Your search keyword '"Isao Sakane"' showing total 10 results

1. Isolation of short peptide fragments from α-synuclein fibril core identifies a residue important for fibril nucleation: A possible implication for diagnostic applications

Author

Hisashi Yagi, Naomi Ito, Tomohiro Mizobata, Yuji Goto, Shiho Ogawa, Kunihiro Hongo, Yasushi Kawata, Isao Sakane, and Hideki Takeuchi

Subjects

Amyloid, Molecular Sequence Data, Biophysics, Nucleation, Phenylalanine, Peptide, macromolecular substances, Microscopy, Atomic Force, Fibril, Biochemistry, Analytical Chemistry, chemistry.chemical_compound, Residue (chemistry), Humans, Insulin, Amino Acid Sequence, Benzothiazoles, Molecular Biology, chemistry.chemical_classification, Edman degradation, Chemistry, Circular Dichroism, GroES, Peptide Fragments, Thiazoles, alpha-Synuclein, Lewy Bodies, Lysozyme

Abstract

alpha-Synuclein is one of the causative proteins of the neurodegenerative disorder, Parkinson's disease. Deposits of alpha-synuclein called Lewy bodies are a hallmark of this disorder, which is implicated in its progression. In order to understand the mechanism of amyloid fibril formation of alpha-synuclein in more detail, in this study we have isolated a specific, ~20 residue peptide region of the alpha-synuclein fibril core, using a combination of Edman degradation and mass-spectroscopy analyses of protease-resistant samples. Starting from this core peptide sequence, we then synthesized a series of peptides that undergo aggregation and fibril formation under similar conditions. Interestingly, in a derivative peptide where a crucial phenylalanine residue was changed to a glycine, the ability to initiate spontaneous fibril formation was abolished, while the ability to extend from preexisting fibril seeds was conserved. This fibril extension occurred irrespective of the source of the initial fibril seed, as demonstrated in experiments using fibril seeds of insulin, lysozyme, and GroES. This interesting ability suggests that this peptide might form the basis for a possible diagnostic tool useful in detecting the presence of various fibrillogenic factors.

Published

2010

2. c-ABL tyrosine kinase stabilizes RAD51 chromatin association

Author

Masahiko Kobayashi, Ken Ichi Yamamoto, Milena Popova, Naoyuki Hayashi, Ashok R. Venkitaraman, Masayuki Takahashi, Isao Sakane, Hitoshi Kurumizaka, Fabrice Fleury, and Hiroko Shimizu

Subjects

DNA repair, DNA damage, genetic processes, Biophysics, RAD51, Biology, Biochemistry, c-ABL, Cell Line, Tyrosine phosphorylation, chemistry.chemical_compound, Humans, Phosphorylation, Kinase activity, Proto-Oncogene Proteins c-abl, Molecular Biology, Cell Biology, BRCA2, Molecular biology, Chromatin, Cell biology, enzymes and coenzymes (carbohydrates), chemistry, ATM, Homologous recombination repair, health occupations, Tyrosine, Rad51 Recombinase, biological phenomena, cell phenomena, and immunity, Homologous recombination, DNA, DNA Damage

Abstract

金沢大学がん研究所がん分子細胞制御, The assembly of RAD51 recombinase on DNA substrates at sites of breakage is essential for their repair by homologous recombination repair (HRR). The signaling pathway that triggers RAD51 assembly at damage sites to form subnuclear foci is unclear. Here, we provide evidence that c-ABL, a tyrosine kinase activated by DNA damage which phosphorylates RAD51 on Tyr-315, works at a previously unrecognized, proximal step to initiate RAD51 assembly. We first show that c-ABL associates with chromatin after DNA damage in a manner dependent on its kinase activity. Using RAD51 mutants that are unable to oligomerize to form a nucleoprotein filament, we separate RAD51 assembly on DNA to form foci into two steps: stable chromatin association followed by oligomerization. We show that phosphorylation on Tyr-315 by c-ABL is required for chromatin association of oligomerization-defective RAD51 mutants, but is insufficient to restore oligomerization. Our findings suggest a new model for the regulation of early steps of HRR. © 2009 Elsevier Inc. All rights reserved.

Published

2009

3. Filament formation and robust strand exchange activities of the rice DMC1A and DMC1B proteins

Author

Hitoshi Kurumizaka, Chiaki Kamataki, Marina Nakashima, Yoshimasa Takizawa, Shukuko Ikawa, Takehiko Shibata, Hiroaki Ichikawa, Isao Sakane, and Seiichi Toki

Subjects

Adenosine Triphosphatases, Base pair, Molecular Sequence Data, food and beverages, Oryza, DNA, Biology, Molecular biology, Recombinases, chemistry.chemical_compound, D-loop, chemistry, Biochemistry, Coding strand, Genetics, Recombinase, DMC1, Amino Acid Sequence, Gene, Replication protein A, Molecular Biology, Sequence Alignment, Plant Proteins

Abstract

The DMC1 protein, a meiosis-specific DNA recombinase, catalyzes strand exchange between homologous chromosomes. In rice, two Dmc1 genes, Dmc1A and Dmc1B, have been reported. Although the Oryza sativa DMC1A protein has been partially characterized, however the biochemical properties of the DMC1B protein have not been defined. In the present study, we expressed the Oryza sativa DMC1A and DMC1B proteins in bacteria and purified them. The purified DMC1A and DMC1B proteins formed helical filaments along single-stranded DNA (ssDNA) and double-stranded DNA (dsDNA), and promoted robust strand exchange between ssDNA and dsDNA over five thousand base pairs in the presence of RPA, as a co-factor. The DMC1A and DMC1B proteins also promoted strand exchange in the absence of RPA with long DNA substrates containing several thousand base pairs. In contrast, the human DMC1 protein strictly required RPA to promote strand exchange with these long DNA substrates. The strand-exchange activity of the Oryza sativa DMC1A protein was much higher than that of the DMC1B protein. Consistently, the DNA-binding activity of the DMC1A protein was higher than that of the DMC1B protein. These biochemical differences between the DMC1A and DMC1B proteins may provide important insight into their functional differences during meiosis in rice.

Published

2008

4. The Lys313 residue of the human Rad51 protein negatively regulates the strand-exchange activity

Author

Takako Ishida, Yoshimasa Takizawa, Isao Sakane, and Hitoshi Kurumizaka

Subjects

Gene isoform, chemistry.chemical_classification, Recombinase activity, RAD51, Cell Biology, Biology, Molecular biology, In vitro, chemistry.chemical_compound, Residue (chemistry), Enzyme, Biochemistry, chemistry, Genetics, Homologous recombination, DNA

Abstract

The Rad51 protein, which catalyzes homologous-pairing and strand-exchange reactions, is an essential enzyme for homologous recombinational repair (HRR) and meiotic homologous recombination in eukaryotes. In humans, the conventional Rad51 (HsRad51) protein has a Lys residue at position 313; however, the HsRad51-Q313 protein, in which the Lys313 residue is replaced by Gln, was reported as an isoform, probably corresponding to a polymorphic variant. In this study, we purified the HsRad51-K313 and HsRad51-Q313 isoforms and analyzed their biochemical activities in vitro. Compared to the conventional HsRad51-K313 protein, the HsRad51-Q313 protein exhibited significantly enhanced strand-exchange activity under conditions with Ca2+, although the difference was not observed without Ca2+. A double-stranded DNA (dsDNA) unwinding assay revealed that the HsRad51-Q313 protein clearly showed enhanced DNA unwinding activity, probably due to its enhanced filament-formation ability. Mutational analyses of the HsRad51-Lys313 residue revealed that positively charged residues (Lys and Arg), but not negatively charged, polar and hydrophobic residues (Glu, Gln and Met, respectively), at position 313 reduced the strand-exchange and DNA unwinding abilities of the HsRad51 protein. These results suggest that the electrostatic environment around position 313 is important for the regulation of the HsRad51 recombinase activity.

Published

2007

5. Recombination Activator Function of the Novel RAD51- and RAD51B-binding Protein, Human EVL*S⃞

Author

Noriko Hosoya, Shugo Nakayama, Yoshimasa Takizawa, Shinichi Machida, Hitoshi Kurumizaka, Kiyoshi Miyagawa, Isao Sakane, Motoki Takaku, and Takehiko Shibata

Subjects

RAD51, Plasma protein binding, Biology, Biochemistry, DNA-binding protein, chemistry.chemical_compound, Cell Line, Tumor, Homologous chromosome, Humans, Molecular Biology, Recombination, Genetic, Activator (genetics), Binding protein, Cell Biology, DNA, DNA repair protein XRCC4, Molecular biology, DNA-Binding Proteins, Chromosome Pairing, chemistry, Gene Knockdown Techniques, DNA: Replication, Repair, Recombination, and Chromosome Dynamics, Rad51 Recombinase, Cell Adhesion Molecules, Protein Binding

Abstract

The RAD51 protein is a central player in homologous recombinational repair. The RAD51B protein is one of five RAD51 paralogs that function in the homologous recombinational repair pathway in higher eukaryotes. In the present study, we found that the human EVL (Ena/Vasp-like) protein, which is suggested to be involved in actin-remodeling processes, unexpectedly binds to the RAD51 and RAD51B proteins and stimulates the RAD51-mediated homologous pairing and strand exchange. The EVL knockdown cells impaired RAD51 assembly onto damaged DNA after ionizing radiation or mitomycin C treatment. The EVL protein alone promotes single-stranded DNA annealing, and the recombination activities of the EVL protein are further enhanced by the RAD51B protein. The expression of the EVL protein is not ubiquitous, but it is significantly expressed in breast cancer-derived MCF7 cells. These results suggest that the EVL protein is a novel recombination factor that may be required for repairing specific DNA lesions, and that may cause tumor malignancy by its inappropriate expression.

Published

2009

6. Mechanical unfolding of covalently linked GroES: evidence of structural subunit intermediates

Author

Tomohiro Mizobata, Kunihiro Hongo, Yasushi Kawata, and Isao Sakane

Subjects

Models, Molecular, Protein Denaturation, Protein Folding, Protein subunit, Escherichia coli Proteins, Equilibrium unfolding, Force spectroscopy, GroES, Microscopy, Atomic Force, Biochemistry, GroEL, chemistry.chemical_compound, Crystallography, Monomer, Immobilized Proteins, chemistry, Covalent bond, For the Record, Chaperonin 10, Protein folding, Protein Structure, Quaternary, Molecular Biology

Abstract

It is difficult to determine the structural stability of the individual subunits or protomers of many proteins in the cell that exist in an oligomeric or complexed state. In this study, we used single-molecule force spectroscopy on seven subunits of covalently linked cochaperonin GroES (ESC7) to evaluate the structural stability of the subunit. A modified form of ESC7 was immobilized on a mica surface. The force-extension profile obtained from the mechanical unfolding of this ESC7 showed a distinctive sawtooth pattern that is typical for multimodular proteins. When analyzed according to the worm-like chain model, the contour lengths calculated from the peaks in the profile suggested that linked-GroES subunits unfold in distinct steps after the oligomeric ring structure of ESC7 is disrupted. The evidence that structured subunits of ESC7 withstand external force to some extent even after the perturbation of the oligomeric ring structure suggests that a stable monomeric intermediate is an important component of the equilibrium unfolding reaction of GroES.

Published

2009

7. Gly192 at hinge 2 site in the chaperonin GroEL plays a pivotal role in the dynamic apical domain movement that leads to GroES binding and efficient encapsulation of substrate proteins

Author

Kodai Machida, Tatsuhide Tanaka, Tomohiro Mizobata, Ryoko Fujiwara, Kunihiro Hongo, Yasushi Kawata, and Isao Sakane

Subjects

Models, Molecular, Protein Folding, Protein Conformation, Protein subunit, Mutant, Biophysics, macromolecular substances, Biology, Biochemistry, Analytical Chemistry, Chaperonin, Adenosine Triphosphate, Chaperonin 10, Escherichia coli, Point Mutation, Surface plasmon resonance, Molecular Biology, Escherichia coli Proteins, GroES, Chaperonin 60, GroEL, enzymes and coenzymes (carbohydrates), biological sciences, Foldase, bacteria, Protein folding, Protein Binding

Abstract

The subunit structure of chaperonin GroEL is divided into three domains; the apical domain, the intermediate domain, and the equatorial domain. Each domain has a specific role in the chaperonin mechanism. The ‘hinge 2’ site of GroEL contains three glycine residues, Gly192, Gly374, and Gly375, connecting the apical domain and the intermediate domain. In this study, to understand the importance of the hinge 2 amino acid residues in chaperonin function, we substituted each of these three glycine residues to tryptophan. The GroEL mutants G374W and G375W were functionally similar to wild-type GroEL. However, GroEL G192W showed a significant decrease in the ability to assist the refolding of stringent substrate proteins. Interestingly, from biochemical assays and characterization using surface plasmon resonance analysis, we found that GroEL G192W was capable of binding GroES even in the absence of ATP to form a very stable GroEL–GroES complex, which could not be dissociated even upon addition of ATP. Electron micrographs showed that GroEL G192W intrinsically formed an asymmetric double ring structure with one ring locked in the ‘open’ conformation, and it is postulated that GroES binds to this open ring in the absence of ATP. Trans-binding of both substrate protein and GroES was observed for this binary complex, but simultaneous binding of both substrate and GroES (a mechanism that ensures substrate encapsulation) was impaired. We postulate that alteration of Gly192 severely compromises an essential movement that allows efficient encapsulation of unfolded protein intermediates.

Published

2008

8. Fibril formation of hsp10 homologue proteins and determination of fibril core regions: differences in fibril core regions dependent on subtle differences in amino acid sequence

Author

Tomohiro Mizobata, Masahiro Hara, Ai Sato, Yoshiki Hattori, Yasushi Kawata, Isao Sakane, Hisashi Yagi, Jun Shimamura, Kunihiro Hongo, and Akihiro Yoshida

Subjects

Amyloid, Protein Folding, Molecular Sequence Data, Peptide, macromolecular substances, Fibril, Microscopy, Atomic Force, chemistry.chemical_compound, Viral Proteins, Microscopy, Electron, Transmission, Structural Biology, Chaperonin 10, Animals, Humans, Amino Acid Sequence, Guanidine, Molecular Biology, Peptide sequence, Chromatography, High Pressure Liquid, chemistry.chemical_classification, Edman degradation, biology, Sequence Homology, Amino Acid, GroES, Hydrogen-Ion Concentration, biology.organism_classification, Rats, Biochemistry, chemistry, Thermotoga maritima, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Protein folding

Abstract

Heat shock protein 10 (hsp10) is a member of the molecular chaperones and works with hsp60 in mediating various protein folding reactions. GroES is a representative protein of hsp10 from Escherichia coli. Recently, we found that GroES formed a typical amyloid fibril from a guanidine hydrochloride (Gdn-HCl) unfolded state at neutral pH. Here, we report that other hsp10 homologues, such as human hsp10 (Hhsp10), rat mitochondrial hsp10 (Rhsp10), Gp31 from T4 phage, and hsp10 from the hyperthermophilic bacteria Thermotoga maritima, also form amyloid fibrils from an unfolded state. Interestingly, whereas GroES formed fibrils from either the Gdn-HCl unfolded state (at neutral pH) or the acidic unfolded state (at pH 2.0-3.0), Hhsp10, Rhsp10, and Gp31 formed fibrils from only the acidic unfolded state. Core peptide regions of these protein fibrils were determined by proteolysis treatment followed by a combination of Edman degradation and mass spectroscopy analyses of the protease-resistant peptides. The core peptides of GroES fibrils were identical for fibrils formed from the Gdn-HCl unfolded state and those formed from the acidic unfolded state. However, a peptide with a different sequence was isolated from fibrils of Hhsp10 and Rhsp10. With the use of synthesized peptides of the determined core regions, it was also confirmed that the identified regions were capable of fibril formation. These findings suggested that GroES homologues formed typical amyloid fibrils under acidic unfolding conditions but that the fibril core structures were different, perhaps owing to differences in local amino acid sequences.

Published

2007

9. Roles of the human Rad51 L1 and L2 loops in DNA binding

Author

Yoshimasa Takizawa, Yusuke Matsuo, Isao Sakane, Masayuki Takahashi, and Hitoshi Kurumizaka

Subjects

Protein Folding, HMG-box, DNA Repair, DNA repair, Molecular Sequence Data, RAD51, Biology, Biochemistry, Protein Structure, Secondary, chemistry.chemical_compound, Humans, Amino Acid Sequence, Binding site, Molecular Biology, Replication protein A, Recombination, Genetic, DNA clamp, Alanine, Binding Sites, Sequence Homology, Amino Acid, Tryptophan, Cell Biology, Protein Structure, Tertiary, DNA binding site, DNA-Binding Proteins, Spectrometry, Fluorescence, chemistry, Amino Acid Substitution, Tyrosine, Rad51 Recombinase, DNA, Protein Binding

Abstract

The human Rad51 protein, a eukaryotic ortholog of the bacterial RecA protein, is a key enzyme that functions in homologous recombination and recombinational repair of double strand breaks. The Rad51 protein contains two flexible loops, L1 and L2, which are proposed to be sites for DNA binding, based on a structural comparison with RecA. In the present study, we performed mutational and fluorescent spectroscopic analyses on the L1 and L2 loops to examine their role in DNA binding. Gel retardation and DNA-dependent ATP hydrolysis measurements revealed that the substitution of the tyrosine residue at position 232 (Tyr232) within the L1 loop with alanine, a short side chain amino acid, significantly decreased the DNA-binding ability of human Rad51, without affecting the protein folding or the salt-induced, DNA-independent ATP hydrolysis. Even the conservative replacement with tryptophan affected the DNA binding, indicating that Tyr232 is involved in DNA binding. The importance of the L1 loop was confirmed by the fluorescence change of a tryptophan residue, replacing the Asp231, Ser233, or Gly236 residue, upon DNA binding. The alanine replacement of phenylalanine at position 279 (Phe279) within the L2 loop did not affect the DNA-binding ability of human Rad51, unlike the Phe203 mutation of the RecA L2 loop. The Phe279 side chain may not be directly involved in the interaction with DNA. However, the fluorescence intensity of the tryptophan replacing the Rad51-Phe279 residue was strongly reduced upon DNA binding, indicating that the L2 loop is also close to the DNA-binding site.

Published

2006

10. 1P036 Cloning and characterization of aspartase-like gene product from Thermotoga maritima

Author

K. Nishida, Kunihiro Hongo, Yasushi Kawata, Isao Sakane, and Tomohiro Mizobata

Subjects

Cloning, Gene product, biology, Biochemistry, Chemistry, Thermotoga maritima, biology.organism_classification

Published

2004