Your search keyword '"Hiroyuki Michiue"' showing total 80 results

1. New Anti‐Angiogenic Therapy for Glioblastoma With the Anti‐Depressant Sertraline

Author

Nobushige Tsuboi, Yoshihiro Otani, Atsuhito Uneda, Joji Ishida, Yasuki Suruga, Yuji Matsumoto, Atsushi Fujimura, Kentaro Fujii, Hideki Matsui, Kazuhiko Kurozumi, Isao Date, and Hiroyuki Michiue

Subjects

anti‐angiogenic therapy, antidepressant sertraline, drug repositioning, glioblastoma, tumor derived endothelial cells, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

ABSTRACT Background and Aims Anti‐angiogenic therapies prolong patient survival in some malignancies but not glioblastoma. We focused on the relationship between the differentiation of glioma stem like cells (GSCs) into tumor derived endothelial cells (TDECs) and, anti‐angiogenic therapy resistance. Especially we aimed to elucidate the mechanisms of drug resistance of TDECs to anti‐angiogenic inhibitors and identify novel anti‐angiogenic drugs with clinical applications. Results The mouse GSCs, 005, were differentiated into TDECs under hypoxic conditions, and TDECs had endothelial cell characteristics independent of the vascular endothelial growth factor (VEGF) pathway. In vivo, inhibition of the VEGF pathway had no anti‐tumor effect and increased the percentage of TDECs in the 005 mouse model. Novel anti‐angiogenic drugs for glioblastoma were evaluated using a tube formation assay and a drug repositioning strategy with existing blood–brain barrier permeable drugs. Drug screening revealed that the antidepressant sertraline inhibited tube formation of TDECs. Sertraline was administered to differentiated TDECs in vitro and 005 mouse models in vivo to evaluate genetic changes by RNA‐Seq and tumor regression effects by immunohistochemistry and MRI. Sertraline reduced Lama4 and Ang2 expressions of TDEC, which play an important role in non‐VEGF‐mediated angiogenesis in tumors. The combination of a VEGF receptor inhibitor axitinib, and sertraline improved survival and reduced tumor growth in the 005 mouse model. Conclusion Collectively, our findings showed the diversity of tumor vascular endothelial cells across VEGF and non‐VEGF pathways led to anti‐angiogenic resistance. The combination of axitinib and sertraline can represent an effective anti‐angiogenic therapy for glioblastoma with safe, low cost, and fast availability.

Published

2024

2. ADAR1 is a promising risk stratification biomarker of remnant liver recurrence after hepatic metastasectomy for colorectal cancer

Author

Nanako Hata, Kunitoshi Shigeyasu, Yuzo Umeda, Shuya Yano, Sho Takeda, Kazuhiro Yoshida, Tomokazu Fuji, Ryuichi Yoshida, Kazuya Yasui, Hibiki Umeda, Toshiaki Takahashi, Yoshitaka Kondo, Hiroyuki Kishimoto, Yoshiko Mori, Fuminori Teraishi, Hideki Yamamoto, Hiroyuki Michiue, Keiichiro Nakamura, Hiroshi Tazawa, and Toshiyoshi Fujiwara

Subjects

Medicine, Science

Abstract

Abstract Adenosine-to-inosine RNA editing is a process mediated by adenosine deaminases that act on the RNA (ADAR) gene family. It has been discovered recently as an epigenetic modification dysregulated in human cancers. However, the clinical significance of RNA editing in patients with liver metastasis from colorectal cancer (CRC) remains unclear. The current study aimed to systematically and comprehensively investigate the significance of adenosine deaminase acting on RNA 1 (ADAR1) expression status in 83 liver metastatic tissue samples collected from 36 patients with CRC. The ADAR1 expression level was significantly elevated in liver metastatic tissue samples obtained from patients with right-sided, synchronous, or RAS mutant-type CRC. ADAR1-high liver metastasis was significantly correlated with remnant liver recurrence after hepatic metastasectomy. A high ADAR1 expression was a predictive factor of remnant liver recurrence (area under the curve = 0.72). Results showed that the ADAR1 expression level could be a clinically relevant predictive indicator of remnant liver recurrence. Patients with liver metastases who have a high ADAR1 expression requires adjuvant chemotherapy after hepatic metastasectomy.

Published

2023

3. RNA editing facilitates the enhanced production of neoantigens during the simultaneous administration of oxaliplatin and radiotherapy in colorectal cancer

Author

Yasuhiro Komatsu, Kunitoshi Shigeyasu, Shuya Yano, Sho Takeda, Kazutaka Takahashi, Nanako Hata, Hibiki Umeda, Kazuhiro Yoshida, Yoshiko Mori, Kazuya Yasui, Ryuichi Yoshida, Yoshitaka Kondo, Hiroyuki Kishimoto, Fuminori Teraishi, Yuzo Umeda, Shunsuke Kagawa, Hiroyuki Michiue, Hiroshi Tazawa, Ajay Goel, and Toshiyoshi Fujiwara

Subjects

Medicine, Science

Abstract

Abstract Most cases of colorectal cancers (CRCs) are microsatellite stable (MSS), which frequently demonstrate lower response rates to immune checkpoint inhibitors (ICIs). RNA editing produces neoantigens by altering amino acid sequences. In this study, RNA editing was induced artificially by chemoradiation therapy (CRT) to generate neoantigens in MSS CRCs. Altogether, 543 CRC specimens were systematically analyzed, and the expression pattern of ADAR1 was investigated. In vitro and in vivo experiments were also performed. The RNA editing enzyme ADAR1 was upregulated in microsatellite instability–high CRCs, leading to their high affinity for ICIs. Although ADAR1 expression was low in MSS CRC, CRT including oxaliplatin (OX) treatment upregulated RNA editing levels by inducing ADAR1. Immunohistochemistry analyses showed the upregulation of ADAR1 in patients with CRC treated with CAPOX (capecitabine + OX) radiation therapy relative to ADAR1 expression in patients with CRC treated only by surgery (p

Published

2022

4. Combination of Ad-SGE-REIC and bevacizumab modulates glioma progression by suppressing tumor invasion and angiogenesis.

Author

Yasuhiko Hattori, Kazuhiko Kurozumi, Yoshihiro Otani, Atsuhito Uneda, Nobushige Tsuboi, Keigo Makino, Shuichiro Hirano, Kentaro Fujii, Yusuke Tomita, Tetsuo Oka, Yuji Matsumoto, Yosuke Shimazu, Hiroyuki Michiue, Hiromi Kumon, and Isao Date

Subjects

Medicine, Science

Abstract

Reduced expression in immortalized cells/Dickkopf-3 (REIC/Dkk-3) is a tumor suppressor and its overexpression has been shown to exert anti-tumor effects as a therapeutic target gene in many human cancers. Recently, we demonstrated the anti-glioma effects of an adenoviral vector carrying REIC/Dkk-3 with the super gene expression system (Ad-SGE-REIC). Anti-vascular endothelial growth factor treatments such as bevacizumab have demonstrated convincing therapeutic advantage in patients with glioblastoma. However, bevacizumab did not improve overall survival in patients with newly diagnosed glioblastoma. In this study, we examined the effects of Ad-SGE-REIC on glioma treated with bevacizumab. Ad-SGE-REIC treatment resulted in a significant reduction in the number of invasion cells treated with bevacizumab. Western blot analyses revealed the increased expression of several endoplasmic reticulum stress markers in cells treated with both bevacizumab and Ad-SGE-REIC, as well as decreased β-catenin protein levels. In malignant glioma mouse models, overall survival was extended in the combination therapy group. These results suggest that the combination therapy of Ad-SGE-REIC and bevacizumab exerts anti-glioma effects by suppressing the angiogenesis and invasion of tumors. Combined Ad-SGE-REIC and bevacizumab might be a promising strategy for the treatment of malignant glioma.

Published

2022

5. PIK3R1Met326Ile germline mutation correlates with cysteine-rich protein 61 expression and poor prognosis in glioblastoma

Author

Yoshihiro Otani, Joji Ishida, Kazuhiko Kurozumi, Tetsuo Oka, Toshihiko Shimizu, Yusuke Tomita, Yasuhiko Hattori, Atsuhito Uneda, Yuji Matsumoto, Hiroyuki Michiue, Shuta Tomida, Takehiro Matsubara, Tomotsugu Ichikawa, and Isao Date

Subjects

Medicine, Science

Abstract

Abstract Despite therapeutic advances, glioblastoma represents a lethal brain tumor. Recently, research to identify prognostic markers for glioblastoma has intensified. Our previous study demonstrated that median progression-free survival (PFS) and overall survival (OS) of patients with high cysteine-rich protein 61 (CCN1) expression was significantly shorter than that of patients with low CCN1 expression. To understand the molecular mechanisms that regulate CCN1 expression, we examined 147 tumour samples from 80 patients with glioblastoma and 67 patients with lower grade glioma. Next-generation and Sanger sequencing showed that PIK3R1Met326Ile was more frequent in the CCN1 high expression group (10/37 cases, 27.0%) than the CCN1 low expression group (3/38 cases, 7.9%) in glioblastoma. This mutation was also detected in corresponding blood samples. In multivariate analysis, high CCN1 expression and PIK3R1Met326Ile in glioblastoma patients were prognostic factors for OS [HR = 2.488 (1.298–4.769), p = 0.006] and [HR = 2.089 (1.020–4.277), p = 0.0439], respectively. Thus, the PIK3R1Met326Ile germline appears to be correlated with CCN1 expression and poor prognosis in glioblastoma.

Published

2017

6. Cyclin G2 Promotes Hypoxia- Driven Local Invasion of Glioblastoma by Orchestrating Cytoskeletal Dynamics

Author

Atsushi Fujimura, Hiroyuki Michiue, Yan Cheng, Atsuhito Uneda, Yasunari Tani, Tei-ichi Nishiki, Tomotsugu Ichikawa, Fan-Yan Wei, Kazuhito Tomizawa, and Hideki Matsui

Subjects

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

Abstract

Microenvironmental conditions such as hypoxia potentiate the local invasion of malignant tumors including glioblastomas by modulating signal transduction and protein modification, yet the mechanism by which hypoxia controls cytoskeletal dynamics to promote the local invasion is not well defined. Here, we show that cyclin G2 plays pivotal roles in the cytoskeletal dynamics in hypoxia-driven invasion by glioblastoma cells. Cyclin G2 is a hypoxia-induced and cytoskeleton-associated protein and is required for glioblastoma expansion. Mechanistically, cyclin G2 recruits cortactin to the juxtamembrane through its SH3 domain-binding motif and consequently promotes the restricted tyrosine phosphorylation of cortactin in concert with src. Moreover, cyclin G2 interacts with filamentous actin to facilitate the formation of membrane ruffles. In primary glioblastoma, cyclin G2 is abundantly expressed in severely hypoxic regions such as pseudopalisades, which consist of actively migrating glioma cells. Furthermore, we show the effectiveness of dasatinib against hypoxia-driven, cyclin G2-involved invasion in vitro and in vivo. Our findings elucidate the mechanism of cytoskeletal regulation by which severe hypoxia promotes the local invasion and may provide a therapeutic target in glioblastoma.

Published

2013

7. CACNA1A variants may modify the epileptic phenotype of Dravet syndrome

Author

Iori Ohmori, Mamoru Ouchida, Katsuhiro Kobayashi, Yoshimi Jitsumori, Akiko Mori, Hiroyuki Michiue, Teiichi Nishiki, Yoko Ohtsuka, and Hideki Matsui

Subjects

CACNA1A, Epilepsy, SCN1A, Electrophysiology, Molecular genetics, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Dravet syndrome is an intractable epileptic syndrome beginning in the first year of life. De novo mutations of SCN1A, which encode the Nav1.1 neuronal voltage-gated sodium channel, are considered the major cause of Dravet syndrome. In this study, we investigated genetic modifiers of this syndrome.We performed a mutational analysis of all coding exons of CACNA1A in 48 subjects with Dravet syndrome. To assess the effects of CACNA1A variants on the epileptic phenotypes of Dravet syndrome, we compared clinical features in two genotype groups: 1) subjects harboring SCN1A mutations but no CACNA1A variants (n=20) and 2) subjects with SCN1A mutations plus CACNA1A variants (n=20). CACNA1A variants detected in patients were studied using heterologous expression of recombinant human Cav2.1 in HEK 293 cells and whole-cell patch-clamp recording.Nine CACNA1A variants, including six novel ones, were detected in 21 of the 48 subjects (43.8%). Based on the incidence of variants in healthy controls, most of the variants seemed to be common polymorphisms. However, the subjects harboring SCN1A mutations and CACNA1A variants had absence seizures more frequently than the patients with only SCN1A mutations (8/20 vs. 0/20, p=0.002). Moreover, the former group of subjects exhibited earlier onset of seizures and more frequent prolonged seizures before one year of age, compared to the latter group of subjects. The electrophysiological properties of four of the five novel Cav2.1 variants exhibited biophysical changes consistent with gain-of-function. We conclude that CACNA1A variants in some persons with Dravet syndrome may modify the epileptic phenotypes.

Published

2013

8. Theranostic protein targeting ErbB2 for bioluminescence imaging and therapy for cancer.

Author

Xiao-Jian Han, Ling-Fei Sun, Yuki Nishiyama, Bin Feng, Hiroyuki Michiue, Masaharu Seno, Hideki Matsui, and Kazuhito Tomizawa

Subjects

Medicine, Science

Abstract

A combination of molecular-targeted cancer imaging and therapy is an emerging strategy to improve cancer diagnosis and minimize the side effects of conventional treatments. Here, we generated a recombinant protein, EC1-GLuc-p53C, by fusing EC1 peptide, an artificial ligand of ErbB2, with Gaussia luciferase (GLuc) and a p53-activating peptide, p53C. EC1-GLuc-p53C was expressed and purified from E. coli BL21. In vitro experiments showed that EC1-GLuc-p53c was stable in luminescent activity and selectively targeted ErbB2-overexpressing BT474 cells for bioluminescence imaging. Moreover, the internalized EC1-GLuc-p53C in BT474 cells exerted its function to reactivate p53 and significantly inhibited cellular proliferation. In tumor-bearing mice, the ErbB2-targeted bioluminescence imaging and therapeutic effect of EC1-GLuc-p53C were also observed specifically in BT474 tumors but not in MCF7 tumors, which does not overexpress ErbB2. Thus, the present study demonstrates EC1-GLuc-p53C to be an effective theranostic reagent targeting ErbB2 for bioluminescence imaging and cancer therapy.

Published

2013

9. Expression of a constitutively active calcineurin encoded by an intron-retaining mRNA in follicular keratinocytes.

Author

Atsushi Fujimura, Hiroyuki Michiue, Tei-ichi Nishiki, Iori Ohmori, Fan-Yan Wei, Hideki Matsui, and Kazuhito Tomizawa

Subjects

Medicine, Science

Abstract

Hair growth is a highly regulated cyclical process. Immunosuppressive immunophilin ligands such as cyclosporin A (CsA) and FK506 are known as potent hair growth modulatory agents in rodents and humans that induce active hair growth and inhibit hair follicle regression. The immunosuppressive effectiveness of these drugs has been generally attributed to inhibition of T cell activation through well-characterized pathways. Specifically, CsA and FK506 bind to intracellular proteins, principally cyclophilin A and FKBP12, respectively, and thereby inhibit the phosphatase calcineurin (Cn). The calcineurin (Cn)/NFAT pathway has an important, but poorly understood, role in the regulation of hair follicle development. Here we show that a novel-splicing variant of calcineurin Aß CnAß-FK, which is encoded by an intron-retaining mRNA and is deficient in the autoinhibitory domain, is predominantly expressed in mature follicular keratinocytes but not in the proliferating keratinocytes of rodents. CnAß-FK was weakly sensitive to Ca(2+) and dephosphorylated NFATc2 under low Ca(2+) levels in keratinocytes. Inhibition of Cn/NFAT induced hair growth in nude mice. Cyclin G2 was identified as a novel target of the Cn/NFATc2 pathway and its expression in follicular keratinocytes was reduced by inhibition of Cn/NFAT. Overexpression of cyclin G2 arrested the cell cycle in follicular keratinocytes in vitro and the Cn inhibitor, cyclosporin A, inhibited nuclear localization of NFATc2, resulting in decreased cyclin G2 expression in follicular keratinocytes of rats in vivo. We therefore suggest that the calcineurin/NFAT pathway has a unique regulatory role in hair follicle development.

Published

2011

10. Particle and Heavy Ion Transport Code System‐Based Microdosimetry for the Development of Boron Agents for Boron Neutron Capture Therapy

Author

Takafumi Shigehira, Tadashi Hanafusa, Kazuyo Igawa, Tomonari Kasai, Shuichi Furuya, Hisakazu Nishimori, Yoshinobu Maeda, Hiroyuki Michiue, and Atsushi Fujimura

Subjects

Statistics and Probability, Numerical Analysis, Multidisciplinary, boron agents, boron neutron capture therapy, Modeling and Simulation, simulation study

Abstract

Boron neutron capture therapy (BNCT) is a radiation therapy that selectively kills cancer cells at the cellular level using the boron neutron capture reaction (BNCR) (10B(n.α)7Li). The amount of boron 10B delivers in boronophenylalanine (BPA)-BNCT to achieve anti-tumor effects is ≈15–40 ppm. The same is true for all boron drugs; however, whether the same amount of 10B is required for other boron drugs with different accumulation characteristics has not been intensively investigated. Therefore, herein, a virtual cell model with intracellular organelles is prepared, and the BPA equivalent dose concentration to the cell nucleus is analyzed using particle and heavy ion transport code system-based microdosimetry. Additionally, the intranuclear minimal region (IMR) is set as a reference for the concept of the intranuclear domain in the microdosimetric kinetic model, and the BPA equivalent dose concentration to the IMR is estimated. The required boron delivery dose greatly varies depending on the dose assessment based on the accumulation characteristics of boron agents in intracellular organelles. Evaluation of the BNCR effect according to the accumulation characteristics without being influenced by the specified value of 15–40 ppm is recommended.

Published

2023

11. Regulatory T cells induce a suppressive immune milieu and promote lymph node metastasis in intrahepatic cholangiocarcinoma

Author

Daisuke Konishi, Yuzo Umeda, Kazuhiro Yoshida, Kunitoshi Shigeyasu, Shuya Yano, Tomohiro Toji, Sho Takeda, Ryuichi Yoshida, Kazuya Yasui, Tomokazu Fuji, Kazuyuki Matsumoto, Hiroyuki Kishimoto, Hiroyuki Michiue, Fuminori Teraishi, Hironari Kato, Hiroshi Tazawa, Hiroyuki Yanai, Takahito Yagi, Ajay Goel, and Toshiyoshi Fujiwara

Subjects

Cholangiocarcinoma, Cancer Research, Bile Ducts, Intrahepatic, Lymphocytes, Tumor-Infiltrating, Bile Duct Neoplasms, Oncology, Lymphatic Metastasis, Humans, Forkhead Transcription Factors, Prognosis, T-Lymphocytes, Regulatory

Abstract

Background Emerging evidence indicates that immunogenicity plays an important role in intrahepatic cholangiocarcinoma (ICC). Herein, we systematically evaluated the clinical relevance of immunogenicity in ICC. Methods Highly immunogenic ICCs identified in the public dataset and the Cancer Immunome Atlas (TCIA) were assessed to determine the prognostic impact of immunogenicity in ICC and key components after curative resection. We also investigated the clinical relevance of the immune milieu in ICC. Results Using the Gene Expression Omnibus dataset 89749 and TCIA, we identified CD8+/forkhead box P3 (FoxP3)+ tumour-infiltrating lymphocytes (TILs), T-cell immunoglobulin and mucin domain 3 (TIM-3) and human leukocyte antigen-A (HLA-A) in highly immunogenic ICCs. Immunohistochemical analysis of the in-house cohort showed that intratumoral FoxP3+ TILs correlated with CD8+ TILs (P = 0.045, Fisher’s exact test) and that high FoxP3+/CD8+ ratio (FCR) was an important marker for poor survival (P P = 0.003, Mann–Whitney U test). Conclusions FCR should be considered an important biomarker that represents the immune environment of ICC based on its potentially important role in tumour progression, especially lymph node metastasis.

Published

2022

12. RNA editing is a valuable biomarker for predicting carcinogenesis in ulcerative colitis

Author

Kazutaka Takahashi, Kunitoshi Shigeyasu, Yoshitaka Kondo, Kazuyoshi Gotoh, Shuya Yano, Yuzo Umeda, Toshihiro Inokuchi, Caiming Xu, Kazuhiro Yoshida, Hibiki Umeda, Toshiaki Takahashi, Sho Takeda, Ryuichi Yoshida, Fuminori Teraishi, Hiroyuki Kishimoto, Yoshiko Mori, Kazuhiro Noma, Yoshinaga Okugawa, Sakiko Hiraoka, Hiroyuki Michiue, Hiroshi Tazawa, Osamu Matsushita, Ajay Goel, and Toshiyoshi Fujiwara

Subjects

Gastroenterology, General Medicine

Abstract

Background and Aims Ulcerative colitis [UC] can lead to colitis-associated colorectal neoplasm [CAN]. Adenosine-to-inosine RNA editing, which is regulated by adenosine deaminase acting on RNA [ADAR], induces the post-transcriptional modification of critical oncogenes, including antizyme inhibitor 1 [AZIN1], leading to colorectal carcinogenesis. Therefore, we hypothesized that ADAR1 might be involved in the development of CAN in UC. Methods We systematically analysed a cohort of 139 UC cases [40 acute phase, 73 remission phase, 26 CAN]. The degree of inflammation was evaluated using the Mayo endoscopic score [MES]. Results The type 1 interferon [IFN]-related inflammation pathway was upregulated in the rectum of active UC, rectum of UC-CAN and tumour site of UC-CAN patients. ADAR1 expression was upregulated in the entire colon of CAN cases, while it was downregulated in non-CAN MES0 cases. ADAR1 expression in the rectum predicted the development of CAN better than p53 or β-catenin, with an area under the curve of 0.93. The high expression of ADAR1 and high AZIN1 RNA editing in UC was triggered by type 1 IFN stimulation from UC-specific microbiomes, such as seen in Fusobacterium in vitro analyses. The induction of AZIN1 RNA editing by ADAR1, whose expression is promoted by Fusobacterium, may induce carcinogenesis in UC. Conclusions The risk of CAN can be evaluated by assessing ADAR1 expression in the rectum of MES0 UC patients, freeing UC patients from unnecessary colonoscopy and reducing their physical burden. RNA editing may be involved in UC carcinogenesis, and may be used to facilitate the prevention and treatment of CAN in UC.

Published

2022

13. Reaction of Chloroacetyl-Modified Peptides with Mercaptoundecahydrododecaborate (BSH) Is Accelerated by Basic Amino Acid Residues in the Peptide

Author

Mizuki Kitamatsu, Ken Inoue, Naoki Yamagata, and Hiroyuki Michiue

Subjects

BSH, peptide, boron neutron capture therapy (BNCT), Process Chemistry and Technology, Chemical Engineering (miscellaneous), Bioengineering

Abstract

We assessed a reactivity of chloroacetyl-modified tripeptides consisting of various amino acid residues (Cl-3X) and mercaptoundecahydrododecaborate (BSH) by converting Cl-3X to its reactant (BS-3X). We showed that the Cl-3X consisting of basic amino acid residues (e.g., Arg) reacted with BSH effectively and its conversion decreased as the number of Arg residues in the Cl-3X decreased. Furthermore, a reactivity of the peptides with introduction of an alkyl linker between the triarginine and the chloroacetyl group (Cl-Cn-3R) with BSH decreased with increasing alkyl linker length. These results indicate that an electrostatic attraction of positively charged amino acid residues in the tripeptides and negatively charged BSH causes BSH to gather in a vicinity of the chloroacetyl group, resulting in an accelerated reaction. This work should aid a development of new boron agents using BSH in boron neutron capture therapy.

Published

2022

14. Combination of Ad-SGE-REIC and Bevacizumab Modulates Glioma Progression by Suppressing Invasion and Angiogenesis

Author

Atsuhito Uneda, Yuji Matsumoto, Yusuke Tomita, Nobushige Tsuboi, Yasuhiko Hattori, Yoshihiro Otani, Tetsuo Oka, Hiroyuki Michiue, Kazuhiko Kurozumi, Yosuke Shimazu, Kentaro Fujii, Hiromi Kumon, and Isao Date

Subjects

Bevacizumab, Angiogenesis, business.industry, Glioma, medicine, Cancer research, medicine.disease, business, medicine.drug

Abstract

Reduced expression in immortalized cells/Dickkopf-3 (REIC/Dkk-3) is a tumor suppressor and its overexpression has been shown to exert anti-tumor effects as a therapeutic target gene in many human cancers. Recently, we demonstrated the anti-glioma effects of an adenoviral vector carrying REIC/Dkk-3 with the super gene expression system (Ad-SGE-REIC). Anti-vascular endothelial growth factor treatments such as bevacizumab have demonstrated convincing therapeutic advantage in patients with glioblastoma. However, bevacizumab could not improve overall survival in patients with newly diagnosed glioblastoma. In this study, we examined the effects of Ad-SGE-REIC on glioma treated with bevacizumab. Treatment of Ad-SGE-REIC resulted in significant reduced numbers of invasion cells treated with bevacizumab.. Western blot analyses revealed increased expression of several endoplasmic reticulum stress markers in cells treated with both bevacizumab and Ad-SGE-REIC and decreased β-catenin protein levels. Expressions of apoptosis markers were also increased in cells with combination therapy. In malignant glioma mouse models, overall survival was extended in the combination therapy group. These results suggest that the combination therapy of Ad-SGE-REIC and bevacizumab exerts anti-glioma effects by suppressing angiogenesis and invasion of tumors. Combined Ad-SGE-REIC and bevacizumab might indicate a promising strategy for the treatment of malignant glioma.

Published

2021

15. Improvement of Water Solubility of Mercaptoundecahydrododecaborate (BSH)-Peptides by Conjugating with Ethylene Glycol Linker and Interaction with Cyclodextrin

Author

Mizuki Kitamatsu, Hiroyuki Michiue, Yoshimichi Ishikawa, and Ayaka Nakamura-Tachibana

Subjects

inorganic chemicals, Bioengineering, Peptide, ethylene glycol, BSH, Conjugated system, 010402 general chemistry, lcsh:Chemical technology, 01 natural sciences, lcsh:Chemistry, chemistry.chemical_compound, Chemical Engineering (miscellaneous), lcsh:TP1-1185, Solubility, chemistry.chemical_classification, Aqueous solution, Cyclodextrin, 010405 organic chemistry, Process Chemistry and Technology, Combinatorial chemistry, 0104 chemical sciences, chemistry, lcsh:QD1-999, cyclodextrin, Ethylene glycol, Linker, cell-penetrating peptide, Conjugate

Abstract

We previously developed a conjugate consisting of 10B cluster BSH and tri-arginine peptide (BSH-3R). This could potentially be used as a boron agent for boron neutron capture therapy, however, it possesses poor water solubility and thus needs to be improved for use as medicine. In this study, we devised several means of improving the water solubility of BSH-3R. As one of them, we used cyclodextrin (CD), which was expected to improve the water solubility resulting from interaction of the BSH-3R with CD. We evaluated the solubility of BSH-3R in aqueous CD solution by using reverse-phase high-performance liquid chromatography. As we expected, the solubility of BSH-3R was increased in a manner dependent on the addition of &beta, CD and &gamma, CD in aqueous solution. Furthermore, we synthesized BSH conjugated to oligoarginine having various chain lengths (BSH-nR) and BSH-3R with ethylene glycol linkers introduced between BSH and 3R (BSH-nEg-3R). The water solubility of these BSH peptides was also evaluated and the results showed that the introduction of nEg to BSH-3R markedly improved the water solubility. Furthermore, we found that the water solubility of these peptides can be further improved by also applying CD.

Published

2021

16. Fibroblast growth factor 13 regulates glioma cell invasion and is important for bevacizumab-induced glioma invasion

Author

Joji Ishida, Atsuhito Uneda, Yoshihiro Otani, Tomotsugu Ichikawa, Yuji Matsumoto, Yasuhiko Hattori, Hiroyuki Michiue, Tetsuo Oka, Toshihiko Shimizu, Kazuhiko Kurozumi, Yousuke Tomita, Satoshi Inoue, and Isao Date

Subjects

0301 basic medicine, Cancer Research, Angiogenesis, Cell, Apoptosis, Mice, SCID, Biology, Fibroblast growth factor, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Glioma, Biomarkers, Tumor, Tumor Cells, Cultured, Genetics, medicine, Animals, Humans, Neoplasm Invasiveness, neoplasms, Molecular Biology, Cell Proliferation, Brain Neoplasms, Cell growth, Prognosis, medicine.disease, Xenograft Model Antitumor Assays, nervous system diseases, Bevacizumab, Fibroblast Growth Factors, Gene Expression Regulation, Neoplastic, 030104 developmental biology, medicine.anatomical_structure, Cell culture, 030220 oncology & carcinogenesis, Neoplastic Stem Cells, Cancer research, Female, Stem cell, Glioblastoma, Intracellular, Follow-Up Studies

Abstract

Glioblastoma has the poorest prognosis, and is characterized by excessive invasion and angiogenesis. To determine the invasive mechanisms, we previously used two glioma cell lines (J3T-1 and J3T-2) with different invasive phenotypes. The J3T-1 showed abundant angiogenesis and tumor cell invasion around neovasculature, while J3T-2 showed diffuse cell infiltration into surrounding healthy parenchyma. Microarray analyses were used to identify invasion-related genes in J3T-2 cells, and the expressed genes and their intracellular and intratumoral distribution patterns were evaluated in J3T-2 cell lines, human glioma cell lines, human glioblastoma stem cells and human glioblastoma specimens. To determine the role of the invasion-related genes, invasive activities were evaluated in vitro and in vivo. Fibroblast growth factor 13 (FGF13) was overexpressed in J3T-2 cells compared to J3T-1 cells, and in human glioma cell lines, human glioblastoma stem cells and human glioblastoma specimens, when compared to that of normal human astrocytes. Immunohistochemical staining and the RNA-seq (sequencing) data from the IVY Glioblastoma Atlas Project showed FGF13 expression in glioma cells in the invasive edges of tumor specimens. Also, the intracellular distribution was mainly in the cytoplasm of tumor cells and colocalized with tubulin. Overexpression of FGF13 stabilized tubulin dynamics in vitro and knockdown of FGF13 decreased glioma invasion both in vitro and in vivo and prolonged overall survival of several xenograft models. FGF13 was negatively regulated by hypoxic condition. Silencing of FGF13 also decreased in vivo bevacizumab-induced glioma invasion. In conclusion, FGF13 regulated glioma cell invasion and bevacizumab-induced glioma invasion, and could be a novel target for glioma treatment.

Published

2017

17. DDIS-01. NEW DRUG DISCOVERY WITH DRUG RE-POSITIONING SYSTEM TOWARD GBM TREATMENT

Author

Hiroyuki Michiue, Keiichiro Hayashi, Kazuhiko Kurozumi, Nobushige Tsuboi, and Hideki Matsui

Subjects

Drug, Oncology, Cancer Research, medicine.medical_specialty, Positioning system, Drug discovery, business.industry, media_common.quotation_subject, Tumor Cell Invasion, medicine.disease, Drug development, Internal medicine, Drug Discovery, medicine, Neurology (clinical), business, Drug toxicity, media_common, Glioblastoma, Mice nude

Abstract

INTRODUCTION Invasion of Glioblastoma (GBM) cells into normal brain is the major cause of poor prognosis and requires dynamic reorganization of the actin cytoskeleton, which includes lamellipodial protrusions, focal adhesions, and stress fibers at the leading edge of GBM cells. Therefore, we hypothesized that the inhibition of actin polymerization with existing medication could lead to clinical GBM treatment directly in short time. The Drug Repositioning system is also known as drug repurposing or drug reprofiling and understood as the process of redeveloping a compound for use in a different disease. In this time, we would show the new direction of drug development with drug repositioning. MATERIALS AND METHODS We adopted a drug repositioning system for screening with a pyrene-actin-based actin polymerization assay and identified fluvoxamine, a clinically used antidepressant. Fluvoxamine, selective serotonin reuptake inhibitor, was a potent inhibitor of actin polymerization and confirmed as drug penetration through the blood–brain barrier (BBB) and accumulation of whole brain including brain tumor with no drug toxicity. RESULTS Fluvoxamine inhibited serum-induced ruffle formation, cell migration, and invasion of human GBM and glioma stem cells in vitro by suppressing FAK signaling. Fluvoxamine showed no drug toxicity. Daily treatment of athymic mice bearing human glioma-initiating cells with fluvoxamine blocked tumor cell invasion and prolonged the survival with almost same doze of anti-depressant effect. CONCLUSIONS The SSRI group has big potential for clinical GBM treatment with low cost, short time and low side effect.

Published

2019

18. ATIM-21. THE CURRENT STATUS OF AD-SGE-REIC GENE THERAPY FOR MALIGNANT GLIOMA

Author

Yasuhiko Hattori, Nobushige Tsuboi, Yusuke Tomita, Kentaro Fujii, Isao Date, Keigo Makino, Hiroyuki Michiue, Yosuke Shimazu, Yuji Matsumoto, Tetsuo Oka, Kazuhiko Kurozumi, Atsuhito Uneda, Hiromi Kumorn, and Keisuke Kaneda

Subjects

Cancer Research, Genetic enhancement, Adult Clinical Trials–Immunologic, Biology, medicine.disease, Viral vector, Oncology, Glioma, Gene expression, Cancer research, medicine, Neurology (clinical), Immortalised cell line, Gene, Human cancer

Abstract

INTRODUCTION Expression of the gene encoding reduced expression in immortalized cells/Dickkopf-3 (REIC/Dkk-3) was reported to be reduced in a variety of human cancer cells. We previously examined the antitumor effect of an adenoviral vector carrying REIC/Dkk-3 gene (Ad-CAG-REIC). Recently, a novel adenoviral vector expressing REIC/Dkk-3 has also been developed based on the cytomegalovirus promoter-driven super gene expression system (Ad-SGE-REIC). We evaluated the anti-glioma effect of the Ad-SGE-REIC and planned a clinical trial of Ad-SGE-REIC for malignant glioma. MATERIALS AND METHODS We evaluated a cytotoxicity assay to treatments with Ad-SGE-REIC, Ad-CAG-REIC, or Ad-LacZ (control) using malignant glioma cells. The survival of mice in each group was analyzed by the Kaplan–Meier method. We also performed Good Laboratory Practice (GLP) toxicology tests and prepared a protocol for this clinical trial. RESULTS In the cytotoxicity assay, after treatment with Ad-SGE-REIC, the number of malignant glioma cells attached to the bottom of culture wells was significantly reduced in a time-dependent manner. Mice treated with Ad-SGE-REIC survived significantly longer than those treated with other vectors. We also performed GLP toxicology tests using intracranial injection of higher doses of Ad-SGE-REIC in rats at Shin Nippon Biomedical Laboratories (SNBL Japan) to determine the injection dose of Ad-SGE-REIC for this clinical trial. After finishing the consultation with Pharmaceuticals and Medical Devices Agency (PMDA), we prepared a protocol for a phase I/IIa clinical trial of Ad-SGE-REIC for the treatment of recurrent malignant glioma supported by Japan Agency for Medical Research and Development (AMED). This protocol was reviewed by institution review board (IRB) in March 2019. We submitted a notification of this trial in April 2019. CONCLUSIONS We demonstrated the anti-glioma effect of Ad-SGE-REIC. We will start a phase I/IIa clinical trial of Ad-SGE-REIC for the treatment of recurrent malignant glioma.

Published

2019

19. Complementary leucine zippering system for effective intracellular delivery of proteins by cell-penetrating peptides

Author

Takashi Ohtsuki, Hiroyuki Michiue, Hiroki Yuasa, and Mizuki Kitamatsu

Subjects

Leucine zipper, Zipper, Green Fluorescent Proteins, Clinical Biochemistry, Pharmaceutical Science, Peptide, Cell-Penetrating Peptides, 01 natural sciences, Biochemistry, Green fluorescent protein, Mice, Leucine, Drug Discovery, Fluorescence microscope, Animals, Molecular Biology, Cells, Cultured, chemistry.chemical_classification, Leucine Zippers, 010405 organic chemistry, Organic Chemistry, 0104 chemical sciences, Mice, Inbred C57BL, 010404 medicinal & biomolecular chemistry, chemistry, Cell-penetrating peptide, Biophysics, Molecular Medicine, Peptides, Intracellular

Abstract

A heterodimeric leucine zipper composed of a pair of leucine zipper peptides containing acidic or basic amino acid residues at appropriate positions in each peptide was used as a molecular glue to connect protein cargos to a cell-penetrating peptide (CPP) carrier. To investigate the hybridization properties by fluorescence experiments, we prepared an enhanced green fluorescent protein (EGFP) fused with an acidic leucine zipper (LzK), EGFP-LzK, and a basic leucine zipper (LzE) modified with a CPP, LzE-CPP. The LzK and LzE formed a 1:1 hybrid when EGFP-LzK and LzE-CPP were mixed in phosphate buffer saline, thereby conjugating the EGFP with the CPP. The formation of the 1:1 hybrid was confirmed by fluorescence spectra and fluorescence titration curves. Results from fluorescence microscopy experiments showed that EGFP was successfully delivered into cells by conjugating with the CPP via formation of the LzK/LzE hybrid. We also fused the apoptotic protein p53 with LzK (p53-LzK) and investigated the inhibition of cell proliferation of various cell lines by incubation with the p53-LzK/LzE-CPP hybrid. This hybrid was found to localize in nuclei and successfully inhibited cell-specific proliferation. The LzE/LzK zipper system inhibited cell proliferation more efficiently than the directly fused conjugate, p53-CPP. Our method will be a useful drug delivery system for delivering bioactive proteins to treat various diseases.

Published

2021

20. Actin bundling by dynamin 2 and cortactin is implicated in cell migration by stabilizing filopodia in human non-small cell lung carcinoma cells

Author

Tadashi Abe, Tetsuya Takeda, Kohji Takei, Hiroshi Yamada, and Hiroyuki Michiue

Subjects

Dynamins, 0301 basic medicine, Cancer Research, Lung Neoplasms, Podosome, Endocytic cycle, macromolecular substances, Biology, migration, Dynamin II, 03 medical and health sciences, filopodia, Cell Movement, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, dynamin, Humans, Pseudopodia, Dynamin, Cell migration, Articles, cortactin, Actins, Cell biology, 030104 developmental biology, Oncology, Gene Knockdown Techniques, Invadopodia, biology.protein, actin, Filopodia, Cortactin

Abstract

The endocytic protein dynamin participates in the formation of actin-based membrane protrusions such as podosomes, pseudopodia, and invadopodia, which facilitate cancer cell migration, invasion, and metastasis. However, the role of dynamin in the formation of actin-based membrane protrusions at the leading edge of cancer cells is unclear. In this study, we demonstrate that the ubiquitously expressed dynamin 2 isoform facilitates cell migration by stabilizing F-actin bundles in filopodia of the lung cancer cell line H1299. Pharmacological inhibition of dynamin 2 decreased cell migration and filopodial formation. Furthermore, dynamin 2 and cortactin mostly colocalized along F-actin bundles in filopodia of serum-stimulated H1299 cells by immunofluorescent and immunoelectron microscopy. Knockdown of dynamin 2 or cortactin inhibited the formation of filopodia in serum-stimulated H1299 cells, concomitant with a loss of F-actin bundles. Expression of wild-type cortactin rescued the punctate-like localization of dynamin 2 and filopodial formation. The incubation of dynamin 2 and cortactin with F-actin induced the formation of long and thick actin bundles, with these proteins colocalizing at F-actin bundles. A depolymerization assay revealed that dynamin 2 and cortactin increased the stability of F-actin bundles. These results indicate that dynamin 2 and cortactin participate in cell migration by stabilizing F-actin bundles in filopodia. Taken together, these findings suggest that dynamin might be a possible molecular target for anticancer therapy.

Published

2016

21. Detection of γH2AX foci in mouse normal brain and brain tumor after boron neutron capture therapy

Author

Shin-ichiro Masunaga, Hiroki Tanaka, Tsubasa Watanabe, Hiroyuki Michiue, Yosuke Nakagawa, Masaru Narabayashi, Yoshinori Sakurai, Minoru Suzuki, Koji Ono, Natsuko Kondo, and Yuko Kinashi

Subjects

0301 basic medicine, Chemistry, DNA damage, business.industry, Brain tumor, Linear energy transfer, Neutron radiation, medicine.disease, Neutron temperature, Ionizing radiation, 03 medical and health sciences, Neutron capture, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, medicine, Cancer research, Radiology, Nuclear Medicine and imaging, Original Research Article, Irradiation, Nuclear medicine, business

Abstract

Aim In this study, we investigated γH2AX foci as markers of DSBs in normal brain and brain tumor tissue in mouse after BNCT. Background Boron neutron capture therapy (BNCT) is a particle radiation therapy in combination of thermal neutron irradiation and boron compound that specifically accumulates in the tumor. 10 B captures neutrons and produces an alpha ( 4 He) particle and a recoiled lithium nucleus ( 7 Li). These particles have the characteristics of extremely high linear energy transfer (LET) radiation and therefore have marked biological effects. High LET radiation causes severe DNA damage, DNA DSBs. As the high LET radiation induces complex DNA double strand breaks (DSBs), large proportions of DSBs are considered to remain unrepaired in comparison with exposure to sparsely ionizing radiation. Materials and methods We analyzed the number of γH2AX foci by immunohistochemistry 30 min or 24 h after neutron irradiation. Results In both normal brain and brain tumor, γH2AX foci induced by 10 B(n,α) 7 Li reaction remained 24 h after neutron beam irradiation. In contrast, γH2AX foci produced by γ-ray irradiation at contaminated dose in BNCT disappeared 24 h after irradiation in these tissues. Conclusion DSBs produced by 10 B(n,α) 7 Li reaction are supposed to be too complex to repair for cells in normal brain and brain tumor tissue within 24 h. These DSBs would be more difficult to repair than those by γ-ray. Excellent anti-tumor effect of BNCT may result from these unrepaired DSBs induced by 10 B(n,α) 7 Li reaction.

Published

2016

22. Self-assembling A6K peptide nanotubes as a mercaptoundecahydrododecaborate (BSH) delivery system for boron neutron capture t (BNCT)

Author

Natsuko Kondo, Tomonari Kasai, Hiroaki Matsushita, Kazuyo Igawa, Mizuki Kitamatsu, Asami Fukunaga, Shuichi Furuya, Nobushige Tsuboi, Hideki Matsui, Atsushi Fujimura, and Hiroyuki Michiue

Subjects

Boron Compounds, Nanotubes, Peptide, inorganic chemicals, Pharmaceutical Science, chemistry.chemical_element, Boron Neutron Capture Therapy, Peptide, Borohydrides, 02 engineering and technology, Mice, 03 medical and health sciences, Transduction (genetics), Boron drug, Pharmacokinetics, Glioma, medicine, Animals, Humans, Sulfhydryl Compounds, Boron, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Nanotubes, Chemistry, Cell growth, Drug delivery system (DDS), 021001 nanoscience & nanotechnology, medicine.disease, Malignant brain tumor, Peptide nanotube, Boron neutron capture therapy (BNCT), A6K peptide, Drug delivery, Cancer research, 0210 nano-technology, Oligopeptides, Intracellular

Abstract

Boron neutron capture therapy (BNCT) is a tumor selective therapy, the effectiveness of which depends on sufficient 10B delivery to and accumulation in tumors. In this study, we used self-assembling A6K peptide nanotubes as boron carriers and prepared new boron agents by simple mixing of A6K and BSH. BSH has been used to treat malignant glioma patients in clinical trials and its drug safety and availability have been confirmed; however, its contribution to BNCT efficacy is low. A6K nanotube delivery improved two major limitations of BSH, including absence of intracellular transduction and non-specific drug delivery to tumor tissue. Varying the A6K peptide and BSH mixture ratio produced materials with different morphologies-determined by electron microscopy-and intracellular transduction efficiencies. We investigated the A6K/BSH 1:10 mixture ratio and found high intracellular boron uptake with no toxicity. Microscopy observation showed intracellular localization of A6K/BSH in the perinuclear region and endosome in human glioma cells. The intracellular boron concentration using A6K/BSH was almost 10 times higher than that of BSH. The systematic administration of A6K/BSH via mouse tail vein showed tumor specific accumulation in a mouse brain tumor model with immunohistochemistry and pharmacokinetic study. Neutron irradiation of glioma cells treated with A6K/BSH showed the inhibition of cell proliferation in a colony formation assay. Boron delivery using A6K peptide provides a unique and simple strategy for next generation BNCT drugs.

Published

2020

23. A leucine zipper-based peptide hybrid delivers functional Nanog protein inside the cell nucleus

Author

Takashi Ohtsuki, Yoshiyuki Hakata, Masaaki Miyazawa, Hiroyuki Michiue, and Mizuki Kitamatsu

Subjects

Leucine zipper, Clinical Biochemistry, Pharmaceutical Science, Peptide, Cell-Penetrating Peptides, 01 natural sciences, Biochemistry, Proper function, Drug Discovery, medicine, Humans, Amino Acid Sequence, Molecular Biology, chemistry.chemical_classification, Cell Nucleus, Leucine Zippers, 010405 organic chemistry, Organic Chemistry, Nanog Homeobox Protein, 0104 chemical sciences, Amino acid, Nanog Protein, 010404 medicinal & biomolecular chemistry, Cell nucleus, medicine.anatomical_structure, chemistry, embryonic structures, Molecular Medicine, Nuclear transport, HeLa Cells

Abstract

We synthesized a pair of compounds containing leucine zipper peptides to deliver protein cargo into cells. One is a cell-penetrating peptide (CPP) with Lz(E), a leucine zipper peptide containing negatively charged amino acids, and the other is a Nanog protein with Lz(K), a leucine zipper peptide containing positively charged amino acids. When cells were treated with these equimolar mixtures, Nanog-Lz(K) hybridized with Lz(E)-CPP was successfully delivered into the cells. Furthermore, Nanog-Lz(K) exerted its proper function after nuclear transport.

Published

2018

24. DDIS-20. NEW A6K BORON DRUG DELIVERY SYSTEM FOR CLINICAL APPLICATION OF BORON NEUTRON CAPTURE THERAPY (BNCT)

Author

Hiroyuki Michiue, Shuichi Furuya, Atsushi Fujimura, Asami Fukunaga, Hideki Matsui, and Kazuyo Igawa

Subjects

Cancer Research, Neutron capture, Abstracts, Materials science, Oncology, chemistry, Radiochemistry, Drug delivery, chemistry.chemical_element, Neurology (clinical), Boron

Abstract

In BNCT in GBM, one of the keys to success can depend on the boron compounds. The combination of BSH and BPA in clinical GBM BNCT showed good results and that meant the multi boron use in BNCT was one answer to next step of BNCT. In this time, we showed that the new self-assembling peptide DDS with BSH toward clinical application of BNCT. The self-assembling A6K peptide was found and reported by Dr. Shuguang Zhang, MIT in 1982. The A6K peptide showed self-assembling feature in water, and worked as drug delivery system of siRNA with only mixture. The A6K drug delivery system was clinically approved to breast cancer trial in Japan since 2015. We observed the complex of A6K and BSH with scanning electron microscope in different mixture ratio. Next, we checked the cell toxicity, measured intracellular boron concentration and observed BSH localization in mouse model. At first, we established the simple A6K/BSH complex making method, as just mixture the BSH and A6K water solution by itself. The BSH/A6K complex with different mixture ratio showed different shape and different diameter of complex in SEM image. The ideal range of particle size of DDS is 20nm to 200 nm, and ours’ complex diameter was about 40nm. Next, we administrated BSH/A6K complex to GBM cells and measured intracellular boron uptake. The concentration with BSH/A6K complex in U87 delta EGFR was 10 times or higher than that with BSH. Finally, we administrated BSH or A6K/BSH complex through mouse tail vein and got brain tumor sample after 12hr. The A6K/BSH mouse brain sample showed specifically accumulated BSH in tumor area. A6K peptide is clinical use in DDS and will spread various drug delivery tool for various clinical fields in future. Our A6K/BSH complex is very promising boron drug for next generation BNCT.

Published

2018

25. ANGI-01. FIBROBLAST GROWTH FACTOR 13 REGULATES GLIOMA CELL INVASION

Author

Toshihiko Shimizu, Atsuhito Uneda, Hiroyuki Michiue, Tetsuo Oka, Joji Ishida, Tomotsugu Ichikawa, Yasuhiko Hattori, Yusuke Tomita, Yuji Matsumoto, Satoshi Inoue, Yoshihiro Otani, Kazuhiko Kurozumi, and Isao Date

Subjects

Cancer Research, biology, Fibroblast growth factor receptor 2, Angiogenesis, Fibroblast growth factor receptor 3, Glioma cell, Fibroblast growth factor, Abstracts, Tubulin, Oncology, Cell culture, biology.protein, Cancer research, Immunohistochemistry, Neurology (clinical)

Published

2017

26. GENE-22. CORRELATION BETWEEN PIK3R1MET326ILE MUTATION, CYSTEINE-RICH PROTEIN 61 EXPRESSION AND POOR PROGNOSIS IN GLIOBLASTOMA

Author

Tetsuo Oka, Atsuhito Uneda, Yusuke Tomita, Joji Ishida, Isao Date, Hiroyuki Michiue, Tomotsugu Ichikawa, Yuji Matsumoto, Kazuhiko Kurozumi, Yoshihiro Otani, Yasuhiko Hattori, Toshihiko Shimizu, and Kentaro Fujii

Subjects

Cancer Research, Poor prognosis, Mutation, Biology, medicine.disease, medicine.disease_cause, Cysteine rich protein, Abstracts, Oncology, Glioma, medicine, Cancer research, Neurology (clinical), Gene, Cysteine, Glioblastoma

Abstract

In spite of the development of treatments, long-term survival in patients with glioblastoma is very rare. Recently, studies about clarifying prognostic markers for glioblastoma have been growing. Previously we reported that median progression-free survival and overall survival (OS) of patients with high cysteine-rich protein 61 (CCN1) expression were significantly shorter than those of patients with low CCN1 expression. To investigate the molecular mechanisms that regulate CCN1 expression, we analysed 147 tumor samples from 80 glioblastoma patients and 67 lower grade glioma patients using next-generation and Sanger sequencing. Sequencing analysis showed that CCN1 high expression group includes PIK3R1Met326Ile more frequently (10/37 cases, 27.0%) than CCN1 low expression group (3/38 cases, 7.9%) in glioblastoma. We also found this mutation in corresponding blood samples. And multivariate analysis indicated that, high CCN1 expression and PIK3R1Met326Ile in glioblastoma patients were prognostic factors for OS ([HR=2.488 (1.298–4.769), p=0.006] and [HR=2.089 (1.020–4.277), p=0.0439], respectively. According to our results, the PIK3R1Met326Ile mutation related to CCN1 expression and poor prognosis in glioblastoma.

Published

2017

27. PIK3R1Met326Ile germline mutation correlates with cysteine-rich protein 61 expression and poor prognosis in glioblastoma

Author

Atsuhito Uneda, Tomotsugu Ichikawa, Yasuhiko Hattori, Isao Date, Toshihiko Shimizu, Yoshihiro Otani, Joji Ishida, Yuji Matsumoto, Tetsuo Oka, Yusuke Tomita, Kazuhiko Kurozumi, Shuta Tomida, Hiroyuki Michiue, and Takehiro Matsubara

Subjects

Adult, Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Science, Brain tumor, Biology, Article, Germline, Phosphatidylinositol 3-Kinases, Young Adult, 03 medical and health sciences, symbols.namesake, Germline mutation, Glioma, medicine, Humans, Progression-free survival, Germ-Line Mutation, Survival analysis, Aged, Neoplasm Staging, Aged, 80 and over, Regulation of gene expression, Sanger sequencing, Multidisciplinary, Brain Neoplasms, Gene Expression Profiling, High-Throughput Nucleotide Sequencing, Sequence Analysis, DNA, Middle Aged, Prognosis, medicine.disease, Survival Analysis, Progression-Free Survival, Up-Regulation, Class Ia Phosphatidylinositol 3-Kinase, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Amino Acid Substitution, Cancer research, symbols, Medicine, Female, Glioblastoma, Cysteine-Rich Protein 61

Abstract

Despite therapeutic advances, glioblastoma represents a lethal brain tumor. Recently, research to identify prognostic markers for glioblastoma has intensified. Our previous study demonstrated that median progression-free survival (PFS) and overall survival (OS) of patients with high cysteine-rich protein 61 (CCN1) expression was significantly shorter than that of patients with low CCN1 expression. To understand the molecular mechanisms that regulate CCN1 expression, we examined 147 tumour samples from 80 patients with glioblastoma and 67 patients with lower grade glioma. Next-generation and Sanger sequencing showed that PIK3R1Met326Ile was more frequent in the CCN1 high expression group (10/37 cases, 27.0%) than the CCN1 low expression group (3/38 cases, 7.9%) in glioblastoma. This mutation was also detected in corresponding blood samples. In multivariate analysis, high CCN1 expression and PIK3R1Met326Ile in glioblastoma patients were prognostic factors for OS [HR = 2.488 (1.298–4.769), p = 0.006] and [HR = 2.089 (1.020–4.277), p = 0.0439], respectively. Thus, the PIK3R1Met326Ile germline appears to be correlated with CCN1 expression and poor prognosis in glioblastoma.

Published

2017

28. P09.24 The germline mutation PIK3R1Met326Ile correlates with the levels of cysteine<->rich protein 61 and poor prognosis of glioblastoma

Author

Joji Ishida, Toshihiko Shimizu, Matsubara T, Yoshihiro Otani, Tetsuo Oka, Shuta Tomida, Yasuhiko Hattori, Yousuke Tomita, Kazuhiko Kurozumi, Isao Date, Hiroyuki Michiue, and Tomotsugu Ichikawa

Subjects

Genetics, Cancer Research, Poor prognosis, business.industry, Biology, medicine.disease, Cysteine rich protein, Germline mutation, Text mining, Oncology, Cancer research, medicine, Neurology (clinical), business, POSTER PRESENTATIONS, Glioblastoma

Abstract

Despite advances in treatment, glioblastoma remains a lethal brain tumor. Efforts to identify prognostic molecular biomarkers for glioblastoma have intensified, and we previously reported that the median progression-free survival (PFS) and overall survival (OS) of patients with high levels of cysteine-rich protein 61 (CCN1/CYR61) are significantly shorter compared with those with low levels of CCN1. To identify the molecular mechanisms that regulate the expression of CCN1 in glioblastomas, we analyzed tumor samples from 42 patients with glioblastoma. Next-generation and Sanger sequencing techniques revealed that the PIK3R1Met326Ile mutation was significantly more frequent in patients with high vs low levels of CCN1 (9/22, 40.9% vs 2/20, 10.0%; respectively). Moreover, this mutation was identified in the corresponding blood samples. Univariate analysis of Kaplan-Meier survival data revealed that high levels of CCN1 and the presence of the PIK3R1Met326Ile mutation were significantly associated with PFS (p=0.0003 and 0.0191, respectively) and that age, high levels of CCN1, and the presence of the PIK3R1Met326Ile mutation were significantly associated with OS (p=0.0016, 0.0019 and 0.0057, respectively). Multivariate analysis identified age >65 years and the presence of the PIK3R1Met326Ile mutation as prognostic factors for OS (HR=3.533 [1.519-8.220], p=0.003) and (HR=2.712 [1.187-6.198], p=0.018, respectively). We conclude that the germline mutation PIK3R1Met326Ile correlates with the levels of CCN1 and poor prognosis of glioblastoma.

Published

2017

29. Reduced neurotoxicity with combined treatment of high-dose methotrexate, cyclophosphamide, doxorubicin, vincristine and prednisolone (M-CHOP) and deferred radiotherapy for primary central nervous system lymphoma

Author

Kazuhiko Kurozumi, Isao Date, Hiroyuki Michiue, Eisei Kondo, Akihiro Kawasaki, Joji Ishida, Yoshinobu Maeda, and Tomotsugu Ichikawa

Subjects

Male, medicine.medical_specialty, Vincristine, Lymphoma, genetic structures, Cyclophosphamide, Prednisolone, medicine.medical_treatment, Kaplan-Meier Estimate, Neuropsychological Tests, CHOP, Gastroenterology, Disease-Free Survival, Central Nervous System Neoplasms, immune system diseases, hemic and lymphatic diseases, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, polycyclic compounds, medicine, Humans, Karnofsky Performance Status, Aged, business.industry, Primary central nervous system lymphoma, Neurotoxicity, General Medicine, Middle Aged, medicine.disease, Survival Analysis, eye diseases, Surgery, Radiation therapy, Methotrexate, Treatment Outcome, Doxorubicin, Female, Neurology (clinical), business, medicine.drug

Abstract

Objective Although high-dose methotrexate and whole-brain radiation therapy (WBRT) is the current standard for primary central nervous system lymphoma (PCNSL), it has a limited response rate and produces radiation-induced neurotoxicity. We report the effect of a combined treatment of high-dose methotrexate, cyclophosphamide, doxorubicin, vincristine and prednisolone (M-CHOP) for immunocompetent patients with PCNSL. Methods We analyzed 24 patients who had received M-CHOP administered in 28-day cycles with or without WBRT. The response rate to M-CHOP, overall survival (OS), and recurrence-free survival (RFS) were analyzed. Results Nine patients were treated with M-CHOP plus WBRT and 15 patients were treated with M-CHOP alone. Twenty-one patients achieved a complete response and three patients achieved a partial response to M-CHOP, for a 100% response rate. With a median follow-up of 70 months, the median OS and RFS were 33 and 13 months, respectively. The median OS for patients treated with M-CHOP plus WBRT and M-CHOP alone was 33 and 32 months, respectively. Of the 13 patients whose age was above 65 years, the median OS for the M-CHOP plus WBRT group (two patients) and the M-CHOP alone group (11 patients) was 14 and 32 months, respectively. Toxicities related to M-CHOP were mostly hematologic and generally mild to moderate. Two patients whose age was above 65 years in the M-CHOP plus WBRT group developed neurotoxicity. Conclusion Combined treatment with M-CHOP was well tolerated and produced a high response rate. Deferring WBRT was associated with reduced neurotoxicity without worsening the prognosis, especially in elderly patients.

Published

2014

30. The 2013 Incentive Award of the Okayama Medical Association in General Medical Science (2013 Yuuki Prize)

Author

Hiroyuki Michiue

Published

2015

31. Inhalation of 10% carbon dioxide rapidly terminates Scn1a mutation-related hyperthermia-induced seizures

Author

Haijiao Wang, Mamoru Ouchida, Teiichi Nishiki, Iori Ohmori, Naohiro Fujita, Hideki Matsui, Hiroyuki Michiue, Keiichiro Hayashi, and Takushi Inoue

Subjects

Male, medicine.medical_specialty, Hiss, Time Factors, Fever, medicine.medical_treatment, Mutation, Missense, Rats, Mutant Strains, pCO2, Epilepsy, Seizures, Internal medicine, Febrile seizure, medicine, Animals, Inhalation, Chemistry, Carbon Dioxide, medicine.disease, Rats, Inbred F344, Rats, NAV1.1 Voltage-Gated Sodium Channel, Respiratory acidosis, Endocrinology, Anticonvulsant, Neurology, Anesthesia, Respiratory alkalosis, Neurology (clinical)

Abstract

The aim of this study was to assess the anticonvulsant effect of carbon dioxide (CO2) on Scn1a mutation-related febrile seizures. We examined physiological changes in the blood gas levels after the induction of hyperthermia-induced seizures (HISs), which were associated with the Scn1a missense mutation. We determined the efficacy of inhalation of 5% or 10% CO2 to treat HISs. HISs were evoked in Scn1a mutant and wild-type (WT) rats by hot water baths. To determine the anticonvulsant effect of CO2 inhalation, rats were placed in a chamber filled with air or mixed gas containing 5% CO2 or 10% CO2 for 3 min, immediately after the induction of HISs. We also analyzed the blood gas levels at the end of inhalation of CO2. Hot water bathing induced a significant reduction in the partial pressure of CO2 (pCO2) and respiratory alkalosis in the WT and Scn1a mutant rats. HISs were evoked in 100% of the Scn1a mutant rats within 5 min, but in none of the WT rats. The Scn1a mutant rats demonstrated a higher HISs susceptibility associated with respiratory alkalosis than the WT rats. Inhalation of 10% CO2 shortened the seizure duration from 62.6±12.1 s to 15.5±1.0 s. Blood gas analysis after the inhalation of 10% CO2 demonstrated an elevated pCO2 level and respiratory acidosis. Inhalation of 10% CO2 demonstrated a potent and fast-acting anticonvulsant effect against HISs.

Published

2013

32. CACNA1A variants may modify the epileptic phenotype of Dravet syndrome

Author

Hiroyuki Michiue, Teiichi Nishiki, Hideki Matsui, Yoshimi Jitsumori, Katsuhiro Kobayashi, Akiko Mori, Iori Ohmori, Mamoru Ouchida, and Yoko Ohtsuka

Subjects

Adult, medicine.medical_specialty, Patch-Clamp Techniques, Genotype, DNA Mutational Analysis, Molecular Sequence Data, Epilepsies, Myoclonic, Biology, CACNA1A, lcsh:RC321-571, Epilepsy, Exon, Dravet syndrome, Molecular genetics, medicine, Humans, SCN1A, Child, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Genetics, Base Sequence, Sodium channel, HEK 293 cells, Electroencephalography, medicine.disease, Phenotype, Electrophysiology, Neurology, Calcium Channels

Abstract

Dravet syndrome is an intractable epileptic syndrome beginning in the first year of life. De novo mutations of SCN1A, which encode the Na(v)1.1 neuronal voltage-gated sodium channel, are considered the major cause of Dravet syndrome. In this study, we investigated genetic modifiers of this syndrome. We performed a mutational analysis of all coding exons of CACNA1A in 48 subjects with Dravet syndrome. To assess the effects of CACNA1A variants on the epileptic phenotypes of Dravet syndrome, we compared clinical features in two genotype groups: 1) subjects harboring SCN1A mutations but no CACNA1A variants (n=20) and 2) subjects with SCN1A mutations plus CACNA1A variants (n=20). CACNA1A variants detected in patients were studied using heterologous expression of recombinant human Ca(v)2.1 in HEK 293 cells and whole-cell patch-clamp recording. Nine CACNA1A variants, including six novel ones, were detected in 21 of the 48 subjects (43.8%). Based on the incidence of variants in healthy controls, most of the variants seemed to be common polymorphisms. However, the subjects harboring SCN1A mutations and CACNA1A variants had absence seizures more frequently than the patients with only SCN1A mutations (8/20 vs. 0/20, p=0.002). Moreover, the former group of subjects exhibited earlier onset of seizures and more frequent prolonged seizures before one year of age, compared to the latter group of subjects. The electrophysiological properties of four of the five novel Ca(v)2.1 variants exhibited biophysical changes consistent with gain-of-function. We conclude that CACNA1A variants in some persons with Dravet syndrome may modify the epileptic phenotypes.

Published

2013

33. Oxytocin Inhibits Corticosterone-induced Apoptosis in Primary Hippocampal Neurons

Author

Hideki Matsui, Yuuri Koga, Kazuhito Tomizawa, Hiroyuki Michiue, Hiroaki Matsushita, Teiichi Nishiki, Hein Min Latt, and Miku Morino

Subjects

0301 basic medicine, endocrine system, medicine.medical_specialty, Hippocampus, Apoptosis, Hippocampal formation, Biology, Inhibitory postsynaptic potential, Oxytocin, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Corticosterone, Internal medicine, medicine, Animals, Receptor, Cells, Cultured, Mice, Knockout, Neurons, Dose-Response Relationship, Drug, General Neuroscience, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Neuroprotective Agents, nervous system, chemistry, Receptors, Oxytocin, Neuroglia, hormones, hormone substitutes, and hormone antagonists, 030217 neurology & neurosurgery, Stress, Psychological, medicine.drug

Abstract

Stress is an adaptive and coordinated response to endogenous or exogenous stressors that pose an unpleasant and aversive threat to an individual's homeostasis and wellbeing. Glucocorticoids, corticosterone (CORT) in rodents and cortisol in humans, are adrenal steroids which are released in response to stressful stimuli. Although they help individuals to cope with stress, their overexposure in animals has been implicated in hippocampal dysfunction and neuronal loss. Oxytocin (OT) plays an active role in adaptive stress-related responses and protects hippocampal synaptic plasticity and memory during stress. In this study, we showed that OT protects primary mouse hippocampal neurons from CORT-induced apoptosis. OT receptors (OTR) were expressed in primary mouse hippocampal neurons and glial cells. CORT induced apoptosis in hippocampal neurons, but had no effect on apoptosis in glial cells. OT inhibited CORT-induced apoptosis in primary hippocampal neurons. OT was unable to protect primary hippocampal neurons prepared from OTR KO mice from CORT-induced apoptosis. These results indicate that OT has inhibitory effects on CORT-induced neuronal death in primary hippocampal neurons via acting on OTR. The findings suggest a therapeutic potential of OT in the treatment of stress-related disorders.

Published

2016

34. OS1.5 Fluvoxamine (SSRI), inhibits glioblastoma invasion by inhibition of actin polymerization

Author

Keiichiro Hayashi and Hiroyuki Michiue

Subjects

Cancer Research, Oncology, Polymerization, Chemistry, medicine, Fluvoxamine, Neurology (clinical), OS1 Cell Biology, Pharmacology, medicine.disease, Actin, Glioblastoma, medicine.drug

Published

2016

35. Bimodal anti-glioma mechanisms of cilengitide demonstrated by novel invasive glioma models

Author

Kentaro Fujii, Isao Date, Koichi Yoshida, Kazuhiko Kurozumi, Manabu Onishi, E. Antonio Chiocca, Tomotsugu Ichikawa, Balveen Kaur, Hiroyuki Michiue, and Satoshi Inoue

Subjects

Pathology, medicine.medical_specialty, Angiogenesis, Cell, Integrin, Cilengitide, General Medicine, Biology, medicine.disease, Pathology and Forensic Medicine, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Cell culture, Glioma, medicine, biology.protein, Immunohistochemistry, Neurology (clinical), Infiltration (medical)

Abstract

Integrins are expressed in tumor cells and tumor endothelial cells, and likely play important roles in glioma angiogenesis and invasion. We investigated the anti-glioma mechanisms of cilengitide (EMD121974), an αvβ3 integrin inhibitor, utilizing the novel invasive glioma models, J3T-1 and J3T-2. Immunohistochemical staining of cells in culture and brain tumors in rats revealed positive αvβ3 integrin expression in J3T-2 cells and tumor endothelial cells, but not in J3T-1 cells. Established J3T-1 and J3T-2 orthotopic gliomas in athymic rats were treated with cilengitide or solvent. J3T-1 gliomas showed perivascular tumor cluster formation and angiogenesis, while J3T-2 gliomas showed diffuse single-cell infiltration without obvious angiogenesis. Cilengitide treatment resulted in a significantly decreased diameter of the J3T-1 tumor vessel clusters and its core vessels when compared with controls, while an anti-invasive effect was shown in the J3T-2 glioma with a significant reduction of diffuse cell infiltration around the tumor center. The survival of cilengitide-treated mice harboring J3T-1 tumors was significantly longer than that of control animals (median survival: 57.5 days and 31.8 days, respectively, P

Published

2012

36. Antidepressant-like effect of sildenafil through oxytocin-dependent cyclic AMP response element-binding protein phosphorylation

Author

Tei-ich Nishiki, Hiroaki Matsushita, Mitsuhiro Matsuzaki, Xiao-Jian Han, Iori Ohmori, Hiroyuki Michiue, Hideki Matsui, and Kazuhito Tomizawa

Subjects

Male, Oxytocin, Piperazines, Mice, Sexual Behavior, Animal, chemistry.chemical_compound, Sulfones, Enzyme Inhibitors, Phosphorylation, Cyclic AMP Response Element-Binding Protein, Mice, Knockout, Aniline Compounds, biology, Depression, General Neuroscience, Antidepressive Agents, medicine.anatomical_structure, Receptors, Oxytocin, Benzamides, cardiovascular system, Female, Signal transduction, medicine.drug, medicine.medical_specialty, Sildenafil, CREB, Sildenafil Citrate, Sex Factors, Posterior pituitary, Internal medicine, medicine, Animals, Swimming, Dose-Response Relationship, Drug, business.industry, Antagonist, Immobility Response, Tonic, respiratory tract diseases, Mice, Inbred C57BL, Disease Models, Animal, Endocrinology, Gene Expression Regulation, chemistry, Purines, Exploratory Behavior, biology.protein, business

Abstract

Oxytocin (OT) levels in plasma increase during sexual response and are significantly lower in patients with depression. A drug for the treatment of sexual dysfunction, sildenafil, enhances the electrically evoked release of OT from the posterior pituitary. In this study, we showed that sildenafil had an antidepressant-like effect through activation of an OT signaling pathway. Application of sildenafil reduced depression-related behavior in male mice. The antidepressant-like effect was blocked by an OT receptor (OTR) antagonist and was absent in OTR knockout (KO) mice. Sildenafil increased the phosphorylation of cAMP response element-binding protein (CREB) in the hippocampus. The OTR antagonist inhibited sildenafil-induced CREB phosphorylation and sildenafil had no effect on CREB phosphorylation in OTR KO mice. These results suggest sildenafil to have an antidepressant-like effect through the activation of OT signaling and to be a promising drug for the treatment of depression.

Published

2012

37. Protein Therapy Using Heme-Oxygenase-1 Fused to a Polyarginine Transduction Domain Attenuates Cerebral Vasospasm after Experimental Subarachnoid Hemorrhage

Author

Kazuhito Tomizawa, Yumei Wu, Hans Jakob Steiger, Daniel Hänggi, Isao Date, Tomoyuki Ogawa, Hideki Matsui, Shigeki Ono, and Hiroyuki Michiue

Subjects

Male, Subarachnoid hemorrhage, Arginine, Cell Survival, Protein Conformation, Recombinant Fusion Proteins, Blotting, Western, Cerebral arteries, Pharmacology, Cisterna magna, Cell Line, Rats, Sprague-Dawley, Cerebral vasospasm, Transduction, Genetic, medicine.artery, Escherichia coli, Basilar artery, medicine, Animals, Vasospasm, Intracranial, business.industry, Vasospasm, Cerebral Arteries, Subarachnoid Hemorrhage, medicine.disease, Immunohistochemistry, Rats, Heme oxygenase, Disease Models, Animal, Neurology, Biochemistry, Basilar Artery, Original Article, Electrophoresis, Polyacrylamide Gel, Neurology (clinical), Peptides, Cardiology and Cardiovascular Medicine, business, Heme Oxygenase-1, Plasmids

Abstract

A sequence of 11 consecutive arginine residues (11R) is one of the best protein transduction domains for introducing proteins into cell membranes. Heme-oxygenase-1 (HO-1) is involved in heme catabolism and reduces the contractile effect of hemoglobin after subarachnoid hemorrhage (SAH). Therefore, we constructed 11R-fused HO-1 protein to achieve successful transduction of the protein into the cerebral arteries and examined the therapeutic effect of the 11R-HO-1 protein for cerebral vasospasm (CV) after SAH. We injected the 11R-HO-1 protein into the cisterna magna of male rats and, several hours after the injection, performed immunofluorescence staining and western blotting analysis of the rat basilar arteries (BAs) to determine transduction efficacy. We also assessed intraarterial HO-1 activity as cGMP (cyclic guanosine 3′, 5′-cyclic monophosphate) accumulation in SAH and determined whether protein transduction of 11R-HO-1 quantified the therapeutic effect in a rat double-hemorrhage model of SAH. The BAs expressed significantly more HO-1 in the group injected with 11R-HO-1 (3.56±0.54 (11R-HO-1) versus control (saline)), and transduction of 11R-HO-1 resulted in higher activity (>3.25-fold) in rat BAs with SAH. Moreover, the results of the rat double-hemorrhage model showed that the 11R-HO-1 protein significantly attenuated CV after SAH (317.59±23.48 μm (11R-HO-1) versus 270.08±14.66 μm (11R-fused enhanced green fluorescent protein), 252.05±13.95 μm (saline), P

Published

2011

38. Physical modification of carbon nanotubes with a dendrimer bearing terminal mercaptoundecahydrododecaborates (Na 2 B 12 H 11 S)

Author

Hideaki Miyake, Yutaka Takaguchi, Kango Ishimoto, Masahiro Yamagami, Tomoyuki Tajima, and Hiroyuki Michiue

Subjects

Bearing (mechanical), Chemistry, 02 engineering and technology, General Chemistry, Carbon nanotube, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, 0104 chemical sciences, law.invention, Terminal (electronics), law, Dendrimer, Polymer chemistry, 0210 nano-technology

Published

2018

39. Induction of in vivo synthetic lethal RNAi responses to treat glioblastoma

Author

Miriam Scadeng, Steven F. Dowdy, Akiko Eguchi, and Hiroyuki Michiue

Subjects

Cancer Research, Small interfering RNA, Immunoblotting, Longevity, Population, Mice, Nude, Apoptosis, Biology, Article, RNAi Therapeutics, Mice, Transduction (genetics), RNA interference, In vivo, In Situ Nick-End Labeling, Tumor Cells, Cultured, Animals, Humans, RNA, Small Interfering, education, RNA, Double-Stranded, Pharmacology, education.field_of_study, Brain Neoplasms, Cell growth, Xenograft Model Antitumor Assays, Molecular biology, Protein Structure, Tertiary, ErbB Receptors, Survival Rate, Oncology, Cancer research, Molecular Medicine, Genes, Lethal, Glioblastoma, Proto-Oncogene Proteins c-akt

Abstract

Glioblastoma multiforme remains one of the most intractable human malignancies. Glioblastomas arise due to activation of multiple oncogenic pathways leading to increased cellular growth, proliferation and tumor cell survival. siRNA induced RNA Interference (RNAi) responses result in the degradation of specific mRNA species. In theory, RNAi responses can selectively target intersecting oncogenic pathways to induce a tumor cell specific RNAi synthetic lethal response. However, the concept of inducing in vivo synthetic lethal RNAi responses has not yet been addressed. Here we tested the in vivo ability of synthetic lethal RNAi responses to treat glioblastoma. To deliver siRNAs into cells, we fused a peptide transduction delivery domain to a dsRNA-binding domain (PTD-DRBD). DRBDs avidly bind to siRNAs, masking the siRNA anionic negative charge and allowing for efficient PTD-mediated siRNA delivery into the entire cell population. Combinatorial targeting of EGF-Receptor (EGFR) and Akt2, but not Ak1 or Akt3, by PTD-DRBD delivered siRNAs synergized to induce tumor cell specific apoptosis. In vivo PTD-DRBD delivery of EGFR and Akt2 siRNAs induced tumor specific apoptosis and significantly increased survival in intracerebral glioblastoma mouse models (p < 0.0005), whereas delivery of irrelevant control siRNAs did not alter longevity. Thus, siRNA induced synthetic lethal RNAi responses have great potential for personalized medicine treatment of cancer.

Published

2009

40. Enhanced Intracellular Delivery Using Arginine-Rich Peptides by the Addition of Penetration Accelerating Sequences (Pas)

Author

Ikuhiko Nakase, Hideki Matsui, Kentaro Takayama, Shiroh Futaki, Kazuhito Tomizawa, Toshihide Takeuchi, and Hiroyuki Michiue

Subjects

Cell Membrane Permeability, Arginine, Membrane permeability, intracellular delivery, Cell Survival, Molecular Sequence Data, Cell Culture Techniques, Pharmaceutical Science, Peptide, Biology, arginine-rich peptide, Cathepsin D, Cytosol, Drug Delivery Systems, Humans, p53 C-terminal segment, Amino Acid Sequence, Peptide sequence, chemistry.chemical_classification, Microscopy, Confocal, Cell Membrane, retro-inverso peptide, Retro-Inverso Peptide, Flow Cytometry, Peptide Fragments, Biochemistry, chemistry, cell penetrating peptide, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Biophysics, Cell-penetrating peptide, Capsid Proteins, Tumor Suppressor Protein p53, Oligopeptides, Intracellular, HeLa Cells

Abstract

Cell penetrating peptides (CPPs), including arginine-rich peptides, are attractive tools for the intracellular delivery of various bioactive molecules with a low membrane permeability. We showed that the accelerated intracellular delivery of arginine-rich peptides was achieved by the addition of a short peptide segment (penetration accelerating sequence, Pas) to arginine-rich CPPs. The cytosolic release of the Pas-attached arginine-rich CPPs was observed within 5 min after the treatment of the cells with the peptides even in the presence of serum. Effectiveness of the Pas segment in the intracellular delivery of bioactive peptides using arginine-rich CPPs was exemplified through the enhanced growth inhibition activity of the malignant glioma cells by a retro-inverso peptide derived from the p53 C-terminal 22-amino-acid segment (positions 361-382).

Published

2009

41. Boron Neutron Capture Therapy for Newly Diagnosed Glioblastoma

Author

Hiroaki Kumada, Shin-Ichi Miyatake, Yoshio Imahori, Yoshinori Sakurai, Taisuke Inomata, Akira Maruhashi, Koji Ono, Shiro Miyata, Toshihiko Kuroiwa, Masatsugu Takahashi, Hiroyuki Michiue, Shinji Kawabata, Atsushi Doi, Mitsunori Kirihata, Naosuke Nonoguchi, Kunio Yokoyama, and Kyoko Iida

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Health, Toxicology and Mutagenesis, medicine.medical_treatment, Boron Neutron Capture Therapy, Newly diagnosed, Sodium Borocaptate, Young Adult, medicine, Humans, Radiology, Nuclear Medicine and imaging, Aged, Chemotherapy, Radiation, Brain Neoplasms, business.industry, Middle Aged, medicine.disease, Combined Modality Therapy, Survival Rate, Radiation therapy, Clinical trial, Treatment Outcome, Tumor progression, Female, Radiology, Glioblastoma, Nuclear medicine, business, Median survival

Abstract

We evaluate the clinical results of a form of tumor selective particle radiation known as boron neutron capture therapy (BNCT) for newly-diagnosed glioblastoma (NDGB) patients, especially in combination with X-ray treatment (XRT). Between 2002 and 2006, we treated 21 patients of NDGB with BNCT utilizing sodium borocaptate and boronophenylalanine simultaneously. The first 10 were treated with only BNCT (protocol 1), and the last 11 were treated with BNCT followed by XRT of 20 to 30 Gy (protocol 2) to reduce the possibility of local tumor recurrence. No chemotherapy was applied until tumor progression was observed. The patients treated with BNCT (protocol 1 plus 2) showed a significant survival prolongation compared with the institutional historical controls. BNCT also showed favorable results in correspondence with the RTOG- and EORTC-RPA subclasses. The median survival time (MST) was 15.6 months for protocols 1 and 2 together. For protocol 2, the MST was 23.5 months. The main causes of death were cerebrospinal fluid dissemination as well as local recurrence. Our modified BNCT protocol showed favorable results of patients with NDGB not only for those with good prognoses but also for those with poor prognoses.

Published

2009

42. Development of bionanocapsules targeting brain tumors

Author

Yumi Tsutsui, Mana Nagita, Teiichi Nishiki, Masaharu Seno, Hideki Matsui, Iori Ohmori, Hiroyuki Michiue, and Kazuhito Tomizawa

Subjects

Male, Genetic enhancement, Antibody Affinity, Brain tumor, Mice, Nude, Pharmaceutical Science, EGFR Antibody, Mice, Nanocapsules, Antibody Specificity, In vivo, Cell Line, Tumor, Glioma, medicine, Animals, Humans, Epidermal growth factor receptor, Rats, Wistar, Staphylococcal Protein A, Fluorescent Dyes, Drug Carriers, Mice, Inbred BALB C, biology, Brain Neoplasms, Rhodamines, Antibodies, Monoclonal, Biological Transport, medicine.disease, Virology, Rats, ErbB Receptors, Animals, Newborn, Astrocytes, Drug delivery, Cancer research, biology.protein, Protein A

Abstract

Bionanocapsules (BNCs) are hollow nanoparticles that are composed of L protein (the hepatitis B virus surface antigen) and show specific affinity for human hepatocytes. The pre-S1 peptide displayed on the surface of BNCs is the specific ligand for binding to the receptor on human hepatocytes. Therefore, BNCs are not delivered to other tissues, such as the brain. The aim of the present study was to develop a novel drug delivery system (DDS) targeting brain tumors using BNCs that selectively targeted brain tumors. Epidermal growth factor receptor (EGFR), especially a constitutively active genomic sequence deletion variant of EGFR (EGFRvIII), is overexpressed in human glioblastoma. In the present study, we replaced the pre-S1 peptide with the antibody affinity motif of protein A and made hybrid BNCs conjugated with anti-human EGFR antibody recognizing EGFRvIII. The hybrid BNCs were efficiently delivered to glioma cells but not normal glial cells. Moreover, we confirmed the specific delivery of the hybrid BNCs to brain tumors in an in vivo brain tumor model. These results suggest that this new approach using BNCs is a promising system for brain tumor-targeted drug delivery.

Published

2007

43. CBIO-25NEW HYPOXIA-INDUCED INVASION FACTOR IN HUMAN GLIOBLASTOMA INVASION

Author

Hideki Matsui, Atsushi Fujimura, Hiroyuki Michiue, Hiroaki Mastushita, and Teiichi Nishiki

Subjects

Cancer Research, Tyrosine phosphorylation, macromolecular substances, Biology, medicine.disease, Filamentous actin, Cell biology, chemistry.chemical_compound, Oncology, chemistry, Glioma, medicine, biology.protein, Neurology (clinical), Signal transduction, Cytoskeleton, Abstracts from the 20th Annual Scientific Meeting of the Society for Neuro-Oncology, Cortactin, Cyclin, Proto-oncogene tyrosine-protein kinase Src

Abstract

Microenvironmental conditions such as hypoxia potentiate the local invasion of malignant tumors including glioblastomas by modulating signal transduction and protein modification, yet the mechanism by which hypoxia controls cytoskeletal dynamics to promote the local invasion is not well defined. Here, we show that cyclin G2 plays pivotal roles in the cytoskeletal dynamics in hypoxia-driven invasion by glioblastoma cells. Cyclin G2 is a hypoxia-induced and cytoskeleton-associated protein and is required for glioblastoma expansion. Mechanistically, cyclin G2 recruits cortactin to the juxtamembrane through its SH3 domain-binding motif and consequently promotes the restricted tyrosine phosphorylation of cortactin in concert with src. Moreover, cyclin G2 interacts with filamentous actin to facilitate the formation of membrane ruffles. In primary glioblastoma, cyclin G2 is abundantly expressed in severely hypoxic regions such as pseudopalisades, which consist of actively migrating glioma cells. Furthermore, we show the effectiveness of dasatinib against hypoxia-driven, cyclin G2-involved invasion in vitro and in vivo. Our findings elucidate the mechanism of cytoskeletal regulation by which severe hypoxia promotes the local invasion and may provide a therapeutic target in glioblastoma.

Published

2015

44. Fluvoxamine, an anti-depressant, inhibits human glioblastoma invasion by disrupting actin polymerization

Author

Hiroshi Tazawa, Kazuhito Tomizawa, Katsuyoshi Takata, Hiroshi Yamada, Akira Asai, Kohji Takei, Keiichiro Hayashi, Hiroyuki Miyachi, Hiroyuki Michiue, Atsushi Fujimura, Hiroki Nakayama, Hideki Matsui, Naohisa Ogo, Teiichi Nishiki, and Fan Yan Wei

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Fluvoxamine, Article, Focal adhesion, 03 medical and health sciences, Mice, 0302 clinical medicine, Cell Movement, Glioma, Cell Line, Tumor, Medicine, Animals, Humans, Neoplasm Invasiveness, Protein kinase B, Multidisciplinary, Dose-Response Relationship, Drug, business.industry, Brain Neoplasms, TOR Serine-Threonine Kinases, Drug Repositioning, Cell migration, medicine.disease, Actin cytoskeleton, Survival Analysis, Xenograft Model Antitumor Assays, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Treatment Outcome, Cell culture, 030220 oncology & carcinogenesis, Focal Adhesion Protein-Tyrosine Kinases, Cancer research, Neoplastic Stem Cells, Stem cell, business, Glioblastoma, Proto-Oncogene Proteins c-akt, medicine.drug, Signal Transduction

Abstract

Glioblastoma multiforme (GBM) is the most common malignant brain tumor with a median survival time about one year. Invasion of GBM cells into normal brain is the major cause of poor prognosis and requires dynamic reorganization of the actin cytoskeleton, which includes lamellipodial protrusions, focal adhesions, and stress fibers at the leading edge of GBM. Therefore, we hypothesized that inhibitors of actin polymerization can suppress GBM migration and invasion. First, we adopted a drug repositioning system for screening with a pyrene-actin-based actin polymerization assay and identified fluvoxamine, a clinically used antidepressant. Fluvoxamine, selective serotonin reuptake inhibitor, was a potent inhibitor of actin polymerization and confirmed as drug penetration through the blood–brain barrier (BBB) and accumulation of whole brain including brain tumor with no drug toxicity. Fluvoxamine inhibited serum-induced ruffle formation, cell migration, and invasion of human GBM and glioma stem cells in vitro by suppressing both FAK and Akt/mammalian target of rapamycin signaling. Daily treatment of athymic mice bearing human glioma-initiating cells with fluvoxamine blocked tumor cell invasion and prolonged the survival with almost same dose of anti-depressant effect. In conclusion, fluvoxamine is a promising anti-invasive treatment against GBM with reliable approach.

Published

2015

45. Tumor-specific delivery of BSH-3R for boron neutron capture therapy and positron emission tomography imaging in a mouse brain tumor model

Author

Yuri Hayashi, Hiroyuki Michiue, Mizuki Kitamatsu, Yoshiya Iguchi, Teiichi Nishiki, Hideki Matsui, and Fumiaki Takenaka

Subjects

Modern medicine, Materials science, Arginine, Cell Survival, Biophysics, Brain tumor, Mice, Nude, Bioengineering, Boron Neutron Capture Therapy, Multimodality Therapy, Biomaterials, chemistry.chemical_compound, Heterocyclic Compounds, 1-Ring, Mice, Drug Delivery Systems, Pharmacokinetics, Glioma, Cell Line, Tumor, medicine, DOTA, Animals, Humans, Boron, Mice, Inbred BALB C, medicine.diagnostic_test, business.industry, Brain Neoplasms, medicine.disease, Boronic Acids, Immunohistochemistry, Disease Models, Animal, chemistry, Mechanics of Materials, Positron emission tomography, Positron-Emission Tomography, Ceramics and Composites, Cancer research, Female, Nuclear medicine, business, Peptides, Tomography, X-Ray Computed, Oligopeptides, Copper, Neoplasm Transplantation

Abstract

Glioblastoma, a malignant brain tumor with poor disease outcomes, is managed in modern medicine by multimodality therapy. Boron neutron capture therapy (BNCT) is an encouraging treatment under clinical investigation. In malignant cells, BNCT consists of two major factors: neutron radiation and boron uptake. To increase boron uptake in cells, we created a mercapto-closo-undecahydrododecaborate ([B12HnSH](2-)2Na(+), BSH) fused with a short arginine peptide (1R, 2R, 3R) and checked cellular uptake in vitro and in vivo. In a mouse brain tumor model, only BSH with at least three arginine domains could penetrate cell membranes of glioma cells in vitro and in vivo. Furthermore, to monitor the pharmacokinetic properties of these agents in vivo, we fused BSH and BSH-3R with 1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid (DOTA); DOTA is a metal chelating agent for labeling positron emission tomography (PET) probe with (64)Cu. We administered BSH-DOTA-(64)Cu and BSH-3R-DOTA-(64)Cu to the tumor model through a mouse tail vein and determined the drugs' pharmacokinetics by PET imaging. BSH-3R showed a high uptake in the tumor area on PET imaging. We concluded that BSH-3R is the ideal boron compound for clinical use during BNCT and that in developing this compound for clinical use, the BSH-3R PET probe is essential for pharmacokinetic imaging.

Published

2014

46. A novel leucine zipper motif-based hybrid peptide delivers a functional peptide cargo inside cells

Author

Mizuki Kitamatsu, S. Tsuchiya, Masaaki Miyazawa, Yoshiyuki Hakata, Takashi Ohtsuki, Hideki Matsui, and Hiroyuki Michiue

Subjects

chemistry.chemical_classification, Leucine zipper, Programmed cell death, Leucine Zippers, Chemistry, Autophagy, Molecular Sequence Data, Metals and Alloys, Peptide, General Chemistry, Cell-Penetrating Peptides, Catalysis, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, Biochemistry, Materials Chemistry, Ceramics and Composites, Humans, Amino Acid Sequence, Functional peptide, Peptides, Peptide sequence, HeLa Cells

Abstract

A hybrid comprising an autophagy-inducing peptide (AIP) and a cell-penetrating peptide (CPP) connected via heterodimeric leucine zippers was generated and delivered into cells. The hybrid successfully induced autophagy without significant cell death, while the same AIP directly connected to a CPP caused both autophagy and significant cell death.

Published

2014

47. [The use of the ubiquitin-proteasome system in neurosurgery and the clinical applications of protein therapy]

Author

Hiroyuki, Michiue and Isao, Date

Subjects

Proteasome Endopeptidase Complex, Drug Delivery Systems, Ubiquitin, Proteolysis, Neurosurgery, Animals, Humans, Tumor Suppressor Protein p53

Published

2014

48. The transdermal inhibition of melanogenesis by a cell-membrane-permeable peptide delivery system based on poly-arginine

Author

Hideki Matsui, Nanako Ookubo, Iori Ohmori, Maho Kamamura, Teiichi Nishiki, Mizuki Kitamatsu, and Hiroyuki Michiue

Subjects

Cell Membrane Permeability, Tyrosinase, Guinea Pigs, Biophysics, Tyrosinase Peptide, Melanoma, Experimental, Bioengineering, Peptide, Skin Pigmentation, Absorption (skin), Pharmacology, Administration, Cutaneous, Biomaterials, Melanin, chemistry.chemical_compound, Drug Delivery Systems, Cell Line, Tumor, Animals, Humans, Amino Acid Sequence, Transdermal, Skin, chemistry.chemical_classification, Melanins, integumentary system, Monophenol Monooxygenase, Amino acid, chemistry, Mechanics of Materials, Ceramics and Composites, Female, Kojic acid, Peptides

Abstract

Topical therapy is the most favored form of treatment for whitening against hyper-pigmentation and sunburn because it lends itself to self-administration, patient compliance and an absence of systemic adverse effects. However, high-molecular-weight, hydrophilic chemicals are difficult to use as transdermal delivery drugs and the use of topical drugs has been highly limited. There are now many potent tyrosinase inhibitors, for example, sulfite or kojic acid, but the efficacy of their skin transduction remains a big problem. Furthermore, melanogenesis inhibitors from natural sources have great potential, as they are considered to be safe and largely free from adverse side effects. We applied 11-arginine (11R), a cell-membrane-permeable peptide, as a transdermal delivery system with a skin delivery enhancer, pyrenbutyrate. We performed intracellular screening for melanogenesis inhibitors with 11R fused with several kinds of tyrosinase inhibitory peptides from natural sources. Of 28 tyrosinase peptides, 13 melanin synthesis inhibitory peptides were selected. Peptide No. 10 found in gliadin protein, a wheat component, most strongly inhibited melanin production. This No. 10 peptide, of only 8 amino acids, fused to 11R showed no cytotoxicity and inhibited melanin synthesis as determined through melanin content measured using an absorption spectrometer and observation with a transmission electron microscope. Next, we transduced this 11R-No. 10 into skin with an 11R transdermal delivery system after previous treatment with pyrenbutyrate and performed daily repetitive topical application for two weeks against a UV-induced sun-tanning guinea pig model. We observed a whitening effect in a model skin sample by Masson-Fontana staining and the 11R-No. 10 peptide-applied area showed significant melanogenesis inhibition. These results show that 11R using a transdermal drug delivery system with melanogenesis inhibitory peptide is a very safe and promising method for applications from cosmetics to the pharmaceutical industry.

Published

2014

49. The acceleration of boron neutron capture therapy using multi-linked mercaptoundecahydrododecaborate (BSH) fused cell-penetrating peptide

Author

Mizuki Kitamatsu, Kazuhito Tomizawa, Koji Ono, Yuki Hirota, Hideki Matsui, Yoshinori Sakurai, Kiichiro Nakajima, Natsuko Kondo, Shin-Ichi Miyatake, Hiroyuki Michiue, Iori Ohmori, Feng Bin, Teiichi Nishiki, and Shinji Kawabata

Subjects

inorganic chemicals, Materials science, Cell, Biophysics, chemistry.chemical_element, Bioengineering, Peptide, Boron Neutron Capture Therapy, Borohydrides, Sodium Borocaptate, Biomaterials, Cell membrane, In vivo, Glioma, medicine, Humans, Sulfhydryl Compounds, Boron, chemistry.chemical_classification, Brain Neoplasms, Radiochemistry, medicine.disease, medicine.anatomical_structure, chemistry, Mechanics of Materials, Ceramics and Composites, Cell-penetrating peptide, Glioblastoma, Peptides

Abstract

New anti-cancer therapy with boron neutron capture therapy (BNCT) is based on the nuclear reaction of boron-10 with neutron irradiation. The median survival of BNCT patients with glioblastoma was almost twice as long as those receiving standard therapy in a Japanese BNCT clinical trial. In this clinical trial, two boron compounds, BPA (boronophenylalanine) and BSH (sodium borocaptate), were used for BNCT. BPA is taken up into cells through amino acid transporters that are expressed highly in almost all malignant cells, but BSH cannot pass through the cell membrane and remains outside the cell. We simulated the energy transfer against the nucleus at different locations of boron from outside the cell to the nuclear region with neutron irradiation and concluded that there was a marked difference between inside and outside the cell in boron localization. To overcome this disadvantage of BSH in BNCT, we used a cell-penetrating peptide system for transduction of BSH. CPP (cell-membrane penetrating peptide) is very common peptide domains that transduce many physiologically active substances into cells in vitro and in vivo. BSH-fused CPPs can penetrate the cell membrane and localize inside a cell. To increase the boron ratio in one BSH-peptide molecule, 8BSH fused to 11R with a dendritic lysine structure was synthesized and administrated to malignant glioma cells and a brain tumor mouse model. 8BSH-11R localized at the cell nucleus and showed a very high boron value in ICP results. With neutron irradiation, the 8BSH-11R administrated group showed a significant cancer killing effect compared to the 100 times higher concentration of BSH-administrated group. We concluded that BSH-fused CPPs were one of the most improved and potential boron compounds in the next-stage BNCT trial and 8BSH-11R may be applied in the clinical setting.

Published

2013

50. Theranostic Protein Targeting ErbB2 for Bioluminescence Imaging and Therapy for Cancer

Author

Bin Feng, Hideki Matsui, Xiao Jian Han, Hiroyuki Michiue, Yuki Nishiyama, Ling Fei Sun, Kazuhito Tomizawa, and Masaharu Seno

Subjects

Receptor, ErbB-2, Recombinant Fusion Proteins, lcsh:Medicine, Gene Expression, Mice, Nude, Antineoplastic Agents, Biology, medicine.disease_cause, Ligands, Gaussia, Mice, Cell Line, Tumor, Neoplasms, Protein targeting, medicine, Bioluminescence, Bioluminescence imaging, Animals, Humans, Luciferase, Molecular Targeted Therapy, lcsh:Science, skin and connective tissue diseases, Cell Proliferation, Multidisciplinary, Protein Stability, lcsh:R, Optical Imaging, Cancer, medicine.disease, biology.organism_classification, Molecular biology, In vitro, Molecular Imaging, Tumor Burden, Disease Models, Animal, Luminescent Measurements, Cancer research, Heterografts, lcsh:Q, Female, Molecular imaging, Research Article, Protein Binding

Abstract

A combination of molecular-targeted cancer imaging and therapy is an emerging strategy to improve cancer diagnosis and minimize the side effects of conventional treatments. Here, we generated a recombinant protein, EC1-GLuc-p53C, by fusing EC1 peptide, an artificial ligand of ErbB2, with Gaussia luciferase (GLuc) and a p53-activating peptide, p53C. EC1-GLuc-p53C was expressed and purified from E. coli BL21. In vitro experiments showed that EC1-GLuc-p53c was stable in luminescent activity and selectively targeted ErbB2-overexpressing BT474 cells for bioluminescence imaging. Moreover, the internalized EC1-GLuc-p53C in BT474 cells exerted its function to reactivate p53 and significantly inhibited cellular proliferation. In tumor-bearing mice, the ErbB2-targeted bioluminescence imaging and therapeutic effect of EC1-GLuc-p53C were also observed specifically in BT474 tumors but not in MCF7 tumors, which does not overexpress ErbB2. Thus, the present study demonstrates EC1-GLuc-p53C to be an effective theranostic reagent targeting ErbB2 for bioluminescence imaging and cancer therapy.

Published

2013