SERIZAWA Kentaro
Department of Medicine | Lecturer |
Last Updated :2024/11/22
■Researcher comments
List of press-related appearances
1
■Researcher basic information
J-Global ID
■Career
■Research activity information
Paper
- Kodai Kuriyama; Shigeo Fuji; Ayumu Ito; Noriko Doki; Yuta Katayama; Hiroyuki Ohigashi; Tetsuya Nishida; Kentaro Serizawa; Tetsuya Eto; Naoyuki Uchida; Yoshinobu Kanda; Masatsugu Tanaka; Ken-Ichi Matsuoka; Hideyuki Nakazawa; Junya Kanda; Takahiro Fukuda; Yoshiko Atsuta; Masao OgataTransplantation and cellular therapy 30 (5) 514.e1-514.e13 2024/05The purine analog fludarabine (Flu) plays a central role in reduced-intensity conditioning and myeloablative reduced-toxicity conditioning regimens because of limited nonhematologic toxicities. Few reports assess the impact of different dose of Flu on the clinical outcomes and the Flu doses vary across reports. To compare the effect of Flu dose, the clinical outcomes of patients who received Flu and busulfan (FB; n = 1647) or melphalan (Flu with melphalan (FM); n = 1162) conditioning for unrelated bone marrow transplantation were retrospectively analyzed using Japanese nationwide registry data. In the FB group, high-dose Flu (180 mg/m2; HFB) and low-dose Flu (150/125 mg/m2; LFB) were given to 1334 and 313 patients, respectively. The 3-year overall survival (OS) rates were significantly higher in the HFB group than in the LFB group (49.5% versus 39.2%, P < .001). In the HFB and LFB groups, the cumulative incidences were 30.4% and 36.6% (P = .058) for 3-year relapse and 25.1% and 28.1% (P = .24) for 3-year nonrelapse mortality (NRM), respectively. In the multivariate analysis for OS and relapse, Flu dose was identified as an independent prognostic factor (hazard ratio: 0.83, P = .03; hazard ratio: 0.80, P = .043). In the FM group, high-dose Flu (180 mg/m2; HFM) and low-dose Flu (150/125 mg/m2; LFM) were given to 118 and 1044 patients, respectively. The OS, relapse, and NRM after 3 years did not differ significantly between the HFM and LFM groups (48.3% versus 48.8%, P = .92; 23.7% versus 27.2%, P = .55; 31.9% versus 30.8%, P = .67). These findings suggest that high-dose Flu was associated with favorable outcomes in the FB group but not in the FM group.
- Koji Kato; Takeshi Sugio; Takashi Ikeda; Kanako Yoshitsugu; Kana Miyazaki; Junji Suzumiya; Go Yamamoto; Sung-Won Kim; Kazuhiro Ikegame; Yasufumi Uehara; Yasuo Mori; Jun Ishikawa; Nobuhiro Hiramoto; Tetsuya Eto; Hideyuki Nakazawa; Hikaru Kobayashi; Kentaro Serizawa; Makoto Onizuka; Takahiro Fukuda; Yoshiko Atsuta; Ritsuro SuzukiBone marrow transplantation 59 (3) 306 - 314 2024/03Allogeneic hematopoietic stem cell transplantation (allo-HSCT) is a currative treatment modality for diffuse large B-cell lymphoma (DLBCL) because of the intrinsic graft-versus-lymphoma effect. However, limited information is available regarding which patients with relapsed or refractory DLBCL are likely to benefit from allo-HSCT. We retrospectively analyzed data from 1268 DLBCL patients who received allo-HSCT. The overall survival and progression-free survival (PFS) rates were 30.3% and 21.6% at 3 years, respectively. Multivariate analysis revealed that stable or progressive disease at transplantation, male patient, poorer performance status at transplantation, and shorter intervals from previous transplantation were associated independently with a lower PFS. Four prognostic factors were used to construct a prognostic index for PFS, predicting 3-year PFS of 55.4%, 43.7%, 20.4% and 6.6%, respectively. The prognostic model predicted relapse rates following allo-HSCT accordingly (P < 0.0001), whereas did not predict transplantation-related mortality (P = 0.249). The prognostic index can identify a subgroup of DLBCL patients who benefit from allo-HSCT and it is worthwhile to evaluate whether this model is also applicable to patients undergoing allo-HSCT in cases of relapse after chimeric antigen receptor engineered T-cell therapy, although the application of allo-HSCT has been declining with the increase of novel immunotherapies.
- Masamitsu Yanada; Satoshi Yamasaki; Tadakazu Kondo; Takahito Kawata; Kaito Harada; Naoyuki Uchida; Noriko Doki; Satoshi Yoshihara; Yuta Katayama; Tetsuya Eto; Masatsugu Tanaka; Satoru Takada; Toshiro Kawakita; Tetsuya Nishida; Shuichi Ota; Kentaro Serizawa; Makoto Onizuka; Yoshinobu Kanda; Takahiro Fukuda; Yoshiko Atsuta; Takaaki KonumaLeukemia 38 (3) 513 - 520 2024/03Allogeneic hematopoietic cell transplantation (HCT) is the last option for long-term survival for patients with chemotherapy-refractory acute myeloid leukemia (AML). By using the Japanese nationwide registry data, we analyzed 6927 adults with AML having undergone first allogeneic HCT while not in complete remission (CR) between 2001 and 2020. The 5-year overall survival (OS), relapse, and non-relapse mortality (NRM) rates were 23%, 53%, and 27%, respectively. Multivariate analysis identified several factors predictive of OS mainly through their effects on relapse (cytogenetics, percentage of blasts in the peripheral blood, and transplantation year) and NRM (age, sex, and performance status). As regards disease status, relapsed disease was associated with a higher risk of overall mortality than primary induction failure (PIF). The shorter duration of the first CR increased the risks of relapse and overall mortality for the relapsed group, and the longer time from diagnosis to transplantation did so for the PIF group. Our experience compiled over the past two decades demonstrated that >20% of patients still enjoy long-term survival with allogeneic HCT performed during non-CR and identified those less likely to benefit from allogeneic HCT. Future efforts are needed to reduce the risk of posttransplant relapse in these patients.
- Hiromi Hayashi; Makoto Iwasaki; Hideki Nakasone; Reo Tanoshima; Masashi Shimabukuro; Wataru Takeda; Tetsuya Nishida; Shinichi Kako; Shin-Ichiro Fujiwara; Yuta Katayama; Masashi Sawa; Kentaro Serizawa; Ken-Ichi Matsuoka; Naoyuki Uchida; Takashi Ikeda; Hiroyuki Ohigashi; Kentaro Fukushima; Moeko Hino; Yoshinobu Kanda; Takahiro Fukuda; Yoshiko Atsuta; Junya KandaCytotherapy 26 (2) 178 - 184 2024/02BACKGROUND AIMS: This study aimed to comprehensively assess the impact of stem cell selection between bone marrow (BM) and peripheral blood (PB) in unrelated hematopoietic stem cell transplantation (HSCT) for hematological malignancies. Our objective was to identify specific factors associated with better transplant outcomes. METHODS: A retrospective analysis was conducted using data from the Japanese HSCT registry. Inclusion criteria were patients aged 0-70 years who underwent their first unrelated HSCT with BM or PB, with an 8/8 or 7/8 allele HLA match for hematological malignancies between 2010 and 2020. RESULTS: Among 10 295 patients, no significant difference was observed in overall survival, relapse, graft-versus-host disease (GVHD)-free, relapse-free survival (GRFS) or non-relapse mortality between the groups. Patients who received PB showed no clear difference in acute GVHD but had a greater rate of chronic GVHD, resulting in poor chronic GVHD-free, relapse-free survival (CRFS). Subgroup analyses highlighted the importance of patient-specific factors in source selection. Patients with non-Hodgkin lymphoma and a greater hematopoietic cell transplantation-comorbidity index showed better CRFS and GRFS when BM was the preferred source. Similar trends were observed among patients with standard-risk disease for CRFS. However, no such trends were evident among patients aged 0-24 years, indicating that both sources are viable choices for young patients. CONCLUSIONS: This real-world retrospective analysis showed similar basic outcomes for BM and PB in an unrelated setting. The results support that BM may still be preferred over PB, especially when the long-term quality of life is a major concern. A consideration of individual factors can further optimize transplant success. Further research is warranted to explore the long-term implications of stem cell source selection.
- Takahiro Haeno; Shinya Rai; Yoshiaki Miyake; Maiko Inoue; Ko Fujimoto; Aki Fujii; Yoshio Iwata; Shuji Minamoto; Takahide Taniguchi; Hiroaki Kakutani; Hiroaki Inoue; Takahiro Kumode; Kentaro Serizawa; Yasuhiro Taniguchi; Chikara Hirase; Yasuyoshi Morita; Hirokazu Tanaka; Yoichi Tatsumi; Takashi Ashida; Itaru MatsumuraJournal of clinical and experimental hematopathology : JCEH 63 (2) 99 - 107 2023/06We retrospectively evaluated long-term outcomes of high dose chemotherapy followed by autologous stem cell transplant (HDC/ASCT) in patients with diffuse large B-cell lymphoma (DLBCL). Between 2004 and 2020, 46 DLBCL patients received HDC/ASCT in our institution, including 12 patients (26.1%), who received as an upfront setting (UFS). At a median follow-up time of 69 months (range, 2-169 months), the 5-year progression-free survival (PFS) rates were 82.5% (95%CI, 46.1-95.3%) in the UFS, and 57.8% (95%CI, 38.1-73.2%) in the relapsed or refractory (R/R) patients (n=34), respectively. The 5-year PFS rates were 62.3% (95%CI, 34.0-81.3%) in primary resistant (n=13) or early relapsing (within 1 year from the initial diagnosis) patients (n=4), and 53.3% (95%CI, 25.9-74.6%) in those relapsing >1 year after the initial diagnosis (n=17), with no statistically significant difference (p=0.498). In R/R patients, multivariate analysis showed that the remission status before HDC/ASCT was an independent poor prognostic factor for progression-free survival (hazard ratio [HR], 17.0; 95%CI, 3.35-86.6; p=0.000630) and high-risk category in the international prognostic index for OS (HR, 9.39; 95%CI, 1.71-51.6; p=0.0100). The incidence of non-relapse mortality by 5 years, and 10 years were 12.2%, and 15.2%, respectively. Eleven patients (23.9%) developed second malignancies, which was the most frequent late complication after HDC/ASCT, with 5-year, and 10-year cumulative incidence of 16.9%, 22.5%, respectively. In conclusion, HDC/ASCT is effective for chemo-sensitive R/R DLBCL regardless of the timing and lines of therapy. However, careful observation is required, considering the long-term complications such as secondary malignancies.
- 田中 宏和; 芹澤 憲太郎; 松村 到日本臨床 (株)日本臨床社 81 (6) 806 - 812 0047-1852 2023/06
- 田中 宏和; 芹澤 憲太郎; 松村 到血液内科 (有)科学評論社 86 (2) 266 - 271 2185-582X 2023/02
- Ryosuke Fujiwara; Yasuhiro Taniguchi; Shinya Rai; Yoshio Iwata; Aki Fujii; Ko Fujimoto; Takahiro Kumode; Kentaro Serizawa; Yasuyoshi Morita; J Luis Espinoza; Hirokazu Tanaka; Hitoshi Hanamoto; Itaru MatsumuraBiochemical and biophysical research communications 626 156 - 166 2022/08We previously reported that the antipsychotic drug chlorpromazine (CPZ), which inhibits the formation of clathrin-coated vesicles (CCVs) essential for endocytosis and intracellular transport of receptor tyrosine kinase (RTK), inhibits the growth/survival of acute myeloid leukemia cells with mutated RTK (KIT D816V or FLT3-ITD) by perturbing the intracellular localization of these molecules. Here, we examined whether these findings are applicable to epidermal growth factor receptor (EGFR). CPZ dose-dependently inhibited the growth/survival of the non-small cell lung cancer (NSCLC) cell line, PC9 harboring an EGFR-activating (EGFR exon 19 deletion). In addition, CPZ not only suppressed the growth/survival of gefitinib (GEF)-resistant PC9ZD cells harboring T790 M, but also restored their sensitivities to GEF. Furthermore, CPZ overcame GEF resistance caused by Met amplification in HCC827GR cells. As for the mechanism of CPZ-induced growth suppression, we found that although CPZ hardly influenced the phosphorylation of EGFR, it effectively reduced the phosphorylation of ERK and AKT. When utilized in combination with trametinib (a MEK inhibitor), dabrafenib (an RAF inhibitor), and everolimus (an mTOR inhibitor), CPZ suppressed the growth of PC9ZD cells cooperatively with everolimus but not with trametinib or dabrafenib. Immunofluorescent staining revealed that EGFR shows a perinuclear pattern and was intensely colocalized with the late endosome marker, Rab11. However, after CPZ treatment, EGFR was unevenly distributed in the cells, and colocalization with the early endosome marker Rab5 and EEA1 became more apparent, indicating that CPZ disrupted the intracellular transport of EGFR. These results suggest that CPZ has therapeutic potential for NSCLC with mutated EGFR by a novel mechanism different from conventional TKIs alone or in combination with other agents.
- Takahiro Kumode; Hirokazu Tanaka; Jorge Luis Esipinoza; Shinya Rai; Yasuhiro Taniguchi; Ryosuke Fujiwara; Keigo Sano; Kentaro Serizawa; Yoshio Iwata; Yasuyoshi Morita; Itaru MatsumuraInternational journal of hematology 115 (3) 310 - 321 2022/03C-type lectin-like receptor 2 (CLEC-2) expressed on megakaryocytes plays important roles in megakaryopoiesis. We found that CLEC-2 was expressed in about 20% of phenotypical long-term hematopoietic stem cells (LT-HSCs), which expressed lower levels of HSC-specific genes and produced larger amounts of megakaryocyte-related molecules than CLEC-2low LT-HSCs. Although CLEC-2high LT-HSCs had immature clonogenic activity, cultured CLEC-2high LT-HSCs preferentially differentiated into megakaryocytes. CLEC-2high HSCs yielded 6.8 times more megakaryocyte progenitors (MkPs) and 6.0 times more platelets 2 weeks and 1 week after transplantation compared with CLEC-2low LT-HSCs. However, platelet yield from CLEC-2high HSCs gradually declined with the loss of MkPs, while CLEC-2low HSCs self-renewed long-term, indicating that CLEC-2high LT-HSCs mainly contribute to early megakaryopoiesis. Treatment with pI:C and LPS increased the proportion of CLEC-2high LT-HSCs within LT-HSCs. Almost all CLEC-2low LT-HSCs were in the G0 phase and barely responded to pI:C. In contrast, 54% of CLEC-2high LT-HSCs were in G0, and pI:C treatment obliged CLEC-2high LT-HSCs to enter the cell cycle and differentiate into megakaryocytes, indicating that CLEC-2high LT-HSCs are primed for cell cycle entry and rapidly yield platelets in response to inflammatory stress. In conclusion, CLEC-2high LT-HSCs appear to act as a reserve for emergent platelet production under stress conditions.
- Kentaro Serizawa; Hirokazu Tanaka; Takeshi Ueda; Ayano Fukui; Hiroaki Kakutani; Takahide Taniguchi; Hiroaki Inoue; Takahiro Kumode; Yasuhiro Taniguchi; Shinya Rai; Chikara Hirase; Yasuyoshi Morita; J. Luis Espinoza; Yoichi Tatsumi; Takashi Ashida; Itaru MatsumuraInternational Journal of Hematology Springer Science and Business Media LLC 115 (3) 336 - 349 0925-5710 2022/03Side population (SP) is known to include therapy-resistant cells in various cancers. Here, we analyzed SP using multiple myeloma (MM) samples. The SP accounted for 2.96% in MM cells from newly diagnosed MM (NDMM). CD34 was expressed in 47.8% of SP cells, but only in 2.11% of bulk MM cells. CD34+ MM cells expressed more immature cell surface markers and a gene signature than CD34- MM cells. CD34+ but not CD34- MM cells possessed clonogenic activities and showed long-term self-renewal activities in xenotransplantation assays. Similarly, whereas 2.20% of MM cells were CD34+ in NDMM (n = 38), this proportion increased to 42.6% in minimal residual disease (MRD) samples (n = 16) (p < 0.001) and to 17.7% in refractory/relapsed MM (RRMM) (n = 30) (p < 0.01). Cell cycle analysis showed that 24.7% of CD34+ MM cells from NDMM were in G0 phase while this proportion was 54.9% in MRD (p < 0.05) and 14.5% in RRMM, reflecting the expansion of MM. Together, CD34+ MM cells with long-term self-renewal activities persist as MRD in cell cycle quiescence or remain as therapy-resistant cells in RRMM, substantiating the necessity of targeting this population to improve clinical outcomes of MM.
- Shinya Rai; Hiroaki Inoue; Kazuko Sakai; Hitoshi Hanamoto; Mitsuhiro Matsuda; Yasuhiro Maeda; Takahiro Haeno; Yosaku Watatani; Takahiro Kumode; Kentaro Serizawa; Yasuhiro Taniguchi; Chikara Hirase; J Luis Espinoza; Yasuyoshi Morita; Hirokazu Tanaka; Takashi Ashida; Yoichi Tatsumi; Kazuto Nishio; Itaru MatsumuraCancer science 113 (2) 660 - 673 2022/02We previously examined the utility of rituximab-bendamustine (RB) in patients with follicular lymphoma (FL) exhibiting less than optimal responses to 2 cycles of the R-CHOP chemotherapy regimen. The aim of this study was to identify molecular biomarkers that can predict prognosis in RB-treated patients in the context of the prospective cohort. We first analyzed the mutational status of 410 genes in diagnostic tumor specimens by target capture and Sanger sequencing. CREBBP, KMT2D, MEF2B, BCL2, EZH2, and CARD11 were recurrently mutated as reported before, however none was predictive for progression-free survival (PFS) in the RB-treated patients (n = 34). A gene expression analysis by nCounter including 800 genes associated with carcinogenesis and/or the immune response showed that expression levels of CD8+ T-cell markers and half of the genes regulating Th1 and Th2 responses were significantly lower in progression of disease within the 24-mo (POD24) group (n = 8) than in the no POD24 group (n = 31). Collectively, we selected 10 genes (TBX21, CXCR3, CCR4, CD8A, CD8B, GZMM, FLT3LG, CD3E, EOMES, GZMK), and generated an immune infiltration score (IIS) for predicting PFS using principal component analysis, which dichotomized the RB-treated patients into immune IIShigh (n = 19) and IISlow (n = 20) groups. The 3-y PFS rate was significantly lower in the IISlow group than in the IIShigh group (50.0% [95% CI: 27.1-69.2%] vs. 84.2% [95% CI: 58.7-94.6%], P = .0237). Furthermore, the IIS was correlates with absolute lymphocyte counts at diagnosis (r = 0.460, P = .00355). These results suggest that the T-cell-associated immune markers could be useful to predict prognosis in RB-treated FL patients. (UMIN:000 013 795, jRCT:051 180 181).
- Yasuhiro Taniguchi; Naoto Takahashi; Masatomo Miura; Chikara Hirase; Sanae Sueda; Jorge Luis Espinoza; Shinya Rai; Shoko Nakayama; Kentaro Serizawa; Takahiro Kumode; Yosaku Watatani; Yasuyoshi Morita; Hirokazu Tanaka; Itaru MatsumuraInternal medicine (Tokyo, Japan) 59 (21) 2745 - 2749 2020/11We recently treated a chronic myeloid leukemia (CML) patient with liver and renal dysfunction, who was undergoing hemodialysis (HD). He was treated with 50 mg dasatinib (DAS) once daily just before HD. The maximum plasma concentration of DAS was 227 ng/mL on a non-HD day and 46.9 ng/mL on a HD day. He was subsequently treated with 200 mg bosutinib (BOS) once daily. The plasma concentration of BOS changed from 74.5 ng/mL before HD to 58.8 ng/mL after HD. Our results indicate that close monitoring of the plasma tyrosine kinase inhibitor concentrations should be considered in CML patients with organ impairment.
- Hiroaki Inoue; Shinya Rai; Hirokazu Tanaka; J Luis Espinoza; Yosaku Watatani; Takahiro Kumode; Kentaro Serizawa; Shoko Nakayama; Yasuhiro Taniguchi; Yasuyoshi Morita; Yoichi Tatsumi; Takashi Ashida; Itaru MatsumuraBritish journal of haematology 191 (2) 243 - 252 2020/05 [Refereed]
Despite duodenal-type follicular lymphoma (DTFL) being morphologically, immunophenotypically and genetically indistinguishable from nodal FL (nFL), this entity typically shows a significantly better prognosis. Here, we analysed the tumour immune microenvironments of diagnostic specimens from patients with DTFL (n = 30), limited-stage FL (LSFL; n = 19) and advanced-stage FL (ASFL; n = 31). The mean number of CD8+ tumour-infiltrating lymphocytes (TILs) in the neoplastic follicles was higher in DTFL (1,827/mm2 ) than in LSFL (1,150/mm2 ) and ASFL (1,188/mm2 ) (P = 0·002, P = 0·002, respectively). In addition, CD8+ PD1- T cells with non-exhausting phenotype were more abundant in the peripheral blood (PB) of DTFL than in LSFL and ASFL, indicating that DTFL may exhibit a better and longer-lasting T cell-mediated immune response. Moreover, whereas FOXP3+ CTLA-4+ effector regulatory T cells (eTregs) were rarely observed in the neoplastic follicles of DTFL (mean: 12/mm2 ), they were more abundant in LSFL (78/mm2 ) and ASFL (109/mm2 ) (P = 2·80 × 10-5 , P = 4·74 × 10-8 , respectively), and the numbers of eTregs correlated inversely with those of CD8+ TILs (r = -0267; P = 0·018). Furthermore, DTFL showed significantly fewer circulating FOXP3hi CD45RA- CD25hi eTregs (0·146%) than ASFL (0·497%) and healthy controls (0·639%) (P = 0·0003, P = 6·79 × 10-7 , respectively). These results suggest that the augmented anti-tumour immune reactions may contribute to a better prognosis on DTFL. - Junichi Miyatake; Hiroaki Inoue; Kentarou Serizawa; Yasuyoshi Morita; J L Espinoza; Hirokazu Tanaka; Takahiro Shimada; Yoichi Tatsumi; Takashi Ashida; Itaru MatsumuraInternal medicine (Tokyo, Japan) 57 (10) 1445 - 1453 0918-2918 2018/05 [Refereed]
Patients with mycosis fungoides (MF), the most common subtype of primary cutaneous T-cell lymphoma, have an increased risk of developing secondary malignancies. We herein report two rare cases of MF concurring with diffuse large B cell lymphoma (B lymphoid lineage) and acute myeloid leukemia (myeloid lineage) in two otherwise healthy elderly patients. Potential etiologic factors, including the impact of the therapy-associated inflammatory response on the development of secondary tumors in patients with MF, are discussed. Further clinical, experimental and genetic studies are needed to elucidate possible physiopathogenic associations among the three concurrent malignancies occurring in the cases presented here. - Kentaro Serizawa; Hirokazu Tanaka; Yasuyoshi Morita; Takahide Taniguchi; Takashi Ashida; Itaru MatsumuraFrontiers in oncology 8 204 - 204 2018 [Refereed]
Myelodysplastic syndrome (MDS) is a heterogeneous group of clonal disorders of hematopoietic stem cells, characterized by dysplastic hematopoiesis and dysregulated immune system resulting in various clinical conditions. Paraneoplastic inflammatory syndromes, which are well known to be associated with MDS, show response to immune-modulated therapy and often disappear during the course of hematologic management. Azacitidine (5-Aza) was shown to prolong survival of high-risk MDS patients, however, the effects of 5-Aza on paraneoplastic inflammation in MDS have yet to be elucidated. 5-Aza was administered to a 60-year-old man with MDS accompanying Sweet's syndrome at a dose of 75 mg/m2/daily subcutaneously for 7 days every 28 days. 5-Aza was not only effective in controlling systemic symptoms caused by paraneoplastic inflammation, but hematologic improvements were also observed after four cycles of the 5-Aza treatment. Immune profiling in peripheral blood before and after 5-Aza treatment revealed that the effector and naive regulatory T cells in lymphocytes drastically increased after the 5-Aza treatment, i.e., 5-Aza might induce a shift in lymphocytic populations toward immunosuppression in this patient. Our results raised the immune-mediated effect of 5-Aza on both dysplastic hematopoiesis and paraneoplastic inflammation in myelodyplastic syndromes. - 芹澤 憲太郎; 芦田 隆司; 谷口 貴英; 谷口 康博; 森田 泰慶; 田中 宏和; 嶋田 高広; 辰巳 陽一; 松村 到臨床血液 (一社)日本血液学会-東京事務局 58 (12) 2386 - 2391 0485-1439 2017/12急性骨髄性白血病に対する同種骨髄移植後に一旦造血機能の回復を認めたものの汎血球減少を来し、二次性生着不全と判断してドナーリンパ球輸注(donor lymphocyte infusion,DLI)を施行したところ著効を示した症例を経験したので報告する。症例は64歳女性。急性骨髄性白血病の部分寛解に対して非血縁者間同種骨髄移植を施行した。速やかに生着し、complete remission with incomplete blood count recovery(CRi)に到達したが、day 110から汎血球減少症が出現した。血液検査および骨髄穿刺では、再発や血球貪食症候群は認めないものの、キメリズム解析でドナー比率が経時的に低下したため、二次性生着不全と診断した。Granulocyte-colony stimulating factor(G-CSF)の投与と輸血にて経過観察したが、造血の改善は認めなかった。患者が再移植を希望しなかったため、DLIを施行した(CD3陽性細胞:1.0×107/kg、単回投与)ところ、有害事象を認めることなく、血球は速やかに改善した。(著者抄録)
- Yasuhiro Taniguchi; Hirokazu Tanaka; Espinoza J. Luis; Kazuko Sakai; Takahiro Kumode; Keigo Sano; Kentarou Serizawa; Shinya Rai; Yasuyoshi Morita; Hitoshi Hanamoto; Kazuo Tsubaki; Kazuto Nishio; Itaru MatsumuraINTERNATIONAL JOURNAL OF HEMATOLOGY SPRINGER JAPAN KK 106 (5) 691 - 703 0925-5710 2017/11 [Refereed]
Myeloproliferative neoplasms (MPNs), including polycythemia vera and essential thrombocythemia, are frequently associated with thrombotic complications. Prevention of thrombotic events is thus a primary aim of the current treatment for these disorders. Although it is known that microparticles (MPs), which are small vesicles released from cell membranes and circulate in the blood, directly contribute to thrombosis via their procoagulant activity, potential associations between plasma levels of MPs and the risk of thrombotic events in MPNs have not been reported. In the present study, we characterized plasma levels of MPs and assessed their potential association with the occurrence of thrombotic events in 59 patients with MPNs. Plasma levels of procoagulant MPs expressing tissue factor (TF+ MPs) were significantly higher in patients suffering thrombotic events than in patients without such events (median/mu l plasma: 33.8 vs 47.2, p = 0.02). Among patients who developed thrombotic events, irrespective of patients' blood counts, TF+ MP were significantly higher in patients without cytoreductive therapy than in those receiving cytoreductive therapy (101.2 vs. 42.5, p < 0.001). These results suggest that elevated levels of TF+ MP may be considered as a novel surrogate marker for thrombotic events in MPN patients. Further studies are needed to clarify the mechanism involved. - T. Kumode; H. Tanaka; R. Fujiwara; K. Sano; K. Serizawa; Y. Taniguchi; S. Rai; I. MatsumuraHAEMATOLOGICA FERRATA STORTI FOUNDATION 102 452 - 453 0390-6078 2017/06
- Serizawa K; Ashida T; Taniguchi T; Taniguchi Y; Morita Y; Tanaka H; Shimada T; Tatsumi Y; Matsumura I[Rinsho ketsueki] The Japanese journal of clinical hematology 58 (12) 2386 - 2391 0485-1439 2017 [Refereed]
Here we report a case of secondary graft failure that was effectively treated with donor lymphocyte infusion (DLI). A 64-year-old female patient with acute myeloid leukemia obtained partial remission with azacitidine therapy and subsequently underwent unrelated allogeneic bone marrow transplantation (BMT). After confirming successful engraftment and achieving complete remission with incomplete blood count recovery, she was subsequently followed up at an outpatient clinic. A routine test performed by day 110 after BMT revealed the presence of pancytopenia. A bone marrow aspirate did not reveal any evidence of disease relapse or hemophagocytic syndrome but demonstrated hematopoietic insufficiency. Donor chimerism also declined over time; thus, the patient was diagnosed with secondary graft failure. Supportive treatment, including granulocyte-colony stimulating factor and blood transfusion, failed to improve the blood parameters. Because the patient refused a second BMT, we performed DLI on day 147 after BMT (CD3+ cells: 1.0×107/kg, single dose). Consequently, the blood cell count improved promptly and dramatically without adverse events. Following this, we discussed the case and analyzed the related literature. - Serizawa Kentaro; Morita Yasuyoshi; Watatani Yosaku; Oyama Yasuyo; Hirase Chikara; Tanaka Hirokazu; Miyatake Junichi; Tatsumi Yoichi; Ashida Takashi; Matsumura ItaruANNALS OF ONCOLOGY 26 108 0923-7534 2015/11 [Refereed]
- Yasuyoshi Morita; Masakatsu Emoto; Kentaro Serizawa; Shinya Rai; Chikara Hirase; Yoshitaka Kanai; Yasuyo Ohyama; Toshihiko Shiga; Hirokazu Tanaka; Junichi Miyatake; Yoichi Tatsumi; Takashi Ashida; Masatomo Kimura; Masafumi Ito; Itaru MatsumuraINTERNAL MEDICINE JAPAN SOC INTERNAL MEDICINE 54 (11) 1393 - 1396 0918-2918 2015 [Refereed]
A 68-year-old man was referred to our hospital due to a high fever and pancytopenia. Neither tumors nor infectious lesions were detected. Hemophagocytosis was observed on the bone marrow (BM) smear, although without abnormal cells. Prednisolone therapy was ineffective for the patient's high fever. Later on, we obtained the results of a BM biopsy indicating the presence of infiltration of atypical Reed-Sternberg cells, leading to a diagnosis of HIV-negative primary bone marrow Hodgkin lymphoma (PBMHL). However, the patient died of multiple organ failure before receiving chemotherapy. As the clinical course of PBMHL is rapid, physicians must keep in mind its possibility in similar cases. - Successful anticoagulant therapy for two pregnant PNH patients, and prospects for the eculizumab eraYasuyoshi Morita; Jun-Ichi Nishimura; Takahiro Shimada; Hirokazu Tanaka; Kentaro Serizawa; Yasuhiro Taniguchi; Mitsuhiro Tsuritani; Yuzuru Kanakura; Itaru MatsumuraInternational Journal of Hematology 97 (4) 491 - 497 0925-5710 2013/04 [Refereed]
Paroxysmal nocturnal hemoglobinuria (PNH) is an acquired stem cell disorder characterized by intravascular hemolysis and thrombosis. The most serious complication is thrombosis, the risk of which is augmented by the hyper-coagulable state that occurs during pregnancy despite this risk, however, young female PNH patients often desire to have a baby. We recently experienced two successful deliveries in PNH patients, who were treated with anticoagulant therapy during their pregnancies. Meanwhile, given the potential benefit of eculizumab (Soliris), a humanized monoclonal antibody against C5, in reducing thrombosis and hemolysis, it represents a promising therapeutic option for the treatment of pregnant PNH patients in combination with, or in replacement of, anticoagulant therapy. © The Japanese Society of Hematology 2013. - Cytokine profiles in relapsed multiple myeloma patients undergoing febrile reactions to lenalidomideYasuyoshi Morita; Takahiro Shimada; Terufumi Yamaguchi; Shinya Rai; Chikara Hirase; Masakatsu Emoto; Kentaro Serizawa; Yasuhiro Taniguchi; Mayuko Ojima; Yoichi Tatsumi; Takashi Ashida; Itaru MatsumuraINTERNATIONAL JOURNAL OF HEMATOLOGY SPRINGER TOKYO 94 (6) 583 - 584 0925-5710 2011/12 [Refereed]
- 芹澤憲太郎; 松村到Progress in Medicine 31 (11) 2631 - 2635 0287-3648 2011/11
- 芹澤憲太郎; 松村到Prog Med 31 (11) 2581 - 2586 0287-3648 2011/11
- 芹澤憲太郎; 川田修平; 金丸昭久血液フロンティア 20 (10) 1809 - 1812 1344-6940 2010/09
MISC
- 鳥畑さやか; 江原裕基; 助臺美帆; 下出孟史; 岩崎早苗; 李篤史; 兵頭咲紀; 宮本あかね; 松浦可歩; 濱田傑; 三宅義昭; 波江野高大; 角谷宏明; 源周治; 口分田貴裕; 芹澤憲太郎; 谷口康博; 森田康慶; 芦田隆司; 芦田隆司 日本造血・免疫細胞療法学会総会プログラム・抄録集 44th- 2022
- 波江野高大; 三宅義昭; 井上舞子; 藤本昂; 角谷宏明; 藤井晶; 源周治; 口分田貴裕; 芹澤憲太郎; 谷口康博; 頼晋也; 平瀬主悦; 森田泰慶; 田中宏和; 辰巳陽一; 芦田隆司; 松村到 日本造血・免疫細胞療法学会総会プログラム・抄録集 44th- 2022
- 鳥畑さやか; 江原裕基; 助臺美帆; 下出孟史; 岩崎早苗; 李篤史; 川口美紅; 木下優子; 渡瀬遂生; 濱田傑; 金澤仁美; 兵頭咲紀; 宮本あかね; 波江野高大; 角谷宏明; 源周治; 口分田貴裕; 芹澤憲太郎; 谷口康博; 森田泰慶; 榎本明史; 芦田隆司; 芦田隆司 日本血液学会学術集会抄録(Web) 83rd- 2021
- KMFに登録されたボルテゾミブとIMiDs両剤に抵抗性の再発骨髄腫の予後解析(Clinical outcomes of relapsed myeloma, dual refractory to bortezomib and IMiDs in KMF registry)藤原 亮介; 田中 宏和; 芹澤 憲太郎; 金子 仁臣; 志村 勇司; 太田 健介; 淵田 真一; 中谷 綾; 諫田 淳也; 八木 秀男; 和田 勝也; 小杉 智; 魚嶋 伸彦; 柴山 浩彦; 小原 尚恵; 中谷 英仁; 内山 人二; 足立 陽子; 飯田 正人; 濱田 常義; 松田 光弘; 高折 晃史; 野村 昌作; 島崎 千尋; 日野 雅之; 黒田 純也; 谷脇 雅史; 今田 和典; 金倉 譲; 松村 到 臨床血液 59- (9) 1739 -1739 2018/09
- 症候性骨髄腫1414例の後方視的解析 関西骨髄腫フォーラムからの最新報告(Retrospective analyses of 1,414 symptomatic multiple myeloma cases: update from Kansai Myeloma Forum)田中 宏和; 芹澤 憲太郎; 中谷 綾; 金子 仁臣; 太田 健介; 小杉 智; 八木 秀男; 花本 仁; 淵田 真一; 志村 勇司; 柴山 浩彦; 小原 尚恵; 中谷 英仁; 諫田 淳也; 魚嶋 伸彦; 和田 勝也; 烏野 隆博; 松井 利充; 内山 人二; 松田 光弘; 足立 陽子; 高折 晃史; 黒田 純也; 谷脇 雅史; 島崎 千尋; 日野 雅之; 今田 和典; 野村 昌作; 金倉 譲; 松村 到 臨床血液 59- (9) 1510 -1510 2018/09
- 山田枝里佳; 斉藤花往里; 藤本昂; 角谷宏明; 岩田吉生; 谷口貴英; 源周治; 大山泰世; 口分田貴裕; 井上宏昭; 芹澤憲太郎; 谷口康博; 頼晋也; 平瀬主税; 森田泰慶; 田中宏和; 岡野意浩; 坂田尚己; 芦田隆司; 松村到 日本アフェレシス学会雑誌 37- (Supplement) 2018
- 芹澤憲太郎; 森田泰慶; 谷口貴英; 岩田吉生; 源周治; 大山泰世; 川内超矢; 金井良高; 頼晋也; 平瀬主税; 田中宏和; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到 日本造血細胞移植学会総会プログラム・抄録集 37th- 2015
- 口分田貴裕; 岩田吉夫; 谷口貴秀; 源周治; 大山泰世; 佐野圭吾; 川内超矢; 芹澤憲太郎; 谷口康博; 頼晋也; 金井良高; 平瀬主税; 森田泰慶; 田中宏和; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到 日本造血細胞移植学会総会プログラム・抄録集 37th- 2015
- 宮武淳一; 岩田吉生; 谷口貴英; 源周治; 大山泰世; 川内超矢; 佐野圭吾; 口分田貴裕; 芹澤憲太郎; 谷口康博; 頼晋也; 金井良高; 平瀬主税; 森田泰慶; 田中宏和; 辰巳陽一; 芦田隆司; 松村到 日本造血細胞移植学会総会プログラム・抄録集 37th- 2015
- 芦田隆司; 芦田隆司; 岩田吉生; 谷口貴英; 源周治; 芹沢憲太郎; 川内超矢; 大山泰世; 金井良高; 頼晋也; 平瀬主税; 森田泰慶; 竹中孝子; 福島靖幸; 川野亜美; 山田枝里佳; 井手大輔; 菅野知恵美; 加藤祐子; 椿本祐子; 松村到; 松村到 日本造血細胞移植学会総会プログラム・抄録集 37th- 2015
- 芦田隆司; 芦田隆司; 福井彩乃; 大山泰世; 芹沢憲太郎; 頼晋也; 平瀬主税; 中野勝彦; 福島靖幸; 川野亜美; 山田枝里佳; 井手大輔; 前田岳宏; 菅野知恵美; 加藤祐子; 椿本祐子; 金光靖; 松村到; 松村到 日本輸血細胞治療学会誌 61- (2) 2015
- 芹澤憲太郎; 森田泰慶; 江本正克; 大山泰世; 福井彩乃; 井上宏昭; 川内超矢; 金井良高; 平瀬主税; 田中宏和; 嶋田高広; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到 日本造血細胞移植学会総会プログラム・抄録集 36th- 2014
- 芦田隆司; 芦田隆司; 芹澤憲太郎; 川内超矢; 江本正克; 谷口康博; 福井彩乃; 大山泰世; 井上宏昭; 金井良高; 平瀬主税; 森田泰慶; 宮武淳一; 福島靖幸; 川野亜美; 井手大輔; 菅野知恵美; 加藤祐子; 椿本祐子; 伊藤志保; 松村到; 松村到 日本造血細胞移植学会総会プログラム・抄録集 36th- 2014
- 芦田隆司; 芦田隆司; 綿谷陽作; 川内超矢; 江本正克; 芹沢憲太郎; 平瀬主税; 谷口康博; 森田泰慶; 川西一信; 宮武淳一; 川野亜美; 山田枝里佳; 井手大輔; 菅野知恵美; 加藤祐子; 椿本祐子; 伊藤志保; 峯佳子; 藤田往子; 松村到; 松村到 日本造血細胞移植学会総会プログラム・抄録集 35th- 2013
- 川西一信; 綿谷陽作; 谷口康博; 川内超矢; 芹澤憲太郎; 江本正克; 金井良高; 頼晋也; 平瀬主税; 森田泰慶; 田中宏和; 嶋田高広; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到 日本造血細胞移植学会総会プログラム・抄録集 35th- 2013
- 芹澤憲太郎; 綿谷陽作; 谷口康博; 森田泰慶; 川内超矢; 江本正克; 平瀬主税; 田中宏和; 嶋田高広; 川西一信; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到 日本造血細胞移植学会総会プログラム・抄録集 35th- 2013
- 芹澤憲太郎; 川西一信; 大山泰世; 尾嶋真由子; 井上宏昭; 口分田貴裕; 江本正克; 谷口康博; 金井良高; 頼晋也; 笹川淳; 平瀬主税; 山口晃史; 森田泰慶; 田中宏和; 嶋田高広; 辰巳陽一; 芦田隆司; 松村到 日本造血細胞移植学会総会プログラム・抄録集 34th- 2012
- 芦田隆司; 川野亜美; 山田枝里佳; 井手大輔; 菅野知恵美; 加藤祐子; 椿本祐子; 伊藤志保; 峯佳子; 藤田往子; 井上宏昭; 口分田貴裕; 芹澤憲太郎; 江本正克; 平瀬主税; 山口晃史; 森田泰慶; 川西一信; 辰巳陽一; 松村到; 松村到 日本造血細胞移植学会総会プログラム・抄録集 34th- 2012
Books and other publications
Lectures, oral presentations, etc.
- フルダラビン+ブスルファンを用いた同種造血幹細胞移植における重症口腔粘膜炎発症のリスク因子の解析(Risk factor of oral mucositis after allogeneic hematopoietic stem cell transplantation using FLU/BU)鳥畑 さやか; 江原 裕基; 助臺 美帆; 下出 孟史; 岩崎 早苗; 李 篤史; 川口 美紅; 木下 優子; 渡瀬 遂生; 濱田 傑; 金澤 仁美; 兵頭 咲紀; 宮本 あかね; 波江野 高大; 角谷 宏明; 源 周治; 口分田 貴裕; 芹澤 憲太郎; 谷口 康博; 森田 泰慶; 榎本 明史; 芦田 隆司日本血液学会学術集会 2021/09 (一社)日本血液学会
- Risk factor of oral mucositis after allogeneic hematopoietic stem cell transplantation using FLU/BU(和訳中)鳥畑 さやか; 江原 裕基; 助臺 美帆; 下出 孟史; 岩崎 早苗; 李 篤史; 川口 美紅; 木下 優子; 渡瀬 遂生; 濱田 傑; 金澤 仁美; 兵頭 咲紀; 宮本 あかね; 波江野 高大; 角谷 宏明; 源 周治; 口分田 貴裕; 芹澤 憲太郎; 谷口 康博; 森田 泰慶; 榎本 明史; 芦田 隆司日本血液学会学術集会 2021/09 (一社)日本血液学会
- Gilteritinib treatment for extramedullary relapse of FLT3-ITD acute myeloid leukemia口分田貴裕; 頼晋也; 波江野高大; 角谷宏明; 源周治; 綿谷陽作; 芹澤憲太郎; 谷口康博; 森田泰慶; 田中宏和; 芦田隆司; 松村到日本造血細胞移植学会総会プログラム・抄録集 2021
- Clinical usefulness of Letermovir for patients with stem cell transplantation谷口康博; 平瀬主税; 芦田隆司; 波江野高大; 角谷宏明; 源周治; 綿谷陽作; 口分田貴裕; 芹澤憲太郎; 頼晋也; 森田泰慶; 田中宏和; 辰巳陽一; 松村到日本造血細胞移植学会総会プログラム・抄録集 2021
- Outcomes of allo-SCT for patients in non-remission especially with chemoresistance谷口康博; 芦田隆司; 森田泰慶; 平瀬主税; 頼晋也; 中山聖子; 芹澤憲太郎; 口分田貴裕; 井上宏昭; 岩田吉男; 谷口貴英; 源周治; 角谷宏明; 藤本昂; 小森舞子; 波江野高大; 三宅義昭; 辰巳陽一; 田中宏和; 松村到日本造血細胞移植学会総会プログラム・抄録集 2020
- 十二指腸原発濾胞性リンパ腫における抗腫瘍免疫の寄与 [Not invited]井上 宏昭; 頼 晋也; 口分田 貴裕; 芹澤 憲太郎; 谷口 康博; 中山 聖子; 森田 泰慶; Luis Espinoza J; 田中 宏和; 辰巳 陽一; 芦田 隆司; 松村 到日本リンパ網内系学会会誌 2019/05
- 診断に難渋した下腿難治性潰瘍の一例西村京子; 西村京子; 竹本剛司; 竹本剛司; 引網梨奈; 引網梨奈; 芹澤憲太郎; 白鳥隆宏日本創傷外科学会総会・学術集会プログラム・抄録集 2019
- KMFに登録されたボルテゾミブとIMiDs両剤に抵抗性の再発骨髄腫の予後解析 [Not invited]藤原亮介; 田中宏和; 芹澤憲太郎; 金子仁臣; 志村勇司; 太田健介; 淵田真一; 中谷 綾; 諫田淳也; 八木秀男; 和田勝也; 小杉智; 魚嶋伸彦; 柴山浩彦; 小原尚恵; 中谷英仁; 内山人二; 足立陽子; 飯田正人; 濱田常義; 松田光弘; 高折晃史; 野村昌作; 島崎千尋; 日野雅之; 黒田純也; 谷脇雅史; 今田和典; 金倉譲; 松村到第80回日本血液学会学術集会 2018/10
- 症候性骨髄腫1414例の後方視的解析:関西骨髄腫フォーラムからの最新報告 [Not invited]田中宏和; 芹澤憲太郎; 中谷 綾; 金子仁臣; 太田健介; 小杉 智; 八木秀男; 花本 仁; 淵田真一; 志村勇司; 柴山浩彦; 小原尚恵; 中谷英仁; 諫田淳也; 魚嶋伸彦; 和田勝也; 烏野隆博; 松井利充; 内山人二; 松田光弘; 足立陽子; 高折晃史; 黒田純也; 谷脇雅史; 島崎千尋; 日野雅之; 今田和典; 野村昌作; 金倉 譲; 松村 到第80回日本血液学会学術集会 2018/10
- 末梢血幹細胞採取前のCD34細胞数測定の有用性 [Not invited]山田 枝里佳; 斉藤 花往里; 藤本 昂; 角谷 宏明; 岩田 吉生; 谷口 貴英; 源 周治; 大山 泰世; 口分田 貴裕; 井上 宏昭; 芹澤 憲太郎; 谷口 康博; 頼 晋也; 平瀬 主税; 森田 泰慶; 田中 宏和; 岡野 意浩; 坂田 尚己; 芦田 隆司; 松村 到日本アフェレシス学会雑誌 2018/10
- KMFに登録されたボルテゾミブとIMiDs両剤に抵抗性の再発骨髄腫の予後解析(Clinical outcomes of relapsed myeloma, dual refractory to bortezomib and IMiDs in KMF registry) [Not invited]藤原 亮介; 田中 宏和; 芹澤 憲太郎; 金子 仁臣; 志村 勇司; 太田 健介; 淵田 真一; 中谷 綾; 諫田 淳也; 八木 秀男; 和田 勝也; 小杉 智; 魚嶋 伸彦; 柴山 浩彦; 小原 尚恵; 中谷 英仁; 内山 人二; 足立 陽子; 飯田 正人; 濱田 常義; 松田 光弘; 高折 晃史; 野村 昌作; 島崎 千尋; 日野 雅之; 黒田 純也; 谷脇 雅史; 今田 和典; 金倉 譲; 松村 到臨床血液 2018/09
- 骨髄異形成症候群に合併したSweet病に対するアザシチジンの免疫学的効果(Immunological effects of azacitidin on Sweet's disease associated with myelodysplastic syndromes) [Not invited]谷口 貴英; 芹澤 憲太郎; 田中 宏和; 森田 泰慶; 谷口 康博; 辰巳 陽一; 芦田 隆司; 松村 到臨床血液 2018/09
- CD34陽性ヒト骨髄腫幹細胞の同定と特性解析(Identification and characterization of CD34+ myeloma cell population as myeloma-initiating cells) [Not invited]芹澤 憲太郎; 田中 宏和; 福井 彩乃; 藤原 亮介; 佐野 圭吾; 口分田 貴裕; 谷口 康博; 森田 泰慶; ルイス・エスピノザ; 辰巳 陽一; 芦田 隆司; 松村 到臨床血液 2018/09
- 十二指腸型濾胞性リンパ腫は、抗腫瘍免疫により良好な予後を示す(Duodenal-type follicular lymphoma exhibits good prognosis through the increased anti-tumor immunity) [Not invited]井上 宏昭; 頼 晋也; 口分田 貴裕; 芹澤 憲太郎; 谷口 康博; 中山 聖子; 森田 泰慶; ルイス・エスピノザ; 田中 宏和; 辰巳 陽一; 芦田 隆司; 松村 到臨床血液 2018/09
- CLEC-2の発現は巨核球にバイアスした長期骨髄再建能を有する造血幹細胞集団を規定する(CLEC-2 identifies a functionally distinct subpopulation of megakaryocyte-biased HSCs) [Not invited]口分田 貴裕; 田中 宏和; Espinoza J. Luis; 岩田 吉生; 佐野 圭吾; 芹澤 憲太郎; 谷口 康博; 頼 晋也; 森田 泰慶; 辰巳 陽一; 芦田 隆司; 松村 到臨床血液 2018/09
- 症候性骨髄腫1414例の後方視的解析 関西骨髄腫フォーラムからの最新報告(Retrospective analyses of 1,414 symptomatic multiple myeloma cases: update from Kansai Myeloma Forum) [Not invited]田中 宏和; 芹澤 憲太郎; 中谷 綾; 金子 仁臣; 太田 健介; 小杉 智; 八木 秀男; 花本 仁; 淵田 真一; 志村 勇司; 柴山 浩彦; 小原 尚恵; 中谷 英仁; 諫田 淳也; 魚嶋 伸彦; 和田 勝也; 烏野 隆博; 松井 利充; 内山 人二; 松田 光弘; 足立 陽子; 高折 晃史; 黒田 純也; 谷脇 雅史; 島崎 千尋; 日野 雅之; 今田 和典; 野村 昌作; 金倉 譲; 松村 到臨床血液 2018/09
- 難治多発性骨髄腫に移植前再寛解導入療法としてKRd療法を用いた1例 [Not invited]大山泰世; 芹澤憲太郎; 森田泰慶; 角谷 宏明; 藤本昂; 谷口貴英; 田中宏和; 辰巳陽一; 芦田隆司; 松村到第219回 日本内科学会近畿地方会 2018/03
- Identification of a Patients-Derived CD34+ Myeloma Cell Population with Tumor-Propagating Capacity and Resistance to Anticancer Drugs [Not invited]Kentaro Serizawa; Hirokazu Tanaka; Ayano Fukui; Ryosuke Fujiwara; Keigo Sano; Hiroaki Inoue; Takahiro Kumode; Yasuhiro Taniguchi; Yasuyoshi Morita; Luis Espinoza; Itaru Matsumurathe 59th Annual Meeting and Exposition 2017/12
- C-TYPE LECTIN-LIKE PECEPTOR 2 SPECIFIES A FINCTIONALLY DISTINCT SUBPOPULATION OF MEGAKARYOCYTE-BIASED LONG-TERM HEMATOPOIETIC STEM CELLS. [Not invited]Takahiro Kumode; Hirokazu Tanaka; Ryosuke Fujiwara; Keigo Sano; Kentaro Serizawa; Yasuhiro Taniguchi; Sinya Rai; Itaru Matsumura第22回欧州血液学会 2017/06
- C-TYPE LECTIN-LIKE RECEPTOR 2 SPECIFIES A FUNCTIONALLY DISTINCT SUBPOPULATION OF MEGAKARYOCYTE-BIASED LONG-TERM HEMATOPOIETIC STEM CELLS [Not invited]T. Kumode; H. Tanaka; R. Fujiwara; K. Sano; K. Serizawa; Y. Taniguchi; S. Rai; I. MatsumuraHAEMATOLOGICA 2017/06 FERRATA STORTI FOUNDATION
- 多発性骨髄腫のpoor mobilizerに対するplerixafor併用下でのPBSCH [Not invited]芹澤憲太郎; 森田泰慶; 口分田貴裕; 田中宏和; 山田枝里佳; 芦田隆司; 松村到日本輸血細胞治療学会誌 2016/04
- 同種造血幹細胞移植後に再発した骨髄異形成症候群(MDS)におけるAzacitidine(AZA)療法 [Not invited]吉川智恵; 芹澤憲太郎; 森田泰慶; 田中宏和; 辰巳陽一; 芦田隆司; 松村到臨床血液 2016/02
- 骨原発ホジキンリンパ腫の1例 [Not invited]角谷 宏明; 芹澤憲太郎; 井上宏昭; 賴晋也; 平瀨主税; 森田泰慶; 田中宏和; 辰巳陽一; 芦田隆司; 松村到第210回 日本内科学会近畿地方会 2015/11
- Analysis of MECP regimen with relapsed or refractory malignant lymphoma in our institution [Not invited]Kentaro Serizawa; Hiroaki Kakutani; Sanae Sueda; Yoshio Iwata; Ayano Hukui; Yasuyo Oyama; Hiroaki Inoue; Shinya Rai; Chikara Hirase; Yasuyoshi Morita; Hirokazu Tanaka; Yoichi Tatsumi; Takashi Ashida; Itaru Matsumura第77回日本血液学会学術集会 2015/10
- CIDPと初期診断したCrow-Fukase症候群の1例 [Not invited]吉川 恵輔; 河合 滋; 加藤 茉莉; 芹澤 憲太郎; 鈴木 秀和; 三井 良之; 楠 進臨床神経学 2015/08
- 臍帯血移植における前処置の比較 全身放射線照射と抗胸腺グロブリン [Not invited]芦田 隆司; 福井 彩乃; 大山 泰世; 芹沢 憲太郎; 頼 晋也; 平瀬 主税; 中野 勝彦; 福島 靖幸; 川野 亜美; 山田 枝里佳; 井手 大輔; 前田 岳宏; 菅野 知恵美; 加藤 祐子; 椿本 祐子; 金光 靖; 松村 到日本輸血細胞治療学会誌 2015/04 (一社)日本輸血・細胞治療学会
- 同種造血幹細胞移植前処置におけるフルダラビン併用下での静注ブスルファン使用量の後方視的解析 [Not invited]芹澤憲太郎; 森田泰慶; 谷口貴英; 岩田吉生; 源周治; 大山泰世; 川内超矢; 金井良高; 頼晋也; 平瀬主税; 田中宏和; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到日本造血細胞移植学会総会プログラム・抄録集 2015/02
- 宮武淳一; 岩田吉生; 谷口貴英; 源周治; 大山泰世; 川内超矢; 佐野圭吾; 口分田貴裕; 芹澤憲太郎; 谷口康博; 頼晋也; 金井良高; 平瀬主税; 森田泰慶; 田中宏和; 辰巳陽一; 芦田隆司; 松村到日本造血細胞移植学会総会プログラム・抄録集 2015/02
- 若年劇症型再生不良性貧血に対する臍帯血移植に成功した一例 [Not invited]口分田貴裕; 岩田吉夫; 谷口貴秀; 源周治; 大山泰世; 佐野圭吾; 川内超矢; 芹澤憲太郎; 谷口康博; 頼晋也; 金井良高; 平瀬主税; 森田泰慶; 田中宏和; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到日本造血細胞移植学会総会プログラム・抄録集 2015/02
- クリオグロブリン血症に対してVCD療法が有効であった1例 [Not invited]吉川智恵; 芹澤憲太郎; 谷口貴英; 森田泰慶; 平瀬主税; 田中宏和; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到第206回 日本内科学会近畿地方会 2014/12
- 同種造血幹細胞移植後、二次生着不全に対してドナーリンパ球輸注が有効であった1例 [Not invited]池田守; 芹澤憲太郎; 谷口貴英; 森田泰慶; 平瀬主税; 田中宏和; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到第206回 日本内科学会近畿地方会 2014/12
- Analysis of conditioning regimen for ASCT with relapsed or refractory malignant lymphoma [Not invited]Kentaro Serizawa; Yasuyoshi Morita; Takahide Taniguchi; Yasuyo Oyama; Masaya Kawauchi; Takahiro Kumode; Yoshitaka Kanai; Chikara Hirase; Hirokazu Tanaka; Zyunichi Miyatake; Yoichi Tatsumi; Takashi Ashida; Itaru Matsumura第76回日本血液学会学術集会 2014/10
- A case of Mogamulizumab treatment for refractory ATLL to DLI following allo-SCT [Not invited]Takahide Taniguchi; Kentaro Serizawa; Yasuyoshi Morita; Yasuyo Oyama; Masaya Kawauchi; Takahiro Kumode; Yoshitaka Kanai; Chikara Hirase; Hirokazu Tanaka; Jyunichi Miyatake; Yoichi Tatsumi; Takashi Ashida; Itaru Matsumura第76回日本血液学会学術集会 2014/10
- 妊娠に合併したヘパリン起因性血小板減少症の1例 [Not invited]池田守; 芹澤憲太郎; 森田泰慶; 辰巳陽一; 芦田隆司; 松村到臨床血液 2014/02
- 当院における同種造血幹細胞移植時のダプトマイシンの有用性と安全性 [Not invited]芹澤憲太郎; 森田泰慶; 江本正克; 大山泰世; 福井彩乃; 井上宏昭; 川内超矢; 金井良高; 平瀬主税; 田中宏和; 嶋田高広; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到日本造血細胞移植学会総会プログラム・抄録集 2014/02
- 造血幹細胞移植後の真菌感染症に対する低用量アムホテリシンBリポソーム製剤の安全性および有用性に関する検討 [Not invited]芦田隆司; 芹澤憲太郎; 川内超矢; 江本正克; 谷口康博; 福井彩乃; 大山泰世; 井上宏昭; 金井良高; 平瀬主税; 森田泰慶; 宮武淳一; 福島靖幸; 川野亜美; 井手大輔; 菅野知恵美; 加藤祐子; 椿本祐子; 伊藤志保; 松村到日本造血細胞移植学会総会プログラム・抄録集 2014/02
- 慢性骨髄単球性白血病に対して骨髄非破壊的移植が有効であった1例 [Not invited]福本雄太; 芹澤憲太郎; 森田泰慶; 平瀬主税; 田中宏和; 嶋田高広; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到第202回 日本内科学会近畿地方会 2013/12
- 高齢者B-cell lymphoma, unclassifiable with features intermediate between diffuse large B-cell lymphoma and Burkitt lympomaに対して自家造血幹細胞移植で長期生存が得られている1例 [Not invited]谷口貴英; 芹澤憲太郎; 森田泰慶; 平瀬主税; 田中宏和; 嶋田高広; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到第202回 日本内科学会近畿地方会 2013/12
- Three hematologic malignancies in different lineages in a patient during the short period [Not invited]宮武 淳一; 川内 超矢; 芹澤 憲太郎; 江本 正克; 谷口 康博; 平瀨 主税; 森田 泰慶; 辰巳 陽一; 芦田 隆司; 川田 暁; 松村 到第75回日本血液学会学術集会 2013/10 札幌 第75回日本血液学会学術集会
- Results of gemcitabine therapy for related of refractory Non-Hodgkin’slymphoma in one institute [Not invited]芹澤 憲太郎; 森田 泰慶; 谷口 康博; 川内 超矢; 江口 剛; 江本 正克; 金井 良高; 賴 晋也; 平瀨 主税; 田中 宏和; 口分田 貴裕; 宮武 淳一; 辰巳 陽一; 芦田 隆司; 松村 到第75回日本血液学会学術集会 2013/10 札幌 第75回日本血液学会学術集会
- 診断に難渋したHELLP症候群の1症例 [Not invited]福本雄太; 芹澤憲太郎; 森田泰慶; 辰巳陽一; 芦田隆司; 松村到; 釣谷充弘臨床血液 2013/08
- フルダラビンをベースとした骨髄非破壊的前処置による移植成績の比較ーフルダラビン/ブルスファン対フルダラビン/メルファラン [Not invited]芦田 隆司; 綿谷 陽作; 川内 超矢; 江本 正克; 芹澤 憲太郎; 平瀨 主税; 谷口 康博; 宮武 淳一; 川野亜美; 森田 泰慶; 山田枝里佳; 井手大輔; 菅野知恵美; 加藤祐子; 椿本祐子; 伊藤志保; 峯 佳子; 藤田往子; 松村 到第35回日本造血細胞移植学会総会 2013/03 金沢 第35回日本造血細胞移植学会総会
- 難治性造血器腫瘍に対するT細胞非除去HLA不一致血縁者間造血幹細胞移植の成績 単一施設の後方視的検討 [Not invited]川西一信; 綿谷陽作; 谷口康博; 川内超矢; 芹澤憲太郎; 江本正克; 金井良高; 頼晋也; 平瀬主税; 森田泰慶; 田中宏和; 嶋田高広; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到日本造血細胞移植学会総会プログラム・抄録集 2013/02
- 高リスクMDSに対する同種造血幹細胞移植前にアザシチジン投与を行った4症例の検討 [Not invited]芹澤憲太郎; 綿谷陽作; 谷口康博; 森田泰慶; 川内超矢; 江本正克; 平瀬主税; 田中宏和; 嶋田高広; 川西一信; 宮武淳一; 辰巳陽一; 芦田隆司; 松村到日本造血細胞移植学会総会プログラム・抄録集 2013/02
- Bioclonal acute myeloid leukemia with t(2;5;15) and t(9;22) [Not invited]芹澤憲太郎; 綿谷陽作; 大山泰世; 江本正克; 大山雄一; 谷口康博; 金井良高; 頼晋也; 平瀬主税; 山口晃史; 森田泰慶; 田中宏和; 嶋田高広; 川西一信; 辰巳陽一; 芦田隆司; 松村到第74回日本血液学会学術集会 2012/10 京都 第74回日本血液学会学術集会
- 真性多血症から移行した急性赤白血病に対して非血縁者間骨髄移植が有効であった1例 [Not invited]芹澤憲太郎; 川西一信; 大山泰世; 尾嶋真由子; 井上宏昭; 口分田貴裕; 江本正克; 谷口康博; 金井良高; 頼晋也; 笹川淳; 平瀬主税; 山口晃史; 森田泰慶; 田中宏和; 嶋田高広; 辰巳陽一; 芦田隆司; 松村到日本造血細胞移植学会総会プログラム・抄録集 2012/02 大阪 第34回日本造血細胞移植学会総会
- 同種造血幹細胞移植前後の血清フェリチン値の移植後の予後に及ぼす影響について [Not invited]芦田隆司; 川野亜美; 山田枝里佳; 井手大輔; 菅野知恵美; 加藤祐子; 椿本祐子; 伊藤志保; 峯佳子; 藤田往子; 井上宏昭; 口分田貴裕; 芹澤憲太郎; 江本正克; 平瀬主税; 山口晃史; 森田泰慶; 川西一信; 辰巳陽一; 松村到日本造血細胞移植学会総会プログラム・抄録集 2012/02
- 急性リンパ性白血病寛解導入療法が著効した芽球性形質細胞様樹状細胞腫瘍の1症例 [Not invited]井上明日圭; 芹澤憲太郎; 川西一信; 山口晃史; 森田泰慶; 田中宏和; 嶋田高広; 辰巳陽一; 芦田隆司; 松村到臨床血液 2012/01
- Experience of indolent malignant lymphoma treated with Bendamustine in our institute [Not invited]谷口 康博; 辰巳 陽一; 川内 超矢; 江本 正克; 頼 晋也; 金井 良高; 平瀬 主税; 森田 泰慶; 田中 宏和; 芹澤 憲太郎; 嶋田 高広; 川西一信; 宮武 淳一; 芦田 隆司; 松村 到第74回日本血液学会学術集会 2012 京都 第74回日本血液学会学術集会
- Analysis of iron overload in patients with transfusion-dependent hematological diseases [Not invited]芦田 隆司; 川野亜美; 山田枝里佳; 井手大輔; 菅野知恵美; 加藤祐子; 椿本祐子; 伊藤志保; 峯 佳子; 藤田往子; 金光 靖; 森嶋祥之; 大山 泰世; 尾嶋 真由子; 井上 宏昭; 口分田 貴裕; 芹澤 憲太郎; 江本 正克; 谷口 康博; 田中 宏和; 金井 良高; 賴 晋也; 笹川 淳; 平瀨 主税; 山口 晃史; 森田 泰慶; 嶋田 高広; 川西 一信; 辰巳 陽一; 松村 到第73回日本血液学会学術集会 2011/10 名古屋 第73回日本血液学会学術集会
- 母児間末梢血幹細胞移植で生着を認めた,維持腹膜透析中の最重症型再生不良性貧血の一例 [Not invited]頼晋也; 松田光弘; 口分田貴裕; 井上宏昭; 川内超矢; 江本正克; 芹澤憲太郎; 金井良高; 山口晃史; 森田泰慶; 嶋田高広; 宮武淳一; 辰巳陽一; 芦田隆司; 前田裕弘; 松村到日本造血細胞移植学会総会プログラム・抄録集 2011
Affiliated academic society
Research Themes
- 日本学術振興会:科学研究費助成事業Date (from‐to) : 2023/04 -2026/03Author : 田中 宏和; 松村 到; 芹澤 憲太郎; 森田 泰慶
- Japan Society for the Promotion of Science:Grants-in-Aid for Scientific ResearchDate (from‐to) : 2016/04 -2019/03Author : TANAKA Hirokazu; SERIZAWA kentaroWe isolated myeloma initiating cells from phenotypically defined CD38+ CD 138+ CD 19- CD 45- multiple myeloma (MM) cells (PhMCs) from a set of 54 bone marrow MM patient samples. And we found PhMCs contains a minor CD34+ fraction that possess myeloma-propagating activities in vitro and in vivo, as well as resistance to anticancer drugs. The percent of CD34+ PhMCs was significantly higher in relapse/refractory than in newly diagnosed samples. Gene expression profiling revealed that CD34- PhMCs had a general myeloma cell signature, whereas CD34+ PhMCs exhibited a more immature pre-germinal center like signature. The presence of e cancer stem cells in MM was proposed for a few decades, however the identity of these cells remains controversial. The identification of these MM propagating cells provides a basis for better understanding the pathogenesis of MM and for designing novel therapeutic strategies aimed to eradicate total MM cells.