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1. Clinical significance of CDKN2A homozygous deletion in combination with methylated MGMT status for IDH-wildtype glioblastoma.

Author

Funakoshi, Yusuke, Hata, Nobuhiro, Takigawa, Kosuke, Arita, Hideyuki, Kuga, Daisuke, Hatae, Ryusuke, Sangatsuda, Yuhei, Fujioka, Yutaka, Sako, Aki, Umehara, Toru, Yoshitake, Tadamasa, Togao, Osamu, Hiwatashi, Akio, Yoshimoto, Koji, Iwaki, Toru, and Mizoguchi, Masahiro

Subjects
CDKN2A, IDH-wildtype, MGMT, glioblastoma, survival, Aged, Antineoplastic Agents, Immunological, Bevacizumab, Brain Neoplasms, Cyclin-Dependent Kinase Inhibitor p16, DNA Methylation, DNA Modification Methylases, DNA Repair Enzymes, Female, Genetic Markers, Glioblastoma, Homozygote, Humans, Isocitrate Dehydrogenase, Male, Middle Aged, Prognosis, Retrospective Studies, Sequence Deletion, Tumor Suppressor Proteins
Abstract

OBJECTIVE: Accumulating evidence from recent molecular diagnostic studies has indicated the prognostic significance of various genetic markers for patients with glioblastoma (GBM). To evaluate the impact of such genetic markers on prognosis, we retrospectively analyzed the outcomes of patients with IDH-wildtype GBM in our institution. In addition, to assess the impact of bevacizumab (BEV) treatment, we compared overall survival (OS) between the pre- and post-BEV eras. METHODS: We analyzed the data of 100 adult patients (over 18 years old) with IDH-wildtype GBM from our database between February 2006 and October 2018. Genetic markers, such as MGMT methylation status, EGFR amplification, CDKN2A homozygous deletion, and clinical factors were analyzed by evaluating the patients OS. RESULTS: CDKN2A homozygous deletion showed no significant impact on OS in patients with methylated MGMT status (p = 0.5268), whereas among patients with unmethylated MGMT status, there was a significant difference in OS between patients with and without CDKN2A homozygous deletion (median OS: 14.7 and 16.9 months, respectively, p = 0.0129). This difference was more evident in the pre-BEV era (median OS: 10.1 and 15.6 months, respectively, p = 0.0351) but has become nonsignificant in the post-BEV era (median OS: 16.0 and 16.9 months, respectively, p = 0.1010) due to OS improvement in patients with CDKN2A homozygous deletion. However, these findings could not be validated in The Cancer Genome Atlas cohort. CONCLUSIONS: MGMT and CDKN2A status subdivided our cohort into three race-specific groups with different prognoses. Our findings indicate that BEV approval in Japan led to OS improvement exclusively for patients with concurrent unmethylated MGMT status and CDKN2A homozygous deletion.

Published
2021

2. Molecular diagnosis of diffuse glioma using a chip-based digital PCR system to analyze IDH, TERT, and H3 mutations in the cerebrospinal fluid.

Author

Fujioka, Yutaka, Hata, Nobuhiro, Akagi, Yojiro, Kuga, Daisuke, Hatae, Ryusuke, Sangatsuda, Yuhei, Michiwaki, Yuhei, Amemiya, Takeo, Takigawa, Kosuke, Funakoshi, Yusuke, Sako, Aki, Iwaki, Toru, Iihara, Koji, and Mizoguchi, Masahiro

Subjects
Cerebrospinal fluid, Chip-based digital PCR, Diffuse glioma, Liquid biopsy, ctDNA, Adolescent, Adult, Aged, Biomarkers, Tumor, Brain Neoplasms, Circulating Tumor DNA, DNA Mutational Analysis, Female, Glioma, Histones, Humans, Isocitrate Dehydrogenase, Liquid Biopsy, Male, Middle Aged, Mutation, Pathology, Molecular, Polymerase Chain Reaction, Telomerase, Young Adult
Abstract

PURPOSE: Conventional genetic analyzers require surgically obtained tumor tissues to confirm the molecular diagnosis of diffuse glioma. Recent technical breakthroughs have enabled increased utilization of cell-free tumor DNA (ctDNA) in body fluids as a reliable resource for molecular diagnosis in various cancers. Here, we tested the application of a chip-based digital PCR system for the less invasive diagnosis (i.e., liquid biopsy) of diffuse glioma using the cerebrospinal fluid (CSF). METHODS: CSF samples from 34 patients with diffuse glioma were collected from the surgical field during craniotomy. Preoperative lumbar CSF collection was also performed in 11 patients. Extracted ctDNA was used to analyze diagnostic point mutations in IDH1 R132H, TERT promoter (C228T and C250T), and H3F3A (K27M) on the QuantStudio® 3D Digital PCR System. These results were compared with their corresponding tumor DNA samples. RESULTS: We detected either of the diagnostic mutations in tumor DNA samples from 28 of 34 patients. Among them, we achieved precise molecular diagnoses using intracranial CSF in 20 (71%). Univariate analyses revealed that the World Health Organization (WHO) grade (p = 0.0034), radiographic enhancement (p = 0.0006), and Mib1 index (p = 0.01) were significant predictors of precise CSF-based molecular diagnosis. We precisely diagnosed WHO grade III or IV diffuse gliomas using lumbar CSF obtained from 6 (87%) of 7 patients with tumors harboring any mutation. CONCLUSION: We established a novel, non-invasive molecular diagnostic method using a chip-based digital PCR system targeting ctDNA derived from CSF with high sensitivity and specificity, especially for high-grade gliomas.

Published
2021

3. Author Correction: Comparative profiling of cortical gene expression in Alzheimer’s disease patients and mouse models demonstrates a link between amyloidosis and neuroinflammation

Author

Castillo, Erika, Leon, Julio, Mazzei, Guianfranco, Abolhassani, Nona, Haruyama, Naoki, Saito, Takashi, Saido, Takaomi, Hokama, Masaaki, Iwaki, Toru, Ohara, Tomoyuki, Ninomiya, Toshiharu, Kiyohara, Yutaka, Sakumi, Kunihiko, LaFerla, Frank M, and Nakabeppu, Yusaku

Subjects
Biochemistry and Cell Biology, Biological Sciences
Abstract

This article contains errors in the Introduction, where “AppNL-G-F/NL-G-F mice carrying the homozygous mutant App gene encoding the humanised Aβ sequence (G601R, F606Y, and R609H) with three pathogenic mutations, namely Swedish (KM595/596NL), Beyreuther/Iberian (I641F), and Arctic (E618G)10, progressively exhibit Aβ accumulation starting at 4 to 6 months of age, dense distributions of microglia and astrocytes from 9 months of age, and behavioural symptoms from 8 to 12 months of age10,11.” should read: “AppNL-G-F/NL-G-F mice carrying the homozygous mutant App gene encoding the humanised Aβ sequence (G676R, F681Y, and R684H) with three pathogenic mutations, namely Swedish (KM670/671NL), Beyreuther/Iberian (I716F), and Arctic (E693G)10, progressively exhibit Aβ accumulation starting at 4 to 6 months of age, dense distributions of microglia and astrocytes from 9 months of age, and behavioural symptoms from 8 to 12 months of age10,11.” In addition, in the Methods section, under the subheading ‘Animals’, “Heterozygous App+/NL-G-F mice carrying humanised Aβ sequence (G601R, F606Y, R609H), Swedish (ML595/596NL), Beyreuther/Iberian (I641F), and Arctic (E618G) mutations, were previously established10.” should read: “Heterozygous App+/NL-G-F mice carrying humanised Aβ sequence (G676R, F681Y, R684H), Swedish (KM670/671NL), Beyreuther/Iberian (I716F), and Arctic (E693G) mutations, were previously established10.”

Published
2021

4. CD206 Expression in Induced Microglia-Like Cells From Peripheral Blood as a Surrogate Biomarker for the Specific Immune Microenvironment of Neurosurgical Diseases Including Glioma.

Author

Tanaka, Shunya, Ohgidani, Masahiro, Hata, Nobuhiro, Inamine, Shogo, Sagata, Noriaki, Shirouzu, Noritoshi, Mukae, Nobutaka, Suzuki, Satoshi, Hamasaki, Hideomi, Hatae, Ryusuke, Sangatsuda, Yuhei, Fujioka, Yutaka, Takigawa, Kosuke, Funakoshi, Yusuke, Iwaki, Toru, Hosoi, Masako, Iihara, Koji, Mizoguchi, Masahiro, and Kato, Takahiro

Subjects
CD206, glioma, induced microglia-like cells, microglia, surrogate biomarker, Antigens, CD, Antigens, Differentiation, Myelomonocytic, Biomarkers, Tumor, Brain Neoplasms, Calcium-Binding Proteins, Cells, Cultured, Feasibility Studies, Female, Glioma, Humans, Male, Membrane Glycoproteins, Microfilament Proteins, Microglia, Monitoring, Immunologic, Phenotype, Prognosis, Receptors, Immunologic, Tumor Microenvironment
Abstract

Targeting the unique glioma immune microenvironment is a promising approach in developing breakthrough immunotherapy treatments. However, recent advances in immunotherapy, including the development of immune checkpoint inhibitors, have not improved the outcomes of patients with glioma. A way of monitoring biological activity of immune cells in neural tissues affected by glioma should be developed to address this lack of sensitivity to immunotherapy. Thus, in this study, we sought to examine the feasibility of non-invasive monitoring of glioma-associated microglia/macrophages (GAM) by utilizing our previously developed induced microglia-like (iMG) cells. Primary microglia (pMG) were isolated from surgically obtained brain tissues of 22 patients with neurological diseases. iMG cells were produced from monocytes extracted from the patients peripheral blood. Quantitative reverse transcription-polymerase chain reaction (qRT-PCR) revealed a significant correlation of the expression levels of representative markers for M1 and M2 microglia phenotypes between pMG and the corresponding iMG cells in each patient (Spearmans correlation coefficient = 0.5225, P

Published
2021

7. Comparative profiling of cortical gene expression in Alzheimers disease patients and mouse models demonstrates a link between amyloidosis and neuroinflammation.

Author

Castillo, Erika, Leon, Julio, Mazzei, Guianfranco, Abolhassani, Nona, Haruyama, Naoki, Saito, Takashi, Saido, Takaomi, Hokama, Masaaki, Iwaki, Toru, Ohara, Tomoyuki, Ninomiya, Toshiharu, Kiyohara, Yutaka, Sakumi, Kunihiko, Nakabeppu, Yusaku, and LaFerla, Frank

Subjects
Aged, Aged, 80 and over, Alzheimer Disease, Amyloid beta-Peptides, Amyloidosis, Animals, Brain, Disease Models, Animal, Female, Gene Expression, Gene Expression Profiling, Genome-Wide Association Study, Gliosis, Humans, Inflammation, Male, Mice, Middle Aged
Abstract

Alzheimers disease (AD) is the most common form of dementia, characterized by accumulation of amyloid β (Aβ) and neurofibrillary tangles. Oxidative stress and inflammation are considered to play an important role in the development and progression of AD. However, the extent to which these events contribute to the Aβ pathologies remains unclear. We performed inter-species comparative gene expression profiling between AD patient brains and the App NL-G-F/NL-G-F and 3xTg-AD-H mouse models. Genes commonly altered in App NL-G-F/NL-G-F and human AD cortices correlated with the inflammatory response or immunological disease. Among them, expression of AD-related genes (C4a/C4b, Cd74, Ctss, Gfap, Nfe2l2, Phyhd1, S100b, Tf, Tgfbr2, and Vim) was increased in the App NL-G-F/NL-G-F cortex as Aβ amyloidosis progressed with exacerbated gliosis, while genes commonly altered in the 3xTg-AD-H and human AD cortices correlated with neurological disease. The App NL-G-F/NL-G-F cortex also had altered expression of genes (Abi3, Apoe, Bin2, Cd33, Ctsc, Dock2, Fcer1g, Frmd6, Hck, Inpp5D, Ly86, Plcg2, Trem2, Tyrobp) defined as risk factors for AD by genome-wide association study or identified as genetic nodes in late-onset AD. These results suggest a strong correlation between cortical Aβ amyloidosis and the neuroinflammatory response and provide a better understanding of the involvement of gender effects in the development of AD.

Published
2017

17. Clinicopathological review of solitary fibrous tumors: dedifferentiation is a major cause of patient death

Author

Yamada, Yuichi, Kohashi, Kenichi, Kinoshita, Izumi, Yamamoto, Hidetaka, Iwasaki, Takeshi, Yoshimoto, Masato, Ishihara, Shin, Toda, Yu, Itou, Yoshihiro, Koga, Yutaka, Hashisako, Mikiko, Nozaki, Yui, Kiyozawa, Daisuke, Kitahara, Daichi, Inoue, Takeshi, Mukai, Munenori, Honda, Yumi, Toyokawa, Gouji, Tsuchihashi, Kenji, Matsushita, Yoshifumi, Fushimi, Fumiyoshi, Taguchi, Kenichi, Tamiya, Sadafumi, Oshiro, Yumi, Furue, Masutaka, Nakashima, Yasuharu, Suzuki, Satoshi, Iwaki, Toru, and Oda, Yoshinao

Published
2019
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22. Neuropathology of spinocerebellar ataxia type 8: Common features and unique tauopathy.

Author

Yonenobu, Yuki, Beck, Goichi, Kido, Kansuke, Maeda, Norihisa, Yamashita, Rika, Inoue, Kimiko, Saito, Yuko, Hasegawa, Masato, Ito, Hidefumi, Hasegawa, Kazuko, Morii, Eiichi, Iwaki, Toru, Murayama, Shigeo, and Mochizuki, Hideki

Subjects
SPINOCEREBELLAR ataxia, TAUOPATHIES, PROGRESSIVE supranuclear palsy, FACIOSCAPULOHUMERAL muscular dystrophy, NEUROLOGICAL disorders, SUBSTANTIA nigra, CEREBELLAR cortex, AUTOPSY
Abstract

Spinocerebellar ataxia type 8 (SCA8) is a neurodegenerative condition that presents with several neurological symptoms, such as cerebellar ataxia, parkinsonism, and cognitive impairment. It is caused by a CTA/CTG repeat expansion on chromosome 13q21 (ataxin 8 opposite strand [ATXN8OS]). However, the pathological significance of this expansion remains unclear. Moreover, abnormal CTA/CTG repeat expansions in ATXN8OS have also been reported in other neurodegenerative diseases, including progressive supranuclear palsy. In this study, we analyzed all available autopsy cases in Japan to investigate common pathological features and profiles of tau pathology in each case. Severe neuronal loss in the substantia nigra and prominent loss of Purkinje cells, atrophy of the molecular layer, and proliferation of Bergmann glia in the cerebellum were common features. Regarding tauopathy, one case presented with progressive supranuclear palsy‐like 4‐repeat tauopathy in addition to mild Alzheimer‐type 3‐ and 4‐repeat tauopathy. Another case showed 3‐ and 4‐repeat tauopathy accentuated in the brainstem. The other two cases lacked tauopathy after extensive immunohistochemical studies. The present study confirmed common pathological features of SCA8 as degeneration of the substantia nigra in addition to the cerebellum. Our study also confirmed unique tauopathy in two of four cases, indicating the necessity to further collect autopsy cases. [ABSTRACT FROM AUTHOR]

Published
2023
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23. Corrigendum to “MUTYH Actively Contributes to Microglial Activation and Impaired Neurogenesis in the Pathogenesis of Alzheimer’s Disease”

Author

Mizuno, Yuri, primary, Abolhassani, Nona, additional, Mazzei, Guianfranco, additional, Sakumi, Kunihiko, additional, Saito, Takashi, additional, Saido, Takaomi C., additional, Ninomiya, Toshiharu, additional, Iwaki, Toru, additional, Yamasaki, Ryo, additional, Kira, Jun-ichi, additional, and Nakabeppu, Yusaku, additional

Published
2023
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29. Early and extensive alterations of glial connexins, distal oligodendrogliopathy type demyelination, and nodal/paranodal pathology are characteristic of multiple system atrophy

Author

Nishimura, Yuji, primary, Masaki, Katsuhisa, additional, Matsuse, Dai, additional, Yamaguchi, Hiroo, additional, Tanaka, Tatsunori, additional, Matsuo, Eriko, additional, Hayashida, Shotaro, additional, Watanabe, Mitsuru, additional, Matsushita, Takuya, additional, Sadashima, Shoko, additional, Sasagasako, Naokazu, additional, Yamasaki, Ryo, additional, Isobe, Noriko, additional, Iwaki, Toru, additional, and Kira, Jun‐ichi, additional

Published
2022
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30. Neuropathology of classic myotonic dystrophy type 1 is characterized by both early initiation of primary age-related tauopathy of the hippocampus and unique 3-repeat tauopathy of the brainstem

Author

Hamasaki, Hideomi, primary, Maeda, Norihisa, additional, Sasagasako, Naokazu, additional, Honda, Hiroyuki, additional, Shijo, Masahiro, additional, Mori, Shin-Ichiro, additional, Yagita, Kaoru, additional, Arahata, Hajime, additional, and Iwaki, Toru, additional

Published
2022
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41. Early and extensive alterations of glial connexins, distal oligodendrogliopathy type demyelination, and nodal/paranodal pathology are characteristic of multiple system atrophy.

Author

Nishimura, Yuji, Masaki, Katsuhisa, Matsuse, Dai, Yamaguchi, Hiroo, Tanaka, Tatsunori, Matsuo, Eriko, Hayashida, Shotaro, Watanabe, Mitsuru, Matsushita, Takuya, Sadashima, Shoko, Sasagasako, Naokazu, Yamasaki, Ryo, Isobe, Noriko, Iwaki, Toru, and Kira, Jun‐ichi

Subjects
MULTIPLE system atrophy, CONNEXINS, MYELIN oligodendrocyte glycoprotein, DEMYELINATION, TUBULINS, ALPHA-synuclein
Abstract

The pathological hallmark of multiple system atrophy (MSA) is aberrant accumulation of phosphorylated α‐synuclein in oligodendrocytes, forming glial cytoplasmic inclusions (GCIs). Extensive demyelination occurs particularly in the olivopontocerebellar and striatonigral pathways, but its precise mechanism remains elusive. Glial connexins (Cxs), which form gap junction channels between astrocytes and oligodendrocytes, play critical roles in myelin maintenance, and have not been studied in MSA. Therefore, we immunohistochemically investigated glial Cx changes in the cerebellar afferent fibers in 15 autopsied patients with MSA. We classified demyelinating lesions into three stages based on Klüver–Barrera staining: early (Stage I), intermediate (Stage II), and late (Stage III) stages showing subtle, moderate, and severe myelin reduction, respectively. Myelin‐associated glycoprotein, but not myelin oligodendrocyte glycoprotein, was preferentially decreased in Stage I, suggesting distal oligodendrogliopathy type demyelination. Accumulation of phosphorylated α‐synuclein in oligodendrocytes was frequently seen in Stage I but less frequently observed in Stages II and III. Tubulin polymerization‐promoting protein (TPPP/p25α)‐positive oligodendrocytes were preserved in Stage I but successively decreased in Stages II and III. Even at Stage I, Cx32 was nearly absent from myelin, despite the relative preservation of other nodal proteins, such as neurofascin, claudin‐11/oligodendrocyte‐specific protein, and contactin‐associated protein 1, which successively decreased in the later stages. Cx32 was re‐distributed in the oligodendrocyte cytoplasm and co‐localized with GCIs. Cx47 gradually decreased at the oligodendrocyte surface in a stage‐dependent manner but was not co‐localized with GCIs. Astrocytic Cx43 was down‐regulated in Stage I but up‐regulated in Stages II and III, reflecting astrogliosis. Cx43/Cx47 gap junctions significantly decreased from Stage I to III. Activated microglia/macrophages and T cells infiltrated in Stage I rather than Stages II and III. Therefore, early and extensive alterations of glial Cxs, particularly Cx32 loss, occur in MSA and may accelerate distal oligodendrogliopathy type demyelination and nodal/paranodal dysfunction through disruption of inter‐glial communication. [ABSTRACT FROM AUTHOR]

Published
2023
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45. A case of ganglioglioma grade 3 with H3 K27M mutation arising in the medial temporal lobe in an elderly patient

Author

Fujii, Yutaro, primary, Hatae, Ryusuke, additional, Hata, Nobuhiro, additional, Suzuki, Satoshi O., additional, Sangatsuda, Yuhei, additional, Takigawa, Kosuke, additional, Funakoshi, Yusuke, additional, Fujioka, Yutaka, additional, Kuga, Daisuke, additional, Mizoguchi, Masahiro, additional, Iwaki, Toru, additional, and Yoshimoto, Koji, additional

Published
2022
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50. MUTYH Actively Contributes to Microglial Activation and Impaired Neurogenesis in the Pathogenesis of Alzheimer’s Disease

Author

Mizuno, Yuri, primary, Abolhassani, Nona, additional, Mazzei, Guianfranco, additional, Sakumi, Kunihiko, additional, Saito, Takashi, additional, Saido, Takaomi C., additional, Ninomiya, Toshiharu, additional, Iwaki, Toru, additional, Yamasaki, Ryo, additional, Kira, Jun-ichi, additional, and Nakabeppu, Yusaku, additional

Published
2021
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