Your search keyword '"Keisuke, Miyazawa"' showing total 279 results

1. Vitamin K2 sensitizes the efficacy of venetoclax in acute myeloid leukemia by targeting the NOXA-MCL-1 pathway.

Author

Tetsuzo Tauchi, Shota Moriya, Seiichi Okabe, Hiromi Kazama, Keisuke Miyazawa, and Naoharu Takano

Subjects

Medicine, Science

Abstract

Promising outcomes have been reported in elder patients with acute myeloid leukemia (AML) using combined therapy of venetoclax (VEN) and azacytidine (AZA) in recent years. However, approximately one-third of patients appear to be refractory to this therapy. Vitamin K2 (VK2) shows apoptosis-inducing activity in AML cells, and daily oral VK2 (menaquinone-4, GlakayR) has been approved for patients with osteoporosis in Japan. We observed a high response rate to AZA plus VEN therapy, with no 8-week mortality in the newly diagnosed AML patients consuming daily VK2 in our hospital. The median age of the patients was 75.9 years (range 66-84) with high-risk features. Patients received AZA 75 mg/m2 on D1-7, VEN 400 mg on D1-28, and daily VK2 45 mg. The CR/CRi ratio was 94.7% (18/19), with a CR rate of 79%. Complete cytogenetic CR was achieved in 15 of 19 (79%) patients, and MRD negativity in 2 of 15 (13%) evaluable CR patients. Owing to the extremely high response rate in clinical settings, we further attempted to investigate the underlying mechanisms. The combination of VK2 and VEN synergistically induced apoptosis in all five AML cell lines tested. VK2, but not VEN, induced mitochondrial reactive oxygen species (ROS), leading to the transcriptional upregulation of NOXA, followed by MCL-1 repression. ROS scavengers repressed VK2 induced-NOXA expression and led to the cancellation of pronounced apoptosis and the downregulation of MCL-1 by VK2 plus VEN. Additionally, knockdown and knockout of NOXA resulted in abrogation of the MCL-1 repression as well as enhanced cytotoxicity by the two-drug combination, indicating that VK2 suppresses MCL-1 via ROS-mediated NOXA induction. These data suggest that the dual inhibition of BCL-2 by VEN and MCL-1 by VK2 is responsible for the remarkable clinical outcomes in our patients. Therefore, large-scale clinical trials are required.

Published

2024

2. Identification of a novel type of focal adhesion remodelling via FAK/FRNK replacement, and its contribution to cancer progression

Author

Masatsune Tsujioka, Keisuke Miyazawa, Masaki Ohmuraya, Yoichi Nibe, Tetsuya Shirokawa, Haruko Hayasaka, Tsunekazu Mizushima, Takeshi Fukuma, and Shigeomi Shimizu

Subjects

Cytology, QH573-671

Abstract

Abstract Numerous studies have investigated the various cellular responses against genotoxic stress, including those mediated by focal adhesions. We here identified a novel type of focal adhesion remodelling that occurs under genotoxic stress conditions, which involves the replacement of active focal adhesion kinase (FAK) with FAK-related non-kinase (FRNK). FRNK stabilized focal adhesions, leading to strong cell-matrix adhesion, and FRNK-depleted cells were easily detached from extracellular matrix upon genotoxic stress. This remodelling occurred in a wide variety of cells. In vivo, the stomachs of Frnk-knockout mice were severely damaged by genotoxic stress, highlighting the protective role of FRNK against genotoxic stress. FRNK was also found to play a vital role in cancer progression, because FRNK depletion significantly inhibited cancer dissemination and progression in a mouse cancer model. Furthermore, in human cancers, FRNK was predominantly expressed in metastatic tissues and not in primary tissues. We hence conclude that this novel type of focal adhesion remodelling reinforces cell adhesion and acts against genotoxic stress, which results in the protection of normal tissues, but in turn facilitates cancer progression.

Published

2023

3. p53 regulates lysosomal membrane permeabilization as well as cytoprotective autophagy in response to DNA-damaging drugs

Author

Gai Yamashita, Naoharu Takano, Hiromi Kazama, Kiyoaki Tsukahara, and Keisuke Miyazawa

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671

Abstract

Abstract Lysosomes are single-membraned organelles that mediate the intracellular degradation of macromolecules. Various stress can induce lysosomal membrane permeabilization (LMP), translocating intralysosomal components, such as cathepsins, to the cytoplasm, which induces lysosomal-dependent cell death (LDCD). This study reports that p53 regulates LMP in response to DNA-damaging drugs. Treating wild-type TP53 A549 cells with DNA-damaging drugs (namely, doxorubicin, carboplatin, and etoposide) induced LMP and accelerated cell death more rapidly than treating TP53-knockout (KO) A549 cells. This suggested p53-dependent LMP and LDCD induction in response to DNA damage. LMP was induced by p53-dependent BID upregulation and activation, followed by translocation of truncated BID to lysosomes. Simultaneously, autophagy for damaged lysosome elimination (lysophagy) was activated via the p53–mTOR–TEFB/TFE3 pathways in response to DNA damage. These data suggested the dichotomous nature of p53 for LMP regulation; LMP induction and repression via the p53–BID axis and p53–mTOR–TFEB/TFE3 pathway, respectively. Blocking autophagy with hydroxychloroquine or azithromycin as well as ATG5 KO enhanced LMP and LDCD induction after exposure to DNA-damaging drugs. Furthermore, lysosomal membrane stabilization using U18666A, a cholesterol transporter Niemann-Pick disease C1 (NPC1) inhibitor, suppressed LMP as well as LDCD in wild-type TP53, but not in TP53-KO, A549 cells. Thus, LMP is finely regulated by TP53 after exposure to DNA-damaging drugs.

Published

2022

4. Protocol for live imaging of intracellular nanoscale structures using atomic force microscopy with nanoneedle probes

Author

Takehiko Ichikawa, Mohammad Shahidul Alam, Marcos Penedo, Kyosuke Matsumoto, Sou Fujita, Keisuke Miyazawa, Hirotoshi Furusho, Kazuki Miyata, Chikashi Nakamura, and Takeshi Fukuma

Subjects

Atomic Force Microscopy, AFM, Cell Biology, Microscopy, Science (General), Q1-390

Abstract

Summary: Atomic force microscopy (AFM) is capable of nanoscale imaging but has so far only been used on cell surfaces when applied to a living cell. Here, we describe a step-by-step protocol for nanoendoscopy-AFM, which enables the imaging of nanoscale structures inside living cells. The protocol consists of cell staining, fabrication of the nanoneedle probes, observation inside living cells using 2D and 3D nanoendoscopy-AFM, and visualization of the 3D data.For complete details on the use and execution of this protocol, please refer to Penedo et al. (2021)1 and Penedo et al. (2021).2 : Publisher’s note: Undertaking any experimental protocol requires adherence to local institutional guidelines for laboratory safety and ethics.

Published

2023

5. Chemical fixation creates nanoscale clusters on the cell surface by aggregating membrane proteins

Author

Takehiko Ichikawa, Dong Wang, Keisuke Miyazawa, Kazuki Miyata, Masanobu Oshima, and Takeshi Fukuma

Subjects

Biology (General), QH301-705.5

Abstract

Atomic force microscopy imaging shows that cell fixation can lead to unwanted aggregation of membrane proteins.

Published

2022

6. Clarithromycin overcomes stromal cell-mediated drug resistance against proteasome inhibitors in myeloma cells via autophagy flux blockage leading to high NOXA expression

Author

Shota Moriya, Hiromi Kazama, Hirotsugu Hino, Naoharu Takano, Masaki Hiramoto, Shin Aizawa, and Keisuke Miyazawa

Subjects

Medicine, Science

Published

2023

7. BRCA1 degradation in response to mitochondrial damage in breast cancer cells

Author

Kana Miyahara, Naoharu Takano, Yumiko Yamada, Hiromi Kazama, Mayumi Tokuhisa, Hirotsugu Hino, Koji Fujita, Edward Barroga, Masaki Hiramoto, Hiroshi Handa, Masahiko Kuroda, Takashi Ishikawa, and Keisuke Miyazawa

Subjects

Medicine, Science

Abstract

Abstract BRCA1 is a well-studied tumor suppressor involved in the homologous repair of DNA damage, whereas PINK1, a mitochondrial serine/threonine kinase, is known to be involved in mitochondrial quality control. Genetic mutations of PINK1 and Parkin cause autosomal recessive early-onset Parkinson’s disease. We found that in breast cancer cells, the mitochondrial targeting reagents, which all induce mitochondrial depolarization along with PINK1 upregulation, induced proteasomal BRCA1 degradation. This BRCA1 degradation was dependent on PINK1, and BRCA1 downregulation upon mitochondrial damage caused DNA double-strand breaks. BRCA1 degradation was mediated through the direct interaction with the E3 ligase Parkin. Strikingly, BRCA1 and PINK1/Parkin expression were inversely correlated in cancerous mammary glands from breast cancer patients. BRCA1 knockdown repressed cancer cell growth, and high BRCA1 expression predicted poor relapse-free survival in breast cancer patients. These observations indicate a novel mechanism by which mitochondrial damage is transmitted to the nucleus, leading to BRCA1 degradation.

Published

2021

8. Cell penetration efficiency analysis of different atomic force microscopy nanoneedles into living cells

Author

Marcos Penedo, Tetsuya Shirokawa, Mohammad Shahidul Alam, Keisuke Miyazawa, Takehiko Ichikawa, Naoko Okano, Hirotoshi Furusho, Chikashi Nakamura, and Takeshi Fukuma

Subjects

Medicine, Science

Abstract

Abstract Over the last decade, nanoneedle-based systems have demonstrated to be extremely useful in cell biology. They can be used as nanotools for drug delivery, biosensing or biomolecular recognition inside cells; or they can be employed to select and sort in parallel a large number of living cells. When using these nanoprobes, the most important requirement is to minimize the cell damage, reducing the forces and indentation lengths needed to penetrate the cell membrane. This is normally achieved by reducing the diameter of the nanoneedles. However, several studies have shown that nanoneedles with a flat tip display lower penetration forces and indentation lengths. In this work, we have tested different nanoneedle shapes and diameters to reduce the force and the indentation length needed to penetrate the cell membrane, demonstrating that ultra-thin and sharp nanoprobes can further reduce them, consequently minimizing the cell damage.

Published

2021

9. Azithromycin, a potent autophagy inhibitor for cancer therapy, perturbs cytoskeletal protein dynamics

Author

Naoharu Takano, Masaki Hiramoto, Yumiko Yamada, Hiroko Kokuba, Mayumi Tokuhisa, Hirotsugu Hino, and Keisuke Miyazawa

Subjects

Cancer Research, Oncology

Abstract

Background Autophagy plays an important role in tumour cell growth and survival and also promotes resistance to chemotherapy. Hence, autophagy has been targeted for cancer therapy. We previously reported that macrolide antibiotics including azithromycin (AZM) inhibit autophagy in various types of cancer cells in vitro. However, the underlying molecular mechanism for autophagy inhibition remains unclear. Here, we aimed to identify the molecular target of AZM for inhibiting autophagy. Methods We identified the AZM-binding proteins using AZM-conjugated magnetic nanobeads for high-throughput affinity purification. Autophagy inhibitory mechanism of AZM was analysed by confocal microscopic and transmission electron microscopic observation. The anti-tumour effect with autophagy inhibition by oral AZM administration was assessed in the xenografted mice model. Results We elucidated that keratin-18 (KRT18) and α/β-tubulin specifically bind to AZM. Treatment of the cells with AZM disrupts intracellular KRT18 dynamics, and KRT18 knockdown resulted in autophagy inhibition. Additionally, AZM treatment suppresses intracellular lysosomal trafficking along the microtubules for blocking autophagic flux. Oral AZM administration suppressed tumour growth while inhibiting autophagy in tumour tissue. Conclusions As drug-repurposing, our results indicate that AZM is a potent autophagy inhibitor for cancer treatment, which acts by directly interacting with cytoskeletal proteins and perturbing their dynamics.

Published

2023

10. Comparison of autophagy inducibility in various tyrosine kinase inhibitors and their enhanced cytotoxicity via inhibition of autophagy in cancer cells in combined treatment with azithromycin

Author

Hideki Tanaka, Hirotsugu Hino, Shota Moriya, Hiromi Kazama, Masaya Miyazaki, Naoharu Takano, Masaki Hiramoto, Kiyoaki Tsukahara, and Keisuke Miyazawa

Subjects

Tyrosine kinase inhibitor, Autophagy, Macrolide antibiotics, Cancer, Biology (General), QH301-705.5, Biochemistry, QD415-436

Abstract

Tyrosine kinase inhibitors (TKIs) induce autophagy in many types of cancer cells. We previously reported that gefitinib (GEF) and imatinib (IMA) induce autophagy in epidermal growth factor receptor (EGFR) knock-out A549 and non-BCR-ABL-expressing leukemia cell lines, respectively. This evidence suggests that TKI-induced autophagy is independent of the original target molecules. The present study compared the autophagy-inducing abilities of various TKIs, regardless of their targets, by quantitative autophagy flux assay. We established stable clones expressing the GFP-LC3-mCherry-LC3ΔG plasmid in A549, PC-9, and CAL 27 cell lines and assessed autophagy inducibility by monitoring the fluorescent ratios of GFP-LC3 to mCherry-LC3ΔG using an IncuCyte live cell imaging system during exposure to TKIs viz; GEF, osimertinib (OSI), lapatinib (LAP), lenvatinib (LEN), sorafenib (SOR), IMA, dasatinib (DAS), and tivantinib (TIV). Among these TKIs, DAS, GEF, and SOR exhibited prominent autophagy induction in A549 and PC-9 cells. In CAL 27 cells, IMA, SOR, and LEN, but not GEF, TIV, or OSI, exhibited autophagy induction. In the presence of azithromycin (AZM), which showed an inhibitory effect on autophagy flux, TKIs with prominent autophagy inducibility exhibited enhanced cytotoxicity via non-apoptotic cell death relative to effects of TKI alone. Therefore, autophagy inducibility of TKIs differed in the context of cancer cells. However, once induced, they appeared to have cytoprotective functions. Thus, blocking TKI-induced autophagy with AZM may improve the therapeutic effect of TKIs in cancer cells.

Published

2020

11. High-veracity functional imaging in scanning probe microscopy via Graph-Bootstrapping

Author

Xin Li, Liam Collins, Keisuke Miyazawa, Takeshi Fukuma, Stephen Jesse, and Sergei V. Kalinin

Subjects

Science

Abstract

Scanning probe microscopy methods can generate high-dimensional data sets that correspond to a low-dimensional sample. Here, Li et al. develop a graphical bootstrapping method to quantitatively visualize large-scale high-dimensional datasets.

Published

2018

12. Highly Stable Triangular Single‐Layer 2D Assemblies: Synthesis and Their Stimuli‐Responsive Elastic and Anisotropic Curling

Author

Yajiao Hao, Lin Yu, Keisuke Miyazawa, Shengrui Zhang, Mo Liu, Zhongqi Yu, Jun Liu, Yang Yu, Song Li, Shujue Xu, Takeshi Fukuma, Sean Xiao‐An Zhang, and Minjie Li

Subjects

General Medicine, General Chemistry, Catalysis

Published

2023

13. Computed Three-Dimensional Atomic Force Microscopy Images of Biopolymers Using the Jarzynski Equality

Author

Takashi Sumikama, Filippo Federici Canova, David Z. Gao, Marcos Penedo, Keisuke Miyazawa, Adam S. Foster, Takeshi Fukuma, Japan Science and Technology Agency, Surfaces and Interfaces at the Nanoscale, Norwegian University of Science and Technology, Swiss Federal Institute of Technology Lausanne, Kanazawa University, Department of Applied Physics, Aalto-yliopisto, and Aalto University

Subjects

Quantitative Biology::Subcellular Processes, Fibers, Quantitative Biology::Biomolecules, Biopolymers, Chemical structure, Polymers, General Materials Science, Probes, Physical and Theoretical Chemistry

Abstract

金沢大学ナノ生命科学研究所, Three-dimensional atomic force microscopy (3D-AFM) has resolved three-dimensional distributions of solvent molecules at solid–liquid interfaces at the subnanometer scale. This method is now being extended to the imaging of biopolymer assemblies such as chromosomes or proteins in cells, with the expectation of being able to resolve their three-dimensional structures. Here, we have developed a computational method to simulate 3D-AFM images of biopolymers by using the Jarzynski equality. It is found that some parts of the fiber structure of biopolymers are indeed resolved in the 3D-AFM image. The dependency of 3D-AFM images on the vertical scanning velocity is investigated, and optimum scanning velocities are found. It is also clarified that forces in nonequilibrium processes are measured in 3D-AFM measurements when the dynamics of polymers are slower than the scanning of the probe., Embargo Period 12 months / CC BY-NC-ND 4.0

Published

2022

14. Visualizing Molecular-Scale Adsorption Structures of Anti-freezing Surfactants on Sapphire (0001) Surfaces at Different Concentrations by 3D Scanning Force Microscopy

Author

Takahiko Ikarashi, Kyosuke Nakayama, Naoki Nakajima, Kazuki Miyata, Keisuke Miyazawa, and Takeshi Fukuma

Subjects

General Materials Science

Abstract

Anti-freezing surfactants form an adsorption layer at the solid-water interface to inhibit the nucleation and growth of ice. However, this mechanism has not been elucidated at the molecular scale because of the difficulties in visualizing such adsorption structures. In this study, we overcome this limitation by directly visualizing the three-dimensional (3D) adsorption structures of anti-freezing surfactants, hexadecyltrimethylammonium bromide (C

Published

2022

15. Identification of a novel type of focal adhesion remodelling via FAK/FRNK replacement, and its contribution to cancer evolution

Author

Masatsune Tsujioka, Keisuke Miyazawa, Masaki Ohmuraya, Yoichi Nibe, Tetsuya Shirokawa, Haruko Hayasaka, Tsunekazu Mizushima, Takeshi Fukuma, and Shigeomi Shimizu

Abstract

Numerous studies have investigated the various cellular responses against genotoxic stress, including those mediated by focal adhesions. Nevertheless, we here identified a novel type of focal adhesion remodelling that occurs under genotoxic stress conditions, which involves the replacement of active focal adhesion kinase (FAK) with FAK-related non-kinase (FRNK). FRNK stabilized focal adhesions, leading to strong cell-matrices adhesion, and FRNK-depleted cells were easily detached from the matrices upon genotoxic stress. This remodelling occurred in a wide variety of cells. In vivo, the stomachs of Frnk-knockout mice were severely damaged by genotoxic stress, highlighting the protective role of FRNK against genotoxic stress. FRNK was also found to play a vital role in cancer progression, because FRNK depletion significantly inhibited cancer dissemination and progression in a mouse cancer model. We hence conclude that this novel type of focal adhesion remodelling reinforces cell adhesion and acts against genotoxic stress, which results in the protection of normal tissues, but, in turn, facilitates cancer evolution.

Published

2022

16. Chemical fixation creates nanoscale clusters on the cell surface by aggregating membrane proteins

Author

Dong Wang, Masanobu Oshima, Takeshi Fukuma, Kazuki Miyata, Takehiko Ichikawa, and Keisuke Miyazawa

Subjects

Chemistry, Cell, Cell Membrane, Membrane Proteins, Medicine (miscellaneous), Microscopy, Atomic Force, General Biochemistry, Genetics and Molecular Biology, Fixation (surgical), Fixatives, medicine.anatomical_structure, Membrane protein, medicine, Biophysics, Artifacts, General Agricultural and Biological Sciences, Nanoscopic scale

Abstract

Chemical fixations have been thought to preserve the structures of the cells or tissues. However, given that the fixatives create crosslinks or aggregate proteins, there is a possibility that these fixatives create nanoscale artefacts by aggregation of membrane proteins which move around freely to some extent on the cell surface. Despite this, little research has been conducted about this problem, probably because there has been no method for observing cell surface structures at the nanoscale. In this study, we have developed a new method to observe cell surfaces stably and with high resolution using atomic force microscopy and a microporous silicon nitride membrane. We demonstrate that the size of the protrusions on the cell surface is increased after treatment with three commonly used fixatives and show that these protrusions were created by the aggregation of membrane proteins by fixatives. These results call attention when observing fixed cell surfaces at the nanoscale.

Published

2022

17. Macrolide Antibiotics Exhibit Cytotoxic Effect under Amino Acid-Depleted Culture Condition by Blocking Autophagy Flux in Head and Neck Squamous Cell Carcinoma Cell Lines.

Author

Kazuhiro Hirasawa, Shota Moriya, Kana Miyahara, Hiromi Kazama, Ayako Hirota, Jun Takemura, Akihisa Abe, Masato Inazu, Masaki Hiramoto, Kiyoaki Tsukahara, and Keisuke Miyazawa

Subjects

Medicine, Science

Abstract

Autophagy, a self-digestive system for cytoplasmic components, is required to maintain the amino acid pool for cellular homeostasis. We previously reported that the macrolide antibiotics azithromycin (AZM) and clarithromycin (CAM) have an inhibitory effect on autophagy flux, and they potently enhance the cytocidal effect of various anticancer reagents in vitro. This suggests that macrolide antibiotics can be used as an adjuvant for cancer chemotherapy. Since cancer cells require a larger metabolic demand than normal cells because of their exuberant growth, upregulated autophagy in tumor cells has now become the target for cancer therapy. In the present study, we examined whether macrolides exhibit cytotoxic effect under an amino acid-starving condition in head and neck squamous cancer cell lines such as CAL 27 and Detroit 562 as models of solid tumors with an upregulated autophagy in the central region owing to hypovascularity. AZM and CAM induced cell death under the amino acid-depleted (AAD) culture condition in these cell lines along with CHOP upregulation, although they showed no cytotoxicity under the complete culture medium. CHOP knockdown by siRNA in the CAL 27 cells significantly suppressed macrolide-induced cell death under the AAD culture condition. CHOP-/- murine embryonic fibroblast (MEF) cell lines also attenuated AZM-induced cell death compared with CHOP+/+ MEF cell lines. Using a tet-off atg5 MEF cell line, knockout of atg5, an essential gene for autophagy, also induced cell death and CHOP in the AAD culture medium but not in the complete culture medium. This suggest that macrolide-induced cell death via CHOP induction is dependent on autophagy inhibition. The cytotoxicity of macrolide with CHOP induction was completely cancelled by the addition of amino acids in the culture medium, indicating that the cytotoxicity is due to the insufficient amino acid pool. These data suggest the possibility of using macrolides for "tumor-starving therapy".

Published

2016

18. Inhibition of Silica Nanoparticle Adhesion to Poly(vinyl alcohol) Surfaces by Ammonia-Mediated Hydration: Implications for Effective Post-Chemical–Mechanical Planarization Cleaning

Author

Takahiko Ikarashi, Chikako Takatoh, Takumi Yoshino, Takeshi Fukuma, Kazuki Miyata, Megumi Uno, Naoki Nakajima, Adam S. Foster, Ygor M. Jaques, and Keisuke Miyazawa

Subjects

Vinyl alcohol, Yield (engineering), Materials science, integumentary system, Abrasive, technology, industry, and agriculture, Nanoparticle, 02 engineering and technology, Adhesion, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, 0104 chemical sciences, carbohydrates (lipids), Silica nanoparticles, Ammonia, chemistry.chemical_compound, Chemical engineering, chemistry, Chemical-mechanical planarization, General Materials Science, 0210 nano-technology

Abstract

Adhesion of silica abrasive nanoparticles to a poly(vinyl alcohol) (PVA) brush surface in post-CMP (chemical–mechanical planarization) cleaning leads to serious problems in yield enhancement of sem...

Published

2020

19. Geometrical Characterization of Glass Nanopipettes with Sub-10 nm Pore Diameter by Transmission Electron Microscopy

Author

Kazuki Shigyou, Shohei Takigaura, Hirotoshi Furusho, Shinji Watanabe, Masashi Tajima, Takeshi Fukuma, Yousuke Kikuchi, Keisuke Miyazawa, Riku Yajima, Azuma Taoka, Linhao Sun, and Toshio Ando

Subjects

Pore diameter, Aperture, Chemistry, business.industry, 010401 analytical chemistry, FOS: Physical sciences, Physics - Applied Physics, Applied Physics (physics.app-ph), Deformation (meteorology), 010402 general chemistry, 01 natural sciences, 0104 chemical sciences, Analytical Chemistry, Characterization (materials science), Electron beam irradiation, Transmission electron microscopy, Thin wall, Optoelectronics, Ligand cone angle, business

Abstract

Glass nanopipettes are widely used for various applications in nanosciences. In most of the applications, it is important to characterize their geometrical parameters, such as the aperture size and the inner cone angle at the tip region. For nanopipettes with sub-10 nm aperture and thin wall thickness, transmission electron microscopy (TEM) must be most instrumental in their precise geometrical measurement. However, this measurement has remained a challenge because heat generated by electron beam irradiation would largely deform sub-10-nm nanopipettes. Here we provide methods for preparing TEM specimens that do not cause deformation of such tiny nanopipettes., Comment: 8 pages, 4 figures

Published

2020

20. Macrolide antibiotics enhance the antitumor effect of lansoprazole resulting in lysosomal membrane permeabilization-associated cell death

Author

Masaki Hiramoto, Keisuke Miyazawa, Akihisa Abe, Hiroko Kokuba, Shota Moriya, Atsuo Takeda, Kiyoaki Tsukahara, Hirotsugu Hino, and Naoharu Takano

Subjects

0301 basic medicine, Cancer Research, Programmed cell death, autophagy, proton pump inhibitor, Cell Survival, Autolysosome, Pharmacology, Biology, Azithromycin, Permeability, Autophagy-Related Protein 5, 03 medical and health sciences, Gene Knockout Techniques, 0302 clinical medicine, Microscopy, Electron, Transmission, Lysosome, Cell Line, Tumor, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, medicine, cancer, Humans, Lansoprazole, Cytotoxicity, Cell Proliferation, A549 cell, Cell Death, Cell growth, apoptosis, Drug Synergism, Articles, Intracellular Membranes, macrolide antibiotics, 030104 developmental biology, medicine.anatomical_structure, Oncology, Apoptosis, 030220 oncology & carcinogenesis, Cancer cell, lysosome, Drug Screening Assays, Antitumor, Lysosomes

Abstract

The proton pump inhibitor lansoprazole (LPZ) inhibits the growth of several cancer cell lines, including A549 and CAL 27. We previously reported that macrolide antibiotics such as azithromycin (AZM) and clarithromycin (CAM) potently inhibit autophagic flux and that combining AZM or CAM with the epidermal growth factor receptor inhibitors enhanced their antitumor effect against various cancer cells. In the present study, we conducted the combination treatment with LPZ and macrolide antibiotics against A549 and CAL 27 cells and evaluated cytotoxicity and morphological changes using cell proliferation and viability assays, flow cytometric analysis, immunoblotting, and morphological assessment. Combination therapy with LPZ and AZM greatly enhanced LPZ‑induced cell death, whereas treatment with AZM alone exhibited negligible cytotoxicity. The observed cytotoxic effect was not mediated through apoptosis or necroptosis. Transmission electron microscopy of A549 cells treated with the LPZ + AZM combination revealed morphological changes associated with necrosis and accumulated autolysosomes with undigested contents. Furthermore, the A549 cell line with ATG5 knockout exhibited complete inhibition of autophagosome formation, which did not affect LPZ + AZM treatment‑induced cytotoxicity, thus excluding the involvement of autophagy‑dependent cell death in LPZ + AZM treatment‑induced cell death. A549 cells treated with LPZ + AZM combination therapy retained the endosomal Alexa‑dextran for extended duration as compared to untreated control cells, thus indicating impairment of lysosomal digestion. Notably, lysosomal galectin‑3 puncta expression induced due to lysosomal membrane permeabilization was increased in cells treated with LPZ + AZM combination as compared to the treatment by either agent alone. Collectively, the present results revealed AZM‑induced autolysosome accumulation, potentiated LPZ‑mediated necrosis, and lysosomal membrane permeabilization, thus suggesting the potential clinical application of LPZ + AZM combination therapy for cancer treatment.

Published

2020

21. Sequestosome 1 (p62) accumulation in breast cancer cells suppresses progesterone receptor expression via argonaute 2

Author

Naoharu Takano, Masaya Miyazaki, Ayuka Yokota, Mayumi Tokuhisa, Hirotsugu Hino, Keisuke Miyazawa, Masaki Hiramoto, and Hiromi Kazama

Subjects

0301 basic medicine, Biophysics, Breast Neoplasms, Biology, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Sequestosome 1, Breast cancer, Cell Line, Tumor, Sequestosome-1 Protein, Gene expression, Progesterone receptor, medicine, Humans, education, Molecular Biology, Cell Nucleus, education.field_of_study, Gene knockdown, Cancer, Signal transducing adaptor protein, Cell Biology, Argonaute, medicine.disease, Gene Expression Regulation, Neoplastic, Protein Transport, 030104 developmental biology, 030220 oncology & carcinogenesis, Argonaute Proteins, Cancer research, Female, Receptors, Progesterone

Abstract

Sequestosome 1 (p62) is a multifunctional adapter protein involved in various physiological functions, such as selective autophagy and oxidative stress response. Hence, aberrant expression and defective regulation of p62 are thought to lead to the onset of various diseases, including cancer. The expression of p62 has been shown to be increased in breast cancer tissues, and is correlated with a poor prognosis. However, the role of p62 in the breast cancer pathophysiology is still unclear. Here, we aimed to analyze the effect of changes in p62 expression on breast cancer cell lines. DNA microarray analysis revealed that the expression of progesterone receptor (PR), which is one of the indices for the classification of breast cancer subtypes, was markedly suppressed by forced expression of p62. The protein expression of PR was also decreased by forced expression of p62, but increased by knockdown of p62. Moreover, we found that p62 knockdown induced the protein expression of argonaute 2 (AGO2). Luciferase reporter assay results showed that the gene expression of PR was promoted by AGO2. Furthermore, results revealed that overexpression of AGO2 partially rescued the decrease in PR expression induced by forced expression of p62. Collectively, our findings indicated that p62 accumulation suppressed the expression of AGO2, which in turn decreased the expression of PR, suggesting that p62 may serve as a marker of aggressive breast cancer and poor prognosis. Moreover, the p62-AGO2-PR axis was identified as a crucial signaling cascade in breast cancer progression.

Published

2020

22. High‐Resolution Electrochemical Mapping of the Hydrogen Evolution Reaction on Transition‐Metal Dichalcogenide Nanosheets

Author

Yasufumi Takahashi, Yu Kobayashi, Ziqian Wang, Yoshikazu Ito, Masato Ota, Hiroki Ida, Akichika Kumatani, Keisuke Miyazawa, Takeshi Fujita, Hitoshi Shiku, Yuri E. Korchev, Yasumitsu Miyata, Takeshi Fukuma, Mingwei Chen, and Tomokazu Matsue

Subjects

General Medicine

Published

2020

23. Selectively Induced Apoptosis in Human Neutrophils in the Presence of Oxidative Phenoxazines, 2-Amino-4,4α-dihydryo-4α-7H-phenoxazine-3-one and 2-Aminophenoxazine-3-one, Preceded by Decrease of Intracellular pH, Depolarization of the Mitochondria, and Inhibition of Superoxide Generation

Author

Takanobu Tabuchi, Xiao-Fang Che, Katsuya Hiraishi, Masakazu Adachi, Kei Miyano, Hideki Sumimoto, Takafumi Tabuchi, Keisuke Miyazawa, and Akio Tomoda

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Abstract.: The present research investigated the effect of the oxidative phenoxazines, 2-amino-4,4α-dihydryo-4α-7H-phenoxazine-3-one (Phx-1) and 2-amino-phenoxazine-3-one (Phx-3) on apoptosis induction and apoptosis-related early events in human neutrophils. When Phx-1 or Phx-3 was administered to freshly drawn human blood for 18 h, these phenoxazines caused apoptotic cell death morphologically characterized by condensation of the nucleus in neutrophils, without causing it in lymphocytes and monocytes. Apoptosis, which was detectable by microscopic analysis and by using flow-cytometry, occurred significantly in human neutrophils isolated from freshly drawn blood, 6 h after the administration of 50 μM Phx-1 and Phx-3. After 24 h, every isolated neutrophil treated with Phx-1 or Phx-3 fell into apoptosis or lost its morphology, while many of the neutrophils without these phenoxazines remained alive, with normal morphology. Apoptosis-related early events including a decrease in intracellular pH (pHi) and depolarization of the mitochondria occurred in the isolated neutrophils, 30 min and 6 h after the administration of Phx-1 or Phx-3, respectively. Superoxide generation from the isolated neutrophils mimicked by phorbol myristate acetate (PMA) was very markedly inhibited by 100 μM Phx-1 or Phx-3. This result could be explained, in part, by the fact that the insufficient supply of NADPH (nicotinamide adenine dinucleotide phosphate, reduced form) was caused by pHi decrease in neutrophils treated with Phx-1 or Phx, because NADPH is necessary for NADPH oxidase responsible for generating superoxide in the cells. The present results suggest that Phx-1 and Phx-3 have the capacity of selectively inducing apoptosis in human neutrophils and that these phenoxazines may be useful as specific drugs to induce apoptotic cell death of human neutrophils and thereby prevent inflammation caused by these phagocytic cells. Keywords:: neutrophil, phenoxazine, apoptosis, mitochondria, pHi

Published

2011

24. Phenoxazine Derivatives Suppress the Infections Caused by Herpes Simplex Virus Type-1 and Herpes Simplex Virus Type-2 Intravaginally Inoculated Into Mice

Author

Kyoko Hayashi, Toshimitsu Hayashi, Keisuke Miyazawa, and Akio Tomoda

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

We examined the in vivo antiviral activities of 2-amino-4,4α-dihydro-4α-7-dimethyl-3H-phenoxazine-3-one (Phx-1), 3-amino-1,4α-dihydro-4α-8-dimethyl-2H-phenoxazine-2-one (Phx-2), and 2-aminophenoxazine-3-one (Phx-3) against herpes viruses. The virus yield three days after administration, changes in the 6-degree’s lesion scores, and the morbidity were assessed after herpes simplex virus type-1 (HSV-1) [acyclovir (ACV)-sensitive KOS strain or ACV-resistant A4-3 strain] or HSV-2 (ACV-sensitive UW 268 strain) was inoculated intravaginally to mice with administration of Phx-1, Phx-2, Phx-3, or ACV (0.2 mg per administration, 3 times daily) for 8 days starting from 1 day before virus inoculation to 7 days after infection. Phx-1, Phx-2, and Phx-3 extensively suppressed the virus yield of HSV-1. Only Phx-2 exerted moderate inhibitory effects against HSV-2 in mice. The lesion scores, as clinical signs manifested by infection of the KOS strain of HSV-1, were extensively suppressed by intravaginal application of Phx-1, Phx-2, or Phx-3. The lesion scores in HSV-2–infected mice indicated moderate suppression, when Phx-1, Phx-2, or Phx-3 was applied. Without treatment by one of the compounds, none of the HSV-1– infected mice died, but all the HSV-2–infected ones did. However, by the administration of Phx-1, Phx-2, or Phx-3 fairly improved the survival rates of the HSV-2–infected mice. Phx-2 showed dose-dependent anti-HSV-2 efficacy when administered at doses of 0.2 and 1 mg per administration. The present in vivo data suggest that the Phx-1, Phx-2, and Phx-3 are attractive candidates for agents to prevent both replication of HSV and aggravation of lesions caused by these viruses. Keywords:: herpes simplex virus type l, herpes simplex virus type 2, phenoxazine, intravaginal application

Published

2010

25. Visualizing intracellular nanostructures of living cells by nanoendoscopy-AFM

Author

Marcos Penedo, Keisuke Miyazawa, Naoko Okano, Hirotoshi Furusho, Takehiko Ichikawa, Mohammad Shahidul Alam, Kazuki Miyata, Chikashi Nakamura, and Takeshi Fukuma

Subjects

Multidisciplinary, microscopy, molecules, cytoskeleton, nanoneedles, force, quantification

Abstract

Atomic force microscopy (AFM) is the only technique that allows label-free imaging of nanoscale biomolecular dynamics, playing a crucial role in solving biological questions that cannot be addressed by other major bioimaging tools (fluorescence or electron microscopy). However, such imaging is possible only for systems either extracted from cells or reconstructed on solid substrates. Thus, nanodynamics inside living cells largely remain inaccessible with the current nanoimaging techniques. Here, we overcome this limitation by nanoendoscopy-AFM, where a needle-like nanoprobe is inserted into a living cell, presenting actin fiber three-dimensional (3D) maps, and 2D nanodynamics of the membrane inner scaffold, resulting in undetectable changes in cell viability. Unlike previous AFM methods, the nanoprobe directly accesses the target intracellular components, exploiting all the AFM capabilities, such as high-resolution imaging, nanomechanical mapping, and molecular recognition. These features should greatly expand the range of intracellular structures observable in living cells.

Published

2021

26. Virtual Replication of the Idalion Tablet.

Author

Bertille Robin, Thibaut Hilpert, Keisuke Miyazawa, Patrick Callet, François-Xavier de Contencin, and Anna Zymla

Published

2010

27. Targeted disruption of GAK stagnates autophagic flux by disturbing lysosomal dynamics

Author

Hirotsugu Hino, Mayumi Tokuhisa, Keisuke Miyazawa, Masaki Hiramoto, Naoharu Takano, Jun Takemura, Hiroko Kokuba, Masaya Miyazaki, and Hiromi Kazama

Subjects

autophagy, autophagic lysosome reformation, Protein Serine-Threonine Kinases, Endocytosis, Rho-associated protein kinase, Lysosome, Genetics, medicine, Humans, ROCK1, Protein kinase A, Cyclin, rho-Associated Kinases, autophagosome-lysosome fusion, actomyosin, Chemistry, cyclin G-associated kinase, Autophagy, Autophagosomes, Intracellular Signaling Peptides and Proteins, Articles, General Medicine, Cell cycle, Cell biology, medicine.anatomical_structure, A549 Cells, Lysosomes, Flux (metabolism)

Abstract

The autophagy‑lysosome system allows cells to adapt to environmental changes by regulating the degradation and recycling of cellular components, and to maintain homeostasis by removing aggregated proteins and defective organelles. Cyclin G‑associated kinase (GAK) is involved in the regulation of clathrin‑dependent endocytosis and cell cycle progression. In addition, a single nucleotide polymorphism at the GAK locus has been reported as a risk factor for Parkinson's disease. However, the roles of GAK in the autophagy‑lysosome system are not completely understood, thus the present study aimed to clarify this. In the present study, under genetic disruption or chemical inhibition of GAK, analyzing autophagic flux and observing morphological changes of autophagosomes and autolysosomes revealed that GAK controlled lysosomal dynamics via actomyosin regulation, resulting in a steady progression of autophagy. GAK knockout (KO) in A549 cells impaired autophagosome‑lysosome fusion and autophagic lysosome reformation, which resulted in the accumulation of enlarged autophagosomes and autolysosomes during prolonged starvation. The stagnation of autophagic flux accompanied by these phenomena was also observed with the addition of a GAK inhibitor. Furthermore, the addition of Rho‑associated protein kinase (ROCK) inhibitor or ROCK1 knockdown mitigated GAK KO‑mediated effects. The results suggested a vital role of GAK in controlling lysosomal dynamics via maintaining lysosomal homeostasis during autophagy.

Published

2021

28. Ricolinostat enhances adavosertib‑induced mitotic catastrophe in TP53‑mutated head and neck squamous cell carcinoma cells

Author

Keitaro Miyake, Naoharu Takano, Hiromi Kazama, Hiroyuki Kikuchi, Masaki Hiramoto, Kiyoaki Tsukahara, and Keisuke Miyazawa

Subjects

Cancer Research, Pyrimidines, Oncology, Head and Neck Neoplasms, Squamous Cell Carcinoma of Head and Neck, Cell Line, Tumor, Humans, Pyrazoles, Apoptosis, Pyrimidinones, Tumor Suppressor Protein p53, Hydroxamic Acids

Published

2021

29. Lysosome‑targeted drug combination induces multiple organelle dysfunctions and non‑canonical death in pancreatic cancer cells

Author

Sumire Suzuki, Masato Ogawa, Masaya Miyazaki, Kohki Ota, Hiromi Kazama, Ayako Hirota, Naoharu Takano, Masaki Hiramoto, and Keisuke Miyazawa

Subjects

Sphingosine 1 Phosphate Receptor Modulators, Cancer Research, hydroxychloroquine, endocrine system diseases, mitochondrial depolarization, Aminopyridines, Antineoplastic Agents, abemaciclib, pancreatic cancer cells, Cell Line, Tumor, Humans, lysosomal membrane permeabilization, lapatinib, fingolimod, skin and connective tissue diseases, non-canonical cell death, lysosome-targeted drug combination, calcium homeostasis, Fingolimod Hydrochloride, Drug Synergism, General Medicine, Articles, Endoplasmic Reticulum Stress, Pancreatic Neoplasms, Oncology, Benzimidazoles, Lysosomes, Carcinoma, Pancreatic Ductal

Abstract

Pancreatic cancer is one of the leading causes of cancer-related mortality and has the lowest 5-year survival rate. Therefore, novel strategies are urgently required to treat pancreatic cancer. Pancreatic ductal adenocarcinoma (PDAC) cells rely on enhanced lysosomal function for survival and proliferation to facilitate the degradation of contents accumulated via autophagy and macropinocytosis. Previously, we have reported that the combination of epidermal growth factor receptor/HER2 inhibitor lapatinib and sphingosine analog fingolimod (FTY720) confers a significant cytostatic effect in lung cancer cells. In the present study, the combined effects of these drugs on PDAC cell lines, BxPC-3, KP-4, PANC-1 and MIA PaCa-2, were examined. It was observed that FTY720 enhanced the lapatinib-induced cytotoxic effect and caused non-canonical and lysosome-dependent death in PDAC cells. Lapatinib and FTY720 induced lysosomal swelling and inhibited lysosomal acidification. Combination treatment with lapatinib and FTY720 increased lysosomal membrane permeability, induced mitochondrial depolarization, induced endoplasmic reticulum stress and disturbed intracellular calcium homeostasis. Additionally, the cytotoxic effect of lapatinib was enhanced by hydroxychloroquine or the CDK4/6 inhibitor abemaciclib, both of which induce lysosomal dysfunction. Collectively, these results indicated that the lysosome-targeted drug combination induces multiple organelle dysfunction and exerts a marked cytotoxic effect in PDAC cells.

Published

2021

30. Induction of synergistic non-apoptotic cell death by simultaneously targeting proteasomes with bortezomib and histone deacetylase 6 with ricolinostat in head and neck tumor cells

Author

Kazuhiro Hattori, Keisuke Miyazawa, Keitaro Miyake, Kiyoaki Tsukahara, Naoharu Takano, Hiromi Kazama, Masaki Hiramoto, and Shota Moriya

Subjects

head and neck tumor, squamous cell carcinoma, Cancer Research, Programmed cell death, Chemistry, Bortezomib, Necroptosis, Autophagy, bortezomib, necroptosis, macromolecular substances, Articles, Cell cycle, histone deacetylase 6, RIPK1, proteasome, Oncology, Apoptosis, Proteasome inhibitor, medicine, Cancer research, ricolinostat, medicine.drug

Abstract

Following surgery and chemoradiation, ~50% of patients with locally advanced head and neck tumors experience relapse within the first two years, with a poor prognosis. Therefore, a novel therapeutic approach is required. The aim of the present study was to investigate the effect of combination treatment with the proteasome inhibitor bortezomib (BTZ), and ricolinostat (RCS), a specific inhibitor of histone deacetylase 6 (HDAC6), on CAL27 and Detroit562 head and neck cancer cells. BTZ and RCS exhibited cytotoxicity in a dose- and time-dependent manner. Simultaneous treatment with BTZ and RCS resulted in the synergistic enhancement of non-apoptotic cell death and autophagy. The receptor-interacting serine/threonine-protein kinase 1 (RIPK1) inhibitor, necrostatin, but not the autophagy inhibitor, 3-methyladenine, attenuated the cytotoxicity of combined BTZ and RCS treatment. Thus, necroptosis [type-III programmed cell death (PCD)], but not autophagic cell death (type-II PCD), appeared to contribute to the pronounced cytotoxicity. However, no phosphorylation of RIPK1 or mixed lineage kinase domain-like protein was detectable in response to BTZ or RCS. Furthermore, RCS induced α-tubulin acetylation and inhibited BTZ-induced aggresome formation along with endoplasmic reticulum stress loading. Combined treatment with BTZ and RCS enhanced the production of reactive oxygen species (ROS). The ROS scavenger, N-acetyl cysteine, abrogated the increase in cytotoxicity. These results suggest the potential therapeutic value of the dual targeting of the proteasome and HDCA6 for head and neck cancers through the induction of necroptosis-like cell death along with ROS generation.

Published

2021

31. Vitamin K2 induces non-apoptotic cell death along with autophagosome formation in breast cancer cell lines

Author

Naoharu Takano, Keisuke Miyazawa, Shota Moriya, Hirotsugu Hino, Hiroko Kokuba, and Shinsuke Miyazawa

Subjects

0301 basic medicine, Programmed cell death, business.industry, Autophagy, General Medicine, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Breast cancer, Oncology, Apoptosis, Cell culture, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, medicine, Cytotoxic T cell, Pharmacology (medical), Radiology, Nuclear Medicine and imaging, business, Triple-negative breast cancer

Abstract

Vitamin K2 (VK2) has been reported to induce apoptosis in many types of cancer cells including leukemia. However, there are no precise reports regarding the breast cancer cells. From the stand point of clinical implications of VK2 including chemoprevention, we investigated the effects of VK2 on breast cancer cell lines. Breast cancer cell lines were cultured with VK2, and the cytotoxicity and cell death phenotype were examined. The HL-60 leukemia cells were used as a control for VK2-induced apoptosis. VK2 exhibited the cytotoxic effect, especially in triple negative breast cancer cell lines, namely, MDA-MB-231 and MDA-MB-468. However, in contrast to HL-60 cells, typical features of the cells undergoing apoptosis, such as chromatin condensation, nuclear fragments, and cleavage of caspase-3 were not detected. Transmission electron microscopy exhibited an increased number of autophagosomes/autolysosomes with plasma membrane integrity. An autophagy inhibitor, 3-methyladenine, apparently attenuated VK2-induced cytotoxicity, which indicated the involvement of autophagy-dependent cell death. Interestingly, both VK2-induced non-apoptotic cell death in MDA-MB-231 cells and VK2-induced apoptosis in HL-60 cells were suppressed in the presence of reactive oxygen species (ROS) scavengers. Therefore, ROS production by VK2 seems to be located up-stream in the molecular machinery for both the types of cell death execution. The VK2 induced non-apoptotic cell death along with autophagy, in triple negative breast cancer cell lines. Cell death phenotype induced by VK2 appears to differ among the type of cancers. This suggests the possibility of using VK2 for the breast cancer therapy.

Published

2019

32. Variations in Atomic-Scale Step Edge Structures and Dynamics of Dissolving Calcite in Water Revealed by High-Speed Frequency Modulation Atomic Force Microscopy

Author

Yuta Kawagoe, Adam S. Foster, John Tracey, Keisuke Miyazawa, Takeshi Fukuma, and Kazuki Miyata

Subjects

Calcite, Materials science, 02 engineering and technology, Edge (geometry), 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, Atomic units, 0104 chemical sciences, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, Ion, chemistry.chemical_compound, General Energy, chemistry, Chemical physics, Monolayer, Intermediate state, Physical and Theoretical Chemistry, 0210 nano-technology, Dissolution, Earth (classical element)

Abstract

Calcite dissolution plays critical roles in the global carbon cycle in the Earth, biomineralizations, and weathering of buildings. However, in spite of the importance, the atomistic events at the step edges during the dissolution have remained elusive because of the difficulties in their direct visualization. In this study, we used high-speed frequency modulation atomic force microscopy (FM-AFM) for visualizing various atomic-scale step edge structures and dynamics during the calcite dissolution in water. The obtained images reveal the coexistence of the steps with and without a transition region (TR); a Ca(OH)2 monolayer formed along the step edge as an intermediate state in the dissolution. The TRs are more frequently observed along the slowly dissolving acute steps than along the rapidly dissolving obtuse steps. This finding and our imaging of the TR formation process suggest that the free energy to form a TR is comparable to that for removing ions directly from the step edge and an increase in the loc...

Published

2019

33. Azithromycin enhances the cytotoxicity of DNA-damaging drugs via lysosomal membrane permeabilization in lung cancer cells

Author

Naoharu Takano, Hiroko Kokuba, Masaki Hiramoto, Shinji Abe, Keisuke Miyazawa, Shota Moriya, Kazutoshi Toriyama, and Hiromi Kazama

Subjects

0301 basic medicine, Autophagosome, p53, Cancer Research, Programmed cell death, autophagy, Cell Membrane Permeability, Lung Neoplasms, Cell Survival, non–small‐cell lung cancer, Carboplatin, 03 medical and health sciences, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, Humans, Topoisomerase II Inhibitors, Doxorubicin, lysosomal membrane permeabilization, Cytotoxicity, Cell Proliferation, azithromycin, Chemistry, Autophagy, Epidemiology and Prevention, Drug Synergism, General Medicine, Original Articles, Cytoprotection, 030104 developmental biology, Oncology, A549 Cells, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, TFEB, Original Article, Lysosomes, medicine.drug, DNA Damage

Abstract

Cancer cells use autophagy for growth, survival, and cytoprotection from chemotherapy. Therefore, autophagy inhibitors appear to be good candidates for cancer treatment. Our group previously reported that macrolide antibiotics, especially azithromycin (AZM), have potent autophagy inhibitory effects, and combination treatment with tyrosine kinase inhibitors or proteasome inhibitors enhances their anti–cancer activity. In this study, we evaluated the effect of combination therapy with DNA‐damaging drugs and AZM in non–small‐cell lung cancer (NSCLC) cells. We found that the cytotoxic activities of DNA‐damaging drugs, such as doxorubicin (DOX), etoposide, and carboplatin, were enhanced in the presence of AZM in NSCLC cell lines, whereas AZM alone exhibited almost no cytotoxicity. This enhanced cell death was dependent on wild‐type‐p53 status and autophagosome‐forming ability because TP53 knockout (KO) and ATG5‐KO cells attenuated AZM‐enhanced cytotoxicity. DOX treatment upregulated lysosomal biogenesis by activating TFEB and led to lysosomal membrane damage as assessed by galectin 3 puncta assay and cytoplasmic leakage of lysosomal enzymes. In contrast, AZM treatment blocked autophagy, which resulted in the accumulation of lysosomes/autolysosomes. Thus, the effects of DOX and AZM were integrated into the marked increase in damaged lysosomes/autolysosomes, leading to prominent lysosomal membrane permeabilization (LMP) for apoptosis induction. Our data suggest that concomitant treatment with DNA‐damaging drugs and AZM is a promising strategy for NSCLC treatment via pronounced LMP induction., In this paper, we showed that coadministration of DNA‐damaging drugs and azithromycin (AZM), a macrolide antibiotic, enhanced cytotoxicity due to increased lysosomal membrane permeabilization (LMP). Because DNA‐damaging drugs induce LMP, cancer cells activate autophagy to remove damaged lysosomes by lysophagy. However, AZM inhibited lysophagy, as well as autophagy, resulting in the prominent cytoplasmic accumulation of damaged lysosomes for induction of LMP‐mediated apoptosis in non–small‐cell lung cancer cells.

Published

2021

34. BRCA1 degradation in response to mitochondrial damage in breast cancer cells

Author

Keisuke Miyazawa, Hiroshi Handa, Edward Barroga, Koji Fujita, Hiromi Kazama, Kana Miyahara, Masahiko Kuroda, Yumiko Yamada, Hirotsugu Hino, Takashi Ishikawa, Mayumi Tokuhisa, Naoharu Takano, and Masaki Hiramoto

Subjects

Cell biology, Carbonyl Cyanide m-Chlorophenyl Hydrazone, endocrine system diseases, DNA damage, Ubiquitin-Protein Ligases, Science, Breast Neoplasms, PINK1, Biochemistry, Article, Parkin, Breast cancer, Downregulation and upregulation, Humans, DNA Breaks, Double-Stranded, skin and connective tissue diseases, Cancer, Cell Nucleus, Gene knockdown, Multidisciplinary, biology, BRCA1 Protein, Kinase, Chemistry, Ubiquitination, Mitochondria, Up-Regulation, Ubiquitin ligase, HEK293 Cells, Proteolysis, Cancer cell, MCF-7 Cells, biology.protein, Cancer research, Medicine, Female, Protein Kinases

Abstract

BRCA1 is a well-studied tumor suppressor involved in the homologous repair of DNA damage, whereas PINK1, a mitochondrial serine/threonine kinase, is known to be involved in mitochondrial quality control. Genetic mutations of PINK1 and Parkin cause autosomal recessive early-onset Parkinson’s disease. We found that in breast cancer cells, the mitochondrial targeting reagents, which all induce mitochondrial depolarization along with PINK1 upregulation, induced proteasomal BRCA1 degradation. This BRCA1 degradation was dependent on PINK1, and BRCA1 downregulation upon mitochondrial damage caused DNA double-strand breaks. BRCA1 degradation was mediated through the direct interaction with the E3 ligase Parkin. Strikingly, BRCA1 and PINK1/Parkin expression were inversely correlated in cancerous mammary glands from breast cancer patients. BRCA1 knockdown repressed cancer cell growth, and high BRCA1 expression predicted poor relapse-free survival in breast cancer patients. These observations indicate a novel mechanism by which mitochondrial damage is transmitted to the nucleus, leading to BRCA1 degradation.

Published

2021

35. Photothermal excitation efficiency enhancement of cantilevers by electron beam deposition of amorphous carbon thin films

Author

Takeshi Fukuma, Marcos Penedo, Ayhan Yurtsever, Hirotoshi Furusho, Kiyo-aki Ishii, and Keisuke Miyazawa

Subjects

Materials science, Cantilever, Molecular imaging, lcsh:Medicine, Imaging techniques, 02 engineering and technology, 01 natural sciences, Article, Techniques and instrumentation, law.invention, Atomic force microscopy, law, 0103 physical sciences, Laser power scaling, Thin film, lcsh:Science, 010302 applied physics, Multidisciplinary, business.industry, lcsh:R, Resonance, Photothermal therapy, 021001 nanoscience & nanotechnology, Laser, Scanning probe microscopy, Amorphous carbon, Optoelectronics, lcsh:Q, 0210 nano-technology, business, Excitation

Abstract

In recent years, the atomic force microscope has proven to be a powerful tool for studying biological systems, mainly for its capability to measure in liquids with nanoscale resolution. Measuring tissues, cells or proteins in their physiological conditions gives us access to valuable information about their real ‘in vivo’ structure, dynamics and functionality which could then fuel disruptive medical and biological applications. The main problem faced by the atomic force microscope when working in liquid environments is the difficulty to generate clear cantilever resonance spectra, essential for stable operation and for high resolution imaging. Photothermal actuation overcomes this problem, as it generates clear resonance spectra free from spurious peaks. However, relatively high laser powers are required to achieve the desired cantilever oscillation amplitude, which could potentially damage biological samples. In this study, we demonstrate that the photothermal excitation efficiency can be enhanced by coating the cantilever with a thin amorphous carbon layer to increase the heat absorption from the laser, reducing the required excitation laser power and minimizing the damage to biological samples.

Published

2020

36. Comparison of autophagy inducibility in various tyrosine kinase inhibitors and their enhanced cytotoxicity via inhibition of autophagy in cancer cells in combined treatment with azithromycin

Author

Naoharu Takano, Hideki Tanaka, Keisuke Miyazawa, Hiromi Kazama, Masaki Hiramoto, Shota Moriya, Hirotsugu Hino, Kiyoaki Tsukahara, and Masaya Miyazaki

Subjects

0301 basic medicine, Sorafenib, Programmed cell death, medicine.drug_class, Biophysics, Tyrosine kinase inhibitor, tivantinib, TIV, imatinib, IMA, Biochemistry, Tyrosine-kinase inhibitor, lcsh:Biochemistry, 03 medical and health sciences, 0302 clinical medicine, receptor tyrosine kinase, RTK, medicine, Autophagy, Osimertinib, lcsh:QD415-436, Epidermal growth factor receptor, bafilomycin A1, BAF, lcsh:QH301-705.5, sorafenib, SOR, Cancer, azithromycin, AZM, lapatinib, LAP, biology, Chemistry, osimertinib, OSI, dasatinib, DAS, Macrolide antibiotics, respiratory tract diseases, Dasatinib, lenvatinib, LEN, 030104 developmental biology, lcsh:Biology (General), 030220 oncology & carcinogenesis, Cancer research, biology.protein, tyrosine kinase inhibitors, TKIs, Tyrosine kinase, Research Article, gefitinib, GEF, medicine.drug

Abstract

Tyrosine kinase inhibitors (TKIs) induce autophagy in many types of cancer cells. We previously reported that gefitinib (GEF) and imatinib (IMA) induce autophagy in epidermal growth factor receptor (EGFR) knock-out A549 and non-BCR-ABL-expressing leukemia cell lines, respectively. This evidence suggests that TKI-induced autophagy is independent of the original target molecules. The present study compared the autophagy-inducing abilities of various TKIs, regardless of their targets, by quantitative autophagy flux assay. We established stable clones expressing the GFP-LC3-mCherry-LC3ΔG plasmid in A549, PC-9, and CAL 27 cell lines and assessed autophagy inducibility by monitoring the fluorescent ratios of GFP-LC3 to mCherry-LC3ΔG using an IncuCyte live cell imaging system during exposure to TKIs viz; GEF, osimertinib (OSI), lapatinib (LAP), lenvatinib (LEN), sorafenib (SOR), IMA, dasatinib (DAS), and tivantinib (TIV). Among these TKIs, DAS, GEF, and SOR exhibited prominent autophagy induction in A549 and PC-9 cells. In CAL 27 cells, IMA, SOR, and LEN, but not GEF, TIV, or OSI, exhibited autophagy induction. In the presence of azithromycin (AZM), which showed an inhibitory effect on autophagy flux, TKIs with prominent autophagy inducibility exhibited enhanced cytotoxicity via non-apoptotic cell death relative to effects of TKI alone. Therefore, autophagy inducibility of TKIs differed in the context of cancer cells. However, once induced, they appeared to have cytoprotective functions. Thus, blocking TKI-induced autophagy with AZM may improve the therapeutic effect of TKIs in cancer cells., Highlights • Tyrosine kinase inhibitors (TKIs) induce autophagy regardless of their main target. • This autophagy inducibility is partially determined in the context of cancer cells. • Azithromycin (AZM) has an inhibitory effect on autophagy. • Blocking TKI-induced autophagy with AZM enhances their cytotoxicity in cancer cells. • This enhanced cytotoxicity is mediated through non-apoptotic cell death.

Published

2020

37. Tip dependence of three-dimensional scanning force microscopy images of calcite-water interfaces investigated by simulation and experiments

Author

Adam S. Foster, John Tracey, Bernhard Reischl, Andrew L. Rohl, Takeshi Fukuma, Peter Spijker, Keisuke Miyazawa, Kanazawa University, Surfaces and Interfaces at the Nanoscale, Curtin University, Department of Applied Physics, Aalto-yliopisto, Aalto University, and INAR Physics

Subjects

Surface (mathematics), Calcite, Materials science, Similarity (geometry), 02 engineering and technology, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, Molecular physics, 114 Physical sciences, DEFLECTION SENSOR, 0104 chemical sciences, ENERGY, chemistry.chemical_compound, chemistry, SOLVATION, Mechanical stability, Microscopy, General Materials Science, HYDRATION LAYERS, Scanning Force Microscopy, 0210 nano-technology, Three dimensional scanning

Abstract

In this study, we have investigated the influence of the tip on the three-dimensional scanning force microscopy (3D-SFM) images of calcite-water interfaces by experiments and simulations. We calculated 3D force images by simulations with the solvent tip approximation (STA), Ca, CO3 and OH tip models. For all the 3D images, the z profiles at the surface Ca and CO3 sites alternately show oscillatory peaks corresponding to the hydration layers. However, the peak heights and spacings become larger when the mechanical stability of the tip becomes higher. For analyzing the xy slices of the 3D force images, we developed the extended STA (E-STA) model which allowed us to reveal the strong correlation between the hydration structure just under the tip and the atomic-scale force contrasts. Based on these understandings on the image features showing the strong tip dependence, we developed a method for objectively estimating the similarity between 3D force images. With this method, we compared the simulated images with the three experimentally obtained ones. Among them, two images showed a relatively high similarity with the image obtained by the simulation with the Ca or the CO3 tip model. Based on these agreements, we characterized the hydration structure and mechanical stability of the experimentally used tips. The understanding and methodology presented here should help us to derive accurate information on the tip and the interfacial structure from experimentally obtained 3D-SFM images.

Published

2020

38. Self-assembly of small molecules at hydrophobic interfaces using group effect

Author

Keisuke Miyazawa, Kislon Voϊtchovsky, William J. Foster, Takeshi Fukuma, and Halim Kusumaatmaja

Subjects

Materials science, Supramolecular chemistry, Oxide, FOS: Physical sciences, 02 engineering and technology, Condensed Matter - Soft Condensed Matter, 010402 general chemistry, 01 natural sciences, law.invention, chemistry.chemical_compound, law, Physics - Chemical Physics, Molecule, General Materials Science, Nanoscopic scale, Chemical Physics (physics.chem-ph), Condensed Matter - Materials Science, Hydrogen bond, Graphene, Materials Science (cond-mat.mtrl-sci), 021001 nanoscience & nanotechnology, Small molecule, 0104 chemical sciences, chemistry, Chemical physics, Soft Condensed Matter (cond-mat.soft), Self-assembly, 0210 nano-technology

Abstract

Although common in nature, the self-assembly of small molecules at sold-liquid interfaces is difficult to control in artificial systems. The high mobility of dissolved small molecules limits their residence at the interface, typically restricting the self-assembly to systems under confinement or with mobile tethers between the molecules and the surface. Small hydrogen-bonding molecules can overcome these issues by exploiting group-effect stabilization to achieve non-tethered self-assembly at hydrophobic interfaces. Significantly, the weak molecular interactions with the solid makes it possible to influence the interfacial hydrogen bond network, potentially creating a wide variety of supramolecular structures. Here we investigate the nanoscale details of water and alcohols mixtures self-assembling at the interface with graphite through group effect. We explore the interplay between inter-molecular and surface interactions by adding small amounts of foreign molecules able to interfere with the hydrogen bond network and systematically varying the length of the alcohol hydrocarbon chain. The resulting supramolecular structures forming at room temperature are then examined using atomic force microscopy with insights from computer simulations. We show that the group-based self-assembly approach investigated here is general and can be reproduced on other substrates such as molybdenum disulphide and graphene oxide, potentially making it relevant for a wide variety of systems., 6 figures, Supporting Information files are available upon request to the authors

Published

2020

39. Wideband Magnetic Excitation System for Atomic Force Microscopy Cantilevers with Megahertz-Order Resonance Frequency

Author

Keisuke Miyazawa, Takumi Igarashi, Keita Suzuki, Takeshi Fukuma, and Kaito Hirata

Subjects

Cantilever, Materials science, lcsh:Medicine, 02 engineering and technology, Imaging techniques, 01 natural sciences, Characterization and analytical techniques, Article, 0103 physical sciences, Wideband, 010306 general physics, lcsh:Science, Electrical impedance, Electronic circuit, Multidisciplinary, business.industry, lcsh:R, Resonance, 021001 nanoscience & nanotechnology, Magnetic field, Scanning probe microscopy, Electromagnetic coil, Optoelectronics, lcsh:Q, 0210 nano-technology, business, Excitation

Abstract

Small cantilevers with a megahertz-order resonance frequency provide excellent sensitivity and speed in liquid-environment atomic force microscopy (AFM). However, stable and accurate oscillation control of a small cantilever requires the photothermal excitation, which has hindered their applications to the studies on photo-sensitive materials. Here, we develop a magnetic excitation system with a bandwidth wider than 4 MHz, enabling a light-free excitation of small cantilevers. In the system, a cantilever with a magnetic bead is driven by a magnetic field generated by a coil. In the coil driver, a differentiation circuit is used for compensating the frequency dependence of the coil impedance and keeping the current constant. By implementing several differentiation circuits with different frequency ranges, we enable to drive various cantilevers having different resonance frequencies with sufficient excitation efficiency. In contrast to the conventional coil driver with a closed-loop circuit, the developed one consists of an open-loop circuit and hence can be stably operated regardless of the coil design. With the developed system, atomic-resolution imaging of mica in liquid using a small cantilever with a megahertz-order resonance frequency is demonstrated. This development should lead to the future applications of AFM with small cantilevers to the studies on various photo-sensitive materials and phenomena.

Published

2020

40. Different intoxication mechanism between paralytic shellfish toxin (PST)- and/or tetrodotoxin-contaminated xanthid crabs and PST-contaminated edible shore crabs in Japan and their food poisonings

Author

Tamao Noguchi, Hiroshi Oikawa, Manabu Asakawa, Osamu Arakawa, Kinue Daigo, and Keisuke Miyazawa

Subjects

Shore, geography, animal structures, Food poisoning, geography.geographical_feature_category, Toxin, fungi, food and beverages, Zoology, Biology, Contamination, medicine.disease, medicine.disease_cause, body regions, chemistry.chemical_compound, Food chain, chemistry, Tetrodotoxin, medicine, Ingestion, Omnivore

Abstract

The intoxication mechanism of xanthid crabs and edible shore crabs in Japan by ‘paralytic shellfish toxin’ (PST) and/or ‘tetrodotoxin’ (TTX) was investigated. Three xanthid crabs were toxic and their toxin consisted of PST and/or TTX. Since great individual and regional variation in toxicity of each specimen, and toxin variety with exposure of toxic crab to each toxin were confirmed, their intoxication mechanism was suggested to be a food chain feeding toxic plankton. However, as they are omnivorous, the conclusion remains uncertain. Two edible shore crabs including Telmessus acutidents were contaminated with PST around 2003, in the Tohoku district of Japan. The intoxication mechanism of the crab was experimentally shown to be through the food chain by feeding on bivalves infested with PST-producing Alexandrium sp. Many food poisoning cases due to ingestion of xanthid crabs have occurred so far, but there are no reports in the case of this shore crab.

Published

2020

41. Contributors

Author

Francisco Gabriel Acién-Fernández, Hossein Ahmadzadeh, Cynthia Alcántara, Allan Victor Martins Almeida, Agostinho Antunes, Osamu Arakawa, Wagner L. Araújo, Neha Arora, Manabu Asakawa, Jose L. Barriada, Laura Barsanti, Eloy Bécares, Saúl Blanco, Aurélie Blanfuné, Silvia Bolado, Charles F. Boudouresque, Cristiane Canan, Naira Valle de Castro, Liliana Cepoi, Channakeshavaiah Chikkaputtaiah, Ann D. Christy, Eliane Colla, Jorge Alberto Vieira Costa, Rosana Aparecida da Silva-Buzanello, Kinue Daigo, Tatenda Dalu, Clinton J. Dawes, Deepi Deka, Deisy Alessandra Drunkler, Maranda Esterhuizen-Londt, Letícia Schneider Fanka, Cecilia Faraloni, José María Fernández-Sevilla, Pedro García-Encina, María Cruz García-González, Reimund Goss, Paolo Gualtieri, David Hernández, Roberto Herrero, Rubén Irusta, Damini Jaiswal, Torsten Jakob, Daneysa Lahis Kalschne, Ozcan Konur, Roberta da Costa Kosinski, Ana Larrán, Daniel A. Lemley, Pablo Lodeiro, Stephen Lyon, Violeta Makareviciene, Giorgos Markou, Joana Martins, Arthur C. Mathieson, Yukihiko Matsuyama, Anne Luize Lupatini Menegotto, J.S. Metcalf, Keisuke Miyazawa, Marziyeh Molazadeh, Michele Greque de Morais, Cristiana Moreira, Juliana Botelho Moreira, Raúl Muñoz, Tamao Noguchi, Bahareh Nowruzi, Adriano Nunes-Nesi, Ellis O’Neill, Tatsuya Oda, Hiroshi Oikawa, Sheyla Ortíz, Stephan Pflugmacher, Yimin Qin, Berta Riaño, Pilar Rodriguez-Barro, Sandrine Ruitton, Beenish Saba, Gisoo Sarvari, Manuel E. Sastre de Vicente, Egle Sendzikiene, Shinjinee Sengupta, Mostafa Shourian, Gavin C. Snow, Shashanka Sonowal, N.R. Souza, Thierry Thibaut, Cristina Tomás, Giuseppe Torzillo, Vitor Vasconcelos, Marcelo Gomes Marçal Vieira Vaz, Natarajan Velmurugan, Teresa Vilariño, Pramod P. Wangikar, Christian Wilhelm, Naicheng Wu, Inga Zinicovscaia, Hussein Znad, and Hamidreza Zohoorian

Published

2020

42. Morphology and Physical Properties of Hydrophilic-Polymer-Modified Lipids in Supported Lipid Bilayers

Author

Yoshihiro Tachihara, Yoshiaki Okamoto, Keisuke Miyazawa, Ryugo Tero, Yasuhiro Kakimoto, and Takeshi Fukuma

Subjects

0301 basic medicine, Morphology (linguistics), Polymers, Lipid Bilayers, macromolecular substances, 02 engineering and technology, Polyethylene glycol, Microscopy, Atomic Force, 03 medical and health sciences, chemistry.chemical_compound, PEG ratio, Microscopy, Electrochemistry, Fluorescence microscope, General Materials Science, Lipid bilayer, Spectroscopy, Chemistry, technology, industry, and agriculture, Fluorescence recovery after photobleaching, Surfaces and Interfaces, 021001 nanoscience & nanotechnology, Condensed Matter Physics, Lipids, 030104 developmental biology, Membrane, Microscopy, Fluorescence, Biophysics, lipids (amino acids, peptides, and proteins), 0210 nano-technology, Hydrophobic and Hydrophilic Interactions

Abstract

Lipid molecules such as glycolipids that are modified with hydrophilic biopolymers participate in the biochemical reactions occurring on cell membranes. Their functions and efficiency are determined by the formation of microdomains and their physical properties. We investigated the morphology and properties of domains induced by the hydrophilic-polymer-modified lipid applying a polyethylene glycol (PEG)-modified lipid as a model modified lipid. We formed supported lipid bilayers (SLBs) using a 0–10 mol % range of PEG-modified lipid concentration (CPEG). We studied their morphology and fluidity by fluorescence microscopy, the fluorescence recovery after photobleaching method, and atomic force microscopy (AFM). Fluorescence images showed that domains rich in the PEG-modified lipid appeared and SLB fluidity decreased when CPEG ≥ 5%. AFM topographies showed that clusters of the PEG-modified lipid appeared prior to domain formation and the PEG-lipid-rich domains were observed as depressions. Frequency-modulati...

Published

2018

43. Quasi-solid-state self-assembly of 1D-branched ZnSe/ZnS quantum rods into parallel monorail-like continuous films for solar devices

Author

Paras N. Prasad, Shaobin Wang, Qiang Sun, Yongsheng Gao, Guohua Jia, Keisuke Miyazawa, Huayang Zhang, Guosheng Shao, Takeshi Fukuma, Qin Li, Dechao Chen, Ryohei Kojima, Dongyuan Zhao, Lei Yang, Peng Zhang, Colin L. Raston, and Nam-Trung Nguyen

Subjects

Photocurrent, Nanostructure, Materials science, Renewable Energy, Sustainability and the Environment, business.industry, Heterojunction, 02 engineering and technology, Photoelectric effect, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, 0104 chemical sciences, Nanomaterials, Optoelectronics, General Materials Science, Charge carrier, Self-assembly, Electrical and Electronic Engineering, 0210 nano-technology, business, Quasi-solid

Abstract

Translating the extraordinary optoelectric properties of colloidal quantum rods (QRs) into functional devices requires multiscale structural control to preserve the nanoscale attributes as well as to introduce micro- and macroscale interactions between the building blocks. Self-assembly of anisotropic QRs into ordered nanostructures can tailor the photoelectric properties of the QRs, such as in light absorption, and charge separation and transfer. However, it remains a challenge to assemble anisotropic nanomaterial into centimeter-sized, multilayered continuous films that retain nanoscale properties in the fabricated macroscopic devices. We have developed a quasi-solid-state self-assembly of randomly oriented nanostructures for overcoming this challenge, demonstrated by the re-assembly of randomly packed ZnSe/ZnS QRs into aligned and ordered parallel monorails (PMs). These ZnSe/ZnS PMs show significant enhancement in photo-excited charge transport, boosting photocatalytic oxygen evolution rates and the enhancement of photoelectrochemical activities, with a photocurrent density of 18 μA/cm2, 5 times higher than the parent random packing of ZnSe/ZnS QRs. The ZnSe/ZnS PMs enrich the p-n heterojunctions, which can modulate charge carrier separation and transport at the interfaces. The new method has applicability for re-assembling randomly packed films of anisotropic nanoparticles into ordered nanostructures. Importantly, the extraordinary photoelectro-energy conversion behavior of the Type-I core/shell quantum materials illuminates the pathways for novel designed materials by tailoring the hierarchical structures at all scales.

Published

2021

44. The cyclin-dependent kinase 4/6 inhibitor, abemaciclib, exerts dose-dependent cytostatic and cytocidal effects and induces autophagy in multiple myeloma cells

Author

Masami Takei, Yoshihiro Hatta, Shota Moriya, Keisuke Miyazawa, Masaki Hiramoto, Hirotsugu Hino, and Noriyoshi Iriyama

Subjects

0301 basic medicine, Cancer Research, Programmed cell death, Aminopyridines, Apoptosis, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Autophagy, medicine, Humans, Protein Kinase Inhibitors, Multiple myeloma, Cell Proliferation, Cyclin, biology, Cell growth, Cyclin-dependent kinase 4, Kinase, Cell Cycle, Cyclin-Dependent Kinase 4, Cyclin-Dependent Kinase 6, Hematology, medicine.disease, Cell biology, 030104 developmental biology, Oncology, Cell culture, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Benzimidazoles, Multiple Myeloma

Abstract

The D-type cyclin (CCND)-cyclin-dependent kinase 4/6 (CDK4/6) complex has been implicated in multiple myeloma development. We investigated the biological activity of CDK4/6 inhibitor abemaciclib on cell growth and survival in three myeloma cell lines, KMS-12-PE, RPMI 8226, and IM-9. Abemaciclib inhibited myeloma cell growth in a dose-dependent manner in all cell lines, with significant differences seen at a concentration of 320 nM. Treatment with 1 μM abemaciclib increased the fraction of cells in the G0/G1 phase and decreased the fraction in the S-G2/M phases. Further, treatment with abemaciclib at a concentration of 3.2 μM or more showed apparent cytocidal activity accompanied with cytoplasmic vacuolization against myeloma cells. Importantly, abemaciclib induced autophagy in a dose-dependent manner in all three cell lines. These results indicate that the CCND-CDK4/6 complex is closely tied to myeloma cell growth and survival.

Published

2017

45. Dissolution Processes at Step Edges of Calcite in Water Investigated by High-Speed Frequency Modulation Atomic Force Microscopy and Simulation

Author

Peter Spijker, Ville Haapasilta, Katsuo Tsukamoto, Kazuki Miyata, Keisuke Miyazawa, Yuta Kawagoe, Adam S. Foster, Takeshi Fukuma, John Tracey, Kanazawa University, Department of Applied Physics, Tohoku University, Aalto-yliopisto, and Aalto University

Subjects

Analytical chemistry, Bioengineering, Crystal growth, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Atomic force microscopy, chemistry.chemical_compound, Monolayer, Microscopy, General Materials Science, Dissolution, Nanoscopic scale, Calcite, ta114, high-speed atomic-resolution imaging, Mechanical Engineering, General Chemistry, 021001 nanoscience & nanotechnology, Condensed Matter Physics, 0104 chemical sciences, Interferometry, chemistry, Chemical physics, Nanometre, 0210 nano-technology, calcite, crystal dissolution process

Abstract

金沢大学ナノ生命科学研究所, The microscopic understanding of the crystal growth and dissolution processes have been greatly advanced by the direct imaging of nanoscale step flows by atomic force microscopy (AFM), optical interferometry, and X-ray microscopy. However, one of the most fundamental events that govern their kinetics, namely, atomistic events at the step edges, have not been well understood. In this study, we have developed high-speed frequency modulation AFM (FM-AFM) and enabled true atomic-resolution imaging in liquid at ∼1 s/frame, which is ∼50 times faster than the conventional FM-AFM. With the developed AFM, we have directly imaged subnanometer-scale surface structures around the moving step edges of calcite during its dissolution in water. The obtained images reveal that the transition region with typical width of a few nanometers is formed along the step edges. Building upon insight in previous studies, our simulations suggest that the transition region is most likely to be a Ca(OH)2 monolayer formed as an intermediate state in the dissolution process. On the basis of this finding, we improve our understanding of the atomistic dissolution model of calcite in water. These results open up a wide range of future applications of the high-speed FM-AFM to the studies on various dynamic processes at solid-liquid interfaces with true atomic resolution. © 2017 American Chemical Society., Embargo Period 12 months

Published

2017

46. Abemaciclib induces atypical cell death in cancer cells characterized by formation of cytoplasmic vacuoles derived from lysosomes

Author

Hiroko Kokuba, Naoharu Takano, Shin Aizawa, Hirotsugu Hino, Keisuke Miyazawa, Noriyoshi Iriyama, Shota Moriya, Masaki Hiramoto, and Hiromi Kazama

Subjects

0301 basic medicine, Cancer Research, Programmed cell death, Necroptosis, Aminopyridines, Antineoplastic Agents, Vacuole, abemaciclib, V‐ATPase, CDK4/6 inhibitor, vacuole formation, 03 medical and health sciences, 0302 clinical medicine, Lysosome, Cell Line, Tumor, Organelle, medicine, Humans, Protein Kinase Inhibitors, Cell Proliferation, Cell Death, Chemistry, Pinocytosis, General Medicine, Original Articles, Cell cycle, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Drug Discovery and Delivery, Oncology, Cytoplasm, 030220 oncology & carcinogenesis, Vacuoles, lysosome, Benzimidazoles, Original Article, Lysosomes

Abstract

In the cell cycle, the G1/S transition is controlled by the cyclin‐dependent kinase (CDK) 4/6‐cyclin D complex. Constitutive activation of CDK4/6 dysregulates G1/S transition, leading to oncogenic transformation. We found that 3 CDK4/6 inhibitors, abemaciclib, ribociclib, and palbociclib, exerted a cytocidal effect as well as a cytostatic effect at the G1 phase in cancer cell lines, including A549 human non–small cell lung cancer cells. Among these inhibitors, abemaciclib exhibited the most potent cytotoxic effect. The cell‐death phenotype induced by abemaciclib, which entailed formation of multiple cytoplasmic vacuoles, was not consistent with apoptosis or necroptosis. Abemaciclib blocked autophagic flux, resulting in accumulation of autophagosomes, however vacuole formation and cell death induced by abemaciclib were independent of autophagy. In addition, methuosis, a cell‐death phenotype characterized by vacuole formation induced by excessive macropinocytosis, was excluded because the vacuoles did not incorporate fluorescent dextran. Of note, both formation of vacuoles and induction of cell death in response to abemaciclib were inhibited by vacuolar‐type ATPase (V‐ATPase) inhibitors such as bafilomycin A1 and concanamycin A. Live‐cell imaging revealed that the abemaciclib‐induced vacuoles were derived from lysosomes that expanded following acidification. Transmission electron microscopy revealed that these vacuoles contained undigested debris and remnants of organelles. Cycloheximide chase assay revealed that lysosomal turnover was blocked by abemaciclib. Furthermore, mTORC1 inhibition along with partial lysosomal membrane permeabilization occurred after abemaciclib treatment. Together, these results indicate that, in cancer cells, abemaciclib induces a unique form of cell death accompanied by swollen and dysfunctional lysosomes., We found that abemaciclib, a CDK4/6 inhibitor, exerted a potent cytocidal effect in cancer cell lines with an atypical cell death phenotype, which entailed formation of multiple cytoplasmic vacuoles, and both the formation of vacuoles and the induction of cell death were inhibited by V‐ATPase inhibitors. Precise live‐cell imaging and transmission electron microscopy revealed that these vacuoles were derived from lysosomes that expanded following acidification and contained undigested debris and remnants of organelles. Thus we here propose a unique form of cell death accompanied by swollen and dysfunctional lysosomes by abemaciclib treatment.

Published

2019

47. High-Resolution Electrochemical Mapping of the Hydrogen Evolution Reaction on Transition-Metal Dichalcogenide Nanosheets

Author

Yoshikazu Ito, Tomokazu Matsue, Takeshi Fujita, Yu Kobayashi, Keisuke Miyazawa, Hitoshi Shiku, Hiroki Ida, Mingwei Chen, Akichika Kumatani, Masato S. Ota, Ziqian Wang, Yasufumi Takahashi, Yuri E. Korchev, Takeshi Fukuma, and Yasumitsu Miyata

Subjects

Materials science, 010405 organic chemistry, Resolution (electron density), Heterojunction, General Chemistry, 010402 general chemistry, Electrochemistry, 01 natural sciences, Catalysis, 0104 chemical sciences, Electrochemical cell, law.invention, Chemical engineering, Optical microscope, law, Microscopy, Nanoscopic scale, Nanosheet

Abstract

High-resolution scanning electrochemical cell microscopy (SECCM) is used to image and quantitatively analyze the hydrogen evolution reaction (HER) catalytically active sites of 1H-MoS2 nanosheets, MoS2 , and WS2 heteronanosheets. Using a 20 nm radius nanopipette and hopping mode scanning, the resolution of SECCM was beyond the optical microscopy limit and visualized a small triangular MoS2 nanosheet with a side length of ca. 130 nm. The electrochemical cell provides local cyclic voltammograms with a nanoscale spatial resolution for visualizing HER active sites as electrochemical images. The HER activity difference of edge, terrace, and heterojunction of MoS2 and WS2 were revealed. The SECCM imaging directly visualized the relationship of HER activity and number of MoS2 nanosheet layers and unveiled the heterogeneous aging state of MoS2 nanosheets. SECCM can be used for improving local HER activities by producing sulfur vacancies using electrochemical reaction at the selected region.

Published

2019

48. Association of BRCA Mutations and BRCAness Status With Anticancer Drug Sensitivities in Triple-Negative Breast Cancer Cell Lines

Author

Takahiko Kawate, Kana Miyahara, Keisuke Miyazawa, Saeko Teraoka, Naoharu Takano, Takashi Ishikawa, Kimito Yamada, Hiroshi Kaise, and Masako Muguruma

Subjects

endocrine system diseases, Antineoplastic Agents, Triple Negative Breast Neoplasms, Docetaxel, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Cell Line, Tumor, Medicine, Humans, skin and connective tissue diseases, Triple-negative breast cancer, Cisplatin, Gene knockdown, business.industry, BRCA1 Protein, Cancer, medicine.disease, Cell culture, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Mutation, Cancer research, 030211 gastroenterology & hepatology, Surgery, Female, business, Epirubicin, medicine.drug

Abstract

Background Many triple-negative breast cancers (TNBCs) show impaired breast cancer susceptibility gene I (BRCA1) function, called BRCAness. BRCAness tumors may show similar sensitivities to anticancer drugs as tumors with BRCA1 mutations. In this study, we investigated the association of BRCA mutations or BRCAness with drug sensitivities in TNBC. Methods BRCAness was evaluated as BRCA1-like scores, using multiplex ligation-dependent probe amplification in 12 TNBC cell lines, including four with mutations. Sensitivities to docetaxel, cisplatin, and epirubicin were compared with BRCA mutations and BRCA1-like scores. Cisplatin sensitivity was examined in BRCA1 knockdown Michigan Cancer Foundation-7 cell lines. Results Eight and four cell lines had characteristics of BRCAness and non-BRCAness, respectively. The 50% inhibitory concentration of docetaxel was higher in BRCA mutant and BRCAness cell lines than their counterparts. BRCA1-like scores showed a weak positive correlation with docetaxel sensitivity (r = 0.377; P = 0.039). Regarding cisplatin, scores were lower in BRCA mutants and BRCAness tumors than their counterparts. A negative correlation was found between BRCA1-like scores and cisplatin sensitivity (r = −0.407; P = 0.013). No differences were found for epirubicin. BRCA1 gene knockdown increased the cisplatin sensitivity of Michigan Cancer Foundation-7 cells. Conclusions BRCA1-like scores were associated with cisplatin sensitivity and docetaxel resistance. BRCA1-like score is hence a promising indicator for estimating drug sensitivities in TNBC.

Published

2019

49. Vitamin K

Author

Shinsuke, Miyazawa, Shota, Moriya, Hiroko, Kokuba, Hirotsugu, Hino, Naoharu, Takano, and Keisuke, Miyazawa

Subjects

Cell Death, Cell Line, Tumor, Autophagosomes, MCF-7 Cells, Humans, Antineoplastic Agents, Apoptosis, Breast Neoplasms, Female, HL-60 Cells, Vitamin K 2, Reactive Oxygen Species, Transcription Factor CHOP

Abstract

Vitamin KBreast cancer cell lines were cultured with VK2, and the cytotoxicity and cell death phenotype were examined. The HL-60 leukemia cells were used as a control for VK2-induced apoptosis.VK2 exhibited the cytotoxic effect, especially in triple negative breast cancer cell lines, namely, MDA-MB-231 and MDA-MB-468. However, in contrast to HL-60 cells, typical features of the cells undergoing apoptosis, such as chromatin condensation, nuclear fragments, and cleavage of caspase-3 were not detected. Transmission electron microscopy exhibited an increased number of autophagosomes/autolysosomes with plasma membrane integrity. An autophagy inhibitor, 3-methyladenine, apparently attenuated VK2-induced cytotoxicity, which indicated the involvement of autophagy-dependent cell death. Interestingly, both VK2-induced non-apoptotic cell death in MDA-MB-231 cells and VK2-induced apoptosis in HL-60 cells were suppressed in the presence of reactive oxygen species (ROS) scavengers. Therefore, ROS production by VK2 seems to be located up-stream in the molecular machinery for both the types of cell death execution.The VK2 induced non-apoptotic cell death along with autophagy, in triple negative breast cancer cell lines. Cell death phenotype induced by VK2 appears to differ among the type of cancers. This suggests the possibility of using VK2 for the breast cancer therapy.

Published

2019

50. Fingolimod sensitizes EGFR wild‑type non‑small cell lung cancer cells to lapatinib or sorafenib and induces cell cycle arrest

Author

Ayuka Yokota, Kohki Ota, Hiromi Kazama, Shota Moriya, Takashi Okuma, Alberto De Lorenzo, Hirotsugu Hino, Keisuke Miyazawa, Naoharu Takano, and Masaki Hiramoto

Subjects

0301 basic medicine, Sorafenib, Cancer Research, Lung Neoplasms, Cell cycle checkpoint, Cell Survival, Autophagy-Related Proteins, Lapatinib, Receptor tyrosine kinase, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, hemic and lymphatic diseases, medicine, Humans, Epidermal growth factor receptor, Lung cancer, Protein Kinase Inhibitors, Cell Proliferation, biology, Fingolimod Hydrochloride, business.industry, Cell Cycle, Drug Repositioning, Cancer, Drug Synergism, General Medicine, Cell cycle, medicine.disease, respiratory tract diseases, ErbB Receptors, 030104 developmental biology, Oncology, A549 Cells, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, biology.protein, business, medicine.drug

Abstract

Epidermal growth factor receptor (EGFR) is a receptor tyrosine kinase and mutations in this gene are major drivers of lung cancer development. EGFR tyrosine kinase inhibitors (TKIs) are standard first‑line therapies for patients with advanced non‑small cell lung cancer (NSCLC) with activating EGFR mutations, but are not effective in patients with wild‑type EGFR. In the present study, the cytotoxic effects of various TKIs against EGFR were investigated in wild‑type NSCLC cells as single treatments or in combination with Fingolimod (FTY720), which has been approved for treating multiple sclerosis and has cytotoxic effects against several tumor cell lines. It was found that the combined treatment with TKIs lapatinib (Lap) or sorafenib (Sor) and FTY720 synergistically suppressed the viability of the NSCLC cell lines A549 and H596. Additionally, FTY720 inhibited lysosomal acidification and suppressed autophagy flux. Immunoblotting and reverse transcription‑quantitative polymerase chain reaction showed that FTY720 combined with Lap or Sor, enhanced endoplasmic reticulum (ER) stress loading and cell cycle arrest in A549 cells. The enhancement of ER stress loading and cell cycle arrest induced by combined treatment with Lap or Sor and FTY720, which was associated with the cytotoxicity induced by the combination of these drugs. These findings suggested that FTY720 improved TKI therapy in NSCLC patients with wild‑type EGFR, by sensitizing NSCLC cells to TKIs.

Published

2019