Your search keyword '"Nobuaki Yasuo"' showing total 7 results

1. In silico, in vitro, X-ray crystallography, and integrated strategies for discovering spermidine synthase inhibitors for Chagas disease

Author

Ryunosuke Yoshino, Nobuaki Yasuo, Yohsuke Hagiwara, Takashi Ishida, Daniel Ken Inaoka, Yasushi Amano, Yukihiro Tateishi, Kazuki Ohno, Ichiji Namatame, Tatsuya Niimi, Masaya Orita, Kiyoshi Kita, Yutaka Akiyama, and Masakazu Sekijima

Subjects

Medicine, Science

Abstract

Abstract Chagas disease results from infection by Trypanosoma cruzi and is a neglected tropical disease (NTD). Although some treatment drugs are available, their use is associated with severe problems, including adverse effects and limited effectiveness during the chronic disease phase. To develop a novel anti-Chagas drug, we virtually screened 4.8 million small molecules against spermidine synthase (SpdSyn) as the target protein using our super computer “TSUBAME2.5” and conducted in vitro enzyme assays to determine the half-maximal inhibitory concentration values. We identified four hit compounds that inhibit T. cruzi SpdSyn (TcSpdSyn) by in silico and in vitro screening. We also determined the TcSpdSyn–hit compound complex structure using X-ray crystallography, which shows that the hit compound binds to the putrescine-binding site and interacts with Asp171 through a salt bridge.

Published

2017

2. Identification of key interactions between SARS-CoV-2 main protease and inhibitor drug candidates

Author

Ryunosuke Yoshino, Masakazu Sekijima, and Nobuaki Yasuo

Subjects

0301 basic medicine, medicine.medical_treatment, viruses, lcsh:Medicine, Viral Nonstructural Proteins, Virtual drug screening, 01 natural sciences, Protein structure, skin and connective tissue diseases, lcsh:Science, media_common, Multidisciplinary, virus diseases, Severe acute respiratory syndrome-related coronavirus, Drug screening, Infectious diseases, Identification (biology), Pharmacophore, medicine.symptom, Coronavirus Infections, Drug, Proteases, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), media_common.quotation_subject, Pneumonia, Viral, Sequence alignment, Computational biology, Molecular Dynamics Simulation, Biology, 010402 general chemistry, Article, Betacoronavirus, 03 medical and health sciences, medicine, Humans, Protease Inhibitors, Amino Acid Sequence, Pandemics, Binding Sites, Protease, SARS-CoV-2, fungi, lcsh:R, COVID-19, Protein Structure, Tertiary, Computational biology and bioinformatics, 0104 chemical sciences, body regions, 030104 developmental biology, Mechanism of action, Drug Design, lcsh:Q, Sequence Alignment

Abstract

The number of cases of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection (COVID-19) has reached over 114,000. SARS-CoV-2 caused a pandemic in Wuhan, China, in December 2019 and is rapidly spreading globally. It has been reported that peptide-like anti-HIV-1 drugs are effective against SARS-CoV Main protease (Mpro). Due to the close phylogenetic relationship between SARS-CoV and SARS-CoV-2, their main proteases share many structural and functional features. Thus, these drugs are also regarded as potential drug candidates targeting SARS-CoV-2 Mpro. However, the mechanism of action of SARS-CoV-2 Mpro at the atomic-level is unknown. In the present study, we revealed key interactions between SARS-CoV-2 Mpro and three drug candidates by performing pharmacophore modeling and 1μs molecular dynamics (MD) simulations. His41, Gly143, and Glu166 formed interactions with the functional groups that were common among peptide-like inhibitors in all MD simulations. These interactions are important targets for potential drugs against SARS-CoV-2 Mpro.

Published

2020

3. Molecular Dynamics Simulation reveals the mechanism by which the Influenza Cap-dependent Endonuclease acquires resistance against Baloxavir marboxil

Author

Ryunosuke Yoshino, Nobuaki Yasuo, and Masakazu Sekijima

Subjects

0301 basic medicine, Models, Molecular, Binding free energy, Protein Conformation, Pyridines, Mutant, lcsh:Medicine, Drug resistance, medicine.disease_cause, Virus Replication, 01 natural sciences, Endonuclease, Molecular dynamics, Influenza A Virus, H1N1 Subtype, Protein analysis, lcsh:Science, Mutation, Multidisciplinary, biology, Molecular Structure, Chemistry, Triazines, Thermodynamics, Thiepins, Protein Binding, Dibenzothiepins, medicine.drug_class, Pyridones, Morpholines, Protein function predictions, Molecular Dynamics Simulation, 010402 general chemistry, Antiviral Agents, Virus, Article, 03 medical and health sciences, Structure-Activity Relationship, Viral Proteins, Drug Resistance, Viral, Endoribonucleases, Oxazines, medicine, Binding Sites, lcsh:R, Molecular biology, 0104 chemical sciences, Influenza B virus, 030104 developmental biology, Amino Acid Substitution, biology.protein, lcsh:Q, Antiviral drug

Abstract

Baloxavir marboxil (BXM), an antiviral drug for influenza virus, inhibits RNA replication by binding to RNA replication cap-dependent endonuclease (CEN) of influenza A and B viruses. Although this drug was only approved by the FDA in October 2018, drug resistant viruses have already been detected from clinical trials owing to an I38 mutation of CEN. To investigate the reduction of drug sensitivity by the I38 mutant variants, we performed a molecular dynamics (MD) simulation on the CEN-BXM complex structure to analyze variations in the mode of interaction. Our simulation results suggest that the side chain methyl group of I38 in CEN engages in a CH-pi interaction with the aromatic ring of BXM. This interaction is abolished in various I38 mutant variants. Moreover, MD simulation on various mutation models and binding free energy prediction by MM/GBSA method suggest that the I38 mutation precludes any interaction with the aromatic ring of BXA and thereby reduces BXA sensitivity.

Published

2019

4. A prospective compound screening contest identified broader inhibitors for Sirtuin 1

Author

Daisuke Kobayashi, Attayeb Mohsen, Masakazu Sekijima, Tomoki Ito, M. Michael Gromiha, Masahiro Mochizuki, Mika Sakamoto, Kenji Mizuguchi, Modong Tan, Hideaki Umeyama, Nobuaki Yasuo, Shuntaro Chiba, Shogo Suzuki, Takashi Ishida, Kazuyoshi Ikeda, Daisuke Kihara, Yoshitaka Moriwaki, Yutaka Akiyama, Reiji Teramoto, A. Mary Thangakani, Shintaro Minami, Vipul Gupta, Mitsuo Iwadate, Chioko Nagao, Takaaki Ichikawa, Kazuki Yamamoto, Masahito Ohue, Itsuo Nakane, Kei Yura, Tatsuya Okuno, George Chikenji, Masahiro Kawatani, Kun Yi Hsin, Sakurako Takashina, Takatsugu Hirokawa, Woong-Hee Shin, Devadasan Velmurugan, Hayase Hakariya, Chandrasekaran Ramakrishnan, Ryunosuke Yoshino, Hironori K. Nakamura, Philip Prathipati, Nobuaki Miura, Hiroaki Kitano, Sergey Zozulya, Mari Ito, Akiko Higuchi, Teruki Honma, Petro Borysko, Keita Oda, Anastasiia Gryniukova, Nanako Uchida, and Kentaroh Kudoh

Subjects

0301 basic medicine, Multidisciplinary, Drug discovery, Sirtuin 1, In silico, lcsh:R, lcsh:Medicine, Computational biology, Information technology, Biology, Virtual drug screening, 01 natural sciences, Article, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, 030104 developmental biology, biology.protein, lcsh:Q, lcsh:Science

Abstract

Potential inhibitors of a target biomolecule, NAD-dependent deacetylase Sirtuin 1, were identified by a contest-based approach, in which participants were asked to propose a prioritized list of 400 compounds from a designated compound library containing 2.5 million compounds using in silico methods and scoring. Our aim was to identify target enzyme inhibitors and to benchmark computer-aided drug discovery methods under the same experimental conditions. Collecting compound lists derived from various methods is advantageous for aggregating compounds with structurally diversified properties compared with the use of a single method. The inhibitory action on Sirtuin 1 of approximately half of the proposed compounds was experimentally accessed. Ultimately, seven structurally diverse compounds were identified.

Published

2019

5. An iterative compound screening contest method for identifying target protein inhibitors using the tyrosine-protein kinase Yes

Author

Shintaro Minami, Chandrasekaran Ramakrishnan, Petro Borysko, Takashi Ishida, Hideaki Umeyama, M. Michael Gromiha, Shuntaro Chiba, Shogo Suzuki, George Chikenji, Mitsuo Iwadate, A. Mary Thangakani, Masakazu Sekijima, Kazuyoshi Ikeda, Keisuke Yanagisawa, Daisuke Kihara, Y-h. Taguchi, Reiji Teramoto, Sergey Zozulya, Devadasan Velmurugan, Woong-Hee Shin, Tatsuya Okuno, Teruki Honma, Masahiro Mochizuki, Kazuki Yamamoto, Yoshitaka Moriwaki, Takatsugu Hirokawa, Ryunosuke Yoshino, Roman Stavniichuk, Yutaka Akiyama, Nobuaki Yasuo, and Koya Kato

Subjects

0301 basic medicine, Computer science, lcsh:Medicine, Tyrosine-Protein Kinase Yes, Computational biology, CONTEST, Bioinformatics, 01 natural sciences, Article, Machine Learning, 03 medical and health sciences, Structure-Activity Relationship, Drug Discovery, Humans, Enzyme Inhibitors, lcsh:Science, Protein Kinase Inhibitors, Proto-Oncogene Proteins c-yes, Multidisciplinary, Molecular Structure, Drug discovery, lcsh:R, Reproducibility of Results, 0104 chemical sciences, High-Throughput Screening Assays, 010404 medicinal & biomolecular chemistry, 030104 developmental biology, lcsh:Q, Target protein, human activities, Protein Binding

Abstract

We propose a new iterative screening contest method to identify target protein inhibitors. After conducting a compound screening contest in 2014, we report results acquired from a contest held in 2015 in this study. Our aims were to identify target enzyme inhibitors and to benchmark a variety of computer-aided drug discovery methods under identical experimental conditions. In both contests, we employed the tyrosine-protein kinase Yes as an example target protein. Participating groups virtually screened possible inhibitors from a library containing 2.4 million compounds. Compounds were ranked based on functional scores obtained using their respective methods, and the top 181 compounds from each group were selected. Our results from the 2015 contest show an improved hit rate when compared to results from the 2014 contest. In addition, we have successfully identified a statistically-warranted method for identifying target inhibitors. Quantitative analysis of the most successful method gave additional insights into important characteristics of the method used.

Published

2017

6. In silico, in vitro, X-ray crystallography, and integrated strategies for discovering spermidine synthase inhibitors for Chagas disease

Author

Yukihiro Tateishi, Daniel Ken Inaoka, Kiyoshi Kita, Takashi Ishida, Yutaka Akiyama, Ichiji Namatame, Kazuki Ohno, Tatsuya Niimi, Yohsuke Hagiwara, Masakazu Sekijima, Masaya Orita, Ryunosuke Yoshino, Nobuaki Yasuo, and Yasushi Amano

Subjects

0301 basic medicine, Chagas disease, 030103 biophysics, In silico, High-throughput screening, Trypanosoma cruzi, Science, Protozoan Proteins, Pharmacology, Biology, Crystallography, X-Ray, Spermidine Synthase, Article, 03 medical and health sciences, Drug Discovery, medicine, Chagas Disease, Computer Simulation, Enzyme Inhibitors, Multidisciplinary, Binding Sites, medicine.disease, biology.organism_classification, Small molecule, In vitro, 030104 developmental biology, Biochemistry, biology.protein, Medicine, Target protein, Spermidine synthase

Abstract

Chagas disease results from infection by Trypanosoma cruzi and is a neglected tropical disease (NTD). Although some treatment drugs are available, their use is associated with severe problems, including adverse effects and limited effectiveness during the chronic disease phase. To develop a novel anti-Chagas drug, we virtually screened 4.8 million small molecules against spermidine synthase (SpdSyn) as the target protein using our super computer “TSUBAME2.5” and conducted in vitro enzyme assays to determine the half-maximal inhibitory concentration values. We identified four hit compounds that inhibit T. cruzi SpdSyn (TcSpdSyn) by in silico and in vitro screening. We also determined the TcSpdSyn–hit compound complex structure using X-ray crystallography, which shows that the hit compound binds to the putrescine-binding site and interacts with Asp171 through a salt bridge.

Published

2017

7. Identification of potential inhibitors based on compound proposal contest: Tyrosine-protein kinase Yes as a target

Author

Hiroaki Kitano, Yuko Tsuchiya, Kun-Yi Hsin, Teruki Honma, Takashi Ishida, Kenji Mizuguchi, Chandrasekaran Ramakrishnan, Devadasan Velmurugan, Masahiro Mochizuki, A. Mary Thangakani, Shuntaro Chiba, Ito Junichi, Keisuke Yanagisawa, Tomohiro Ban, Hideaki Umeyama, Koya Kato, Yutaka Akiyama, George Chikenji, Masakazu Sekijima, Kazuyoshi Ikeda, Y-h. Taguchi, Reiji Teramoto, Nobuaki Yasuo, M. Michael Gromiha, Ryunosuke Yoshino, Tatsuya Okuno, Kazuki Yamamoto, Nobuyoshi Sugaya, Takatsugu Hirokawa, Philip Prathipati, and Mitsuo Iwadate

Subjects

Proto-Oncogene Proteins c-yes, Principal Component Analysis, Multidisciplinary, Research groups, Drug discovery, Drug Evaluation, Preclinical, Reproducibility of Results, Tyrosine-Protein Kinase Yes, Computational biology, Biology, CONTEST, Bioinformatics, Article, Chemical space, Identification (information), src-Family Kinases, Humans, Target protein, Protein Kinase Inhibitors

Abstract

A search of broader range of chemical space is important for drug discovery. Different methods of computer-aided drug discovery (CADD) are known to propose compounds in different chemical spaces as hit molecules for the same target protein. This study aimed at using multiple CADD methods through open innovation to achieve a level of hit molecule diversity that is not achievable with any particular single method. We held a compound proposal contest, in which multiple research groups participated and predicted inhibitors of tyrosine-protein kinase Yes. This showed whether collective knowledge based on individual approaches helped to obtain hit compounds from a broad range of chemical space and whether the contest-based approach was effective.

Published

2015