研究者業績
基本情報
研究キーワード
4研究分野
1経歴
7-
2020年4月 - 現在
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2019年4月 - 2020年3月
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2018年10月 - 2019年3月
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2010年4月 - 2018年10月
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2006年6月 - 2013年3月
学歴
1-
1987年4月 - 現在
委員歴
7-
2012年6月 - 2024年6月
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2011年4月 - 2021年9月
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2018年6月 - 2020年6月
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2016年6月 - 2020年6月
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2016年6月 - 2020年6月
論文
86-
Cancer medicine 2023年7月27日BACKGROUND: Distinguishing between central nervous system lymphoma (CNSL) and CNS infectious and/or demyelinating diseases, although clinically important, is sometimes difficult even using imaging strategies and conventional cerebrospinal fluid (CSF) analyses. To determine whether detection of genetic mutations enables differentiation between these diseases and the early detection of CNSL, we performed mutational analysis using CSF liquid biopsy technique. METHODS: In this study, we extracted cell-free DNA from the CSF (CSF-cfDNA) of CNSL (N = 10), CNS infectious disease (N = 10), and demyelinating disease (N = 10) patients, and performed quantitative mutational analysis by droplet-digital PCR. Conventional analyses were also performed using peripheral blood and CSF to confirm the characteristics of each disease. RESULTS: Blood hemoglobin and albumin levels were significantly lower in CNSL than CNS infectious and demyelinating diseases, CSF cell counts were significantly higher in infectious diseases than CNSL and demyelinating diseases, and CSF-cfDNA concentrations were significantly higher in infectious diseases than CNSL and demyelinating diseases. Mutation analysis using CSF-cfDNA detected MYD88L265P and CD79Y196 mutations in 60% of CNSLs each, with either mutation detected in 80% of cases. Mutual existence of both mutations was identified in 40% of cases. These mutations were not detected in either infectious or demyelinating diseases, and the sensitivity and specificity of detecting either MYD88/CD79B mutations in CNSL were 80% and 100%, respectively. In the four cases biopsied, the median time from collecting CSF with the detected mutations to definitive diagnosis by conventional methods was 22.5 days (range, 18-93 days). CONCLUSIONS: These results suggest that mutation analysis using CSF-cfDNA might be useful for differentiating CNSL from CNS infectious/demyelinating diseases and for early detection of CNSL, even in cases where brain biopsy is difficult to perform.
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Annals of hematology 101(12) 2813-2815 2022年12月
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Blood advances 6(11) 3230-3233 2022年1月13日
MISC
195-
日本リンパ網内系学会会誌 = The journal of the Japanese Society of Lymphoreticular Tissue 47 57-57 2007年5月11日
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BLOOD 106(11) 795A-795A 2005年11月
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内科 95(5) 948-953 2005年5月
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医学のあゆみ 212(5) 479-484 2005年1月29日
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BLOOD 104(11) 902A-902A 2004年11月
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日本リンパ網内系学会会誌 = The journal of the Japanese Society of Lymphoreticular Tissue 44 63-63 2004年6月10日
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Serum levels of the nm23-H1 protein and their clinical implication in extranodal NK/T-cell lymphoma.Leukemia. 2003 May; 2003年
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Blood 99 815-821 2002年
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BLOOD 96(11) 506A-506A 2000年11月
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BLOOD 96(11) 129A-129A 2000年11月
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医学のあゆみ 188(10) 949-953 1999年3月6日
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無菌生物 = Japanese journal of germfree life and gnotobiology 28(2) 78-79 1998年12月1日
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無菌生物 = Japanese journal of germfree life and gnotobiology 27(1) 29-32 1997年6月
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BLOOD 88(10) 3461-3461 1996年11月
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臨床血液 35(7) p635-641 1994年7月
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European Journal of Cancer 29(10) 1499 1993年
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New England Journal of Medicine 324(18) 1290 1991年5月2日To the Editor: Liver damage in primary human herpesvirus-6 infection has been reported in infants1,2 and adults.3 4 5 All patients had a benign, self-limited course except one infant with fatal fulminant hepatitis.1 We describe here an adult with fulminant hepatitis associated with lymphadenopathy and marked atypical lymphocytosis presumably caused by herpesvirus-6 infection. A 29-year-old man was admitted to our hospital on October 17, 1989, with fever, jaundice, skin rash, and lymphadenopathy, which had developed 10 days earlier. The bilirubin concentration (2.4 mg per deciliter), aminotransferase activities, and prothrombin time (18 percent) confirmed hepatic involvement. Generalized lymphadenopathy with leukocytosis (33,100 per. © 1991, Massachusetts Medical Society. All rights reserved.