Your search keyword '"Masashi Sanada"' showing total 134 results

1. Oncogenic lesions and molecular subtypes in adults with B‐cell acute lymphoblastic leukemia

Author

Takahiko Yasuda, Masashi Sanada, Shinobu Tsuzuki, and Fumihiko Hayakawa

Subjects

Gene Rearrangement, Young Adult, Cancer Research, Adolescent, Oncology, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, Mutation, Humans, General Medicine, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Prognosis, Burkitt Lymphoma

Abstract

B-cell acute lymphoblastic leukemia (B-ALL), a genetically heterogeneous disease, is classified into different molecular subtypes that are defined by recurrent gene rearrangements, gross chromosomal abnormalities, or specific gene mutations. Cells with these genetic alterations acquire a leukemia-initiating ability and show unique expression profiles. The distribution of B-ALL molecular subtypes is greatly dependent on age, which also affects treatment responsiveness and long-term survival, partly accounting for the inferior outcome in adolescents and young adults (AYA) and (older) adults with B-ALL. Recent advances in sequencing technology, especially RNA sequencing and the application of these technologies in large B-ALL cohorts have uncovered B-ALL molecular subtypes prevalent in AYA and adults. These new insights supply more precise estimations of prognoses and targeted therapies informed by sequencing results, as well as a deeper understanding of the genetic basis of AYA/adult B-ALL. This article provides an account of these technological advances and an overview of the recent major findings of B-ALL molecular subtypes in adults.

Published

2022

2. Functional inhibition of MEF2 by C/EBP is a possible mechanism of leukemia development by CEBP-IGH fusion gene

Author

Koya Odaira, Takahiko Yasuda, Kentaro Okada, Takuya Shimooka, Yukino Kojima, Mina Noura, Shogo Tamura, Shingo Kurahashi, Eisuke Iwamoto, Masashi Sanada, Itaru Matsumura, Yasushi Miyazaki, Tetsuhito Kojima, Hitoshi Kiyoi, Shinobu Tsuzuki, and Fumihiko Hayakawa

Subjects

Cancer Research, Oncology, General Medicine

Abstract

CEBPA-IGH, a fusion gene of the immunoglobulin heavy-chain locus (IGH) and the CCAAT enhancer-binding protein α (C/EBPα) gene, is recurrently found in B-ALL cases and causes aberrant expression of C/EBPα, a master regulator of granulocyte differentiation, in B cells. Forced expression of C/EBPα in B cells was reported to cause loss of B-cell identity due to the inhibition of Pax5, a master regulator of B-cell differentiation; however, it is not known whether the same mechanism is applicable for B-ALL development by CEBPA-IGH. It is known that a full-length isoform of C/EBPα, p42, promotes myeloid differentiation, whereas its N-terminal truncated isoform, p30, inhibits myeloid differentiation through the inhibition of p42; however, the differential role between p42 and p30 in ALL development has not been clarified. In the present study, we examined the effect of the expression of p42 and p30 in B cells by performing RNA-seq of mRNA from LCL stably transfected with p42 or p30. Unexpectedly, suppression of PAX5 target genes was barely observed. Instead, both isoforms suppressed the target genes of MEF2 family members (MEF2s), other regulators of B-cell differentiation. Similarly, MEF2s target genes rather than PAX5 target genes were suppressed in CEBP-IGH-positive ALL (n = 8) compared with other B-ALL (n = 315). Furthermore, binding of both isoforms to MEF2s target genes and the reduction of surrounding histone acetylation were observed in ChIP-qPCR. Our data suggest that the inhibition of MEF2s by C/EBPα plays a role in the development of CEBPA-IGH-positive ALL and that both isoforms work co-operatively to achieve it.

Published

2022

3. Clinical characteristics and outcomes of B-cell precursor ALL with MEF2D rearrangements: a retrospective study by the Ponte di Legno Childhood ALL Working Group

Author

Kentaro Ohki, Ellie R. Butler, Nobutaka Kiyokawa, Shinsuke Hirabayashi, Anke K. Bergmann, Anja Möricke, Judith M. Boer, Hélène Cavé, Giovanni Cazzaniga, Allen Eng Juh Yeoh, Masashi Sanada, Toshihiko Imamura, Hiroto Inaba, Charles G. Mullighan, Mignon L. Loh, Ulrika Norén-Nyström, Lee-Yung Shih, Marketa Zaliova, Ching-Hon Pui, Oskar A. Haas, Christine J. Harrison, Anthony V. Moorman, and Atsushi Manabe

Subjects

Cancer och onkologi, Cancer Research, Oncology, Cancer and Oncology, Pediatrik, Hematology, Pediatrics

Published

2022

4. Clinical utility of target capture‐based panel sequencing in hematological malignancies: A multicenter feasibility study

Author

Masashi Sanada, Hiroaki Miyoshi, Takahiko Yasuda, Yasushi Miyazaki, Ryoji Kobayashi, Hirohiko Shibayama, Koichi Ohshima, Yuichi Shiraishi, Akihiro Tomita, Tadao Ishida, Yuichi Ishikawa, Masaki Ri, Shinsuke Iida, Kenichi Yoshida, Keisuke Kataoka, Takashi Kanamori, Dai Nishijima, Norio Asou, Hiroshi Handa, Akiko Saito, Hitoshi Kiyoi, Kensuke Usuki, Souichi Adachi, Hiroki Kurahashi, Atsushi Manabe, Hiroyoshi Hattori, Kennosuke Karube, Keizo Horibe, Yuka Iijima, Motohiro Kato, Hisayuki Yokoyama, Shinsuke Hirabayashi, Chisako Iriyama, Momoko Nishikori, Seishi Ogawa, Masahiro Abe, and Hiroaki Goto

Subjects

Male, 0301 basic medicine, Oncology, Cancer Research, clinical sequencing, potentially actionable finding, 0302 clinical medicine, hemic and lymphatic diseases, Child, Genetics, Genomics, and Proteomics, Multiple myeloma, Aged, 80 and over, High-Throughput Nucleotide Sequencing, feasibility study, Myeloid leukemia, General Medicine, Middle Aged, Child, Preschool, Hematologic Neoplasms, 030220 oncology & carcinogenesis, Female, Original Article, Adult, medicine.medical_specialty, Adolescent, Childhood leukemia, Genetic counseling, panel testing, Young Adult, 03 medical and health sciences, Internal medicine, Biomarkers, Tumor, medicine, Humans, Genetic Predisposition to Disease, Clinical significance, Genetic Testing, Genetic Association Studies, Germ-Line Mutation, Aged, hematological malignancy, business.industry, Infant, Newborn, Computational Biology, Infant, Reproducibility of Results, Adult Acute Myeloid Leukemia, Original Articles, medicine.disease, Lymphoma, Clinical trial, 030104 developmental biology, business

Abstract

Although next‐generation sequencing‐based panel testing is well practiced in the field of cancer medicine for the identification of target molecules in solid tumors, the clinical utility and clinical issues surrounding panel testing in hematological malignancies have yet to be fully evaluated. We conducted a multicenter prospective clinical sequencing study to verify the feasibility of a panel test for hematological tumors, including acute myeloid leukemia, acute lymphoblastic leukemia, multiple myeloma, and diffuse large B‐cell lymphoma. Out of 96 eligible patients, 79 patients (82%) showed potentially actionable findings, based on the clinical sequencing assays. We identified that genetic alterations with a strong clinical significance were found at a higher frequency in terms of diagnosis (n = 60; 63%) and prognosis (n = 61; 64%) than in terms of therapy (n = 8; 8%). Three patients who harbored a germline mutation in either DDX41 (n = 2) or BRCA2 (n = 1) were provided with genetic counseling. At 6 mo after sequencing, clinical actions based on the diagnostic (n = 5) or prognostic (n = 3) findings were reported, but no patients were enrolled in a clinical trial or received targeted therapies based on the sequencing results. These results suggest that panel testing for hematological malignancies would be feasible given the availability of useful diagnostic and prognostic information. This study is registered with the UMIN Clinical Trial Registry (UMIN000029879, multiple myeloma; UMIN000031343, adult acute myeloid leukemia; UMIN000033144, diffuse large B‐cell lymphoma; and UMIN000034243, childhood leukemia)., This multicenter prospective study investigated feasibility of target capture‐based panel testing, focusing on hematological malignancies. Our results suggest that panel testing for hematological malignancies is feasible given the availability of useful diagnostic and prognostic information.

Published

2020

5. Frequent mutations that converge on the NFKBIZ pathway in ulcerative colitis

Author

Kenichi Chiba, Tomonori Hirano, Norihiro Goto, Akira Yokoyama, Yusuke Shiozawa, Hironori Haga, Ayana Kon, Seishi Ogawa, Yosaku Watatani, Yasunori Kogure, Tsutomu Chiba, Makoto Mark Taketo, Yuichi Shiraishi, Hideki Makishima, Takaaki Sato, Kenichi Yoshida, Takaki Sakurai, Ryosaku Inagaki, Takako Kihara, Takashi Maruyama, Takahiro Horimatsu, Jun Oishi, Kotaro Akaki, Eiji Sugihara, Hiroko Tanaka, Hiroki Ikeuchi, Osamu Takeuchi, Yoichi Fujii, Akinori Yoda, Hiroyuki Miyoshi, Yasuhito Nanya, Motoi Uchino, Tetsuichi Yoshizato, Yoshikage Inoue, Yoshiharu Sakai, Satoshi Nagayama, Kenji Kawada, Hiroshi Nakase, Seiichi Hirota, Yasuhide Takeuchi, Soo Ki Kim, Minoru Matsuura, Hideaki Okajima, Shinya Okamoto, Yotaro Ochi, Shuji Yamamoto, Hiroshi Seno, Masahiro Nakagawa, Nobuyuki Kakiuchi, Yutaka Ueda, Hiroyuki Marusawa, Satoru Miyano, Keisuke Kataoka, and Masashi Sanada

Subjects

0301 basic medicine, Multidisciplinary, Colorectal cancer, Cancer, Inflammation, Biology, medicine.disease, medicine.disease_cause, Ulcerative colitis, 03 medical and health sciences, Negative selection, 030104 developmental biology, 0302 clinical medicine, Downregulation and upregulation, 030220 oncology & carcinogenesis, medicine, Cancer research, Colitis, medicine.symptom, Carcinogenesis

Abstract

Chronic inflammation is accompanied by recurring cycles of tissue destruction and repair and is associated with an increased risk of cancer1–3. However, how such cycles affect the clonal composition of tissues, particularly in terms of cancer development, remains unknown. Here we show that in patients with ulcerative colitis, the inflamed intestine undergoes widespread remodelling by pervasive clones, many of which are positively selected by acquiring mutations that commonly involve the NFKBIZ, TRAF3IP2, ZC3H12A, PIGR and HNRNPF genes and are implicated in the downregulation of IL-17 and other pro-inflammatory signals. Mutational profiles vary substantially between colitis-associated cancer and non-dysplastic tissues in ulcerative colitis, which indicates that there are distinct mechanisms of positive selection in both tissues. In particular, mutations in NFKBIZ are highly prevalent in the epithelium of patients with ulcerative colitis but rarely found in both sporadic and colitis-associated cancer, indicating that NFKBIZ-mutant cells are selected against during colorectal carcinogenesis. In further support of this negative selection, we found that tumour formation was significantly attenuated in Nfkbiz-mutant mice and cell competition was compromised by disruption of NFKBIZ in human colorectal cancer cells. Our results highlight common and discrete mechanisms of clonal selection in inflammatory tissues, which reveal unexpected cancer vulnerabilities that could potentially be exploited for therapeutics in colorectal cancer. In patients with ulcerative colitis, chronic inflammation can lead to remodelling of the colorectal epithelium through positive selection of clones with mutations in genes related to IL-17 signalling, which, however, might be negatively selected during colitis-associated carcinogenesis.

Published

2019

6. Genetic features of B-cell lymphoblastic lymphoma with TCF3-PBX1

Author

Masashi Sanada, Motohiro Kato, Takeshi Mori, Nobutaka Kiyokawa, Mikiya Endo, Kenichiro Hata, Takako Yoshioka, Masatoshi Takagi, Seishi Ogawa, Mika Kohri, Tomoo Osumi, Aiko Sato-Otsubo, Ryota Shirai, Kazuhiko Nakabayashi, Masanori Yoshida, Kentaro Ohki, Toshihiko Imamura, Satoshi Miyamoto, Shiho Yasue, Takashi Ishihara, and Kaoru Yoshida

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Oncogene Proteins, Fusion, business.industry, Somatic cell, Lymphoblastic lymphoma, Pre-B-Cell Leukemia Transcription Factor 1, Clone (cell biology), Disease, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, medicine.anatomical_structure, Internal medicine, medicine, Basic Helix-Loop-Helix Transcription Factors, Humans, Bone marrow, Stage (cooking), business, Exome sequencing, B cell

Abstract

Background Lymphoblastic lymphoma (LBL) and acute lymphoblastic leukemia (ALL) are categorized as the same entity under precursor lymphoid neoplasms in the World Health Organization classification. However, compared to B-cell ALL, the molecular genetic makeup of B-cell LBL remains to be understood, mainly due to its rarity. We performed whole exome sequencing (WES) on seven patients with TCF3-PBX1-positive B-cell LBL. Methods WES was performed using DNA extracted from tumor specimens and paired blood samples at remission for six patients, and tumor-only analysis was performed for one patient whose remission sample was not available. For one patient, a relapsed sample was also analyzed. Results KMT2D variants and 6q LOH were found as recurrent alterations. Somatic variants of KMT2D were identified in three of the seven patients. Of note, the two patients with heterozygous nonsense variant of KMT2D were at stage III, without bone marrow infiltration. 6q LOH was also identified in two others, out of the seven patients. The common 6q deleted region of the two patients ranged from 6q12 to 6q16.3. Both patients had bone marrow infiltration. Analysis of recurrent case also revealed that the relapsed clone might be derived from a minor clone of the bone marrow at diagnosis. Conclusion In this study, through WES for seven patients with TCF3-PBX1-positive B-LBL, we identified KMT2D mutations and 6q LOH as recurrent alterations. In order to elucidate the relationship between these recurrent alterations and disease specificity or outcomes, further studies comparing with TCF3-PBX1-positive B-ALL are required.

Published

2021

7. DNA methylation-based classification reveals difference between pediatric T-cell acute lymphoblastic leukemia and normal thymocytes

Author

Kentaro Watanabe, Akira Ohara, Atsushi Manabe, Masao Kobayashi, Akira Oka, Tomoko Kawai, Atsushi Sato, Seishi Ogawa, Katsuyoshi Koh, Satoru Miyano, Yusuke Shiozawa, Hiromichi Suzuki, Motohiro Kato, Shunsuke Kimura, Yoshiko Hashii, Masashi Sanada, Yasuo Kubota, Keizo Horibe, Hiroo Ueno, Junko Takita, Yasuhide Hayashi, Yasuhito Nannya, Nobutaka Kiyokawa, Yuichi Shiraishi, Ryoji Kobayashi, Masafumi Seki, Hiroaki Goto, Marc R. Mansour, Masahiro Sekiguchi, Kenichiro Hata, Takao Deguchi, Toshihiko Imamura, Kenichi Yoshida, Tomoya Isobe, and Kentaro Ohki

Subjects

Regulation of gene expression, Cancer Research, medicine.anatomical_structure, Oncology, T cell, Lymphoblastic Leukemia, DNA methylation, medicine, Cancer research, Hematology, Biology, Epigenesis

Published

2019

8. Molecular heterogeneity in peripheral T-cell lymphoma, not otherwise specified revealed by comprehensive genetic profiling

Author

Tetsuichi Yoshizato, Yuichi Shiraishi, Nobuyuki Kakiuchi, Kengo Takeuchi, Ryota Matsuoka, Hiroko Tanaka, Yusuke Kito, Kazuya Shimoda, Tadashi Yoshino, Kenji Nishida, Takayuki Ishikawa, Kenichi Chiba, Kana Sakamoto, Lanying Zhao, Yusuke Shiozawa, Hiroaki Miyoshi, Hiroo Ueno, Nobuhiro Hiramoto, Kenichi Yoshida, Koichi Ohshima, Junichi Kitagawa, Shigeru Chiba, Yasuhito Nanya, Hisashi Tsurumi, Masashi Sanada, Nobuhiko Nakamura, Yasunobu Nagata, Yasuhide Takeuchi, Satoru Miyano, Hideki Makishima, Masayuki Noguchi, June Takeda, Keisuke Kataoka, Tatsuhiko Miyazaki, Yasuharu Sato, Mamiko Sakata-Yanagimoto, Masahiro Nakagawa, Yotaro Ochi, Yasunori Kogure, Seishi Ogawa, Yosaku Watatani, and Yuka Gion

Subjects

Male, 0301 basic medicine, Genome instability, Cancer Research, DNA Copy Number Variations, Peripheral T-cell lymphoma not otherwise specified, Genomics, Computational biology, Biology, Genomic Instability, Genetic Heterogeneity, 03 medical and health sciences, 0302 clinical medicine, CDKN2A, Exome Sequencing, Biomarkers, Tumor, medicine, Humans, Genetic Predisposition to Disease, Allele, Alleles, Genetic Association Studies, Exome sequencing, Genetic heterogeneity, Gene Expression Profiling, Computational Biology, Genetic Variation, High-Throughput Nucleotide Sequencing, Lymphoma, T-Cell, Peripheral, Hematology, medicine.disease, Gene expression profiling, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Mutation, Female, Tumor Escape, Signal Transduction

Abstract

Peripheral T-cell lymphoma, not otherwise specified (PTCL, NOS) is a diagnosis of exclusion, being the most common entity in mature T-cell neoplasms, and its molecular pathogenesis remains significantly understudied. Here, combining whole-exome and targeted-capture sequencing, gene-expression profiling, and immunohistochemical analysis of tumor samples from 133 cases, we have delineated the entire landscape of somatic alterations, and discovered frequently affected driver pathways in PTCL, NOS, with and without a T-follicular helper (TFH) cell phenotype. In addition to previously reported mutational targets, we identified a number of novel recurrently altered genes, such as KMT2C, SETD1B, YTHDF2, and PDCD1. We integrated these genetic drivers using hierarchical clustering and identified a previously undescribed molecular subtype characterized by TP53 and/or CDKN2A mutations and deletions in non-TFH PTCL, NOS. This subtype exhibited different prognosis and unique genetic features associated with extensive chromosomal instability, which preferentially affected molecules involved in immune escape and transcriptional regulation, such as HLA-A/B and IKZF2. Taken together, our findings provide novel insights into the molecular pathogenesis of PTCL, NOS by highlighting their genetic heterogeneity. These results should help to devise a novel molecular classification of PTCLs and to exploit a new therapeutic strategy for this group of aggressive malignancies.

Published

2019

9. Frequent structural variations involving programmed death ligands in Epstein-Barr virus-associated lymphomas

Author

Masahiro Onozawa, Koji Izutsu, Tetsuichi Yoshizato, Kenshi Suzuki, Kenichi Chiba, Koichi Ohshima, Akihiro Tomita, Seiji Sakata, Yasunori Kogure, Kenichi Yoshida, Yumiko Yoshiki, Hiroko Tanaka, Lucile Couronné, Tadao Ishida, Kengo Takeuchi, Yuichi Shiraishi, Hiroaki Miyoshi, Yasuharu Sato, Masashi Sanada, Kazuyuki Shimada, Nobuyuki Kakiuchi, Olivier Hermine, Yoshiki Akatsuka, Yasunori Ota, Tadashi Yoshino, Ayako Demachi-Okamura, Yusuke Shiozawa, Kenji Nishida, Akito Dobashi, Philippe Gaulard, Motohiro Kato, Yuka Gion, Hideki Makishima, Seishi Ogawa, Yosaku Watatani, Takanori Teshima, Satoru Miyano, and Keisuke Kataoka

Subjects

0301 basic medicine, Epstein-Barr Virus Infections, Herpesvirus 4, Human, Cancer Research, Cellular immunity, Biology, Ligands, medicine.disease_cause, B7-H1 Antigen, Article, Virus, 03 medical and health sciences, 0302 clinical medicine, CDKN2A, hemic and lymphatic diseases, Biomarkers, Tumor, Cancer genomics, medicine, Humans, Tumour virus infections, Immunosurveillance, Genetic Variation, Lymphoma, T-Cell, Peripheral, Hematology, CD79B, Programmed Cell Death 1 Ligand 2 Protein, medicine.disease, Epstein–Barr virus, Immune checkpoint, Lymphoma, Gene Expression Regulation, Neoplastic, Lymphoma, Extranodal NK-T-Cell, Leukemia, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, Lymphoma, Large B-Cell, Diffuse

Abstract

Viral infection induces potent cellular immunity and activated intracellular signaling, which may dictate the driver events involved in immune escape and clonal selection of virus-associated cancers, including Epstein-Barr virus (EBV)-positive lymphomas. Here, we thoroughly interrogated PD-L1/PD-L2-involving somatic aberrations in 384 samples from various lymphoma subtypes using high-throughput sequencing, particularly focusing on virus-associated lymphomas. A high frequency of PD-L1/PD-L2-involving genetic aberrations was observed in EBV-positive lymphomas [33 (22%) of 148 cases], including extranodal NK/T-cell lymphoma (ENKTL, 23%), aggressive NK-cell leukemia (57%), systemic EBV-positive T-cell lymphoproliferative disorder (17%) as well as EBV-positive diffuse large B-cell lymphoma (DLBCL, 19%) and peripheral T-cell lymphoma-not otherwise specified (15%). Predominantly causing a truncation of the 3′-untranslated region, these alterations represented the most prevalent somatic lesions in ENKTL. By contrast, the frequency was much lower in EBV-negative lymphomas regardless of histology type [12 (5%) of 236 cases]. Besides PD-L1/PD-L2 alterations, EBV-positive DLBCL exhibited a genetic profile distinct from EBV-negative one, characterized by frequent TET2 and DNMT3A mutations and the paucity of CD79B, MYD88, CDKN2A, and FAS alterations. Our findings illustrate unique genetic features of EBV-associated lymphomas, also suggesting a potential role of detecting PD-L1/PD-L2-involving lesions for these lymphomas to be effectively targeted by immune checkpoint blockade.

Published

2019

10. Clinical characteristics and outcomes of B-ALL with ZNF384 rearrangements: a retrospective analysis by the Ponte di Legno Childhood ALL Working Group

Author

Christine J. Harrison, Anja Möricke, Ching-Hon Pui, Marketa Zaliova, Hiroto Inaba, Ulrika Norén-Nyström, Kentaro Ohki, Toshihiko Imamura, Judith M. Boer, Atsushi Manabe, Shinsuke Hirabayashi, Allen Eng Juh Yeoh, Oskar A. Haas, Masashi Sanada, Nobutaka Kiyokawa, Ellie Butler, Anke K. Bergmann, Giovanni Cazzaniga, Lee Yung Shih, Hélène Cavé, Anthony V. Moorman, Charles G. Mullighan, Agata Pastorczak, Mignon L. Loh, Hirabayashi, S, Butler, E, Ohki, K, Kiyokawa, N, Bergmann, A, Moricke, A, Boer, J, Cave, H, Cazzaniga, G, Yeoh, A, Sanada, M, Imamura, T, Inaba, H, Mullighan, C, Loh, M, Noren-Nystrom, U, Pastorczak, A, Shih, L, Zaliova, M, Pui, C, Haas, O, Harrison, C, Moorman, A, and Manabe, A

Subjects

Adult, Male, Cancer Research, Pediatrics, medicine.medical_specialty, Letter, Adolescent, MEDLINE, Acute lymphoblastic leukemia, Young Adult, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, Biomarkers, Tumor, Retrospective analysis, Humans, Medicine, Child, Cancer genetics, Childhood all, Retrospective Studies, Gene Rearrangement, Cancer och onkologi, Acute lymphocytic leukaemia, business.industry, Infant, Hematology, Prognosis, Survival Rate, Oncology, Child, Preschool, Cancer and Oncology, Trans-Activators, Female, business, Follow-Up Studies

Published

2021

11. Clonal evolution and clinical implications of genetic abnormalities in blastic transformation of chronic myeloid leukaemia

Author

Yotaro Ochi, Tomoiku Takaku, Yuichi Shiraishi, Kenichi Chiba, Masashi Sanada, Kazuma Ohyashiki, Lanying Zhao, Nobuhiko Nakamura, Takayuki Ishikawa, Hiroko Tanaka, Akifumi Takaori-Kondo, Nobuhiro Hiramoto, Lee-Yung Shih, June Takeda, Kenichi Yoshida, Satoru Miyano, Nobuhiro Kanemura, Kinuko Mitani, Rurika Okuda, Hideki Makishima, Susan Branford, Ming-Chung Kuo, Yasunori Ueda, Yasuhito Nannya, Rabindranath Bera, Naranie Shanmuganathan, Noriko Hosoya, Shun Tsuchiya, Naoto Takahashi, Yusuke Shiozawa, Satoshi Yoshihara, Ying-Jung Huang, Seishi Ogawa, Yosaku Watatani, Ko Sasaki, Ochi, Yotaro, Yoshida, Kenichi, Huang, Ying-Jung, Kuo, Ming-Chung, Branford, Susan, Shanmuganathan, Naranie, and Shih, Lee-Yung

Subjects

0301 basic medicine, TKIs, Male, Oncogene Proteins, Fusion, genetic abnormalities, General Physics and Astronomy, medicine.disease_cause, Somatic evolution in cancer, Cohort Studies, 0302 clinical medicine, hemic and lymphatic diseases, tyrosine kinase inhibitors, Medicine, Exome, CML, Cancer genetics, Aged, 80 and over, Mutation, Multidisciplinary, Transition (genetics), Blood Proteins, Middle Aged, Protein-Tyrosine Kinases, Prognosis, 030220 oncology & carcinogenesis, Cohort, Core Binding Factor Alpha 2 Subunit, Leukemia, Myeloid, Chronic-Phase, Female, Tyrosine kinase, Adult, Lineage (genetic), Adolescent, chronic myeloid leukaemia, Science, General Biochemistry, Genetics and Molecular Biology, Article, Proto-Oncogene Protein c-ets-2, Clonal Evolution, 03 medical and health sciences, Young Adult, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Exome Sequencing, Humans, Protein Kinase Inhibitors, Aged, Haematological cancer, business.industry, General Chemistry, Transformation (genetics), 030104 developmental biology, Cancer research, business, Blast Crisis, human activities

Abstract

Blast crisis (BC) predicts dismal outcomes in patients with chronic myeloid leukaemia (CML). Although additional genetic alterations play a central role in BC, the landscape and prognostic impact of these alterations remain elusive. Here, we comprehensively investigate genetic abnormalities in 136 BC and 148 chronic phase (CP) samples obtained from 216 CML patients using exome and targeted sequencing. One or more genetic abnormalities are found in 126 (92.6%) out of the 136 BC patients, including the RUNX1-ETS2 fusion and NBEAL2 mutations. The number of genetic alterations increase during the transition from CP to BC, which is markedly suppressed by tyrosine kinase inhibitors (TKIs). The lineage of the BC and prior use of TKIs correlate with distinct molecular profiles. Notably, genetic alterations, rather than clinical variables, contribute to a better prediction of BC prognosis. In conclusion, genetic abnormalities can help predict clinical outcomes and can guide clinical decisions in CML., In chronic myeloid leukaemia (CML), the drivers of blast crisis and resistance to tyrosine kinase inhibitors are not fully characterised. Here, the authors analyse a cohort of CML samples with genomic technologies and find that at least one driver alteration is associated with progression and worse prognosis.

Published

2020

12. Molecular classification and diagnostics of upper urinary tract urothelial carcinoma

Author

Satoru Miyano, Yusuke Sato, Genta Nagae, Yuichi Shiraishi, Akira Yokoyama, Keisuke Kataoka, Masashi Sanada, Jonathan A. Coleman, Hiroyuki Aburatani, Hiromichi Suzuki, Kenichi Yoshida, Tetsuo Ushiku, Yoshikage Inoue, Taketo Kawai, Tetsuichi Yoshizato, Yasuhito Nannya, Eiji Sugihara, Yukio Homma, Seishi Ogawa, David B. Solit, Jimpei Miyakawa, Shigekatsu Maekawa, Nobuyuki Kakiuchi, Hideki Makishima, Yasuhide Takeuchi, Masashi Fukayama, Yoichi Fujii, Andrew T. Lenis, Haruki Kume, Kenichi Chiba, Yotaro Ochi, Kosuke Aoki, Yusuke Shiozawa, Takaaki Sato, Tohru Nakagawa, Teppei Morikawa, Hiroko Tanaka, and Masahiro Nakagawa

Subjects

0301 basic medicine, Oncology, Male, Cancer Research, 2019-20 coronavirus outbreak, medicine.medical_specialty, integrated molecular study, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), upper urinary tract urothelial carcinoma, Gene Dosage, Polymorphism, Single Nucleotide, 03 medical and health sciences, 0302 clinical medicine, Molecular classification, Internal medicine, Biomarkers, Tumor, Medicine, Mutational status, Humans, Receptor, Fibroblast Growth Factor, Type 3, TP53, Tumor location, urothelial carcinoma, Urothelial carcinoma, Upper urinary tract, Aged, Carcinoma, Transitional Cell, molecular classification, business.industry, Ureteral Neoplasms, hypermutation, Molecular pathogenesis, Proto-Oncogene Proteins c-mdm2, molecular diagnostic, DNA Methylation, Middle Aged, Gene Expression Regulation, Neoplastic, 030104 developmental biology, FGFR3, 030220 oncology & carcinogenesis, Mutation, ras Proteins, Female, Tumor Suppressor Protein p53, business, transcriptome, RAS

Abstract

Upper urinary tract urothelial carcinoma (UTUC) is one of the common urothelial cancers. Its molecular pathogenesis, however, is poorly understood, with no useful biomarkers available for accurate diagnosis and molecular classification. Through an integrated genetic study involving 199 UTUC samples, we delineate the landscape of genetic alterations in UTUC enabling genetic/molecular classification. According to the mutational status of TP53, MDM2, RAS, and FGFR3, UTUC is classified into five subtypes having discrete profiles of gene expression, tumor location/histology, and clinical outcome, which is largely recapitulated in an independent UTUC cohort. Sequencing of urine sediment-derived DNA has a high diagnostic value for UTUC with 82.2% sensitivity and 100% specificity. These results provide a solid basis for better diagnosis and management of UTUC., 上部尿路上皮がんの分子分類と新規分子診断 --尿中遺伝子変異の検出で高精度の診断が可能--. 京都大学プレスリリース. 2021-06-15.

Published

2020

13. Exosomes secreted from cancer-associated fibroblasts elicit anti-pyrimidine drug resistance through modulation of its transporter in malignant lymphoma

Author

Masashi Sanada, Mika Takai, Satoko Shimada, Eisuke Iwamoto, Fumihiko Hayakawa, Akihiko Sakamoto, Tomoya Hikita, Kazuyuki Shimada, Shunsuke Kunou, Tomohiro Aoki, Hitoshi Kiyoi, Yusuke Kagaya, and Chitose Oneyama

Subjects

0301 basic medicine, Male, Cancer microenvironment, Cancer Research, Antimetabolites, Antineoplastic, Lymphoma, Primary Cell Culture, Mice, SCID, Biology, Equilibrative nucleoside transporter 2, Exosomes, Exosome, Deoxycytidine, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Cancer-Associated Fibroblasts, Mice, Inbred NOD, Cell Line, Tumor, microRNA, Genetics, medicine, Tumor Microenvironment, Animals, Humans, Secretion, Equilibrative-Nucleoside Transporter 2, Molecular Biology, Cell Proliferation, Tumor microenvironment, B-cell lymphoma, Cytarabine, medicine.disease, Xenograft Model Antitumor Assays, Gemcitabine, Microvesicles, MicroRNAs, 030104 developmental biology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, biology.protein

Abstract

The tumor microenvironment is deeply involved in the process of tumor growth and development. In this study, we focused on cancer-associated fibroblasts (CAFs) and their derived exosomes on the lymphoma microenvironment to uncover their clinical significance. CAFs were established from primary lymphoma samples, and exosomes secreted from CAFs were obtained by standard procedures. We then investigated the roles of CAFs and their derived exosomes in the survival and drug resistance of lymphoma cells. CAFs supported the survival of lymphoma cells through increased glycolysis, and the extent differed among CAFs. Exosomes were identified as a major component of the extracellular vesicles from CAFs, and they also supported the survival of lymphoma cells. The suppression of RAB27B, which is involved in the secretion of exosomes, using a specific siRNA resulted in reduced exosome secretion and decreased survival of lymphoma cells. Moreover, anti-pyrimidine drug resistance was induced in the presence of exosomes through the suppression of the pyrimidine transporter, equilibrative nucleoside transporter 2 (ENT2), and the suppression of ENT2 was significant in in vivo experiments and clinical samples. RNA sequencing analysis of miRNAs in exosomes identified miR-4717-5p as one of the most abundant miRNAs in the exosome, which suppressed the expression of ENT2 and induced anti-pyrimidine drug resistance in vitro. Our results suggest that exosomes including miR-4717-5p secreted from CAFs play a pivotal role in the lymphoma microenvironment, indicating that they are a promising therapeutic target.

Published

2020

14. Frequent genetic alterations in immune checkpoint-related genes in intravascular large B-cell lymphoma

Author

Kei Kohno, Hitoshi Kiyoi, Kenichi Chiba, Hiroaki Miyoshi, Yachiyo Kuwatsuka, Masashi Sanada, Seishi Ogawa, Akinao Okamoto, Yuichi Shiraishi, Koichi Ohshima, Yoshiko Atsuta, Akihiro Tomita, Yasufumi Masaki, Masaaki Yuge, Takahiko Ito, Hiroko Tanaka, Shigeru Kusumoto, Yusuke Takagi, Satoko Shimada, Asako Okabe, Yuichiro Inagaki, Shigeo Nakamura, Yusuke Shiozawa, Yoshikage Inoue, Masahiro Nakatochi, Chisako Iriyama, Yasuhito Nannya, Yasuhiro Suzuki, Satoru Miyano, Keisuke Kataoka, Kenichi Yoshida, and Kazuyuki Shimada

Subjects

Male, Immunology, Programmed Cell Death 1 Receptor, Biology, medicine.disease_cause, Biochemistry, B7-H1 Antigen, Biopsy, Exome Sequencing, medicine, Animals, Humans, Aged, Aged, 80 and over, Mutation, Intravascular large B-cell lymphoma, medicine.diagnostic_test, Cell Biology, Hematology, CD79B, Middle Aged, medicine.disease, Programmed Cell Death 1 Ligand 2 Protein, Immune checkpoint, Vascular Neoplasms, Lymphoma, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Cancer research, Female, Tumor Escape, Bone marrow, Lymphoma, Large B-Cell, Diffuse, Diffuse large B-cell lymphoma, Cell-Free Nucleic Acids

Abstract

Intravascular large B-cell lymphoma (IVLBCL) is a unique type of extranodal lymphoma characterized by selective growth of tumor cells in small vessels without lymphadenopathy. Greater understanding of the molecular pathogenesis of IVLBCL is hampered by the paucity of lymphoma cells in biopsy specimens, creating a limitation in obtaining sufficient tumor materials. To uncover the genetic landscape of IVLBCL, we performed whole-exome sequencing (WES) of 21 patients with IVLBCL using plasma-derived cell-free DNA (cfDNA) (n = 18), patient-derived xenograft tumors (n = 4), and tumor DNA from bone marrow (BM) mononuclear cells (n = 2). The concentration of cfDNA in IVLBCL was significantly higher than that in diffuse large B-cell lymphoma (DLBCL) (P < .0001) and healthy donors (P = .0053), allowing us to perform WES; most mutations detected in BM tumor DNA were successfully captured in cfDNA and xenograft. IVLBCL showed a high frequency of genetic lesions characteristic of activated B-cell–type DLBCL, with the former showing conspicuously higher frequencies (compared with nodal DLBCL) of mutations in MYD88 (57%), CD79B (67%), SETD1B (57%), and HLA-B (57%). We also found that 8 IVLBCL (38%) harbored rearrangements of programmed cell death 1 ligand 1 and 2 (PD-L1/PD-L2) involving the 3′ untranslated region; such rearrangements are implicated in immune evasion via PD-L1/PD-L2 overexpression. Our data demonstrate the utility of cfDNA and imply important roles for immune evasion in IVLBCL pathogenesis and PD-1/PD-L1/PD-L2 blockade in therapeutics for IVLBCL.

Published

2020

15. Integrated multiomics analysis of hepatoblastoma unravels its heterogeneity and provides novel druggable targets

Author

Satoru Miyano, Keisuke Kataoka, Yasuhide Hayashi, Mureo Kasahara, Akira Oka, Yuichi Shiraishi, Kenichi Kohashi, Misa Yoshida, Junko Takita, Hiroko Tanaka, Motohiro Kato, Kenichi Chiba, Shunsuke Kimura, Yuki Arakawa, Mio Tanaka, Yutaka Kanamori, Mitsuteru Hiwatari, Teppei Shimamura, Yusuke Sato, Hiromichi Suzuki, Ryota Souzaki, Yasuo Kubota, Yasuhito Nannya, Masahiro Sekiguchi, Noriko Hoshino, Masafumi Seki, Tomoko Kawai, Katsuyoshi Koh, Ryota Shirai, Takako Yoshioka, Kimikazu Matsumoto, Tomoaki Taguchi, Kentaro Watanabe, Seishi Ogawa, Kenichiro Hata, Masashi Sanada, Kenichi Yoshida, Yukichi Tanaka, Aiko Sato-Otsubo, Tomoya Isobe, and Yoichi Fujii

Subjects

0301 basic medicine, Cancer Research, Hepatoblastoma, Druggability, Biology, lcsh:RC254-282, DNA sequencing, Article, Transcriptome, Paediatric cancer, 03 medical and health sciences, 0302 clinical medicine, medicine, Cancer genomics, Genetic heterogeneity, Cell cycle, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, digestive system diseases, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, DNA methylation, Cancer research, Next-generation sequencing, Liver cancer

Abstract

Although hepatoblastoma is the most common pediatric liver cancer, its genetic heterogeneity and therapeutic targets are not well elucidated. Therefore, we conducted a multiomics analysis, including mutatome, DNA methylome, and transcriptome analyses, of 59 hepatoblastoma samples. Based on DNA methylation patterns, hepatoblastoma was classified into three clusters exhibiting remarkable correlation with clinical, histological, and genetic features. Cluster F was largely composed of cases with fetal histology and good outcomes, whereas clusters E1 and E2 corresponded primarily to embryonal/combined histology and poor outcomes. E1 and E2, albeit distinguishable by different patient age distributions, were genetically characterized by hypermethylation of the HNF4A/CEBPA-binding regions, fetal liver-like expression patterns, upregulation of the cell cycle pathway, and overexpression of NQO1 and ODC1. Inhibition of NQO1 and ODC1 in hepatoblastoma cells induced chemosensitization and growth suppression, respectively. Our results provide a comprehensive description of the molecular basis of hepatoblastoma and rational therapeutic strategies for high-risk cases.

Published

2020

16. ASXL2 regulates hematopoiesis in mice and its deficiency promotes myeloid expansion

Author

Henry Yang, Ling-Wen Ding, Janani Sundaresan, Pavithra Shyamsunder, Pushkar Dakle, Qiao-Yang Sun, Norimichi Hattori, Masashi Sanada, Tsuyoshi Nakamaki, Lin Han, Manja Meggendorfer, Lee-Yung Shih, Vikas Madan, H. Phillip Koeffler, Q. Tian Wang, Hazimah Binte Mohd Nordin, Der-Cherng Liang, Anand Mayakonda, Seishi Ogawa, Aiko Sato-Otsubo, Su Lin Lim, Jonathan W. Said, Ngan B. Doan, Weoi Woon Teoh, and Torsten Haferlach

Subjects

Myeloid, 0301 basic medicine, Chromosomal translocation, 129 Strain, Cardiorespiratory Medicine and Haematology, Inbred C57BL, Strain, Mice, hemic and lymphatic diseases, 2.1 Biological and endogenous factors, Myeloid Cells, Aetiology, Exome sequencing, Cancer, Mice, Knockout, Myelopoiesis, Pediatric, Leukemia, Cell Differentiation, Hematology, Extramedullary hematopoiesis, Haematopoiesis, medicine.anatomical_structure, Leukemia, Myeloid, Acute Disease, Mice, 129 Strain, Childhood Leukemia, Pediatric Cancer, Knockout, Immunology, Biology, Article, 03 medical and health sciences, Myelogenous, Rare Diseases, Genetics, medicine, Animals, Humans, Cell Proliferation, Gene Expression Profiling, Human Genome, medicine.disease, Hematopoiesis, Mice, Inbred C57BL, Repressor Proteins, Transplantation, 030104 developmental biology, Cancer research

Abstract

Chromosomal translocation t(8;21)(q22;q22) which leads to the generation of oncogenic RUNX1-RUNX1T1 (AML1-ETO) fusion is observed in approximately 10% of acute myelogenous leukemia (AML). To identify somatic mutations that co-operate with t(8;21)-driven leukemia, we performed whole and targeted exome sequencing of an Asian cohort at diagnosis and relapse. We identified high frequency of truncating alterations in ASXL2 along with recurrent mutations of KIT, TET2, MGA, FLT3, and DHX15 in this subtype of AML. To investigate in depth the role of ASXL2 in normal hematopoiesis, we utilized a mouse model of ASXL2 deficiency. Loss of ASXL2 caused progressive hematopoietic defects characterized by myeloid hyperplasia, splenomegaly, extramedullary hematopoiesis, and poor reconstitution ability in transplantation models. Parallel analyses of young and >1-year old Asxl2-deficient mice revealed age-dependent perturbations affecting, not only myeloid and erythroid differentiation, but also maturation of lymphoid cells. Overall, these findings establish a critical role for ASXL2 in maintaining steady state hematopoiesis, and provide insights into how its loss primes the expansion of myeloid cells.

Published

2018

17. Intensification of Early-Phase Therapy to Diminish the Prognostic Effect of Myeloid Antigen Expression in Infants with KMT2A-Rearranged Acute Lymphoblastic Leukemia: A Report from the JPLSG MLL-10 Trial

Author

Yuki Arakawa, Takayuki Takachi, Keizo Horibe, Takashi Ishihara, Takako Miyamura, Daisuke Tomizawa, Tomomi Yamada, Takao Deguchi, Sae Ishimaru, Akiko Saito, Mio Yano, Toshihiko Imamura, Toshinori Hori, Masashi Sanada, Atsushi Manabe, Yuki Aoki, and Shinya Sasaki

Subjects

biology, business.industry, Lymphoblastic Leukemia, Immunology, Cell Biology, Hematology, Biochemistry, Myeloid antigen, KMT2A, hemic and lymphatic diseases, biology.protein, Cancer research, Medicine, Early phase, business

Abstract

Background KMT2A-rearranged acute lymphoblastic leukemia (KMT2A-r ALL) is a rare and dismal disease in infants. Despite restriction of the indication of allogeneic hematopoietic stem cell transplantation to the high-risk group (patients aged Methods We analyzed and compared the MM expression (defined as at least one positive marker [with a positive blast subset ≥ 10%] among CD117, CD13, CD33, and CD65/CD15) by using flow cytometry (FCM) in infants with KMT2A-r ALL who were registered in the JPLSG MLL-10 trial. We also compared the results of immunoglobulin/T-cell receptor (Ig/TCR) gene-based polymerase chain reaction (PCR)-MRD analyses or 4-color FCM-MRD assay between the MM-positive and MM-negative groups at EOI and end of early consolidation. The Ig/TCR-MRD results were classified as negative if Results and Discussion Among the patients with KMT2A-rALL, 74 were included in this study, excluding one who was not evaluated with FCM at diagnosis. Of these patients, 42 were MM-positive and 32 were MM-negative. The 3-year EFS rates of the MM-positive and MM-negative patients were 62.3% (95% confidence interval [CI], 45.5-75.3) and 70.0% (95% CI, 50.3-83.1), respectively (p = 0.61). Their 3-year overall survival rates were 80.6% (95% CI, 65.0-89.8) and 87.5% (95% CI, 70.0-95.1), respectively (p = 0.74). The numbers of MM-positive and MM-negative patients according to age group are summarized in Table 1, and the difference in age distribution between the two groups was not significant. The MRD statuses of the patients at EOI in the two groups are also summarized in Table 1. No significant difference in MRD clearance was found between the MM-positive and MM-negative groups. Conclusion In this study, we found no significant difference in survival rate between the MM-positive and MM-negative groups. The MM expression was not a prognostic marker in the infants with KMT2A-r ALL in the MLL-10 cohort. We believe that rapid MRD clearance in the early phase of treatment with enhanced chemotherapy would have the greatest contribution to the improvement of prognosis. In this study, the MM-positive patients from the MLL-10 cohort might have benefited from early-phase treatment intensification in terms of MRD clearance. Figure 1 Figure 1. Disclosures No relevant conflicts of interest to declare.

Published

2021

18. Topic: AS04-MDS Biology and Pathogenesis/AS04b-Clonal diversity & evolution

Author

Satoru Miyano, A. Kondo-Takaori, Hidehiro Itonaga, Makoto Onizuka, Yasushi Miyazaki, Kazuma Ohyashiki, Jurjen Jansen, Yusuke Shiozawa, T Haferlach, Yoshiko Atsuta, Luca Malcovati, June Takeda, S. Kasahara, Yasuyuki Nagata, Tetsuichi Yoshizato, Yuichi Shiraishi, Toru Kiguchi, Masashi Sanada, Magnus Tobiasson, J. Maciejewski, Mario Cazzola, Y. Iijima-Yamashita, Elli Papaemmanuil, Yasuhito Nannya, F. Matsuda, Maria Creignou, R. Saiki, Kenichi Yoshida, Carmelo Gurnari, Hisashi Tsurumi, Y. Momozawa, Chantana Polprasert, Masahiro Nakagawa, Hideki Makishima, Yoshinobu Kanda, Eva Hellström-Lindberg, Austin G. Kulasekararaj, Seishi Ogawa, and Y. Kamatani

Subjects

Pathogenesis, Cancer Research, Oncology, Evolutionary biology, Hematology, Biology, Clonal diversity

Published

2021

19. A novel genetic and morphologic phenotype of ARID2-mediated myelodysplasia

Author

Masashi Sanada, Bartlomiej P Przychodzen, Ayana Kon, Seishi Ogawa, Kenichi Chiba, Hiroo Ueno, Naoko Hosono, Mikkael A. Sekeres, Kenichi Yoshida, June Takeda, Chantana Polprasert, Hideyuki Nakazawa, Hideki Makishima, Tetsuichi Yoshizato, Masahiro Nakagawa, Richard A. Padgett, Jarnail Singh, Yusuke Shiozawa, Hitoshi Sakai, Hetty E. Carraway, Yasuhito Nannya, Satoru Miyano, Keisuke Kataoka, Tomas Radivoyevitch, Yuichi Shiraishi, and Jaroslaw P. Maciejewski

Subjects

0301 basic medicine, Genetics, Cancer Research, Extramural, Myelodysplastic syndromes, Genetic Variation, Hematology, Biology, medicine.disease, Phenotype, Article, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, Myelodysplastic Syndromes, 030220 oncology & carcinogenesis, Genetic variation, medicine, Humans, Transcription factor, Genetic Association Studies, Transcription Factors

Published

2017

20. Copy number analysis identifies tumor suppressive lncRNAs in human osteosarcoma

Author

De-Chen Lin, Marc F. Hansen, Masashi Sanada, Jian-Jun Xie, H. Phillip Koeffler, Motohiro Kato, Seishi Ogawa, Norihiko Kawamata, Tadayuki Akagi, Dhong Hyun Lee, Carl W. Miller, and Jennifer D. Akunowicz

Subjects

0301 basic medicine, Cancer Research, DNA Copy Number Variations, Transplantation, Heterologous, Gene Dosage, Copy number analysis, Mice, Nude, Single-nucleotide polymorphism, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, Gene dosage, Loss of heterozygosity, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Cell Line, Tumor, Chromosome instability, medicine, Animals, Humans, Genes, Tumor Suppressor, Cell Proliferation, Oligonucleotide Array Sequence Analysis, Osteosarcoma, Uniparental Disomy, medicine.disease, Uniparental disomy, Transplantation, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, RNA, Long Noncoding, Carcinogenesis, Neoplasm Transplantation

Abstract

Osteosarcoma (OS) has a high degree of chromosomal instability and total copy number (CN) changes. We examined 58 human OS samples including 40 primary tumors, 11 explants, and 7 cell lines using single nucleotide polymorphism (SNP) arrays, and revealed that 70% of the samples had one or more recurrent CN-neutral loss of heterozygosity (CNN‑LOH) also known as uniparental disomy (UPD). Importantly, 17% of the samples showed prominent homozygous deletion of 3q13.31, suggesting its role in tumorigenesis. We identified and characterized two novel lncRNAs, LOC285194 and BC040587, within this genomic locus, strongly suggesting their tumor suppressor activity. Frequent deletions and UPD suggest that OS often has mutant or non-expressed tumor suppressor genes including two lncRNAs.

Published

2017

21. Prognostic Relevance of Genetic Abnormalities in Blastic Transformation of Chronic Myeloid Leukemia

Author

Ying-Jung Huang, Seishi Ogawa, Yosaku Watatani, Yotaro Ochi, Kenichi Chiba, Ko Sasaki, Hiroko Tanaka, Noriko Hosoya, Akifumi Takaori-Kondo, Kinuko Mitani, Yuichi Shiraishi, Rabindranath Bera, Nobuhiro Hiramoto, Yasuhito Nannya, Takayuki Ishikawa, Masashi Sanada, Hideki Makishima, Kenichi Yoshida, June Takeda, Yusuke Shiozawa, Lee-Yung Shih, Satoru Miyano, and Ming-Chung Kuo

Subjects

Transformation (genetics), business.industry, Immunology, Cancer research, Medicine, Myeloid leukemia, Relevance (information retrieval), Cell Biology, Hematology, business, Biochemistry

Abstract

Background Chronic myeloid leukemia (CML) is characterized by the BCR-ABL1 fusion gene. Despite the use of tyrosine kinase inhibitors (TKIs), a minority of chronic phase (CP) CML patients fail TKI therapies and progress to blast crisis (BC), showing dismal outcomes. Although genetic studies have revealed that CML-BC frequently carries not only ABL1 mutations but other driver mutations, our knowledge about the mechanism of TKI resistance and progression to BC is still limited by a relatively small number of patients and/or genes analyzed in each study. Moreover, it remains elusive whether mutations can predict clinical outcomes of BC patients, in which few biomarkers are known. Here, we investigated a large cohort of CML patients to reveal the landscape of genetic lesions and those predicting clinical outcomes in CML. Methods We performed whole-exome sequencing (WES) of paired CP and BC samples from 52 patients and targeted-capture sequencing that covered myeloid driver genes in 32 BC and 19 CP samples. Combined with public WES data for 24 BC and 77 CP, we analyzed a total of 108 BC and 148 CP samples. Results In WES analysis of paired CP and BC samples, an average of 5.3 nonsynonymous mutations were acquired during disease progression from CP to BC. Notably, a Poisson regression model revealed that the number of acquired mutations was positively correlated with time to progression from CP to BC (P < 0.001) and negatively with TKI therapy after CP diagnosis (P = 0.0093), although the correlation of the number of driver mutations in CML-BC with time to progression was not clear. These results suggest that the use of TKI effectively reduces the size of tumor populations at risk for clonal evolution by acquiring random mutations, by which prevents BC. In CML-BC, we found frequent mutations not only in known mutational targets in other hematological malignancies, such as RUNX1, ABL1, ASXL1, BCOR/BCORL1, TP53, and WT1, but also in other genes recently reported in BC (UBE2A and SETD1B) and previously unreported mutational targets in cancer (KLC2 and NBEAL2). Deep amplicon-sequencing revealed that ASXL1 mutations were already present at the time of CP diagnosis in most cases, whereas others such as RUNX1, ABL1, and TP53 mutations were absent in CP and newly emerged during progression to BC. Some abnormalities, such as +21, +8, and ASXL1 mutations, were more enriched in myeloid than lymphoid crisis, while others, including CDKN2A/B and IKZF1 deletions, -7/del(7p), -9/del(9p), and ABL1 mutations, vice versa. By contrast, abnormalities such as RUNX1 mutations and double Ph were almost equally observed in both crises. In univariate analysis of clinical factors for overall survival (OS) in 77 CML-BC cases for whom survival information was available, TKI-containing therapy for BC was significantly associated with a better OS, whereas genetic lesions including ASXL1 and TP53 mutations, del(17p), amp(17q), +19, and +21 had a negative impact on OS. Conspicuously, patients with TP53 mutations, del(17p), and amp(17q) showed an especially dismal outcome. We then performed a multivariate analysis using a Cox proportional hazard regression model, focusing on 36 TKI-treated patients, because TKI-containing therapy has been shown to improve OS and therefore, is a standard choice of therapy. We found that ASXL1 and BCOR mutations, complex copy-number alterations, amp(17q), and +21 were independent predictors for worse prognosis. Based on the number of these unfavorable factors, patients were classified into three subgroups showing distinct prognosis, where the 2-year OS rate was 71.8%, 15.6%, and 0% for patients with 0, 1, and ≥2 risk factors, respectively (P < 0.001). Finally, we explored the genetic abnormalities and clinical outcomes in CML-CP. In CP, only ASXL1 was mutated at a frequency comparable to that in BC, while others, including TET2, KMT2D, PTPN11, RUNX1, and WT1, were mutated at much lower frequencies. Of interest, patients who later developed BC more frequently had at least one genetic abnormality, suggesting that mutations found at the time of CP might play a role in driving CML cells to BC under the pressure of TKI treatment. Conclusion Our study clarified a comprehensive registry of genetic lesions in BC in a large cohort of CML patients and their prognostic impact, which should provide a clue to the development of better therapy/management for patients with CML. Disclosures Takaori-Kondo: Celgene: Honoraria, Research Funding; Bristol-Myers Squibb: Honoraria, Research Funding; Kyowa Kirin: Honoraria, Research Funding; Astellas Pharma: Honoraria, Research Funding; Ono Pharmaceutical: Research Funding; Thyas Co. Ltd.: Research Funding; Takeda: Research Funding; CHUGAI: Research Funding; Eisai: Research Funding; Nippon Shinyaku: Research Funding; Otsuka Pharmaceutical: Research Funding; Pfizer: Research Funding; OHARA Pharmaceutical: Research Funding; Sanofi: Research Funding; Novartis Pharma: Honoraria; MSD: Honoraria. Mitani:CHUGAI: Research Funding; Takeda: Research Funding; KYOWA KIRIN: Consultancy, Research Funding. Ogawa:Chordia Therapeutics, Inc.: Membership on an entity's Board of Directors or advisory committees, Research Funding; Asahi Genomics Co., Ltd.: Current equity holder in private company; Eisai Co., Ltd.: Research Funding; Otsuka Pharmaceutical Co., Ltd.: Research Funding; KAN Research Institute, Inc.: Membership on an entity's Board of Directors or advisory committees, Research Funding; Sumitomo Dainippon Pharma Co., Ltd.: Research Funding. Shih:Novartis: Research Funding; Celgene: Research Funding; PharmaEssentia: Consultancy, Membership on an entity's Board of Directors or advisory committees; Bristol-Myers Squibb: Consultancy, Membership on an entity's Board of Directors or advisory committees.

Published

2020

22. Frequent germline mutations of HAVCR2 in sporadic subcutaneous panniculitis-like T-cell lymphoma

Author

Masashi Sanada, Arunrat Pirunsarn, June Takeda, Hiromichi Suzuki, Kenichi Yoshida, Noppacharn Uaprasert, Ponlapat Rojnuckarin, Hiroko Tanaka, Kenichi Chiba, Satoru Miyano, Sunisa Kongkiatkamon, Chatphatai Moonla, Hideki Makishima, Yuichi Shiraishi, Nobuyuki Kakiuchi, Panisinee Lawasut, Seishi Ogawa, Chantana Polprasert, Nobuhiro Akita, Kitsada Wudhikarn, Udomsak Bunworasate, Thamathorn Assanasen, Yasuhito Nannya, Wimonmas Sitthi, Yoichi Fujii, and Yasuhide Takeuchi

Subjects

Adult, Panniculitis, Biology, medicine.disease_cause, Compound heterozygosity, Lymphoma, T-Cell, Germline, Epigenesis, Genetic, Young Adult, Germline mutation, Subcutaneous Panniculitis-Like T-Cell Lymphoma, medicine, Missense mutation, Humans, Hepatitis A Virus Cellular Receptor 2, Exome sequencing, Alleles, Germ-Line Mutation, Hemophagocytic lymphohistiocytosis, Mutation, Lymphoid Neoplasia, Hematology, Middle Aged, medicine.disease, Child, Preschool, Cancer research

Abstract

Subcutaneous panniculitis-like T-cell lymphoma (SPTCL) is a rare subtype of peripheral T-cell lymphoma affecting younger patients and associated with hemophagocytic lymphohistiocytosis. To clarify the molecular pathogenesis of SPTCL, we analyzed paired tumor and germline DNAs from 13 patients by whole-exome sequencing. All cases were Asians and were phenotypically sporadic with no family history of SPTCL. Consistent with a recent report, germline mutations in HAVCR2, encoding T-cell immunoglobulin mucin 3 (TIM3), were identified in 11 of 13 (85%) cases. All mutated cases were primary SPTCL, whereas the 2 cases without mutation were secondary SPTCL associated with underlying diseases, including viral infection and autoimmune disease. Ten patients harbored homozygous p.Y82C mutations, and 1 showed compound heterozygous mutations (p.Y82C and p.T101I). Both missense mutations altered highly conserved residues located in the extracellular immunoglobulin variable–like domain. According to the Genome Aggregation Database of >138 500 general individuals, both mutations were documented with minor allele frequencies < 0.007, indicating remarkable enrichment of these HAVCR2 alleles in SPTCL. SPTCL cells also harbored somatic mutations (6.2 per patient) that are frequently identified in genes associated with epigenetic regulation and signal transduction. In conclusion, individuals harboring biallelic HAVCR2 (TIM3) germline mutations were highly susceptible to sporadic SPTCL, which was also associated with clonal somatic mutations.

Published

2019

23. Somatic PHF6 mutations in 1760 cases with various myeloid neoplasms

Author

T Haferlach, Hiraku Mori, Hirotoshi Tanaka, S Miyawaki, Wolfgang Kern, Hitoshi Kiyoi, Yasunobu Nagata, Tetsuichi Yoshizato, Yusuke Shiozawa, Yuichi Shiraishi, Kenichi Yoshida, Claudia Haferlach, Hideki Makishima, Rika Kihara, Shih Ly, Satoru Miyano, Ken Ishiyama, Keisuke Kataoka, H P Koeffler, Aiko Sato-Otsubo, Ayana Kon, Seishi Ogawa, Tomoki Naoe, Masashi Sanada, Tsuyoshi Nakamaki, T. Mori, and Kenichi Chiba

Subjects

0301 basic medicine, Cancer Research, medicine.medical_specialty, Myeloid, Somatic cell, medicine.disease_cause, 03 medical and health sciences, Internal medicine, medicine, Humans, Mutation, Hematology, business.industry, medicine.disease, Lymphoma, Repressor Proteins, Leukemia, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Oncology, Bone marrow neoplasm, Core Binding Factor Alpha 2 Subunit, Immunology, Cancer research, Bone Marrow Neoplasms, Carrier Proteins, business

Abstract

Leukemia accepted article preview online, 01 August 2016. doi:10.1038/leu.2016.212.

Published

2016

24. Whole-exome sequencing reveals the spectrum of gene mutations and the clonal evolution patterns in paediatric acute myeloid leukaemia

Author

Etsuro Ito, Motohiro Kato, Kentaro Ohki, Kenichi Chiba, Keizo Horibe, Takashi Taga, Yasuhide Hayashi, Seishi Ogawa, Kiminori Terui, Masashi Sanada, Yuichi Shiraishi, Kazuko Kudo, Junko Takita, Kenichi Yoshida, Hiroko Tanaka, Souichi Adachi, Norio Shiba, Daisuke Tomizawa, Yasunobu Nagata, Myoung-ja Park, Yusuke Hara, Satoru Miyano, Genki Yamato, Akio Tawa, Hirokazu Arakawa, Yusuke Okuno, and Akira Shimada

Subjects

Male, 0301 basic medicine, NPM1, Cohesin complex, DNA Mutational Analysis, Biology, Gene mutation, Somatic evolution in cancer, Deep sequencing, Epigenesis, Genetic, Clonal Evolution, 03 medical and health sciences, Recurrence, hemic and lymphatic diseases, CEBPA, Humans, Exome, Genetic Predisposition to Disease, Child, Genetic Association Studies, Exome sequencing, Genetics, Massive parallel sequencing, High-Throughput Nucleotide Sequencing, Hematology, Prognosis, Leukemia, Myeloid, Acute, 030104 developmental biology, Mutation, Disease Progression, Cancer research, Female, Nucleophosmin

Abstract

Acute myeloid leukaemia (AML) is a molecularly and clinically heterogeneous disease. Targeted sequencing efforts have identified several mutations with diagnostic and prognostic values in KIT, NPM1, CEBPA and FLT3 in both adult and paediatric AML. In addition, massively parallel sequencing enabled the discovery of recurrent mutations (i.e. IDH1/2 and DNMT3A) in adult AML. In this study, whole-exome sequencing (WES) of 22 paediatric AML patients revealed mutations in components of the cohesin complex (RAD21 and SMC3), BCORL1 and ASXL2 in addition to previously known gene mutations. We also revealed intratumoural heterogeneities in many patients, implicating multiple clonal evolution events in the development of AML. Furthermore, targeted deep sequencing in 182 paediatric AML patients identified three major categories of recurrently mutated genes: cohesion complex genes [STAG2, RAD21 and SMC3 in 17 patients (8·3%)], epigenetic regulators [ASXL1/ASXL2 in 17 patients (8·3%), BCOR/BCORL1 in 7 patients (3·4%)] and signalling molecules. We also performed WES in four patients with relapsed AML. Relapsed AML evolved from one of the subclones at the initial phase and was accompanied by many additional mutations, including common driver mutations that were absent or existed only with lower allele frequency in the diagnostic samples, indicating a multistep process causing leukaemia recurrence.

Published

2016

25. Aberrant PD-L1 expression through 3′-UTR disruption in multiple cancers

Author

Koichi Kashiwase, Kyoko Masuda, Hidehiro Itonaga, Yuichi Shiraishi, Satoshi Ito, Nagahiro Minato, Yasunobu Nagata, Misako Matsumoto, Tatsuhiro Shibata, Kengo Takeuchi, Natsuko Hama, Hiroko Tanaka, Wataru Munakata, Hiromi Nakamura, Seishi Ogawa, Yosaku Watatani, Koji Izutsu, Akifumi Takaori-Kondo, Masashi Sanada, Kotaro Shide, Kenichi Yoshida, Tomonori Hidaka, Takuro Kameda, Akira Kitanaka, Kenichi Chiba, Seiji Sakata, Yasushi Miyazaki, Tetsuichi Yoshizato, Yohei Takeda, Takuya Maeda, Seiya Mizuno, Yoshitaka Imaizumi, Hiroshi Kawamoto, Yasushi Totoki, Nobuyuki Kakiuchi, Kazuya Shimoda, Hiromichi Suzuki, Yoshiki Akatsuka, Seiji Nagano, Tsukasa Seya, Satoru Miyano, Keisuke Kataoka, Satoru Takahashi, and Yoko Kubuki

Subjects

Genetic Markers, 0301 basic medicine, Untranslated region, RNA Stability, Programmed Cell Death 1 Receptor, Chromosomal translocation, Adenocarcinoma, Antibodies, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Stomach Neoplasms, Cell Line, Tumor, Neoplasms, Gene duplication, medicine, Animals, Humans, Leukemia-Lymphoma, Adult T-Cell, RNA, Messenger, Clonal Selection, Antigen-Mediated, 3' Untranslated Regions, Gene, Multidisciplinary, biology, Three prime untranslated region, medicine.disease, Up-Regulation, Lymphoma, Gene Expression Regulation, Neoplastic, 030104 developmental biology, 030220 oncology & carcinogenesis, Immunology, biology.protein, Cancer research, Female, Tumor Escape, Lymphoma, Large B-Cell, Diffuse, CRISPR-Cas Systems, Antibody

Abstract

Successful treatment of many patients with advanced cancer using antibodies against programmed cell death 1 (PD-1; also known as PDCD1) and its ligand (PD-L1; also known as CD274) has highlighted the critical importance of PD-1/PD-L1-mediated immune escape in cancer development. However, the genetic basis for the immune escape has not been fully elucidated, with the exception of elevated PD-L1 expression by gene amplification and utilization of an ectopic promoter by translocation, as reported in Hodgkin and other B-cell lymphomas, as well as stomach adenocarcinoma. Here we show a unique genetic mechanism of immune escape caused by structural variations (SVs) commonly disrupting the 3' region of the PD-L1 gene. Widely affecting multiple common human cancer types, including adult T-cell leukaemia/lymphoma (27%), diffuse large B-cell lymphoma (8%), and stomach adenocarcinoma (2%), these SVs invariably lead to a marked elevation of aberrant PD-L1 transcripts that are stabilized by truncation of the 3'-untranslated region (UTR). Disruption of the Pd-l1 3'-UTR in mice enables immune evasion of EG7-OVA tumour cells with elevated Pd-l1 expression in vivo, which is effectively inhibited by Pd-1/Pd-l1 blockade, supporting the role of relevant SVs in clonal selection through immune evasion. Our findings not only unmask a novel regulatory mechanism of PD-L1 expression, but also suggest that PD-L1 3'-UTR disruption could serve as a genetic marker to identify cancers that actively evade anti-tumour immunity through PD-L1 overexpression.

Published

2016

26. Comprehensive mutational analysis of primary and relapse acute promyelocytic leukemia

Author

Michael Heuser, Manoj Garg, T Haferlach, L. Z. Liu, Shih Ly, Yuichi Shiraishi, Takayuki Ikezoe, Michael Lill, Hwei-Fang Tien, Henry Yang, Ling-Wen Ding, Hagop M. Kantarjian, H P Koeffler, T. Ma, Yasunobu Nagata, Wolf-K. Hofmann, Qiao-Yang Sun, Satoru Miyano, Richard A. Larson, Noreen Fulton, Seishi Ogawa, Pavithra Shyamsunder, Masashi Sanada, Kamran Alimoghaddam, W. J. Chng, Norimichi Hattori, Saravanan Ganesan, Wendy Stock, Tamara Alpermann, S. Rostami, Ezhilarasi Chendamarai, Vikram Mathews, Kenichi Yoshida, Anand Mayakonda, Steve Kornblau, M. C. Kuo, Gregory Malnassy, Vikas Madan, Lin Han, A. Ghavamzadeh, Hsin-An Hou, Andrea Biondi, Bayard L. Powell, W. Chien, Jairo Matthews, Janani Sundaresan, Michael Lübbert, Daniel Nowak, Deepika Kanojia, Arnold Ganser, Kar Tong Tan, Maya Koren-Michowitz, Madan, V, Shyamsunder, P, Han, L, Mayakonda, A, Nagata, Y, Sundaresan, J, Kanojia, D, Yoshida, K, Ganesan, S, Hattori, N, Fulton, N, Tan, K, Alpermann, T, Kuo, M, Rostami, S, Matthews, J, Sanada, M, Liu, L, Shiraishi, Y, Miyano, S, Chendamarai, E, Hou, H, Malnassy, G, Ma, T, Garg, M, Ding, L, Sun, Q, Chien, W, Ikezoe, T, Lill, M, Biondi, A, Larson, R, Powell, B, Lubbert, M, Chng, W, Tien, H, Heuser, M, Ganser, A, Koren-Michowitz, M, Kornblau, S, Kantarjian, H, Nowak, D, Hofmann, W, Yang, H, Stock, W, Ghavamzadeh, A, Alimoghaddam, K, Haferlach, T, Ogawa, S, Shih, L, Mathews, V, and Koeffler, H

Subjects

0301 basic medicine, Neuroblastoma RAS viral oncogene homolog, Acute promyelocytic leukemia, Cancer Research, ARID1A, DNA-Binding Protein, DNA Mutational Analysis, Clinical Sciences, Oncology and Carcinogenesis, Immunology, Acute, Biology, DNA Mutational Analysi, Fusion gene, 03 medical and health sciences, 0302 clinical medicine, Leukemia, Promyelocytic, Acute, Recurrence, immune system diseases, medicine, Humans, Exome, neoplasms, Nuclear Protein, Promyelocytic, Genetics, Leukemia, Gene Expression Profiling, Nuclear Proteins, Myeloid leukemia, Cell Differentiation, Hematology, medicine.disease, DNA-Binding Proteins, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Original Article, Human, Transcription Factors

Abstract

Acute promyelocytic leukemia (APL) is a subtype of myeloid leukemia characterized by differentiation block at the promyelocyte stage. Besides the presence of chromosomal rearrangement t(15;17), leading to the formation of PML-RARA (promyelocytic leukemia-retinoic acid receptor alpha) fusion, other genetic alterations have also been implicated in APL. Here, we performed comprehensive mutational analysis of primary and relapse APL to identify somatic alterations, which cooperate with PML-RARA in the pathogenesis of APL. We explored the mutational landscape using whole-exome (n=12) and subsequent targeted sequencing of 398 genes in 153 primary and 69 relapse APL. Both primary and relapse APL harbored an average of eight non-silent somatic mutations per exome. We observed recurrent alterations of FLT3, WT1, NRAS and KRAS in the newly diagnosed APL, whereas mutations in other genes commonly mutated in myeloid leukemia were rarely detected. The molecular signature of APL relapse was characterized by emergence of frequent mutations in PML and RARA genes. Our sequencing data also demonstrates incidence of loss-of-function mutations in previously unidentified genes, ARID1B and ARID1A, both of which encode for key components of the SWI/SNF complex. We show that knockdown of ARID1B in APL cell line, NB4, results in large-scale activation of gene expression and reduced in vitro differentiation potential.

Published

2016

27. Abstract 1309: Distinct molecular subtypes and a high diagnostic urinary biomarker of upper urinary tract urothelial carcinoma

Author

Tetsuichi Yoshizato, Haruki Kume, Seishi Ogawa, Taketo Kawai, Tohru Nakagawa, Yusuke Sato, Hideki Makishima, Hiroaki Nishimatsu, Hiromichi Suzuki, Yoichi Fujii, Satoru Miyano, Masashi Sanada, Toshikazu Nishimatsu, Kenichi Yoshida, and Yuichi Shiraishi

Subjects

Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Urinary system, Cancer, Gene mutation, medicine.disease, Gastroenterology, Lynch syndrome, Oncology, CDKN2A, Internal medicine, Medicine, business, Exome, Urine cytology, Upper urinary tract

Abstract

[Backgrounds] Upper urinary tract urothelial carcinomas (UTUCs) are rare malignancies with a histological similarity to urothelial bladder carcinomas (UBCs). Unlike UBCs, little is known about the genetic basis of UTUCs, for which no useful biomarkers are currently available. [Material & Methods] Surgical specimens and matched normal samples were obtained from 209 UTUC patients with various stages and were subjected to integrated molecular analysis including whole exome/transcriptome sequencing. We also investigated a possibility of UTUC diagnosis using urinary sediment-derived DNA. [Result] Hypermutation (≥20/Mb) was observed in 15 samples (6.7%), of which 12 harbored biallelic mismatch repair genes alterations suggestive of Lynch syndrome. The most frequently affected driver genes included TERT (promoter) (50%), followed by KMT2D (46%), FGFR3 (44%), CDKN2A (44%), and TP53 (36%). Mutually exclusive patterns were observed among alterations in FGFR3, RAS (H-/K-/NRAS), TP53, and MDM2, which covered 93.8% of the entire cohort. Approximately 40% of the samples showed highly complexed karyotype (CK) with frequent aneuploidy and chromothripsis. Based on these findings, UTUC cases were classified into 5 genetic subgroups: hypermutated, FGFR3-mutated, RAS-mutated, TP53-mutated with CK, and other cases with none of these features, which were significantly associated distinct clinical outcomes. While hypermutated and FGFR3 subtypes showed favorable prognosis, the TP53/CK subtype exhibited an aggressive clinical course and a shorter survival. Expression-based molecular classification identified unique gene expression subtypes: clusters 1-5, which showed a strong correlation with the mutation-based classification. Of interest, cluster 3 was highly enriched for TP53/CK and showed high expression of PDL1 and PDL2, suggesting a possible role of checkpoint inhibitions. The sequencing analysis of urinary sediment-derived DNA successfully captured those mutations and copy number alterations (CNAs) that had been detected in the corresponding preoperative samples in 84.4% of the cases (38/45), which was significantly higher than the positive diagnosis in urine cytology (class 4 and 5, 31.1%). Failure of detecting mutations were found in 5 tumors that were associated with severe hydronephrosis, which might prevented tumor-containing urinary flow. None of the post operative (0/34) and control (0/19) samples showed mutations/CNAs, including two with positive cytology (class4), both of which were diagnosed as benign pelvis tumors after surgery. [Conclusion] UTUC are classified into 5 distinct genetic subtypes characterized by unique profiles of gene mutations, expression and clinical outcomes, which help an optimal choice of therapeutics, including novel molecular-targeted drugs and checkpoint-inhibitors. Sequencing urinary sediments is a useful, non-invasive biomarker for precise diagnosis and proper treatment. Citation Format: Yoichi Fujii, Yusuke Sato, Hiromichi Suzuki, Tetsuichi Yoshizato, Kenichi Yoshida, Yuichi Shiraishi, Taketo Kawai, Tohru Nakagawa, Hiroaki Nishimatsu, Toshikazu Nishimatsu, Masashi Sanada, Hideki Makishima, Satoru Miyano, Haruki Kume, Seishi Ogawa. Distinct molecular subtypes and a high diagnostic urinary biomarker of upper urinary tract urothelial carcinoma [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 1309.

Published

2020

28. Genetic and transcriptional landscape of plasma cells in POEMS syndrome

Author

June Takeda, Tohru Iseki, Kensuke Kayamori, Seishi Ogawa, Chiaki Nakaseko, Kenichi Yoshida, Satoru Miyano, Chikako Ohwada, Sonoko Misawa, Yusuke Takeda, Atsunori Saraya, Yusuke Shiozawa, Osamu Ohara, Kenichi Chiba, Emiko Sakaida, Shio Mitsukawa, Koutaro Yokote, Dai Nishijima, Hiroko Tanaka, Yoshinori Hasegawa, Shokichi Tsukamoto, Nagisa Oshima-Hasegawa, Ola Rizq, Masashi Sanada, Shuhei Koide, Chika Kawajiri-Manako, Motohiko Oshima, Satoshi Kuwabara, Kazumasa Aoyama, Yuhei Nagao, Naoya Mimura, Atsushi Iwama, Yuichi Shiraishi, Yusuke Isshiki, and Masahiro Takeuchi

Subjects

0301 basic medicine, Neuroblastoma RAS viral oncogene homolog, Adult, Male, Cancer Research, Adolescent, Plasma Cells, Gene mutation, Biology, medicine.disease_cause, Monoclonal Gammopathy of Undetermined Significance, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Antineoplastic Combined Chemotherapy Protocols, Exome Sequencing, medicine, Biomarkers, Tumor, Humans, Multiple myeloma, Exome sequencing, POEMS syndrome, Aged, Gene Expression Profiling, High-Throughput Nucleotide Sequencing, Hematology, Middle Aged, medicine.disease, Prognosis, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Monoclonal, Mutation, POEMS Syndrome, Cancer research, Female, KRAS, Neoplasm Recurrence, Local, Multiple Myeloma, Monoclonal gammopathy of undetermined significance

Abstract

POEMS syndrome is a rare paraneoplastic disease associated with monoclonal plasma cells; however, the pathogenic importance of plasma cells remains unclear. We performed comprehensive genetic analyses of plasma cells in 20 patients with POEMS syndrome. Whole exome sequencing was performed in 11 cases and found a total of 308 somatic mutations in 285 genes. Targeted sequencing was performed in all 20 cases and identified 20 mutations in 7 recurrently mutated genes, namely KLHL6, LTB, EHD1, EML4, HEPHL1, HIPK1, and PCDH10. None of the driver gene mutations frequently found in multiple myeloma (MM) such as NRAS, KRAS, BRAF, and TP53 was detected. Copy number analysis showed chromosomal abnormalities shared with monoclonal gammopathy of undetermined significance (MGUS), suggesting a partial overlap in the early development of MGUS and POEMS syndrome. RNA sequencing revealed a transcription profile specific to POEMS syndrome when compared with normal plasma cells, MGUS and MM. Unexpectedly, disease-specific VEGFA expression was not increased in POEMS syndrome. Our study illustrates that the genetic and transcriptional profiles of plasma cells in POEMS syndrome are distinct from MM and MGUS, indicating unique function of clonal plasma cells in its pathogenesis.

Published

2018

29. INTEGRATED PROFILING OF DNA METHYLATION AND MUTATIONS IN PATIENTS WITH MYELODYSPLASTIC SYNDROMES

Author

Niroshan Nadarajah, T Haferlach, Masashi Sanada, Hiroko Tanaka, Yasuhito Nannya, G. Nagae, Y. Takeuchi, Masahiro Nakagawa, Claudia Haferlach, Constance Baer, Kenichi Chiba, S. Morimoto, Yasushi Miyazaki, S. Ogawa, Y. Fujii, Hiroo Ueno, Yuichi Shiraishi, H. Makishima, Tetsuichi Yoshizato, Wolfgang Kern, H. Aburatani, S. Miyano, R. Inagaki, K. Yoshida, Yasunobu Nagata, and June Takeda

Subjects

business.industry, Myelodysplastic syndromes, DNA methylation, Cancer research, Medicine, Profiling (information science), In patient, Hematology, business, medicine.disease

Published

2019

30. PF532 INTEGRATED PROFILING OF DNA METHYLATION AND MUTATIONS IN PATIENTS WITH MYELODYSPLASTIC SYNDROMES

Author

S. Miyano, Y. Fujii, Yasuhito Nannya, Claudia Haferlach, Y. Takeuchi, Kenichi Chiba, Yasushi Miyazaki, S. Ogawa, G. Nagae, Yasunobu Nagata, Wolfgang Kern, T Haferlach, Masashi Sanada, Hiroko Tanaka, June Takeda, K. Yoshida, Niroshan Nadarajah, H. Aburatani, R. Inagaki, Yuichi Shiraishi, S. Morimoto, Constance Baer, H. Makishima, Hiroo Ueno, Masahiro Nakagawa, and Tetsuichi Yoshizato

Subjects

business.industry, Myelodysplastic syndromes, DNA methylation, Cancer research, medicine, Profiling (information science), In patient, Hematology, medicine.disease, business

Published

2019

31. Profiling of somatic mutations in acute myeloid leukemia with FLT3-ITD at diagnosis and relapse

Author

Li Zhen Liu, Koiti Inokuchi, Torsten Haferlach, Ming Chung Kuo, Henry Yang, Michael Lill, Ling-Wen Ding, Masashi Sanada, Anand Mayakonda, Kenichi Chiba, Manoj Garg, Abhishek Sampath, Satoshi Wakita, Joanna Schiller, Hiroki Yamaguchi, H. Phillip Koeffler, Qiao-Yang Sun, Allen Eng Juh Yeoh, Igor Wolfgang Blau, Wee Joo Chng, Hagop M. Kantarjian, Deepika Kanojia, Yusuke Okuno, Lee Yung Shih, Hiroko Tanaka, Olga Blau, Kar Tong Tan, Steven M. Kornblau, Zhi Jiang Zang, Kenichi Yoshida, Tamara Alpermann, Satoru Miyano, Vikas Madan, Yuichi Shiraishi, Seishi Ogawa, Karl Anton Kreuzer, De-Chen Lin, Yasunobu Nagata, Wenwen Chien, Shirley Kow Yin Kham, Sreya Haridas Keloth, and Subhashree Venkatesan

Subjects

Male, Mutation rate, medicine.medical_specialty, Cohesin complex, Immunology, Biochemistry, Somatic evolution in cancer, Recurrence, hemic and lymphatic diseases, medicine, Humans, Exome, Retrospective Studies, Myeloid Neoplasia, business.industry, food and beverages, Myeloid leukemia, Induction Chemotherapy, Cell Biology, Hematology, DNA Methylation, medicine.disease, Chromatin, Surgery, Leukemia, Myeloid, Acute, Leukemia, fms-Like Tyrosine Kinase 3, Mutation, embryonic structures, Fms-Like Tyrosine Kinase 3, DNA methylation, Cancer research, Female, business

Abstract

Acute myeloid leukemia (AML) with an FLT3 internal tandem duplication (FLT3-ITD) mutation is an aggressive hematologic malignancy with a grave prognosis. To identify the mutational spectrum associated with relapse, whole-exome sequencing was performed on 13 matched diagnosis, relapse, and remission trios followed by targeted sequencing of 299 genes in 67 FLT3-ITD patients. The FLT3-ITD genome has an average of 13 mutations per sample, similar to other AML subtypes, which is a low mutation rate compared with that in solid tumors. Recurrent mutations occur in genes related to DNA methylation, chromatin, histone methylation, myeloid transcription factors, signaling, adhesion, cohesin complex, and the spliceosome. Their pattern of mutual exclusivity and cooperation among mutated genes suggests that these genes have a strong biological relationship. In addition, we identified mutations in previously unappreciated genes such as MLL3, NSD1, FAT1, FAT4, and IDH3B. Mutations in 9 genes were observed in the relapse-specific phase. DNMT3A mutations are the most stable mutations, and this DNMT3A-transformed clone can be present even in morphologic complete remissions. Of note, all AML matched trio samples shared at least 1 genomic alteration at diagnosis and relapse, suggesting common ancestral clones. Two types of clonal evolution occur at relapse: either the founder clone recurs or a subclone of the founder clone escapes from induction chemotherapy and expands at relapse by acquiring new mutations. Relapse-specific mutations displayed an increase in transversions. Functional assays demonstrated that both MLL3 and FAT1 exert tumor-suppressor activity in the FLT3-ITD subtype. An inhibitor of XPO1 synergized with standard AML induction chemotherapy to inhibit FLT3-ITD growth. This study clearly shows that FLT3-ITD AML requires additional driver genetic alterations in addition to FLT3-ITD alone.

Published

2015

32. Genomic analysis of clonal origin of Langerhans cell histiocytosis following acute lymphoblastic leukaemia

Author

Motohiro Kato, Kenichi Chiba, Yusuke Sato, Masaharu Akiyama, Katsuyoshi Koh, Masashi Sanada, Seishi Ogawa, Michiko Kajiwara, Shuki Mizutani, Kenichi Yoshida, Hiroshi Kishimoto, Yuichi Shiraishi, Junko Takita, Hiroko Tanaka, Yuki Arakawa, Tomohiko Taki, Noriko Mitsuiki, Satoru Miyano, Masafumi Seki, and Ryo Oyama

Subjects

business.industry, Hematology, medicine.disease, Genetic analysis, Precursor Cell Lymphoblastic Leukemia Lymphoma, 03 medical and health sciences, 0302 clinical medicine, Langerhans cell histiocytosis, 030220 oncology & carcinogenesis, DNA Mutational Analysis, Cancer research, Medicine, Lymphoblastic leukaemia, Human genome, business, Histiocyte, 030215 immunology

Published

2015

33. Integrated Molecular Characterization of the Lethal Pediatric Cancer Pancreatoblastoma

Author

Yukichi Tanaka, Tomoya Isobe, Motohiro Kato, Hajime Hosoi, Yoshikage Inoue, Kenichiro Hata, Takao Deguchi, Chikako Kiyotani, Masafumi Seki, Hiromichi Suzuki, Tsuyoshi Ito, Akihiro Iguchi, Yuichi Shiraishi, Tomoko Iehara, Satoru Miyano, Yusuke Sato, Yusuke Shiozawa, Junko Takita, Hiroko Tanaka, Akira Yokoyama, Masahiro Sekiguchi, Shunsuke Kimura, Keisuke Kataoka, Akiko Inoue, Asahito Hama, Teppei Shimamura, Junya Fujimura, Tomoaki Taguchi, Tomoko Kawai, Misa Yoshida, Masaharu Akiyama, Akira Oka, Nobuyuki Kakiuchi, Masashi Sanada, Kenichi Chiba, Kenichi Yoshida, and Seishi Ogawa

Subjects

0301 basic medicine, Male, Cancer Research, Gene Expression Profiling, Wnt signaling pathway, Pancreatoblastoma, LGR5, Biology, medicine.disease, Pediatric cancer, Loss of heterozygosity, Transcriptome, Pancreatic Neoplasms, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Oncology, medicine, Cancer research, Humans, Exome, Female, Allele, Pancreas, Child

Abstract

Pancreatoblastoma is a rare pediatric pancreatic malignancy for which the molecular pathogenesis is not understood. In this study, we report the findings of an integrated multiomics study of whole-exome and RNA sequencing as well as genome-wide copy number and methylation analyses of ten pancreatoblastoma cases. The pancreatoblastoma genome was characterized by a high frequency of aberrant activation of the Wnt signaling pathway, either via somatic mutations of CTNNB1 (90%) and copy-neutral loss of heterozygosity (CN-LOH) of APC (10%). In addition, imprinting dysregulation of IGF2 as a consequence of CN-LOH (80%), gain of paternal allele (10%), and gain of methylation (10%) was universally detected. At the transcriptome level, pancreatoblastoma exhibited an expression profile characteristic of early pancreas progenitor-like cells along with upregulation of the R-spondin/LGR5/RNF43 module. Our results offer a comprehensive description of the molecular basis for pancreatoblastoma and highlight rational therapeutic targets for its treatment. Significance: Molecular genetic analysis of a rare untreatable pediatric tumor reveals Wnt/IGF2 aberrations and features of early pancreas progenitor-like cells, suggesting cellular origins and rational strategies for therapeutic targeting. Cancer Res; 78(4); 865–76. ©2017 AACR.

Published

2017

34. Integrated molecular profiling of juvenile myelomonocytic leukemia

Author

Xinan Wang, Asahito Hama, Nozomu Kawashima, Kyogo Suzuki, Masashi Sanada, Atsushi Narita, Hiroyuki Aburatani, Yuichi Shiraishi, Arata Watanabe, Hideki Muramatsu, Seishi Ogawa, Genta Nagae, Seiji Kojima, Kenichi Yoshida, Masashi Hirayama, Hiroko Tanaka, Toshihide Ueno, Yoshiyuki Takahashi, Satoru Miyano, Hirotoshi Sakaguchi, Yusuke Okuno, Hiroyuki Mano, Norihiro Murakami, Masafumi Ito, Kenichi Chiba, and Yinyan Xu

Subjects

0301 basic medicine, Neuroblastoma RAS viral oncogene homolog, Male, Adolescent, Oncogene Proteins, Fusion, Immunology, Gene mutation, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Crizotinib, hemic and lymphatic diseases, ROS1, Medicine, Humans, Child, Protein Kinase Inhibitors, Myeloproliferative neoplasm, Cell Proliferation, Juvenile myelomonocytic leukemia, business.industry, Gene Expression Profiling, Myeloid leukemia, Infant, Cell Biology, Hematology, DNA, Neoplasm, DNA Methylation, medicine.disease, Leukemia, 030104 developmental biology, Leukemia, Myelomonocytic, Juvenile, 030220 oncology & carcinogenesis, Child, Preschool, Mutation, Cancer research, Female, business, medicine.drug, Genome-Wide Association Study

Abstract

Juvenile myelomonocytic leukemia (JMML), a rare and aggressive myelodysplastic/myeloproliferative neoplasm that occurs in infants and during early childhood, is characterized by excessive myelomonocytic cell proliferation. More than 80% of patients harbor germ line and somatic mutations in RAS pathway genes (eg, PTPN11, NF1, NRAS, KRAS, and CBL), and previous studies have identified several biomarkers associated with poor prognosis. However, the molecular pathogenesis of 10% to 20% of patients and the relationships among these biomarkers have not been well defined. To address these issues, we performed an integrated molecular analysis of samples from 150 JMML patients. RNA-sequencing identified ALK/ROS1 tyrosine kinase fusions (DCTN1-ALK, RANBP2-ALK, and TBL1XR1-ROS1) in 3 of 16 patients (18%) who lacked canonical RAS pathway mutations. Crizotinib, an ALK/ROS1 inhibitor, markedly suppressed ALK/ROS1 fusion-positive JMML cell proliferation in vitro. Therefore, we administered crizotinib to a chemotherapy-resistant patient with the RANBP2-ALK fusion who subsequently achieved complete molecular remission. In addition, crizotinib also suppressed proliferation of JMML cells with canonical RAS pathway mutations. Genome-wide methylation analysis identified a hypermethylation profile resembling that of acute myeloid leukemia (AML), which correlated significantly with genetic markers with poor outcomes such as PTPN11/NF1 gene mutations, 2 or more genetic mutations, an AML-type expression profile, and LIN28B expression. In summary, we identified recurrent activated ALK/ROS1 fusions in JMML patients without canonical RAS pathway gene mutations and revealed the relationships among biomarkers for JMML. Crizotinib is a promising candidate drug for the treatment of JMML, particularly in patients with ALK/ROS1 fusions.

Published

2017

35. Prognostic relevance of genetic alterations in diffuse lower-grade gliomas

Author

Tetsuichi Yoshizato, Hiromichi Suzuki, Hironori Yajima, Masahiro Mizoguchi, Yasutomo Momii, Satoru Miyano, Hideo Nakamura, Teppei Shimamura, Keitaro Matsuo, Keisuke Kataoka, Seishi Ogawa, Atsushi Natsume, Reiko Watanabe, Ichiro Ito, Fumiharu Ohka, Satoshi Shiina, Toshihiko Wakabayashi, Yoshihiro Muragaki, Yasunobu Nagata, Masashi Sanada, Tatsuya Abe, Takashi Yamamoto, Kazuya Motomura, Naoya Morita, Ichiro Takeuchi, and Kosuke Aoki

Subjects

Oncology, Adult, Male, Cancer Research, medicine.medical_specialty, DNA Copy Number Variations, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, CDKN2A, Internal medicine, Glioma, medicine, Humans, Copy-number variation, Aged, business.industry, Retinoblastoma, Brain Neoplasms, Astrocytoma, Middle Aged, medicine.disease, Prognosis, Isocitrate Dehydrogenase, Isocitrate dehydrogenase, 030220 oncology & carcinogenesis, Cohort, Basic and Translational Investigations, Mutation, Female, Neurology (clinical), Oligodendroglioma, Neoplasm Grading, business, 030217 neurology & neurosurgery

Abstract

Background Diffuse lower-grade gliomas (LGGs) are genetically classified into 3 distinct subtypes based on isocitrate dehydrogenase (IDH) mutation status and codeletion of chromosome 1p and 19q (1p/19q). However, the subtype-specific effects of additional genetic lesions on survival are largely unknown. Methods Using Cox proportional hazards regression modeling, we investigated the subtype-specific effects of genetic alterations and clinicopathological factors on survival in each LGG subtype, in a Japanese cohort of LGG cases fully genotyped for driver mutations and copy number variations associated with LGGs (n = 308). The results were validated using a dataset from 414 LGG cases available from The Cancer Genome Atlas (TCGA). Results In Oligodendroglioma, IDH-mutant and 1p/19q codeleted, NOTCH1 mutations (P = 0.0041) and incomplete resection (P = 0.0019) were significantly associated with shorter survival. In Astrocytoma, IDH-mutant, PIK3R1 mutations (P = 0.0014) and altered retinoblastoma pathway genes (RB1, CDKN2A, and CDK4) (P = 0.013) were independent predictors of poor survival. In IDH-wildtype LGGs, co-occurrence of 7p gain, 10q loss, mutation in the TERT promoter (P = 0.024), and grade III histology (P < 0.0001) independently predicted poor survival. IDH-wildtype LGGs without any of these factors were diagnosed at a younger age (P = 0.042), and were less likely to have genetic lesions characteristic of glioblastoma, in comparison with other IDH-wildtype LGGs, suggesting that they likely represented biologically different subtypes. These results were largely confirmed in the cohort of TCGA. Conclusions Subtype-specific genetic lesions can be used to stratify patients within each LGG subtype. enabling better prognostication and management.

Published

2017

36. Recurrent SPI1 (PU.1) fusions in high-risk pediatric T cell acute lymphoblastic leukemia

Author

Motohiro Kato, Takao Deguchi, Atsushi Manabe, Yoshiko Hashii, Atsushi Iwama, Yoichi Fujii, Kenichi Yoshida, Katsuyoshi Koh, Masaharu Akiyama, Akira Ohara, Masafumi Seki, Kenichi Chiba, Yasuhide Hayashi, Ryoji Kobayashi, Keizo Horibe, Masashi Sanada, Akira Oka, Changshan Wang, Ayana Kon, Seishi Ogawa, Hiroyuki Mano, Kentaro Ohki, Kyoko Masuda, Shunsuke Kimura, Satoru Miyano, Lin Lin, Hiroo Ueno, Hiromichi Suzuki, Hiroshi Moritake, Hiroshi Kawamoto, Nobutaka Kiyokawa, Yaeko Nakajima-Takagi, Junko Takita, Hiroko Tanaka, Yuki Arakawa, Ryoji Hanada, Yuichi Shiraishi, Masatoshi Takagi, Teppei Shimamura, Atsushi Sato, Yusuke Shiozawa, Keisuke Kataoka, Toshihiko Imamura, and Tomoya Isobe

Subjects

0301 basic medicine, Male, Adolescent, T cell, Biology, Transcriptome, Fusion gene, 03 medical and health sciences, T-Lymphocyte Subsets, Proto-Oncogene Proteins, Genetics, medicine, Humans, Genetic Predisposition to Disease, Progenitor cell, Child, Cell growth, Gene Expression Profiling, Infant, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Fusion protein, Survival Analysis, Gene expression profiling, 030104 developmental biology, medicine.anatomical_structure, Child, Preschool, Cancer research, Trans-Activators, Female, Gene Fusion, CD8

Abstract

The outcome of treatment-refractory and/or relapsed pediatric T cell acute lymphoblastic leukemia (T-ALL) is extremely poor, and the genetic basis for this is not well understood. Here we report comprehensive profiling of 121 cases of pediatric T-ALL using transcriptome and/or targeted capture sequencing, through which we identified new recurrent gene fusions involving SPI1 (STMN1-SPI1 and TCF7-SPI1). Cases positive for fusions involving SPI1 (encoding PU.1), accounting for 3.9% (7/181) of the examined pediatric T-ALL cases, showed a double-negative (DN; CD4-CD8-) or CD8+ single-positive (SP) phenotype and had uniformly poor overall survival. These cases represent a subset of pediatric T-ALL distinguishable from the known T-ALL subsets in terms of expression of genes involved in T cell precommitment, establishment of T cell identity, and post-β-selection maturation and with respect to mutational profile. PU.1 fusion proteins retained transcriptional activity and, when constitutively expressed in mouse stem/progenitor cells, induced cell proliferation and resulted in a maturation block. Our findings highlight a unique role of SPI1 fusions in high-risk pediatric T-ALL.

Published

2017

37. Mutational Landscape of Pediatric Acute Lymphoblastic Leukemia

Author

Lucía Fernández, Manoj Garg, H. Phillip Koeffler, Lee Yung Shih, Qiao-Yang Sun, Yan-Yi Jiang, Der Cherng Liang, Masashi Sanada, Yasunobu Nagata, Xin-Yi Loh, Wenwen Chien, Kar Tong Tan, De-Chen Lin, Hema Preethi, Hagop M. Kantarjian, Henry Yang, Li Zhen Liu, Ling-Wen Ding, Su Lin Lim, Steven M. Kornblau, Anand Mayakonda Thippeswamy, Jin Fen Xiao, Vikas Madan, Norihiko Kawamata, Seishi Ogawa, Liang Xu, Allen Eng Juh Yeoh, Michael Lill, and Satoru Miyano

Subjects

0301 basic medicine, Male, Cancer Research, ARID1A, DNA Mutational Analysis, Bioinformatics, Receptor tyrosine kinase, Mice, 2.1 Biological and endogenous factors, Aetiology, Child, Cancer, Pediatric, biology, Blotting, High-Throughput Nucleotide Sequencing, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Oncology, Child, Preschool, Female, Tyrosine kinase, Western, Biotechnology, Pediatric Research Initiative, Adolescent, Pediatric Cancer, Childhood Leukemia, Blotting, Western, Oncology and Carcinogenesis, Article, 03 medical and health sciences, Rare Diseases, Clinical Research, medicine, Genetics, Animals, Humans, Epigenetics, Oncology & Carcinogenesis, Preschool, Transcription factor, Infant, medicine.disease, 030104 developmental biology, Good Health and Well Being, CTCF, Mutation, biology.protein

Abstract

Current standard of care for patients with pediatric acute lymphoblastic leukemia (ALL) is mainly effective, with high remission rates after treatment. However, the genetic perturbations that give rise to this disease remain largely undefined, limiting the ability to address resistant tumors or develop less toxic targeted therapies. Here, we report the use of next-generation sequencing to interrogate the genetic and pathogenic mechanisms of 240 pediatric ALL cases with their matched remission samples. Commonly mutated genes fell into several categories, including RAS/receptor tyrosine kinases, epigenetic regulators, transcription factors involved in lineage commitment, and the p53/cell-cycle pathway. Unique recurrent mutational hotspots were observed in epigenetic regulators CREBBP (R1446C/H), WHSC1 (E1099K), and the tyrosine kinase FLT3 (K663R, N676K). The mutant WHSC1 was established as a gain-of-function oncogene, while the epigenetic regulator ARID1A and transcription factor CTCF were functionally identified as potential tumor suppressors. Analysis of 28 diagnosis/relapse trio patients plus 10 relapse cases revealed four evolutionary paths and uncovered the ordering of acquisition of mutations in these patients. This study provides a detailed mutational portrait of pediatric ALL and gives insights into the molecular pathogenesis of this disease. Cancer Res; 77(2); 390–400. ©2016 AACR.

Published

2017

38. KLF5 regulates the integrity and oncogenicity of intestinal stem cells

Author

Takeo Nakaya, Hans Clevers, Ryozo Nagai, Masashi Sanada, Kazuki Nakao, Masami Tanaka, Toshiro Sato, Masashi Fukayama, Makoto Mark Taketo, Ichiro Manabe, Seishi Ogawa, Masahiko Kuroda, and Hubrecht Institute for Developmental Biology and Stem Cell Research

Subjects

Cancer Research, Kruppel-Like Transcription Factors, Mice, Transgenic, Biology, Cell Transformation, Small, Inbred C57BL, Transgenic, Mice, Cancer stem cell, Intestine, Small, Animals, Humans, Induced pluripotent stem cell, Neoplastic, LGR5, Embryonic stem cell, Intestinal epithelium, Intestine, Mice, Inbred C57BL, Endothelial stem cell, Cell Transformation, Neoplastic, Oncology, Cancer research, Neoplastic Stem Cells, Stem cell, Colorectal Neoplasms, Adult stem cell

Abstract

The intestinal epithelium maintains homeostasis by a self-renewal process involving resident stem cells, including Lgr5+ crypt-base columnar cells, but core mechanisms and their contributions to intestinal cancer are not fully defined. In this study, we examined a hypothesized role for KLF5, a zinc-finger transcription factor that is critical to maintain the integrity of embryonic and induced pluripotent stem cells, in intestinal stem-cell integrity and cancer in the mouse. Klf5 was indispensable for the integrity and oncogenic transformation of intestinal stem cells. In mice, inducible deletion of Klf5 in Lgr5+ stem cells suppressed their proliferation and survival in a manner associated with nuclear localization of β-catenin (Catnb), generating abnormal apoptotic cells in intestinal crypts. Moreover, production of lethal adenomas and carcinomas by specific expression of an oncogenic mutant of β-catenin in Lgr5+ stem cells was suppressed completely by Klf5 deletion in the same cells. Given that activation of the Wnt/β-catenin pathway is the most frequently altered pathway in human colorectal cancer, our results argue that KLF5 acts as a fundamental core regulator of intestinal oncogenesis at the stem-cell level, and they suggest KLF5 targeting as a rational strategy to eradicate stem-like cells in colorectal cancer. Cancer Res; 74(10); 2882–91. ©2014 AACR.

Published

2014

39. Integrated Analysis of Copy-Number Alterations and Gene Mutations in 2,000 Patients with Myeloid Neoplasms

Author

Shigeo Fuji, Nobuhiko Uoshima, Takayuki Ishikawa, Satoru Miyano, Yuichi Shiraishi, Luca Malcovati, Hidehiro Itonaga, Kenichi Yoshida, Kazunori Imada, Masataka Taguchi, Senji Kasahara, Ryunosuke Saiki, Toru Kiguchi, Yasunori Ueda, Makoto Onizuka, Yusuke Shiozawa, Shuichi Miyawaki, Kensuke Usuki, Yoshinobu Kanda, Mikkael A. Sekeres, June Takeda, Nana Sasaki, Yogenthiran Saunthararajah, Hisashi Tsurumi, Masashi Sanada, Kenichi Chiba, Tsuyoshi Nakamaki, Kathryn M Guinta, Tetsuichi Yoshizato, Yasushi Miyazaki, Hideki Makishima, Lee-Yung Shih, Bartlomiej P Przychodzen, Hiroko Tanaka, Seishi Ogawa, Yoshiko Atsuta, Yasuhito Nannya, Jaroslaw P. Maciejewski, Mario Cazzola, Akifumi Takaori-Kondo, and Shigeru Chiba

Subjects

Monosomy, Myeloid, business.industry, Immunology, Disease progression, Myeloproliferative disease, Cancer, Cell Biology, Hematology, Gene mutation, Trisomy 8, medicine.disease, Biochemistry, medicine.anatomical_structure, Mutation (genetic algorithm), medicine, Cancer research, business

Abstract

Background Copy-number alterations (CNAs) and gene mutations are hallmarks of cancer genomes, and they are implicated in the development of myeloid neoplasm. However, their relationships have not been fully examined. To address this issue, we have recently developed a novel, next-generation sequencing-based platform for copy-number analysis, which enabled us to detect mutations and CNAs simultaneously. We applied this platform to around 2,000 cases with myeloid neoplasms. Aims We aimed at delineating the landscape of CNAs and their relationships with gene mutations in myeloid neoplasms. Methods We examined 2,101 cases with myeloid neoplasms by whole-exome sequencing (WES) or targeted deep sequencing. Excluding 116 samples showing low qualities of copy-number signals, we performed subsequent analysis on the remaining 1,985 cases with myelodysplastic syndromes (MDS, n = 1,102), myelodysplastic/myeloproliferative neoplasms (MDS/MPN, n = 140), de novo acute myeloid leukemia (de novo AML, n = 448), and secondary AML (sAML, n = 295). In copy-number analysis, total copy numbers and allele-specific copy numbers (ASCNs) were quantified based on sequencing depths and allelic ratios on genome-wide probes. Copy-number signals were corrected for multiple biases (e.g. GC content, ASCN, and fragment length). We also validated the performance of this platform through comparison with SNP-array karyotyping data in 115 de novo AML cases. CNAs longer than 5 Mb were regarded as arm-level CNAs, and those shorter than 5 Mb were regarded as focal CNAs. Results In total, we identified 4,141 CNAs (52.9 % of cases with at least one CNA), and 3,863 mutations (73.9 % of cases with at least one mutation). Most frequent alterations included -7/del(7q) (13.2 %), del(5q) (11.4 %), trisomy 8 (7.2 %), and del(20q) (5.2 %), and mutations of TET2 (12 .3 %), TP53 (11.3 %), ASXL1 (10.1%), and DNMT3A (9.9 %). To evaluate the difference of copy-number landscapes between de novo AML and myelodysplasia (MDS, MDS/MPN, and sAML), we compared the frequencies of CNAs between them. Uni-parental disomy (UPD) of 13q (FLT3) and 11p (WT1), and amplifications of 11q, 13q, and 21q (ERG) were more enriched in de novo AML, while der(1;7), UPD of 11q (CBL), and del(20q) were enriched in myelodysplasia, suggesting differential involvements of CNAs. We next analyzed the correlations between CNA profiles and prognosis in cases with myelodysplasia. Since TP53 status implies a large impact on both patients' prognosis and CNA profiles, we separately analyzed TP53-positive (n = 53) and negative (n = 686) cases with available survival data. In TP53-negative cases, -7/7qLOH (Hazard ratio(HR): 2.28, q < 0.001), and UPD of 11q (CBL) (HR: 2.60, q = 0.0034) significantly correlated with shorter overall survivals (OS), while, in TP53-positive cases, amp(11q), +19, and amp(21q) were marginally associated with shorter OS. To delineate the relationships between CNAs and mutations, we interrogated correlations between both lesions among MDS cases without TP53 alterations (n = 937). A number of significant correlations were detected, such as those between trisomy 8 and del(20q) with U2AF1 mutations (q < 0.05, for each), and monosomy 7 and amp(21q) with mutations of RUNX1 and NRAS (q < 0.01, for each). These correlations were also revealed in clustering analysis based on CNA and mutation profiles, which identified 5 unique clusters: Cluster 1 (n = 171) with trisomy 8, del(20q), and mutations of U2AF1 and ETV6, Cluster 2 (n = 43) with monosomy 7, amp(21q), and mutations of NRAS, SETBP1, and RUNX1, Cluster 3 (n = 19) with amp(1q) and amp(3q), Cluster 4 (n = 127) with those of SF3B1, TET2, and DNMT3A, and Cluster 5 (n = 50) with those of SRSF2, STAG2, ASXL1, and RUNX1. The remaining 527 cases were not assigned into any cluster due to lack of significantly correlated alterations. Finally, the temporal relationships of coexisting alterations were estimated based on their cell fractions; monosomy 7 had significantly greater cell fractions (P = 0.031) and is predicted to precede NRAS mutations, while the cell fractions of U2AF1 mutations tended to be greater than those of trisomy 8 (P = 0.063), suggesting their implications in different stages of disease progression. Conclusion An integrated analysis of CNAs and mutations in >2,000 cases revealed the impacts of CNAs on disease characteristics and provided novel insight into the interplay between CNAs and mutations in the pathogenesis of MDS. Figure Disclosures Atsuta: CHUGAI PHARMACEUTICAL CO., LTD.: Honoraria; Kyowa Kirin Co., Ltd: Honoraria. Kanda:Celgene: Consultancy, Research Funding; Novartis: Research Funding; Shionogi: Consultancy, Honoraria, Research Funding; Nippon-Shinyaku: Research Funding; Taiho: Research Funding; Asahi-Kasei: Research Funding; Bristol-Myers Squibb: Consultancy, Honoraria; Takeda: Consultancy, Honoraria, Research Funding; Eisai: Consultancy, Honoraria, Research Funding; Eisai: Consultancy, Honoraria, Research Funding; Dainippon Sumitomo: Consultancy, Honoraria, Research Funding; Otsuka: Research Funding; Kyowa-Hakko Kirin: Consultancy, Honoraria, Research Funding; Ono: Consultancy, Honoraria, Research Funding; MSD: Research Funding; Chugai: Consultancy, Honoraria, Research Funding; CSL Behring: Research Funding; Taisho-Toyama: Research Funding; Tanabe Mitsubishi: Research Funding; Dainippon Sumitomo: Consultancy, Honoraria, Research Funding; Takeda: Consultancy, Honoraria, Research Funding; Kyowa-Hakko Kirin: Consultancy, Honoraria, Research Funding; Bristol-Myers Squibb: Consultancy, Honoraria; Astellas: Consultancy, Honoraria, Research Funding; Takara-bio: Consultancy, Honoraria; Novartis: Research Funding; Astellas: Consultancy, Honoraria, Research Funding; Sanofi: Research Funding; Pfizer: Research Funding; Asahi-Kasei: Research Funding; Alexion: Consultancy, Honoraria; CSL Behring: Research Funding; Takara-bio: Consultancy, Honoraria; Mochida: Consultancy, Honoraria; Taiho: Research Funding; Celgene: Consultancy, Research Funding; Tanabe Mitsubishi: Research Funding; Taisho-Toyama: Research Funding; Pfizer: Research Funding; Sanofi: Research Funding; Mochida: Consultancy, Honoraria; Alexion: Consultancy, Honoraria; Otsuka: Research Funding. Sekeres:Celgene: Membership on an entity's Board of Directors or advisory committees; Millenium: Membership on an entity's Board of Directors or advisory committees; Syros: Membership on an entity's Board of Directors or advisory committees. Saunthararajah:EpiDestiny: Consultancy, Equity Ownership, Patents & Royalties; Novo Nordisk: Consultancy. Miyazaki:Chugai: Research Funding; Otsuka: Honoraria; Novartis: Honoraria; Nippon-Shinyaku: Honoraria; Dainippon-Sumitomo: Honoraria; Kyowa-Kirin: Honoraria. Usuki:Boehringer-Ingelheim Japan: Other: Received Research ; Daiichi Sankyo: Other: Received Research ; SymBio Pharmaceuticals Limited.,: Other: Received Research ; Novartis: Speakers Bureau; Ono Pharmaceutical: Speakers Bureau; Takeda Pharmaceutica: Speakers Bureau; Chugai Pharmaceutical: Speakers Bureau; Nippon Shinyaku: Speakers Bureau; Mochida Pharmaceutical: Speakers Bureau; MSD K.K.: Speakers Bureau; Celgene Corporation: Other: Received Research , Speakers Bureau; Sumitomo Dainippon Pharma: Other: Received Research , Speakers Bureau; Pfizer Japan: Other: Received Research ; Stellas Pharma: Other: Received Research ; Otsuka: Other: Received Research ; Kyowa Kirin: Other: Received Research ; GlaxoSmithKline K.K.: Other: Received Research ; Sanofi K.K.: Other: Received Research ; Shire Japan: Other: Received Research ; Janssen Pharmaceutical K.K: Other: Received Research . Imada:Bristol-Meyer Squibb K.K.: Honoraria; Celgene K.K.: Honoraria; Chugai Pharmaceutical Co., Ltd.: Honoraria; Kyowa Hakko Kirin Co., Ltd.: Honoraria; Ono Pharmaceutical Co., Ltd.: Honoraria; Otsuka Pharmaceutical Co., Ltd.: Honoraria; Astellas Pharma Inc.: Honoraria; Novartis Pharma K.K.: Honoraria; Takeda Pharmaceutical Co.,LTD.: Honoraria; Nippon Shinyaku Co.,Ltd.: Honoraria. Takaori-Kondo:Kyowa Kirin: Research Funding; Pfizer: Honoraria; Janssen: Honoraria; Chugai: Research Funding; Takeda: Research Funding; Ono: Research Funding; Bristol-Myers Squibb: Honoraria, Research Funding; Novartis: Honoraria; Celgene: Honoraria, Research Funding. Kiguchi:Celltrion, Inc.: Research Funding; Astellas Pharmaceutical Co., Ltd.: Research Funding; Nippon Shinyaku Co., Ltd.: Research Funding; Otsuka Pharmaceutical Co., Ltd.: Research Funding; Kyowa Hakko Kirin Co., Ltd.: Research Funding; MSD CO., Ltd.: Research Funding; Novartis Pharmaceutical Co., Ltd.: Research Funding; Sumitomo Dainippon Pharmaceutical Co., Ltd.: Research Funding; Bristol-Myeres Squibb Co., Ltd.: Research Funding; Janssen Pharmaceutical Co., Ltd.: Research Funding; Celgene Co., Ltd.: Research Funding; SymBio Pharmaceutical Co., Ltd.: Research Funding; Taiho Pharmaceutical Co., Ltd.: Research Funding; Tejin Co., Ltd.: Research Funding; Sanofi K.K., Ltd.: Research Funding. Maciejewski:Alexion: Consultancy; Novartis: Consultancy. Ogawa:Asahi Genomics: Equity Ownership; Qiagen Corporation: Patents & Royalties; Dainippon-Sumitomo Pharmaceutical, Inc.: Research Funding; RegCell Corporation: Equity Ownership; ChordiaTherapeutics, Inc.: Consultancy, Equity Ownership; Kan Research Laboratory, Inc.: Consultancy.

Published

2019

40. PPM1D and DNMT3A Mutations in Myelodysplasia and Clonal Hematopoiesis

Author

Hidehiro Itonaga, Yasuhito Nannya, Yoshikage Inoue, Satoru Miyano, Yuka Iijima-Yamashita, Yuichi Shiraishi, Masanori Motomura, Yukihide Momozawa, Hideki Makishima, Makoto Onizuka, Kenichi Chiba, Keizo Horibe, Yoshiko Atsuta, Hiroko Tanaka, Tetsuichi Yoshizato, Seishi Ogawa, Yasunobu Nagata, Wolfgang Kern, Yasushi Miyazaki, Michiaki Kubo, Masashi Sanada, Yoichiro Kamatani, Niroshan Nadarajah, Constance Baer, Claudia Haferlach, Kenichi Yoshida, and Torsten Haferlach

Subjects

Mutation, medicine.medical_treatment, Immunology, Treatment outcome, Preleukemia, Clonal hematopoiesis, Cell Biology, Hematology, Hematopoietic stem cell transplantation, Biology, medicine.disease, medicine.disease_cause, Biochemistry, Haematopoiesis, Leukemia, hemic and lymphatic diseases, medicine, Cancer research, Chromosome abnormality

Abstract

Introduction: Age-related clonal hematopoiesis (CH) has been implicated in an increased risk of myeloid neoplasms. While common driver genes mutated in CH largely overlap to those in myeloid neoplasms, a notable exception is protein phosphatase Mg2+/Mn2+dependent 1D gene (PPM1D), encoding a p53-targeting phosphatase. Although it is known to be involved in DNA damage response pathways and more frequently mutated in therapy-related myeloid neoplasms than in primary ones, its role in CH and myeloid neoplasms has not been fully understood. Aim: To identify genetic features associated with PPM1D mutations, we examined genetic profiles in the large cohorts of healthy elderly individuals and patients with myelodysplasia. Methods: We enrolled 10,826 healthy individuals (>60y) and 1,213 cases with myelodysplasia, including myelodysplastic syndromes (MDSs), myelodysplastic/myeloproliferative neoplasms (MDS/MPNs) (n=1,080), and secondary acute myeloid leukemia (sAML) (n=133), of which 567 cases were treated by hematopoietic stem cell transplantation (HSCT) through the Japan Marrow Donor Program just after sampling, and 332 of them underwent any therapy before sampling. Samples from healthy individuals were subjected to multiplex-amplicon sequencing for 22 genes, including PPM1D and other genes, related to CH or myeloid neoplasms. Myelodysplasia samples had previously been sequenced for major myeloid drivers, except for PPM1D, which was newly sequenced in this study. Results: Frequency of PPM1D mutations in myelodysplasia and healthy individuals was 3.1% and 0.42%, with a median variant allele frequency (VAF) of 0.043 and 0.056, respectively. PPM1D mutations were more frequent in cases with previous treatment (4.8%) than in those without known history of therapy (2.3%) (P=0.038). In MDS and MDS/MPN cases, 59.5% of PPM1D mutations had accompanying mutations, in which DNMT3A mutations were the most frequently identified (16.2%, n=6). These 6 cases were diagnosed with RCUD (n=1), RCMD (n=2), RAEB-2 (n=2), or CMML (n=1). The association between PPM1D and DNMT3A mutations was also seen in 7 of 45 healthy individuals with PPM1D mutations, of which one had a DNMT3A-R882 mutation. In the HSCT cohort, 192 cases harbored ≥2 mutations of the 22 CH-related genes, and the relative temporal order of these mutations was investigated using Bradley-Terry model relying on their tumor cell fractions. The estimate of PPM1D mutations tended to be smaller than that of DNMT3A mutations. To further confirm chronological order of these mutations, VAF values were compared between them in the individuals with concurrent PPM1D and DNMT3A mutations (n=13; 6 myeloid neoplasms and 7 healthy donors). In the combined cohort, the VAFs of PPM1D and DNMT3A mutations were correlated (Spearman; correlation coefficient=0.87, P=1.2x10e-5). In both neoplastic and healthy cohort, the VAFs of DNMT3A-R882 mutations were larger than those of accompanying PPM1D mutations. These findings suggest that these mutations should be acquired in the same cell populations and that DNMT3A mutations might occur prior to PPM1D mutations. With regard to copy number alterations associated with PPM1D-mutated myelodysplasia, del(5q) (16.7%) and complex(-like) karyotypes (13.9%) were among the most frequent chromosomal abnormalities. Approximately 65% of PPM1D-mutated tumor samples had normal karyotype, which was similar to PPM1D-unmutated cases. PPM1D mutations did not significantly influence overall survival, although PPM1D mutations tended to negatively affect clinical outcome among patients who were treated with HSCT (Hazard ratio, 1.61; 95% confidence interval, 0.95 to 2.70). Conclusion: PPM1D mutations were more enriched in myelodysplasia than in CH, and the median value of VAF in PPM1D mutations in CH was not significantly different from that in myelodysplasia. The size of PPM1D-mutated clones tended to be relatively smaller compared with that of clones with other mutations in myelodysplasia. PPM1D and DNMT3A mutations might be cooperatively associated in the pathogenesis of myelodysplasia and CH. Disclosures Baer: MLL Munich Leukemia Laboratory: Employment. Nadarajah:MLL Munich Leukemia Laboratory: Employment. Haferlach:MLL Munich Leukemia Laboratory: Employment, Equity Ownership. Kern:MLL Munich Leukemia Laboratory: Employment, Equity Ownership. Atsuta:CHUGAI PHARMACEUTICAL CO., LTD.: Honoraria; Kyowa Kirin Co., Ltd: Honoraria. Miyazaki:Chugai: Research Funding; Otsuka: Honoraria; Novartis: Honoraria; Nippon-Shinyaku: Honoraria; Dainippon-Sumitomo: Honoraria; Kyowa-Kirin: Honoraria. Haferlach:MLL Munich Leukemia Laboratory: Employment, Equity Ownership. Ogawa:Dainippon-Sumitomo Pharmaceutical, Inc.: Research Funding; Qiagen Corporation: Patents & Royalties; Asahi Genomics: Equity Ownership; RegCell Corporation: Equity Ownership; Kan Research Laboratory, Inc.: Consultancy; ChordiaTherapeutics, Inc.: Consultancy, Equity Ownership.

Published

2019

41. Abstract 3405: Integrated analysis of urothelial carcinoma

Author

Yoichi Fujii, Yusuke Sato, Hiromichi Suzuki, Tetsuichi Yoshizato, Kenichi Yoshida, Yuichi Shiraishi, Taketo Kawai, Tohru Nakagawa, Hiroaki Nishimatsu, Toshikazu Okaneya, Masashi Sanada, Hideki Makishima, Hiroyuki Aburatani, Satoru Miyano, Haruki Kume, and Seishi Ogawa

Subjects

Cancer Research, Oncology

Abstract

[Introduction] Accounting for 5-10% of all urothelial malignancies, upper urinary tract urothelial carcinoma (UTUC) is a relatively rare, whose molecular pathogenesis is poorly understood. We performed comprehensive genetic analysis in a large cohort of UTUC. [Materials and Methods] Surgical specimens of UTUC and matched normal samples were obtained from 209 patients with various stages who underwent nephroureterectomy, and were subjected to whole exome/RNA sequencing and methylation array. [Results] In total, we identified 33 significantly mutated genes (SMG) in UTUC, of which most frequently observed was the TERT promoter (53%), followed by KMT2D (46%), FGFR3 (42%), CDKN2A (42%), TP53 (35%), and RAS family genes (H-/K-/NRAS, 18%). More than 94% cases harbored either TP53, MDM2, FGFR3, or RASalterations in a largely mutually exclusive manner. Dirichlet process clustering based on the SMG identified 3 distinct subgroups. Group 1 cases were frequently affected by TP53, MDM2, and CCND1 alterations with complex copy number alterations (CNAs) and characterized by high stage/grade and poor prognosis. Group2 tumors were characterized by FGFR3 and CDKN2A alterations and associated with lower stage/grade and favorable prognosis, while all cases in Group3 harbored RAS-family gene alterations, showing intermediate prognosis. Gene expression analysis using unsupervised clustering identified 5 clusters. These subtypes showed strong correlation with the mutation status; cluster 1 was enriched for FGFR3 mutations, while clusters 3-5 were dominated by TP53 mutations. Most of the RAS-mutated cases were classified into cluster 2. Cluster 1,2, and 5 showed high expression of luminal markers, while clusters 3 and 4 showed high expression of basal markers. Cluster 5 also had strong expression of p53-like and EMT markers, showing a worse prognosis than other 2 luminal (+) subtypes. Cluster 3 was characterized by strong expression of SCC and immune markers, including CD274 and PDCD1LG2, with frequent squamous differentiation. Finally, clustering analysis combining UBC from TCGA revealed a close association between UTUC and UBC expression subtypes: cluster 1 was similar to the ‘luminal-papillary’ and ‘luminal’, cluster 5 to luminal-infiltrated’, and clusters 3 and 4 to ‘basal-squamous’. Interestingly, cluster 2 was totally different from any of the TCGA subgroups, which might represent an expression profile unique to UTUC. Hierarchical analysis of methylation data revealed that approximately 60% of examined samples showed CpG island methylator phenotype (CIMP). Although there was no correlation between mutation/expression subgroups and methylation profile, KMT2D mutations were significantly enriched in CIMP (-) cases (p=0.0063). [Conclusion] UTUC showed a distinct genetic landscape, associated with various clinical features. Our findings of molecular characteristics in UTUC will contribute to the development of novel diagnostics and therapeutics. Citation Format: Yoichi Fujii, Yusuke Sato, Hiromichi Suzuki, Tetsuichi Yoshizato, Kenichi Yoshida, Yuichi Shiraishi, Taketo Kawai, Tohru Nakagawa, Hiroaki Nishimatsu, Toshikazu Okaneya, Masashi Sanada, Hideki Makishima, Hiroyuki Aburatani, Satoru Miyano, Haruki Kume, Seishi Ogawa. Integrated analysis of urothelial carcinoma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 3405.

Published

2019

42. Abstract 3322: Chronology and risk-dependence of age-related remodelling of oesophageal epithelia

Author

Shigeru Tsunoda, Tomonori Hirano, Seishi Ogawa, Hiroko Tanaka, Yasuhide Takeuchi, Koshi Mimori, Kenichi Chiba, Yoichi Fujii, Hideki Makishima, Akira Yokoyama, Hiromichi Suzuki, Sachiko Minamiguchi, Manabu Muto, Yusuke Sato, Shin'ichi Miyamoto, Yusuke Shiozawa, Kosuke Aoki, Yasuhito Nannya, Nobuyuki Kakiuchi, Yoshikage Inoue, Masahiro Nakagawa, Satoru Miyano, Masashi Sanada, Keisuke Kataoka, Shinya Ohashi, Tetsuichi Yoshizato, Soo Ki Kim, Kenichi Yoshida, and Yuichi Shiraishi

Subjects

Genetics, Cancer Research, Heavy smoking, Positive selection, Cancer, Biology, medicine.disease, Oncology, CDKN2A, Age related, medicine, Cancer development, Allele frequency, Exome sequencing

Abstract

Clonal expansion in aged normal tissues has been implicated in cancer development. However, its chronology and risk-dependence are poorly understood. Esophageal squamous cell carcinoma (ESCC) is a predominant esophageal cancer among Asian populations and substantially affected by heavy smoking and drinking, likely through a ‘field effect’. To elucidate the role of these lifestyle risks on ESCC development, we investigated clonal expansion in physiologically normal esophageal epithelia (PNE) using multiple microscale sampling, as small as 0.2 mm2 in size, followed by an unbiased detection of somatic mutations with whole exome sequencing. Mutations were detected in most of PNE samples (151/157), where none of the mutations were shared between samples collected >10 mm apart. The number of mutations and their allele frequency increased with age, suggesting age-related clonal expansion in PNE (ARCE), which was significantly promoted by heavy smoking and drinking. Mutations were dominated by age-related patterns and a still poorly-defined, ‘esophagus-specific signature, as well as a COSMIC 16-like signature. The latter has recently been related to alcohol drinking and was enriched in high-risk samples, which was confirmed by whole genome sequencing of single cell-derived colonies. As many as 10 genes were significantly mutated or positively selected in ARCE. Among most commonly affected genes were NOTCH1, TP53, FAT1, PPM1D, NOTCH2, and NOTCH3, which substantially differed from those in ESCC, showing prominent over-representation of NOTCH1, PPM1D, FAT1 and NOTCH2, and significant underrepresentation of TP53, NFE2L2, and CDKN2A were significantly underrepresented, suggesting different mechanisms of positive selection between ARCE and ESCC. Driver mutations were detected more frequently and in higher numbers in high-risk PNE samples than low-risk ones, with accentuated NOTCH1, TP53 and PPM1D mutations. Analyses of densely collected micro-scale samples (0.2 mm2) disclosed fine structure of ARCE with its chronological history. Driver-mutated clones emerge multifocally from early childhood as early as Citation Format: Akira Yokoyama, Nobuyuki Kakiuchi, Tetsuichi Yoshizato, Yasuhito Nannya, Hiromichi Suzuki, Yasuhide Takeuchi, Yusuke Shiozawa, Yusuke Sato, Kosuke Aoki, Soo kim, Yoichi Fujii, Kenichi Yoshida, Keisuke Kataoka, Masahiro M. Nakagawa, Yoshikage Inoue, Tomonori Hirano, Yuichi Shiraishi, Kenichi Chiba, Hiroko Tanaka, Masashi Sanada, Shinya Ohashi, Shin’ichi Miyamoto, Shigeru Tsunoda, Koshi Mimori, Sachiko Minamiguchi, Satoru Miyano, Hideki Makishima, Manabu Muto, Seishi Ogawa. Chronology and risk-dependence of age-related remodelling of oesophageal epithelia [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 3322.

Published

2019

43. Landscape of genetic lesions in 944 patients with myelodysplastic syndromes

Author

Vera Grossmann, Yasunobu Nagata, Susanne Schnittger, Satoru Miyano, Hiroyuki Aburatani, Yusuke Okuno, Kenichi Yoshida, Claudia Haferlach, Kenichi Chiba, Hans-Ulrich Klein, Martin Dugas, Andreas Roller, Masashi Sanada, Yusuke Shiozawa, Genta Nagae, H. Phillip Koeffler, Ulrike Bacher, Ayana Kon, Seishi Ogawa, Yuichi Shiraishi, Hiroko Tanaka, Niroshan Nadarajah, Alexander Kohlmann, Wolfgang Kern, Tamara Alpermann, and Torsten Haferlach

Subjects

Neuroblastoma RAS viral oncogene homolog, Oncology, Male, Cancer Research, Leading Article, Gene mutation, Bioinformatics, Biochemistry, Somatic evolution in cancer, Risk groups, Gene Frequency, Mutation Rate, hemic and lymphatic diseases, 80 and over, Significant risk, Cancer, Aged, 80 and over, Univariate analysis, Myeloid leukemia, High-Throughput Nucleotide Sequencing, Single Nucleotide, Hematology, Middle Aged, Prognosis, myelodysplastic syndromes, prognostic score, Leukemia, Female, Biotechnology, Adult, Genetic Markers, medicine.medical_specialty, molecular markers, Clinical Sciences, Oncology and Carcinogenesis, Immunology, and over, Biology, Polymorphism, Single Nucleotide, Deep sequencing, DNA sequencing, Young Adult, Rare Diseases, Clinical Research, Internal medicine, Genetics, medicine, Humans, In patient, Genetic Testing, Polymorphism, Gene, Genetic Association Studies, Aged, Proportional Hazards Models, business.industry, Proportional hazards model, Myelodysplastic syndromes, Human Genome, Cell Biology, medicine.disease, ETV6, Mutation, next-generation sequencing, business

Abstract

Background Myelodysplastic syndromes (MDS) are a heterogeneous group of myeloid neoplasms characterized by varying degrees of cytopenias and a predisposition to acute myeloid leukemia (AML). With conspicuous clinical and biological heterogeneity in MDS, an optimized choice of treatment based on accurate diagnosis and risk stratification in individual patients is central to the current therapeutic strategy. Diagnosis and prognostication in patients with myelodysplastic syndromes (MDS) may be improved by high-throughput mutation/copy number profiling. Methods A total of 944 patients with various MDS subtypes were screened for gene mutations and deletions in 104 known/putative genes relevant to MDS using targeted deep-sequencing and/or array-based genomic hybridization. Impact of genetic lesions on overall survival (OS) was investigated by univariate analysis and a conventional Cox regression, in which the Least Absolute Shrinkage and Selection Operator (lasso) was used for selecting variables. The linear predictor from the Cox regression was then used to assign the patients into discrete risk groups. Prognostic models were constructed in a training set (n=611) and confirmed using an independent validation cohort (n=175). Results After excluding sequencing/mapping errors and known or possible polymorphisms, a total of 2,764 single nucleotide variants (SNVs) and insertions/deletions (indels) were called in 96 genes as high-probability somatic changes. A total of 47 genes were considered as statistically significantly mutated (p10% of the cases. Less common mutations (2−10%) involved U2AF1, ZRSR2, STAG2, TP53, EZH2, CBL, JAK2, BCOR, IDH2, NRAS, MPL, NF1, ATM, IDH1, KRAS, PHF6, BRCC3, ETV6, and LAMB4. Intratumoral heterogeneity was evident in as many as 456 cases (48.3%), even though the small number of gene mutations available for evaluation was thought substantially to underestimate the real frequency. The number of observed intratumoral subpopulations tended to correlate with the number of detected mutations and therefore, advanced WHO subtypes and risk groups with poorer prognosis. Mean variant allele frequencies (VAFs) showed significant variations among major gene targets, suggesting the presence of clonogenic hierarchy among these common mutations during clonal evolution in MDS. The impact of these genetic lesions on clinical outcomes was initially investigated in 875 patients. In univariate analysis, 25 out of 48 genes tested significantly affected overall survival negatively (P A total of 14 genes, together with age, gender, white blood cell counts, hemoglobin, platelet counts, cytogenetic score in IPSS-R, were finally selected for the Cox regression in a proportional hazard model and based on the linear predictor of the regression model, we constructed a prognostic model (novel molecular model), in which patients were classified into 4 risk groups showing significantly different OS (“low”, “intermediate”, “high”, and “very high risk”) with 3-year survival of 95.2%, 69.3%, 32.8%, and 5.3%, respectively (P Conclusions Large-scale genetic and molecular profiling by cytogenetics, NGS and array-CGH not only provided novel insights into the pathogenesis and clonal evolution of MDS, but also helped to develop a powerful prognostic model based on gene mutations and other clinical variables that could be used for risk prediction. Molecular profiling of multiple target genes in MDS is feasible and provides an invaluable tool for improved diagnosis, biologic subclassification and especially prognostication for patients with MDS. Disclosures: Grossmann: MLL Munich Leukemia Laboratory: Employment. Bacher:MLL Munich Leukemia Laboratory: Employment. Schnittger:MLL Munich Leukemia Laboratory: Employment, Equity Ownership. Alpermann:MLL Munich Leukemia Laboratory: Employment. Roller:MLL Munich Leukemia Laboratory: Employment. Nadarajah:MLL Munich Leukemia Laboratory: Employment. Kohlmann:MLL Munich Leukemia Laboratory: Employment. Haferlach:MLL Munich Leukemia Laboratory: Employment, Equity Ownership. Kern:MLL Munich Leukemia Laboratory: Employment, Equity Ownership. Haferlach:MLL Munich Leukemia Laboratory: Employment, Equity Ownership.

Published

2013

44. The landscape of somatic mutations in Down syndrome–related myeloid disorders

Author

Kazuhiro Nakamura, Yuichi Shiraishi, Kiminori Terui, Hiroko Tanaka, Shai Izraeli, Yasuhide Hayashi, Aiko Sato-Otsubo, Norio Shiba, Daisuke Hasegawa, Masashi Sanada, Kenichi Yoshida, Hiromichi Suzuki, Satoru Miyano, Tsutomu Toki, Asahito Hama, Myoung-ja Park, Kenichi Chiba, Rika Kanezaki, Yasunobu Nagata, Souichi Adachi, Koji Kato, Kiyoshi Kawakami, Yusuke Okuno, Ryosei Nishimura, Ru Nan Wang, Hideki Muramatsu, Yusuke Sato, Ayana Kon, Seishi Ogawa, Keiko Tsukamoto, Hirokazu Kanegane, Etsuro Ito, and Seiji Kojima

Subjects

CCCTC-Binding Factor, Down syndrome, Myeloid, Chromosomal Proteins, Non-Histone, Chromosomes, Human, Pair 21, Clone (cell biology), Cell Cycle Proteins, Biology, Leukemoid Reaction, Acute megakaryoblastic leukemia, stomatognathic system, Leukemia, Megakaryoblastic, Acute, Genetics, medicine, Humans, Enhancer of Zeste Homolog 2 Protein, GATA1 Transcription Factor, Myeloid Cells, Epigenetics, Cell Proliferation, Myeloproliferative Disorders, Base Sequence, Gene Expression Profiling, Polycomb Repressive Complex 2, Nuclear Proteins, GATA1, Sequence Analysis, DNA, medicine.disease, Repressor Proteins, Leukemia, medicine.anatomical_structure, CTCF, Cancer research, Down Syndrome

Abstract

Transient abnormal myelopoiesis (TAM) is a myeloid proliferation resembling acute megakaryoblastic leukemia (AMKL), mostly affecting perinatal infants with Down syndrome. Although self-limiting in a majority of cases, TAM may evolve as non-self-limiting AMKL after spontaneous remission (DS-AMKL). Pathogenesis of these Down syndrome-related myeloid disorders is poorly understood, except for GATA1 mutations found in most cases. Here we report genomic profiling of 41 TAM, 49 DS-AMKL and 19 non-DS-AMKL samples, including whole-genome and/or whole-exome sequencing of 15 TAM and 14 DS-AMKL samples. TAM appears to be caused by a single GATA1 mutation and constitutive trisomy 21. Subsequent AMKL evolves from a pre-existing TAM clone through the acquisition of additional mutations, with major mutational targets including multiple cohesin components (53%), CTCF (20%), and EZH2, KANSL1 and other epigenetic regulators (45%), as well as common signaling pathways, such as the JAK family kinases, MPL, SH2B3 (LNK) and multiple RAS pathway genes (47%).

Published

2013

45. Clonal leukemic evolution in myelodysplastic syndromes with TET2 and IDH1/2 mutations

Author

Yasunobu Nagata, Chang-Liang Lai, Masashi Sanada, Kenichi Chiba, Satoru Miyano, Yuichi Shiraishi, Seishi Ogawa, Ming-Chung Kuo, Lee-Yung Shih, Hiroko Tanaka, Chein-Fuang Huang, Jin-Hou Wu, Der-Cherng Liang, Tung-Huei Lin, Tung-Liang Lin, En-Hui Lee, Hsiao-Wen Kao, Yu-Shu Shih, and Yusuke Okuno

Subjects

Male, Karyotype, Gene Dosage, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, IDH2, Dioxygenases, chemistry.chemical_compound, Gene Frequency, Bone Marrow, Proto-Oncogene Proteins, hemic and lymphatic diseases, CEBPA, medicine, Humans, Secondary Acute Myeloid Leukemia, Aged, Aged, 80 and over, Mutation, Leukemia, Myelodysplastic syndromes, Myeloid leukemia, De novo Myelodysplastic Syndrome, Articles, Hematology, Middle Aged, medicine.disease, Isocitrate Dehydrogenase, Clone Cells, DNA-Binding Proteins, Cell Transformation, Neoplastic, RUNX1, chemistry, Myelodysplastic Syndromes, Immunology, Disease Progression, Cancer research, Female

Abstract

Somatic mutations of TET2, IDH1, and IDH2 have been described in myelodysplastic syndrome. The impact of these mutations on outcome of myelodysplastic syndrome and their progression to secondary acute myeloid leukemia remains unclear. Mutation status of TET2, IDH1 and IDH2 was investigated in a cohort of 46 paired myelodysplastic syndrome/acute myeloid leukemia samples and 122 non-paired cases with de novo myelodysplastic syndrome, to clarify their roles in the evolution of myelodysplastic syndrome to acute myeloid leukemia. Among the 168 de novo myelodysplastic syndrome patients, the frequency of TET2, IDH1, and IDH2 mutations was 18.5%, 4.2% and 6.0%, respectively. TET2/IDH mutations had no impact on survivals, while TET2 mutations were significantly associated with rapid progression to acute myeloid leukemia. Seventeen of the 46 paired myelodysplastic syndrome/secondary acute myeloid leukemia samples harbored TET2/IDH mutations; none acquired these mutations in acute myeloid leukemia phase. Progression to acute myeloid leukemia was accompanied by evolution of a novel clone or expansion of a minor pre-existing subclone of one or more distinct mutations in 12 of the 17 cases with TET2/IDH mutations. A minor subclone in 3 cases with biallelic TET2 inactivation subsequently expanded, indicating biallelic TET2 mutations play a role in acute myeloid leukemia progression. Twelve patients acquired other genetic lesions, and/or showed increased relative mutant allelic burden of FLT3-ITD, N/K-RAS, CEBPA or RUNX1 during acute myeloid leukemia progression. Our findings provide a novel insight into the role of TET2/IDH mutation in the pathogenesis of myelodysplastic syndrome and subsequent progression to acute myeloid leukemia.

Published

2013

46. Exome sequencing identifies secondary mutations of SETBP1 and JAK3 in juvenile myelomonocytic leukemia

Author

Hideki Makishima, Kenichi Yoshida, Seiji Kojima, Xinan Wang, Hiroko Tanaka, Koji Nakanishi, Satoru Miyano, Sayoko Doisaki, Kenichi Chiba, Hideki Muramatsu, Ayana Kon, Seishi Ogawa, Nao Yoshida, Mariko Takahashi, Yoshiyuki Takahashi, Asahito Hama, Yuichi Shiraishi, Jaroslaw P. Maciejewski, Masashi Sanada, Hirotoshi Sakaguchi, Yusuke Okuno, and Yinyan Xu

Subjects

Male, Neuroblastoma RAS viral oncogene homolog, Biology, Gene mutation, medicine.disease_cause, Article, Proto-Oncogene Proteins p21(ras), Germline mutation, hemic and lymphatic diseases, Genetics, medicine, Humans, Exome, Child, Germ-Line Mutation, Exome sequencing, Mutation, Juvenile myelomonocytic leukemia, Infant, Newborn, High-Throughput Nucleotide Sequencing, Infant, Janus Kinase 3, Nuclear Proteins, medicine.disease, PTPN11, Leukemia, Myelomonocytic, Juvenile, Child, Preschool, Disease Progression, Cancer research, Female, Carrier Proteins, Signal Transduction

Abstract

Juvenile myelomonocytic leukemia (JMML) is an intractable pediatric leukemia with poor prognosis whose molecular pathogenesis is poorly understood, except for somatic or germline mutations of RAS pathway genes, including PTPN11, NF1, NRAS, KRAS and CBL, in the majority of cases. To obtain a complete registry of gene mutations in JMML, whole-exome sequencing was performed for paired tumor-normal DNA from 13 individuals with JMML (cases), which was followed by deep sequencing of 8 target genes in 92 tumor samples. JMML was characterized by a paucity of gene mutations (0.85 non-silent mutations per sample) with somatic or germline RAS pathway involvement in 82 cases (89%). The SETBP1 and JAK3 genes were among common targets for secondary mutations. Mutations in the latter were often subclonal and may be involved in the progression rather than the initiation of leukemia, and these mutations associated with poor clinical outcome. Our findings provide new insights into the pathogenesis and progression of JMML.

Published

2013

47. Somatic SETBP1 mutations in myeloid malignancies

Author

Inés Gómez-Seguí, Bartlomiej P Przychodzen, Kenichi Yoshida, Yuichi Shiraishi, Kenichi Chiba, Seiji Kojima, Ronald Paquette, Jaroslaw P. Maciejewski, Hiraku Mori, Mariko Takahashi, Nhu Nguyen, Hiroko Tanaka, Kristbjorn O. Gudmundsson, Satoru Miyano, Michael A. McDevitt, Bandana A. Vishwakarma, Yang Du, Andres Jerez, Masashi Sanada, Kathryn M Guinta, Yogen Saunthararajah, Hideki Muramatsu, Seishi Ogawa, Lee-Yung Shih, Yasunobu Nagata, Mikkael A. Sekeres, Hideki Makishima, Kwok Peng Ng, Hirotoshi Sakaguchi, and Yusuke Okuno

Subjects

Myeloid, Somatic cell, SETBP1, Chronic myelomonocytic leukemia, SECONDARY AML, Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, hemic and lymphatic diseases, Genetics, medicine, MUTATION, Exome, 030304 developmental biology, 0303 health sciences, CMML, Myelodysplastic syndromes, medicine.disease, 3. Good health, Leukemia, medicine.anatomical_structure, MONOSOMY 7, 030220 oncology & carcinogenesis, Immunology, Cancer research, Atypical chronic myeloid leukemia

Abstract

Here we report whole-exome sequencing of individuals with various myeloid malignancies and identify recurrent somatic mutations in SETBP1, consistent with a recent report on atypical chronic myeloid leukemia (aCML). Closely positioned somatic SETBP1 mutations encoding changes in Asp868, Ser869, Gly870, Ile871 and Asp880, which match germline mutations in Schinzel-Giedion syndrome (SGS), were detected in 17% of secondary acute myeloid leukemias (sAML) and 15% of chronic myelomonocytic leukemia (CMML) cases. These results from deep sequencing demonstrate a higher mutational detection rate than reported with conventional sequencing methodology. Mutant cases were associated with advanced age and monosomy 7/deletion 7q (-7/del(7q)) constituting poor prognostic factors. Analysis of serially collected samples indicated that SETBP1 mutations were acquired during leukemic evolution. Transduction with mutant Setbp1 led to the immortalization of mouse myeloid progenitors that showed enhanced proliferative capacity compared to cells transduced with wild-type Setbp1. Somatic mutations of SETBP1 seem to cause gain of function, are associated with myeloid leukemic transformation and convey poor prognosis in myelodysplastic syndromes (MDS) and CMML.

Published

2013

48. Adult T-cell leukemia cells are characterized by abnormalities ofHeliosexpression that promote T cell growth

Author

Seishi Ogawa, Tadanori Yamochi, Kaoru Uchimaru, Katsuaki Kawanami, Masashi Sanada, Satomi Asanuma, Kazunari Yamaguchi, Toshiki Watanabe, Kazumi Nakano, Atae Utsunomiya, Aiko Sato-Otsubo, Seiichiro Kobayashi, Satsuki Muto, Makoto Yamagishi, and Masako Iwanaga

Subjects

Cytoplasm, Cancer Research, T-Lymphocytes, T cell, T-cell leukemia, Cell Growth Processes, HeliOS, Lymphocyte proliferation, Biology, Cell Line, Ikaros Transcription Factor, immune system diseases, Cell Line, Tumor, hemic and lymphatic diseases, medicine, Humans, Leukemia-Lymphoma, Adult T-Cell, Protein Isoforms, Human T-lymphotropic virus 1, Gene knockdown, Exons, Original Articles, General Medicine, medicine.disease, Phenotype, Leukemia, HEK293 Cells, medicine.anatomical_structure, Oncology, Immunology, Cancer research, Ectopic expression, HeLa Cells, Signal Transduction

Abstract

Molecular abnormalities involved in the multistep leukemogenesis of adult T-cell leukemia (ATL) remain to be clarified. Based on our integrated database, we focused on the expression patterns and levels of Ikaros family genes, Ikaros, Helios, and Aiolos, in ATL patients and HTLV-1 carriers. The results revealed profound deregulation of Helios expression, a pivotal regulator in the control of T-cell differentiation and activation. The majority of ATL samples (32/37 cases) showed abnormal splicing of Helios expression, and four cases did not express Helios. In addition, novel genomic loss in Helios locus was observed in 17/168 cases. We identified four ATL-specific short Helios isoforms and revealed their dominant-negative function. Ectopic expression of ATL-type Helios isoform as well as knockdown of normal Helios or Ikaros promoted T-cell growth. Global mRNA profiling and pathway analysis showed activation of several signaling pathways important for lymphocyte proliferation and survival. These data provide new insights into the molecular involvement of Helios function in the leukemogenesis and phenotype of ATL cells, indicating that Helios deregulation is one of the novel molecular hallmarks of ATL.

Published

2013

49. Concurrent loss of Ezh2 and Tet2 cooperates in the pathogenesis of myelodysplastic disorders

Author

George R. Wendt, Atsushi Iwama, Genta Nagae, Koutaro Yokote, Haruhiko Koseki, Yutaka Suzuki, Asuka Kamio, Motohiko Oshima, Seishi Ogawa, Tomoya Muto, Satoru Miyagi, Chiaki Nakaseko, Yasunobu Nagata, Kazuya Shimoda, Masashi Sanada, Makiko Mochizuki-Kashio, Sumio Sugano, Atsunori Saraya, Goro Sashida, and Hiroyuki Aburatani

Subjects

Myeloid, Immunology, macromolecular substances, Gene mutation, Biology, medicine.disease_cause, Article, Dioxygenases, Cohort Studies, Mice, Myeloproliferative Disorders, hemic and lymphatic diseases, Proto-Oncogene Proteins, medicine, Immunology and Allergy, Animals, Humans, Enhancer of Zeste Homolog 2 Protein, Myeloproliferative neoplasm, Mice, Knockout, Mutation, Myelodysplastic syndromes, Tumor Suppressor Proteins, Tet methylcytosine dioxygenase 2, fungi, Polycomb Repressive Complex 2, food and beverages, medicine.disease, Hematopoietic Stem Cells, Hematopoiesis, DNA-Binding Proteins, Mice, Inbred C57BL, Haematopoiesis, Disease Models, Animal, medicine.anatomical_structure, Myelodysplastic Syndromes, Cancer research, Genome-Wide Association Study

Abstract

Deletion of Ezh2 results in transcriptional repression of developmental regulator genes, derepression of oncogenic polycomb targets, and induction of MDS/MPN-like disease in mice that is exacerbated by concurrent deletion of Tet2., Polycomb group (PcG) proteins are essential regulators of hematopoietic stem cells. Recent extensive mutation analyses of the myeloid malignancies have revealed that inactivating somatic mutations in PcG genes such as EZH2 and ASXL1 occur frequently in patients with myelodysplastic disorders including myelodysplastic syndromes (MDSs) and MDS/myeloproliferative neoplasm (MPN) overlap disorders (MDS/MPN). In our patient cohort, EZH2 mutations were also found and often coincided with tet methylcytosine dioxygenase 2 (TET2) mutations. Consistent with these findings, deletion of Ezh2 alone was enough to induce MDS/MPN-like diseases in mice. Furthermore, concurrent depletion of Ezh2 and Tet2 established more advanced myelodysplasia and markedly accelerated the development of myelodysplastic disorders including both MDS and MDS/MPN. Comprehensive genome-wide analyses in hematopoietic progenitor cells revealed that upon deletion of Ezh2, key developmental regulator genes were kept transcriptionally repressed, suggesting compensation by Ezh1, whereas a cohort of oncogenic direct and indirect polycomb targets became derepressed. Our findings provide the first evidence of the tumor suppressor function of EZH2 in myeloid malignancies and highlight the cooperative effect of concurrent gene mutations in the pathogenesis of myelodysplastic disorders.

Published

2013

50. Long-term outcome of 6-month maintenance chemotherapy for acute lymphoblastic leukemia in children

Author

Masashi Sanada, Yuichi Shiraishi, Akira Ohara, Motohiro Kato, Ayumu Manabe, Takeshi Inukai, Tomoo Osumi, Takahiro Aoki, Nobuyuki Kakiuchi, Yuichi Taneyama, Masatoshi Takagi, Daisuke Hasegawa, Hiroo Ueno, Katsuyoshi Koh, Daisuke Tomizawa, Masahiro Tsuchida, K Kaizu, Hiroaki Goto, Junko Takita, Yasuhiro Arakawa, Shinya Ishimaru, Keisuke Kato, Yusuke Sato, Satoru Miyano, Tomohiko Taki, Seishi Ogawa, Kenichi Yoshida, Kenichi Chiba, Masafumi Seki, Hirotoshi Tanaka, and Mayuko Okuya

Subjects

Male, Cancer Research, medicine.medical_specialty, Time Factors, Microarray, Adolescent, Translocation, Genetic, Maintenance Chemotherapy, 03 medical and health sciences, 0302 clinical medicine, Maintenance therapy, Recurrence, Risk Factors, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Genetic Predisposition to Disease, Child, Childhood Acute Lymphoblastic Leukemia, Survival analysis, Maintenance chemotherapy, Bone Marrow Smear, business.industry, Cytogenetics, Infant, Newborn, Infant, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Prognosis, Survival Analysis, Surgery, Treatment Outcome, Oncology, 030220 oncology & carcinogenesis, Child, Preschool, Female, Hyperdiploidy, business, 030215 immunology

Abstract

In the treatment of childhood acute lymphoblastic leukemia (ALL), excess shortening of maintenance therapy resulted in high relapse rate, as shown by our previous trial, TCCSG L92-13, in which maintenance therapy was terminated at 1 year from initiation of treatment. In this study, we aimed to confirm the long-term outcome of L92-13, and to identify who can or cannot be cured by shorter duration of maintenance therapy. To obtain sentinel cytogenetics information that had been missed before, we performed genetic analysis with genomic microarray and target intron-capture sequencing from diagnostic bone marrow smear. Disease-free survival (DFS) at 10 years from the end of therapy was 66.0±2.8%. Females (n=138) had better DFS (74.6±3.7%) than males (n=142, 57.5±4.2%, P=0.002). Patients with TCF3-PBX1 (n=11) and ETV6-RUNX1 (n=16) had excellent DFS (90.9±8.7% and 93.8±6.1%, respectively), whereas high hyperdiploidy (n=23) was the most unfavorable subgroup, with 56.6±10.3% of DFS. Short duration of therapy can cure more than half of pediatric ALL, especially females, TCF3-PBX1 and ETV6-RUNX1. Our retrospective observations suggest a gender/karyotype inhomogeneity on the impact of brief therapy.

Published

2016