the structures of both types of relaxed states. Despite the large quaternary structural difference between the R and R2 state, both crystals exhibit similar noncooperative oxygen equilibrium curves with a very high affinity for oxygen, comparable with the fourth oxygen equilibrium constant (K4) of human hemoglobin in solution. One small difference is that the R2 crystals have an oxygen affinity that is 2-3 times higher than that of the R crystals. These results demonstrate that the functional difference between the two typical relaxed quaternary conformations is small and physiologically less important, indicating that these relaxed conformations simply reflect a structural polymorphism of a high affinity relaxed state. [ABSTRACT FROM AUTHOR]

Published

2011

4. Structural insight into the essential PB1–PB2 subunit contact of the influenza virus RNA polymerase.

Author

Sugiyama, Kanako, Obayashi, Eiji, Kawaguchi, Atsushi, Suzuki, Yukari, Tame, Jeremy R. H., Nagata, Kyosuke, and Park, Sam-Yong

Subjects

*INFLUENZA viruses, *RNA polymerases, *ENZYME activation, *ENZYME regulation, *VIRAL genetics, *GENETICS

Abstract

Influenza virus RNA-dependent RNA polymerase is a multi-functional heterotrimer, which uses a ‘cap-snatching’ mechanism to produce viral mRNA. Host cell mRNA is cleaved to yield a cap-bearing oligonucleotide, which can be extended using viral genomic RNA as a template. The cap-binding and endonuclease activities are only activated once viral genomic RNA is bound. This requires signalling from the RNA-binding PB1 subunit to the cap-binding PB2 subunit, and the interface between these two subunits is essential for the polymerase activity. We have defined this interaction surface by protein crystallography and tested the effects of mutating contact residues on the function of the holo-enzyme. This novel interface is surprisingly small, yet, it has a crucial function in regulating the 250 kDa polymerase complex and is completely conserved among avian and human influenza viruses. [ABSTRACT FROM AUTHOR]

Published

2009

5. Elevated levels of interferon γ-inducible protein-10 and epithelial neutrophil-activating peptide-78 in patients with pulmonary sarcoidosis.

Author

Sugiyama, Kanako, Mukae, Hiroshi, Ishii, Hiroshi, Kakugawa, Tomoyuki, Ishimoto, Hiroshi, Nakayama, Seiko, Shirai, Ryo, Fujii, Takeshi, Mizuta, Yohei, and Kohno, Shigeru

Subjects

*SARCOIDOSIS, *CHEMOKINES, *INTERFERONS, *LYMPHOCYTES, *LUNG diseases, *NEUTROPHILS

Abstract

Objective and background: Interferon γ-inducible protein (IP)-10 and epithelial neutrophil-activating peptide (ENA)-78 belong to the CXC chemokine family and are important factors in inflammatory lung diseases. In sarcoidosis, the potential role of IP-10 to regulate the migration and activation of T-cells towards sites of sarcoid activity has been suggested. Methods: In this study, the concentrations of IP-10 and ENA-78 in the serum and BAL fluid of patients with different stages of active pulmonary sarcoidosis ( n = 41) and healthy subjects ( n = 12) were measured by enzyme-linked immunosorbent assay to evaluate the contribution of these CXC chemokines to this disease. Results: Serum and BAL fluid concentrations of IP-10 and BAL fluid levels of ENA-78 in patients with sarcoidosis were significantly higher than those in control subjects. The serum levels of IP-10 were significantly increased only in patients with stages I and II sarcoidosis, while BAL fluid levels of ENA-78 were increased only in stage III sarcoidosis. In addition, serum concentrations of IP-10 were elevated in patients with extrapulmonary lesions compared with those without such lesions. In patients with sarcoidosis, IP-10 concentrations in BAL fluid correlated with lymphocyte proportions in BAL fluid. Conclusion: IP-10 may play an important role in regulating lymphocytes into the lung and that ENA-78 may be associated with lung parenchymal disease in pulmonary sarcoidosis. [ABSTRACT FROM AUTHOR]

Published

2006

6. Structural characterization of the photoswitchable fluorescent protein Dronpa-C62S

Author

Nam, Ki-Hyun, Kwon, Oh Yeun, Sugiyama, Kanako, Lee, Won-Ho, Kim, Young Kwan, Song, Hyun Kyu, Kim, Eunice Eunkyung, Park, Sam-Yong, Jeon, Hyesung, and Hwang, Kwang Yeon

Subjects

*GREEN fluorescent protein, *FLUORESCENT polymers, *GENETIC mutation, *HYDROGEN bonding

Abstract

Abstract: The photoswitching behavior of green fluorescent proteins (GFPs) or GFP-like proteins is increasingly recognized as a new technique for optical marking. Recently, Ando and his colleagues developed a new green fluorescent protein Dronpa, which possesses the unique photochromic property of being photoswitchable in a non-destructive manner. To better understand this mechanism, we determined the crystal structures of a new GFP Dronpa and its mutant C62S, at 1.9Å and 1.8Å, respectively. Determination of the structures demonstrates that a unique hydrogen-bonding network and the sulfur atom of the chromophore are critical to the photoswitching property of Dronpa. Reversible photoswitching was lost in cells expressing the Dronpa-C62S upon repetitive irradiation compared to the native protein. Structural and mutational analyses reveal the chemical basis for the functional properties of photoswitchable fluorescent proteins and provide the basis for subsequent coherent engineering of this subfamily of Dronpa homolog’s. [Copyright &y& Elsevier]

Published

2007

7. Crystallization and preliminary crystallographic studies of the butyrolactone autoregulator receptor protein (BarA) from Streptomyces virginiae.

Author

Yoon, Young-Ho, Kawai, Fumihiro, Sugiyama, Kanako, Park, Sam-Yong, Nihira, Takuya, Choi, Sun-Uk, and Hwang, Yong-Il

Subjects

*BACTERIAL protein crystallography, *BUTYROLACTONES, *STREPTOMYCES, *CRYSTALLIZATION, *DNA-binding proteins, *VIRGINIAMYCIN

Abstract

The Streptomyces butyrolactone autoregulator receptor protein (BarA) is a DNA-binding protein that regulates the biosynthesis of the antibiotic virginiamycin. In this study, BarA from S. virginiae was overexpressed in Escherichia coli, purified and crystallized. Crystals of purified protein have been grown that diffracted to beyond 3.0 Å resolution at 100 K using synchrotron radiation. The protein crystals belonged to the hexagonal space group P6522, with unit-cell parameters a = b = 128.0, c = 286.2 Å. With four molecules per asymmetric unit, the crystal volume per unit protein mass ( VM) was 3.2 Å3 Da−1 and the solvent content was 62%. [ABSTRACT FROM AUTHOR]

Published

2010

8. Successful Bridge-to-Recovery Treatment in a Young Patient with Fulminant Eosinophilic Myocarditis: Roles of a Percutaneous Ventricular Assist Device and Endomyocardial Biopsy.

Author

Hasegawa-Tamba, Saki, Sugi, Keiki, Gatate, Yodo, Sugiyama, Kanako, Muramatsu, Toshihiro, Nishimura, Shigeyuki, Yasuda, Masanori, Fukushima, Kenji, and Nakano, Shintaro

Subjects

*HEART assist devices, *THERAPEUTICS, *CARDIOGENIC shock, *CARDIAC magnetic resonance imaging, *MYOCARDITIS, *MYOCARDIAL perfusion imaging

Abstract

Eosinophilic myocarditis (EM) is a rare condition characterized by myocardial eosinophilic infiltration due to various underlying etiologies. The patient with EM may benefit from appropriate use of mechanical circulatory support (MCS) that acts as a bridge to myocardial recovery in response to effective immunosuppressive therapy. A 16-year-old boy presented with cardiogenic shock due to fulminant myocarditis, for which a percutaneous ventricular assist device (PVAD) was immediately inserted. Based on the histological diagnosis of EM, immunosuppressive therapy was immediately commenced, leading to improvement of left-ventricular ejection fraction (27% to 47%). The PVAD was successfully removed on day 7. Cardiac magnetic resonance imaging and dual-tracer myocardial scintigraphy suggested limited extent of irreversible myocardial damage. For fulminant EM, the short-term use of PVAD, together with immunosuppressive therapy guided by an immediate histological investigation, may be an effective bridging strategy to myocardial recovery. [ABSTRACT FROM AUTHOR]

Published

2019

9. Homopiperazine Derivatives as a Novel Class of Proteasome Inhibitors with a Unique Mode of Proteasome Binding.

Author

Kikuchi, Jiro, Shibayama, Naoya, Yamada, Satoshi, Wada, Taeko, Nobuyoshi, Masaharu, Izumi, Tohru, Akutsu, Miyuki, Kano, Yasuhiko, Sugiyama, Kanako, Ohki, Mio, Park, Sam-Yong, and Furukawa, Yusuke

Subjects

*PROTEASOME inhibitors, *PIPERAZINE, *HOMEOSTASIS, *MULTIPLE myeloma treatment, *INTRAVENOUS injections, *DRUG resistance, *APOPTOSIS, *ONCOLOGY

Abstract

The proteasome is a proteolytic machinery that executes the degradation of polyubiquitinated proteins to maintain cellular homeostasis. Proteasome inhibition is a unique and effective way to kill cancer cells because they are sensitive to proteotoxic stress. Indeed, the proteasome inhibitor bortezomib is now indispensable for the treatment of multiple myeloma and other intractable malignancies, but is associated with patient inconvenience due to intravenous injection and emerging drug resistance. To resolve these problems, we attempted to develop orally bioavailable proteasome inhibitors with distinct mechanisms of action and identified homopiperazine derivatives (HPDs) as promising candidates. Biochemical and crystallographic studies revealed that some HPDs inhibit all three catalytic subunits (ß 1, ß 2 and ß 5) of the proteasome by direct binding, whereas bortezomib and other proteasome inhibitors mainly act on the ß5 subunit. Proteasome-inhibitory HPDs exhibited cytotoxic effects on cell lines from various hematological malignancies including myeloma. Furthermore, K-7174, one of the HPDs, was able to inhibit the growth of bortezomib-resistant myeloma cells carrying a ß5-subunit mutation. Finally, K-7174 had additive effects with bortezomib on proteasome inhibition and apoptosis induction in myeloma cells. Taken together, HPDs could be a new class of proteasome inhibitors, which compensate for the weak points of conventional ones and overcome the resistance to bortezomib. [ABSTRACT FROM AUTHOR]

Published

2013

10. Interstitial pneumonia caused by inhalation of fumes of nickel and chrome.

Author

Hisatomi, Keiko, Ishii, Hiroshi, Hashiguchi, Koji, Seki, Masafumi, Ide, Mioko, Sugiyama, Kanako, Ishimoto, Hiroshi, Nakayama, Seiko, Mukae, Hiroshi, and Kohno, Shigeru

Subjects

*PULMONARY fibrosis, *COUGH, *LEUCOCYTOSIS, *CYTOKINES, *SERUM

Abstract

Two male industrial painters were admitted to hospital with dry cough and dyspnoea on exertion following a tank coating operation using a high-temperature spray paint consisting of a nickel-chromium alloy. Both patients showed hypoxaemia, peripheral leukocytosis, high levels of serum cytokines and bilateral ground-glass opacities on a chest CT scan. They were diagnosed with interstitial pneumonia caused by inhalation of nickel and chrome fumes and successfully treated with corticosteroid. These are rare cases of interstitial pneumonia associated with nickel/chromium inhalation. [ABSTRACT FROM AUTHOR]

Published

2006

11. Differential effects of α- and β-defensin on cytokine production by cultured human bronchial epithelial cells.

Author

Sakamoto, Noriho, Mukae, Hiroshi, Fujii, Takeshi, Ishii, Hiroshi, Yoshioka, Sumako, Kakugawa, Tomoyuki, Sugiyama, Kanako, Mizuta, Yohei, Jun-ichi Kadota, Nakazato, Masamitsu, and Kohno, Shigeru

Subjects

*CYTOKINES, *NEUTROPHILS, *PEPTIDES, *INTERLEUKIN-8, *INTERLEUKINS, *EPITHELIAL cells, *CELLULAR immunity, *IMMUNOREGULATION

Abstract

Defensins are cysteine-rich cationic antimicrobial peptides that play an important role in innate immunity and are known to contribute to the regulation of host adaptive immunity. In addition to direct antimicrobial activities, it has been recently reported that α-defensins, mainly present in neutrophils in the lung, have a cytotoxic effect and induce IL-8 production from airway epithelial cells. Although β-defensins are expressed in epithelial cells in various tissues, including lung, there are no reports of their effects on cytokine synthesis in airway epithelial cells. The aim of the present study was to determine the effects of both α- and β-defensins on the cytokine production, transcription factor binding activity, and cytotoxicity in primary cultured human bronchial epithelial cells (HBECs). We used human neutrophil peptide-1 (HNP-1; α-defensin) and human β-defensin-2 (HBD-2) to stimulate HBECs. The results showed that treatment of HBECs with HNP-1, but not HBD-2, increased IL-8 and IL-1β mRNA expression in a dose-dependent manner and also enhanced IL-8 protein secretion and NF-κB DNA binding activity. The 24-h treatments with >20 μg/ml of HNP-1 or >50 μg/ml of HBD-2 were cytotoxic to HBECs. These results suggest that α- and β-defensins have different effects on cytokine synthesis by airway epithelial cells, and we speculate that they play different roles in inflammatory lung diseases. [ABSTRACT FROM AUTHOR]

Published

2005

12. Expression of HSP47 in Usual Interstitial Pneumonia and Nonspecific Interstitial Pneumonia.

Author

Kakugawa, Tomoyuki, Mukae, Hiroshi, Hayashi, Tomayoshi, Ishii, Hiroshi, Nakayama, Seiko, Sakamoto, Noriho, Yoshioka, Sumako, Sugiyama, Kanako, Mine, Mariko, Mizuta, Yohei, and Kohno, Shigeru

Subjects

*PULMONARY fibrosis, *PNEUMONIA, *HEAT shock proteins, *MOLECULAR chaperones, *LUNG diseases, *PATIENTS, *MEDICAL research

Abstract

Background: Heat shock protein (HSP) 47, a collagen-specific molecular chaperone, is involved in the processing and/or secretion of procollagens, and its expression is increased in various fibrotic diseases. The aim of this study was to determine whether quantitative immunohistochemical evaluation of the expression levels of HSP47, type I procollagen and α-smooth muscle actin (SMA) allows the differentiation of idiopathic usual interstitial pneumonia (UIP) from UIP associated with collagen vascular disease (CVD) and idiopathic nonspecific interstitial pneumonia (NSIP). Methods: We reviewed surgical lung biopsy specimens of 19 patients with idiopathic UIP, 7 with CVD-associated UIP and 16 with idiopathic NSIP and assigned a score for the expression of HSP47, type I procollagen and α-SMA in type II pneumocytes and/or lung fibroblasts (score 0 = no; 1 = weak; 2 = moderate; 3 = strong staining). Results: The expression level of HSP47 in type II pneumocytes of idiopathic UIP was significantly higher than in CVD-associated UIP and idiopathic NSIP. The expression of HSP47 in fibroblasts was significantly higher in idiopathic UIP and idiopathic NSIP than in CVD-associated UIP. The expression of type I procollagen in type II pneumocytes was significantly higher in idiopathic UIP than in idiopathic NSIP. The expression of type I procollagen in fibroblasts was not different in the three groups, while the expression of a-SMA in fibroblasts was significantly higher in idiopathic UIP than in idiopathic NSIP. Conclusion: Our results suggest the existence of different fibrotic pathways among these groups involved in the expression of HSP47 and type I procollagen. [ABSTRACT FROM AUTHOR]

Published

2005