Your search keyword '"Shojiro Kadono"' showing total 7 results

1. Crystal structure of human factor VIIa/tissue factor in complex with peptide mimetic inhibitor

Author

Masateru Ohta, Yoshiaki Watanabe, Hirofumi Kodama, Toshiro Kozono, Takuya Shiraishi, Susumu Itoh, Haruhiko Sato, Takaki Koga, Masayuki Haramura, Yasufumi Kikuchi, Kunihiro Hattori, Akihisa Sakamoto, Naohiro Yabuta, Toru Esaki, Masayoshi Oh-eda, and Shojiro Kadono

Subjects

Models, Molecular, Biophysics, Factor VIIa, Crystallography, X-Ray, Biochemistry, Thromboplastin, chemistry.chemical_compound, Residue (chemistry), Tissue factor, Thrombin, medicine, Humans, Molecular Biology, Serine protease, Methionine, biology, Anticoagulants, Dipeptides, Cell Biology, Benzamidines, chemistry, biology.protein, Peptides, Discovery and development of direct thrombin inhibitors, medicine.drug

Abstract

The 3D structure of human factor VIIa/soluble tissue factor in complex with a peptide mimetic inhibitor, propylsulfonamide-D-Thr-Met-p-aminobenzamidine, is determined by X-ray crystallography. As compared with the interactions between thrombin and thrombin inhibitors, the interactions at S2 and S3 sites characteristic of factor VIIa and factor VIIa inhibitors are revealed. The S2 site has a small pocket, which is filled by the hydrophobic methionine side chain in P2. The small S3 site fits the small size residue, D-threonine in P3. The structural data and SAR data of the peptide mimetic inhibitor show that these interactions in the S2 and S3 sites play an important role for the improvement of selectivity versus thrombin. The results will provide valuable information for the structure-based drug design of specific inhibitors for FVIIa/TF.

Published

2004

2. The crystal structure of thermostable mutants of chimeric 3–isopropylmalate dehydrogenase, 2T2M6T

Author

AkJhiro Yamagishi, Masahiro Sakurai, Tairo Oshima, Jitsutaro Kawaguchi, Shojiro Kadono, Yoko Hayashi, Hideaki Moriyama, Koichi Numata, Nobuo Tanaka, and Ko Onodera

Subjects

Models, Molecular, Hot Temperature, 3-Isopropylmalate Dehydrogenase, Stereochemistry, Recombinant Fusion Proteins, Molecular Sequence Data, Bioengineering, Dehydrogenase, Bacillus subtilis, Crystallography, X-Ray, Protein Engineering, Biochemistry, Protein Structure, Secondary, Enzyme Stability, Serine, Amino Acid Sequence, Isoleucine, Site-directed mutagenesis, Molecular Biology, Thermostability, chemistry.chemical_classification, biology, Chemistry, Thermus thermophilus, biology.organism_classification, Amino acid, Models, Structural, Alcohol Oxidoreductases, Mutagenesis, Site-Directed, Thermodynamics, Biotechnology

Abstract

A chimeric 3-isopropylmalate dehydrogenase (IPMDH), 2T2M6T, was produced by replacing the amino acid sequences of the Thermus thermophilus enzyme with those of the Bacillus subtilis enzyme from residues 75 to 113. Decreased thermostability of the chimeric enzyme was recovered by either evolutionary engineering (I93L) or site-directed mutagenesis (S82R). The 3-D structures of the mutants have been determined by X-ray diffraction at 2.1 A resolution. Although S82R was refined routinely, I93L required the preliminary rigid-body refinement of each domain. The R-factors were reduced to 0.18 for both mutants. Removal of the unfavorable torsion angle at isoleucine 93 may have made I93L more thermostable than 2T2M6T. In the case of S82R, the replaced arginine residue contributed to the extra hydrogen bond with water molecules. The large replaced residue decreased the entropy of the solvent, which may have caused the improvement in enzyme thermostability. Denaturation by heating may be interpreted from these structural results.

Published

1995

3. Chemical modification and site-directed mutagenesis of Tyr36 of 3-isopropylmalate dehydrogenase from Thermits thermophUus HB8

Author

Kentaro Miyazaki, Nobuo Tanaka, Masahiro Sakurai, Shojiro Kadono, Hideaki Moriyama, and Tairo Oshima

Subjects

Models, Molecular, 3-Isopropylmalate Dehydrogenase, Protein Conformation, Stereochemistry, Molecular Sequence Data, Bioengineering, Dehydrogenase, Biochemistry, Michaelis–Menten kinetics, Enzyme catalysis, Structure-Activity Relationship, chemistry.chemical_compound, Animals, Site-directed mutagenesis, Molecular Biology, Binding Sites, Base Sequence, biology, Chemistry, Thermus thermophilus, Active site, Tetranitromethane, biology.organism_classification, Alcohol Oxidoreductases, Mutagenesis, Site-Directed, biology.protein, Tyrosine, Rabbits, Biotechnology

Abstract

3-Isopropylmalate dehydrogenase from an extreme thermophile, Thermus thermophilus HB8, was chemically modified with tetranitromethane which nitrated 1.5-2.0 Tyr residues per subunit. The nitration was biphasic and parallel to the loss of activity. The modified residue in the first phase was identified to be Tyr36, which is distantly located from the active site of the enzyme. The function of Tyr36 was investigated by site-specific replacement with Phe. The Michaelis constant for the substrate or co-enzyme was not altered by the replacement, whereas the catalytic constant decreased down to approximately 5%. X-ray analysis of the mutant enzyme revealed that Arg94 moved the largest distance among the active site residues, that is, the NH1 and NH2 of the guanidino group moved 1.11 and 1.32 A respectively. The results suggest that Arg94 is responsible for the enzyme catalysis.

Published

1994

4. Design and synthesis of peptidomimetic factor VIIa inhibitors

Author

Masateru Ohta, Takaki Koga, Kunihiro Hattori, Keiko Esaki, Toshiro Kozono, Yoshiyuki Ono, Tohru Esaki, Hirofumi Kodama, Kazutaka Yoshihashi, Takehisa Kitazawa, Akihisa Sakamoto, Shojiro Kadono, Haruhiko Sato, Yoshiaki Watanabe, Hitoshi Iikura, Takuya Shiraishi, and Masayuki Haramura

Subjects

Indole test, Models, Molecular, Proteases, Chemistry, Hydrogen bond, Stereochemistry, Peptidomimetic, General Chemistry, General Medicine, Factor VIIa, Ring (chemistry), Crystallography, X-Ray, Combinatorial chemistry, Thromboplastin, Serine, Tissue factor, Biomimetics, Drug Discovery, Selectivity, Peptides, Protein Binding

Abstract

Selective factor VIIa-tissue factor complex (FVIIa/TF) inhibition is regarded as a promising target for developing new anticoagulant drugs. In previous reports, we described a S3 subsite found in the X-ray crystal structure of compound 2 that bound to FVIIa/soluble tissue factor (sTF). Based on the X-ray crystal structure information and with the aim of improving the inhibition activity for FVIIa/TF and selectivity against other serine proteases, we synthesized derivatives by introducing substituents at position 5 of the indole ring of compound 2. Among them, compound 16 showed high selectivity against other serine proteases. Contrary to our expectations, compound 16 did not occupy the S3-subsite; X-ray structure analysis revealed that compound 16 improved selectivity by forming hydrogen bonds with Gln217, Thr99 and Asn100.

Published

2010

5. Structure-based design of P3 moieties in the peptide mimetic factor VIIa inhibitor

Author

Masayuki Haramura, Yoshiaki Watanabe, Hirofumi Kodama, Yoshiyuki Ono, Naohiro Yabuta, Masateru Ohta, Akihisa Sakamoto, Takehisa Kitazawa, Toshiro Kozono, Toru Esaki, Haruhiko Sato, Masayoshi Oh-eda, Takuya Shiraishi, Shojiro Kadono, Yasufumi Kikuchi, Tsukasa Suzuki, Kazutaka Yoshihashi, Takaki Koga, Susumu Itoh, and Kunihiro Hattori

Subjects

Models, Molecular, Stereochemistry, Molecular Sequence Data, Biophysics, Factor VIIa, Crystallography, X-Ray, Biochemistry, Inhibitory Concentration 50, Structure-Activity Relationship, Protein structure, Biomimetic Materials, Structure–activity relationship, Moiety, Humans, Amino Acid Sequence, Binding site, Enzyme Inhibitors, Molecular Biology, Peptide sequence, Serine protease, Binding Sites, biology, Chemistry, Cell Biology, Protein Structure, Tertiary, Coagulation, Drug Design, biology.protein, Selectivity, Peptides, Sequence Alignment

Abstract

Selective factor VIIa-tissue factor complex (FVIIa/TF) inhibition is seen as a promising target for developing new anticoagulant drugs. Structure-based designs of the P3 moiety in the peptide mimetic factor VIIa inhibitor successfully lead to novel inhibitors with selectivity for FVIIa/TF and extrinsic coagulation the same as or even higher than those of previously reported peptide mimetic factor VIIa inhibitors. X-ray crystal structure analysis reveals that one of the novel inhibitors shows improved selectivity by forming interactions between the inhibitor and FVIIa as expected. Another of the novel inhibitors achieves improved selectivity through an unexpected hydrogen bond with Gln217, with a unique bent conformation in FVIIa/TF accompanied by conformational changes of the inhibitor and the protein.

Published

2004

6. Structure of human factor VIIa/tissue factor in complex with a peptide-mimetic inhibitor: high selectivity against thrombin by introducing two charged groups in P2 and P4

Author

Yoshiyuki Ono, Toshiro Kozono, Hirofumi Kodama, Masayuki Haramura, Shojiro Kadono, Toru Esaki, Masayoshi Oh-eda, Yoshiaki Watanabe, Naohiro Yabuta, Yasufumi Kikuchi, Takaki Koga, Masateru Ohta, Akihisa Sakamoto, Susumu Itoh, Kunihiro Hattori, Takuya Shiraishi, and Haruhiko Sato

Subjects

Models, Molecular, Stereochemistry, Macromolecular Substances, High selectivity, Biophysics, Factor VIIa, Crystallography, X-Ray, Biochemistry, Antithrombins, Protein Structure, Secondary, Thromboplastin, chemistry.chemical_compound, Tissue factor, Thrombin, Structural Biology, Genetics, medicine, otorhinolaryngologic diseases, Humans, Protein Structure Communications, Carboxylate, Blood Coagulation, Chemistry, Anticoagulants, Condensed Matter Physics, Drug Design, Selectivity, Peptides, medicine.drug, circulatory and respiratory physiology

Abstract

The crystal structure of human factor VIIa/soluble tissue factor (FVIIa/sTF) in complex with a highly selective peptide-mimetic FVIIa inhibitor which shows 1670-fold selectivity against thrombin inhibition has been solved at 2.6 A resolution. The inhibitor is bound to FVIIa/sTF at the S1, S2 and S3 sites and at the additional S1 subsite. Two charged groups, the amidino group in P2 and the carboxylate group in P4, form ionic interactions with Asp60 and Lys192 of FVIIa, respectively. Structural comparisons between factor VIIa and thrombin show that thrombin has oppositely charged residues, Lys60F and Glu192, in the S2 site and the S1 subsites, respectively. These data suggest that the utilization of the differences of charge distribution in the S2 site and the S1 subsites between FVIIa and thrombin is critical for achieving high selectivity against thrombin inhibition. These results will provide valuable information for the structure-based drug design of specific inhibitors for FVIIa/TF.

Published

2004

7. Novel interactions of large P3 moiety and small P4 moiety in the binding of the peptide mimetic factor VIIa inhibitor

Author

Yasufumi Kikuchi, Tsukasa Suzuki, Hirofumi Kodama, Masayuki Haramura, Haruhiko Sato, Yoshiaki Watanabe, Masayoshi Oh-eda, Shojiro Kadono, Takehisa Kitazawa, Kazutaka Yoshihashi, Toru Esaki, Toshiro Kozono, Akihisa Sakamoto, Kunihiro Hattori, Takaki Koga, Takuya Shiraishi, Susumu Itoh, Yoshiyuki Ono, Masateru Ohta, and Naohiro Yabuta

Subjects

Models, Molecular, Proteases, Stereochemistry, Protein Conformation, Molecular Sequence Data, Biophysics, Factor VIIa, Crystallography, X-Ray, Biochemistry, Substrate Specificity, Serine, Thrombin, Biomimetics, medicine, Moiety, Humans, Computer Simulation, Amino Acid Sequence, Molecular Biology, Peptide sequence, Serine protease, Binding Sites, biology, Blood Coagulation Factor Inhibitors, Chemistry, Cell Biology, Enzyme Activation, Coagulation, Models, Chemical, biology.protein, Peptides, medicine.drug, Protein Binding

Abstract

Selective factor VIIa-tissue factor complex (FVIIa/TF) inhibition is seen as a promising target for developing new anticoagulant drugs. A novel peptide mimetic factor VIIa inhibitor, ethylsulfonamide-d-biphenylalanine-Gln-p-aminobenzamidine, shows 100-fold selectivity against thrombin in spite of its large P3 moiety, unlike previously reported FVIIa/TF selective inhibitors. X-ray crystal structure analysis reveals that the large P3 moiety, d-biphenylalanine, and the small P4 moiety, ethylsulfonamide, make novel interactions with the 170-loop and Lys192 of FVIIa/TF, respectively, accompanying ligand-induced conformational changes of the 170-loop, Gln217, and Lys192. Structural comparisons of FVIIa with thrombin and amino acid sequence comparisons among coagulation serine proteases suggest that these interactions play an important role in achieving selective inhibition for FVIIa/TF.

Published

2004