研究者業績

西村 基

ニシムラ モトイ  (Nishimura Motoi)

基本情報

所属
千葉大学 医学部附属病院検査部 講師
(兼任)遺伝子診療部 講師
学位
医学博士(2004年3月 千葉大学)

研究者番号
80400969
J-GLOBAL ID
201901001893625153
researchmap会員ID
B000380375

外部リンク

学歴

 1

論文

 123
  • Yuri Matsuki, Kiyoshi Ichihara, Yoshihisa Itoh, Kazuo Mori, Hiroshi Ihara, Masato Maekawa, Motoi Nishimura, Sachiko Kiuchi, Fumio Nomura, Naotaka Hashizume, Nobue Itoh, Satoshi Matsumura
    Clinical nutrition ESPEN 61 119-130 2024年6月  
    BACKGROUND & AIMS: Serum retinol (ROH) is commonly used for population level assessment of vitamin A status. High-performance liquid chromatography (HPLC) is considered most accurate method for measuring ROH. However, with the technical difficulty of using HPLC for routine assays, serum retinol-binding protein (RBP) measured by immunological assays is expected to be a surrogate marker for ROH, with reports of a close correlation between serum RBP and ROH. Nevertheless, RBP is not commonly tested to assess vitamin A status with concerns over RBP alterations under various physiopathological conditions. Thus, we reappraised the extent to which RBP could be used as a surrogate marker in representative disorders that alter serum RBP levels. As a related marker, diagnostic utility of transthyretin (TTR) was also evaluated. METHODS: To evaluate the reliability of ROH and RBP assays, specimen stability was assessed in terms of (1) storage at 25, 4, -20, and -80 °C for 1-28 days, (2) five-cycle freeze-thawing, and (3) fluorescent light exposure for 1-14 days. Sources of variation (sex, age, body mass index [BMI], and drinking habits) and reference intervals for ROH, RBP, and TTR were determined in 617 well-defined healthy individuals. To investigate the influence of disorders that affect serum RBP, patients with five diagnostic groups were enrolled: 26 with chronic kidney disease (CKD); 13 with various malignancies in advanced stages (AdM), 12 with acute bacterial infections (ABI), 6 with liver cirrhosis (LC), and 26 with simple obesity (BMI ≥ 27 kg/m2). RESULTS: The stability of RBP and ROH in serum was confirmed under all conditions. In healthy individuals, serum ROH, RBP, and TTR were appreciably high in males with a slight increase in proportion to age and BMI. The major-axis regression line between RBP (x) and ROH (y) in healthy individuals was y = x, with a correlation coefficient of 0.986. In the LC, AdM, and ABI groups, similar strong correlations were observed; however, the regression lines were shifted slightly rightward from the healthy group line, indicating a positive bias in estimating ROH. Interestingly, the same analyses between TTR and ROH revealed similar strong linear relationships in all groups; however, the regression line of each group showed a leftward (opposite) shift from the healthy group line. Based on these observations, we developed a novel regression model composed of RBP and TTR, which gave much improved accuracy in estimating ROH, even under these pathological conditions. CONCLUSIONS: The perfect RBP-ROH correlation in healthy individuals indicates the utility of RPB as a surrogate marker for ROH. Nevertheless, under RBP-altered conditions, a slight overestimation of ROH is inevitable. However, when the TTR was tested together, the bias can be corrected almost perfectly using the novel ROH estimation formula comprising RBP and TTR.
  • 大野 泉, 西村 基, 大内 麻愉, 菅 元泰, 永嶌 裕樹, 高橋 幸治, 大山 広, 平野 翔, 中島 裟文, 鬼澤 歩, 渡辺 奈未, 宇津野 恵美, 高野 重紹, 市川 智彦, 松下 一之, 滝口 裕一, 加藤 直也
    日本消化器病学会雑誌 120(臨増大会) A842-A842 2023年10月  
  • 大野 泉, 西村 基, 大内 麻愉, 菅 元泰, 永嶌 裕樹, 高橋 幸治, 大山 広, 平野 翔, 中島 裟文, 鬼澤 歩, 渡辺 奈未, 宇津野 恵美, 高野 重紹, 市川 智彦, 松下 一之, 滝口 裕一, 加藤 直也
    日本消化器病学会雑誌 120(臨増大会) A842-A842 2023年10月  
  • 坂井 元春, 石渡 一樹, 五十嵐 活志, 類家 裕太郎, 内藤 久美子, 藤本 真徳, 鈴木 佐和子, 小出 尚史, 横手 幸太郎, 大橋 優美, 岡野 公亮, 西村 基
    千葉医学雑誌 99(4) 106-106 2023年8月  
  • 坂井 元春, 石渡 一樹, 五十嵐 活志, 類家 裕太郎, 内藤 久美子, 藤本 真徳, 鈴木 佐和子, 小出 尚史, 横手 幸太郎, 大橋 優美, 岡野 公亮, 西村 基
    千葉医学雑誌 99(4) 106-106 2023年8月  
  • Ikki Sakuma, Hidekazu Nagano, Naoko Hashimoto, Masanori Fujimoto, Akitoshi Nakayama, Takahiro Fuchigami, Yuki Taki, Tatsuma Matsuda, Hiroyuki Akamine, Satomi Kono, Takashi Kono, Masataka Yokoyama, Motoi Nishimura, Koutaro Yokote, Tatsuki Ogasawara, Yoichi Fujii, Seishi Ogawa, Eunyoung Lee, Takashi Miki, Tomoaki Tanaka
    Communications biology 6(1) 787-787 2023年7月28日  
    Fructose-1,6-bisphosphatase (FBPase) deficiency, caused by an FBP1 mutation, is an autosomal recessive disorder characterized by hypoglycemic lactic acidosis. Due to the rarity of FBPase deficiency, the mechanism by which the mutations cause enzyme activity loss still remains unclear. Here we identify compound heterozygous missense mutations of FBP1, c.491G>A (p.G164D) and c.581T>C (p.F194S), in an adult patient with hypoglycemic lactic acidosis. The G164D and F194S FBP1 mutants exhibit decreased FBP1 protein expression and a loss of FBPase enzyme activity. The biochemical phenotypes of all previously reported FBP1 missense mutations in addition to G164D and F194S are classified into three functional categories. Type 1 mutations are located at pivotal residues in enzyme activity motifs and have no effects on protein expression. Type 2 mutations structurally cluster around the substrate binding pocket and are associated with decreased protein expression due to protein misfolding. Type 3 mutations are likely nonpathogenic. These findings demonstrate a key role of protein misfolding in mediating the pathogenesis of FBPase deficiency, particularly for Type 2 mutations. This study provides important insights that certain patients with Type 2 mutations may respond to chaperone molecules.
  • 西村 基, 上田 希彦, 松下 一之, 市川 智彦
    日本遺伝カウンセリング学会誌 44(2) 131-131 2023年6月  
  • Naoki Akizue, Kenichiro Okimoto, Yosuke Hirotsu, Kenji Amemiya, Tatsuya Kaneko, Yuki Ohta, Takashi Taida, Keiko Saito, Tomoaki Matsumura, Motoi Nishimura, Kazuyuki Matsushita, Hitoshi Mochizuki, Tetsuhiro Chiba, Makoto Arai, Jun Kato, Masao Omata, Naoya Kato
    Journal of gastroenterology and hepatology 2023年5月16日  
    BACKGROUND AND AIM: Little is known about genetic mutations in the regenerated mucosa (RM) after endoscopic resection (ER) of esophageal carcinoma. Thus, this study investigates the status of genetic variation in RM after ER of esophageal squamous cell carcinoma (ESCC). METHODS: The study cohort included 19 patients with ESCC. We used an esophageal carcinoma panel to identify target sequences for squamous cell carcinoma (SCC), background mucosa (BM), and RM after ER of ESCC. We used OncoKB to check whether each mutation was a putative driver. RESULTS: We identified 77 mutations of 32 genes in SCC, 133 mutations of 34 genes in BM, and 100 mutations of 29 genes in RM. Putative driver mutations were identified in 20 mutations in 14 cases in SCC, 16 mutations in 10 cases in BM, and 7 mutations in 11 cases in RM. The rate of putative driver mutations to total mutations was significantly lower in RM (26% in SCC vs 12% in BM vs 7% in RM, P = 0.009). Additionally, the rate of cases with TP53 putative driver mutations was significantly lower in RM (63% in SCC vs 37% in BM vs 16% in RM, P = 0.011). The percentage of putative driver mutations and the percentage of cases with a putative driver of TP53 were significantly lower in RM. CONCLUSION: Esophageal RM after ER of ESCC could have a lower risk of carcinogenesis.
  • 松谷 智郎, 廣野 誠一郎, 小林 正芳, 石毛 崇之, 西村 基, 糸賀 栄, 松下 一之, 岩立 康男
    Brain Tumor Pathology 40(Suppl.) 128-128 2023年5月  
  • Motoi Nishimura, Tomoaki Tanaka, Syota Murata, Akiko Miyabe, Takayuki Ishige, Kenji Kawasaki, Masataka Yokoyama, Naoko Hashimoto, Kazuyuki Yamagata, Hidekazu Nagano, Satomi Tojo-Nishimura, Kazuyuki Matsushita
    Scientific reports 13(1) 5731-5731 2023年4月7日  
    Although polymerase chain reaction (PCR) amplification and sequencing of the bacterial 16S rDNA region has numerous scientific applications, it does not provide DNA methylation information. Herein, we propose a simple extension for bisulfite sequencing to investigate 5-methylcytosine residues in the bacterial 16S rDNA region from clinical isolates or flora. Multiple displacement amplification without DNA denaturation was used to preferentially pre-amplify single-stranded bacterial DNA after bisulfite conversion. Following the pre-amplification, the 16S rDNA region was analyzed using nested bisulfite PCR and sequencing, enabling the simultaneous identification of DNA methylation status and sequence data. We used this approach (termed sm16S rDNA PCR/sequencing) to identify novel methylation sites and a methyltransferase (M. MmnI) in Morganella morganii and different methylation motifs among Enterococcus faecalis strains from small volumes of clinical specimens. Further, our analysis suggested that M. MmnI may be correlated to erythromycin resistance. Thus, sm16S rDNA PCR/sequencing is a useful extension method for analyzing the DNA methylation of 16S rDNA regions in a microflora, providing additional information not provided by conventional PCR. Given the relationship between DNA methylation status and drug resistance in bacteria, we believe this technique can be effectively applied in clinical sample testing.
  • Kenichiro Okimoto, Yosuke Hirotsu, Makoto Arai, Kenji Amemiya, Naoki Akizue, Yuki Ohta, Takashi Taida, Keiko Saito, Hiroshi Ohyama, Tomoaki Matsumura, Motoi Nishimura, Kazuyuki Matsushita, Keisuke Matsusaka, Toshio Oyama, Hitoshi Mochizuki, Tetsuhiro Chiba, Jun Kato, Jun-Ichiro Ikeda, Osamu Yokosuka, Naoya Kato, Masao Omata
    Cancer medicine 12(7) 8490-8498 2023年2月3日  
    BACKGROUND: This study aimed to investigate the validity of pathological diagnosis of early CRC (E-CRC) from the genetic background by comparing data of E-CRC to colorectal adenoma (CRA) and The Cancer Genome Atlas (TCGA) on advanced CRC (AD-CRC). METHODS: TCGA data on AD-CRC were studied in silico, whereas by next-generation sequencer, DNA target sequences were performed for endoscopically obtained CRA and E-CRC samples. Immunohistochemical staining of mismatch repair genes and methylation of MLH1 was also performed. The presence of oncogenic mutation according to OncoKB for the genes of the Wnt, MAPK, and cell-cycle-signaling pathways was compared among CRA, E-CRC, and AD-CRC. RESULTS: The study included 22 CRA and 30 E-CRC lesions from the Chiba University Hospital and 212 AD-CRC lesions from TCGA data. Regarding the number of lesions with driver mutations in the Wnt and cell-cycle-signaling pathways, E-CRC was comparable to AD-CRC, but was significantly greater than CRA. CRA had significantly more lesions with a driver mutation for the Wnt signaling pathway only, versus E-CRC. CONCLUSIONS: In conclusion, the definition of E-CRC according to the Japanese criteria had a different genetic profile from CRA and was more similar to AD-CRC. Based on the main pathway, it seemed reasonable to classify E-CRC as adenocarcinoma. The pathological diagnosis of E-CRC according to Japanese definition seemed to be valid from a genetic point of view.
  • 坂井 元春, 石渡 一樹, 岡野 公亮, 大橋 優美, 渡邉 涼香, 五十嵐 活志, 類家 裕太郎, 内藤 久美子, 藤本 真徳, 鈴木 佐和子, 小出 尚史, 西村 基, 横手 幸太郎
    日本内分泌学会雑誌 98(4) 900-900 2023年2月  
  • 西村 基, 宮部 安規子, 村田 正太, 石毛 崇之, 川崎 健治, 松下 一之
    日本臨床微生物学会雑誌 33(Suppl.1) 273-273 2022年12月  
  • Azusa Yamato, Hidekazu Nagano, Yue Gao, Tatsuma Matsuda, Naoko Hashimoto, Akitoshi Nakayama, Kazuyuki Yamagata, Masataka Yokoyama, Yingbo Gong, Xiaoyan Shi, Siti Nurul Zhahara, Takashi Kono, Yuki Taki, Naoto Furuki, Motoi Nishimura, Kentaro Horiguchi, Yasuo Iwadate, Masaki Fukuyo, Bahityar Rahmutulla, Atsushi Kaneda, Yoshinori Hasegawa, Yusuke Kawashima, Osamu Ohara, Tetsuo Ishikawa, Eiryo Kawakami, Yasuhiro Nakamura, Naoko Inoshita, Shozo Yamada, Noriaki Fukuhara, Hiroshi Nishioka, Tomoaki Tanaka
    Communications biology 5(1) 1304-1304 2022年11月27日  査読有り
  • Alimasi Aersilan, Naoko Hashimoto, Kazuyuki Yamagata, Masataka Yokoyama, Akitoshi Nakayama, Xiaoyan Shi, Hidekazu Nagano, Ikki Sakuma, Nijiro Nohata, Takashi Kinoshita, Naohiko Seki, Bahityar Rahmutulla, Atsushi Kaneda, Siti Nurul Zhahara, Yingbo Gong, Motoi Nishimura, Shoichiro Kawauchi, Eiryo Kawakami, Tomoaki Tanaka
    Scientific reports 12(1) 18443-18443 2022年11月2日  査読有り
    The microRNA (miR) miR-874, a potential tumour suppressor, causes cell death via target gene suppression in various cancer types. Mevalonate pathway inhibition also causes cell death in breast cancer. However, the relationship between the mevalonate pathway and miR-874-induced apoptosis or its association with the tumour suppressor p53 has not been elucidated. We identified phosphomevalonate kinase (PMVK), a key mevalonate pathway enzyme, and sterol regulatory element-binding factor 2 (SREBF2), the master cholesterol biosynthesis regulator, as direct miR‑874 targets. Next-generation sequencing analysis revealed a significant miR-874-mediated downregulation of PMVK and SREBF2 gene expression and p53 pathway enrichment. Luciferase reporter assays showed that miR-874 directly regulated PMVK and SREBF2. miR-874-induced apoptosis was p53 dependent, and single-cell RNA sequencing analysis demonstrated that miR-874 transfection resulted in apoptosis and p53 pathway activation. Downregulation of PMVK expression also caused cell cycle arrest and p53 pathway activation, which was rescued by geranylgeranyl pyrophosphate (GGPP) supplementation. Analysis of The Cancer Genome Atlas (TCGA) database indicated a negative correlation between miR-874 and PMVK expression and between miR-874 and SREBF2 expression. These findings suggest that miR-874 suppresses the mevalonate pathway by targeting SREBF2 and PMVK, resulting in GGPP depletion, which activates the p53 pathway and promotes cycle arrest or apoptosis.
  • Yuri Imaizumi, Takayuki Ishige, Tatsuki Fujikawa, Akiko Miyabe, Shota Murata, Kenji Kawasaki, Motoi Nishimura, Toshibumi Taniguchi, Hidetoshi Igari, Kazuyuki Matsushita
    Clinica chimica acta; international journal of clinical chemistry 536 6-11 2022年9月14日  査読有り
    BACKGROUND: Tracking SARS-CoV-2 variants of concern (VOC) by genomic sequencing is time-consuming. The rapid screening of VOCs is necessary for clinical laboratories. In this study, we developed a rapid screening method based on multiplex RT-PCR by extended S-gene target failure (eSGTF), a false negative result caused by S-gene mutations. METHODS: Three S-gene target (SGT) regions (SGT1, codons 65-72; SGT2, codons 152-159; and SGT3, codons 370-377) and an N-gene region (for internal control) were detected in single-tube. Four types of VOC (Alpha, Delta, Omicron BA.1, and Omicron BA.2) are classified by positive/negative patterns of 3 S-gene regions (eSGTF pattern). RESULTS: The eSGTF patterns of VOCs were as follows (SGT1, SGT2, SGT3; P, positive; N, negative): Alpha, NPP; Delta, PNP; Omicron BA.1, NPN pattern; and Omicron BA.2, PPN. As compared with the S-gene sequencing, eSGTF patterns were identical to the specific VOCs (concordance rate = 96.7%, N = 206/213). Seven samples with discordant results had a minor mutation in the probe binding region. The epidemics of VOCs estimated by eSGTF patterns were similar to those in Japan. CONCLUSIONS: Multiplex RT-PCR and eSGTF patterns enable high-throughput screening of VOCs. It will be useful for the rapid determination of VOCs in clinical laboratories.
  • 今泉 優理, 石毛 崇之, 藤川 樹, 宮部 安規子, 村田 正太, 川崎 健治, 西村 基, 谷口 俊文, 猪狩 英俊, 松下 一之
    医療検査と自動化 47(4) 437-437 2022年8月  
  • Mirai Matsubara, Yuri Imaizumi, Tatsuki Fujikawa, Takayuki Ishige, Motoi Nishimura, Akiko Miyabe, Shota Murata, Kenji Kawasaki, Toshibumi Taniguchi, Hidetoshi Igari, Kazuyuki Matsushita
    Clinica chimica acta; international journal of clinical chemistry 530 94-98 2022年3月16日  査読有り
    INTRODUCTION: Genomic surveillance of the SARS-CoV-2 virus is important to assess transmissibility, disease severity, and vaccine effectiveness. The SARS-CoV-2 genome consists of approximately 30 kb single-stranded RNA that is too large to analyze the whole genome by Sanger sequencing. Thus, in this study, we performed Sanger sequencing following long-range RT-PCR of the entire SARS-CoV-2 S-gene and analyzed the mutational dynamics. METHODS: The 4 kb region, including the S-gene, was amplified by two-step long-range RT-PCR. Then, the entire S-gene sequence was determined by Sanger sequencing. The amino acid mutations were identified as compared with the reference SARS-CoV-2 genome. RESULTS: The S:D614G mutation was found in all samples. The R.1 variants were detected after January 2021. Alpha variants started to emerge in April 2021. Delta variants replaced Alpha in July 2021. Then, Omicron variants were detected after December 2021. These mutational dynamics in samples collected in the Chiba University Hospital were similar to those in Japan. CONCLUSION: The emergence of variants of concern (VOC) has been reported by the entire S-gene analysis. As the VOCs have unique mutational patterns of the S-gene region, analysis of the entire S-gene will be useful for molecular surveillance of the SARS-CoV-2 in clinical laboratories.
  • 石毛 崇之, 川崎 健治, 宇津野 恵美, 澤井 摂, 西村 基, 野村 文夫, 松下 一之
    臨床化学 51(1) 36-37 2022年1月  
    発端者は検診でアルカリフォスファターゼ(ALP)高値を指摘され、ALPアイソザイム分析では小腸由来のALP5が71.7%と高値を示し、父と妹にも認めたため優性遺伝性の家族性高ALP血症であると考えられた。塩基配列解析にてALPI遺伝子のコード領域のC末端に挿入欠失バリアントが発見され、このバリアントが家族性高ALP血症の原因となっている可能性が高く、GPIアンカーシグナルの疎水性を減弱させていた。細胞株を用いた蛋白質発現の実験にて、野生型ALPI遺伝子を導入した細胞では培養上清のALP活性はわずかであったが細胞膜分画のALP活性は高くALPは細胞膜に局在した一方、バリアント型ALPI遺伝子を導入した細胞では逆に培養上清のALP活性が高く細胞膜分画には全く活性がなかった。ALPI遺伝子のC末端バリアントは、GPIアンカーシグナルの疎水性低下による膜結合能の喪失により、小腸型ALPの良性家族性高ALP血症を引き起こす可能性がある。
  • Kenji Ohira, Hajime Yokota, Shigeki Hirano, Motoi Nishimura, Hiroki Mukai, Takuro Horikoshi, Setsu Sawai, Yoshitaka Yamanaka, Tatsuya Yamamoto, Shingo Kakeda, Satoshi Kuwabara, Tomoaki Tanaka, Takashi Uno
    Parkinson's disease 2022 8649195-8649195 2022年  
    Taq1A polymorphism is a DRD2 gene variant located in an exon of the ANKK1 gene and has an important role in the brain's dopaminergic functions. Some studies have indicated that A1 carriers have an increased risk of developing Parkinson's disease (PD) and show poorer clinical performance than A2 homo carriers. Previous studies have suggested that A1 carriers had fewer dopamine D2 receptors in the caudate and increased cortical activity as a compensatory mechanism. However, there is little information about morphological changes associated with this polymorphism in patients with PD. The study's aim was to investigate the relationship between brain volume and Taq1A polymorphism in PD using voxel-based morphometry (VBM). Based on Taq1A polymorphism, 103 patients with PD were divided into two groups: A1 carriers (A1/A1 and A1/A2) and A2 homo carriers (A2/A2). The volume of the left prefrontal cortex (PFC) was significantly decreased in A2 homo carriers compared to A1 carriers. This finding supports the association between Taq1A polymorphism and brain volume in PD and may explain the compensation of cortical function in A1 carriers with PD.
  • 村田 正太, 宮部 安規子, 齊藤 知子, 瀬川 俊介, 堀田 恵海, 山下 晃司, 松原 未来, 鈴木 眞, 川崎 健治, 西村 基, 松下 一之
    日本化学療法学会雑誌 70(1) 124-124 2022年1月  
  • 村田 正太, 宮部 安規子, 齊藤 知子, 瀬川 俊介, 堀田 恵海, 山下 晃司, 松原 未来, 鈴木 眞, 川崎 健治, 西村 基, 松下 一之
    日本化学療法学会雑誌 70(1) 124-124 2022年1月  
  • 村田 正太, 土田 祥央, 宮部 安規子, 齊藤 知子, 瀬川 俊介, 堀田 恵海, 山下 晃司, 松原 未来, 鈴木 眞, 川崎 健治, 西村 基, 松下 一之
    日本臨床微生物学会雑誌 32(Suppl.1) 168-168 2021年12月  
  • 松原 未来, 石毛 崇之, 西村 基, 村田 正太, 藤川 樹, 谷口 俊文, 猪狩 英俊, 川崎 健治, 松下 一之
    日本臨床微生物学会雑誌 32(Suppl.1) 246-246 2021年12月  
  • 松原 未来, 石毛 崇之, 西村 基, 村田 正太, 藤川 樹, 谷口 俊文, 猪狩 英俊, 川崎 健治, 松下 一之
    日本臨床微生物学会雑誌 32(Suppl.1) 246-246 2021年12月  
  • 村田 正太, 土田 祥央, 宮部 安規子, 齊藤 知子, 瀬川 俊介, 堀田 恵海, 山下 晃司, 松原 未来, 鈴木 眞, 川崎 健治, 西村 基, 松下 一之
    日本臨床微生物学会雑誌 32(Suppl.1) 168-168 2021年12月  
  • Mamoru Tokunaga, Kenichiro Okimoto, Naoki Akizue, Kentaro Ishikawa, Yosuke Hirotsu, Kenji Amemiya, Masayuki Ota, Keisuke Matsusaka, Motoi Nishimura, Kazuyuki Matsushita, Tsubasa Ishikawa, Ariki Nagashima, Wataru Shiratori, Tatsuya Kaneko, Hirotaka Oura, Kengo Kanayama, Yuki Ohta, Takashi Taida, Keiko Saito, Tomoaki Matsumura, Tetsuhiro Chiba, Hitoshi Mochizuki, Makoto Arai, Jun Kato, Jun-ichiro Ikeda, Masao Omata, Naoya Kato
    Scientific Reports 11(1) 2021年12月  査読有り
    <title>Abstract</title>The genetic characteristics of Barrett’s esophagus (BE) and esophageal adenocarcinoma (EAC) in the Japanese population is unclear. This study aims to investigate the genetic characteristics from nondysplastic BE (NDBE) to early EAC in Japan. Clinical information was collected. Moreover, the genetic profile of NDBE without concurrent dysplasia, early EAC, and surrounding BE were also investigated using endoscopic biopsy samples and formalin-fixed, paraffin-embedded specimens from Japanese patients by targeted next-generation sequencing. Immunohistochemical staining for p53 was also performed for EAC lesions. Targeted NGS was performed for 33 cases with 77 specimens. No significant difference exists in the NDBE group between the number of putative drivers per lesion in the short-segment Barrett’s esophagus (SSBE) and long-segment Barrett’s esophagus (LSBE) [0 (range, 0–1) vs. 0 (range, 0–1). <italic>p</italic> = 1.00]. <italic>TP53</italic> putative drivers were found in two patients (16.7%) with nondysplastic SSBE. <italic>TP53</italic> was the majority of putative drivers in both BE adjacent to EAC and EAC, accounting for 66.7% and 66.7%, respectively. More putative drivers per lesion were found in the EAC than in the NDBE group [1 (range, 0–3) vs. 0 (range, 0–1). <italic>p</italic> &lt; 0.01]. The genetic variants of <italic>TP53</italic> in the Japanese early EAC were similar to those in western countries. However, <italic>TP53</italic> putative drivers were detected even in Japanese patients with nondysplastic SSBE. This is significant because such nondysplastic SSBE might have higher risk of progressing to high-grade dysplasia or EAC. The risks of progression may not be underestimated and appropriate follow-ups may be necessary even in patients with SSBE. <bold>Trial registration:</bold> This study was registered at the University Hospital Medical Information Network (UMIN000034247).
  • 松原 未来, 石毛 崇之, 西村 基, 村田 正太, 藤川 樹, 谷口 俊文, 猪狩 英俊, 川崎 健治, 松下 一之
    医療検査と自動化 46(4) 492-492 2021年8月  
  • 藤川 樹, 石毛 崇之, 西村 基, 松原 未来, 村田 正太, 谷口 俊文, 猪狩 英俊, 川崎 健治, 松下 一之
    医療検査と自動化 46(4) 492-492 2021年8月  
  • 北村 浩一, 藤澤 陽子, 川崎 健治, 西村 基, 松下 一之
    医療検査と自動化 46(4) 502-502 2021年8月  
  • 横山 真隆, 中山 哲俊, 赤嶺 博行, 古木 直人, 石 暁彦, Siti Zhahara, 村田 和貴, 山形 一行, 西村 基, 田中 知明
    日本内分泌学会雑誌 97(3) 649-649 2021年7月  
  • 山形 一行, 田村 愛, 長濱 博章, 藤本 真徳, 中山 哲俊, 横山 真隆, 橋本 直子, 村田 和貴, 西村 基, 田中 知明
    日本内分泌学会雑誌 97(3) 642-642 2021年7月  
  • 山形 一行, 田村 愛, 長濱 博章, 藤本 真徳, 中山 哲俊, 横山 真隆, 橋本 直子, 村田 和貴, 西村 基, 田中 知明
    日本内分泌学会雑誌 97(3) 642-642 2021年7月  
  • 横山 真隆, 中山 哲俊, 赤嶺 博行, 古木 直人, 石 暁彦, Siti Zhahara, 村田 和貴, 山形 一行, 西村 基, 田中 知明
    日本内分泌学会雑誌 97(3) 649-649 2021年7月  
  • 大平 健司, 横田 元, 平野 成樹, 田中 知明, 西村 基, 澤井 摂, 山本 達也, 山中 義崇, 桑原 聡, 宇野 隆
    パーキンソン病・運動障害疾患コングレスプログラム・抄録集 15回 100-100 2021年7月  
  • 中津川 智子, 宇津野 恵美, 関根 瑞香, 山本 寛人, 佐藤 明日香, 吉野 有希子, 藤本 浩司, 縣 靖子, 神津 三佳, 松下 一之, 西村 基, 稲田 麻里, 野村 文夫, 羽田 明, 市川 智彦
    日本遺伝カウンセリング学会誌 42(2) 68-68 2021年6月  
  • 松下 一之, 宮内 英聡, 石毛 崇之, 西村 基, 川崎 健治, 糸賀 栄, 関根 瑞香, 宇津野 恵美, 滝口 裕一, 稲田 麻里, 長嶋 健, 藤本 浩司, 松原 久裕, 市川 智彦
    日本遺伝カウンセリング学会誌 42(2) 78-78 2021年6月  
  • Naoki Akizue, Kenichiro Okimoto, Makoto Arai, Yosuke Hirotsu, Kenji Amemiya, Hirotaka Oura, Tatsuya Kaneko, Mamoru Tokunaga, Kentaro Ishikawa, Yuki Ohta, Takashi Taida, Keiko Saito, Daisuke Maruoka, Tomoaki Matsumura, Tomoo Nakagawa, Motoi Nishimura, Tetsuhiro Chiba, Kazuyuki Matsushita, Hitoshi Mochizuki, Osamu Yokosuka, Masao Omata, Naoya Kato
    CANCER MEDICINE 2021年5月  査読有り
    Somatic mutations including the background mucosa in patients with Lugol-voiding lesions (LVLs) are still not well known. The aim of this study was to evaluate the somatic mutations of the background mucosa in patients with LVLs (Squamous cell carcinoma (SCC), intraepithelial neoplasia (IN), and hyperplasia). Twenty-five patients with LVLs (9 with SCC, 6 with IN, and 10 with hyperplasia) were included. A targeted sequence was performed for LVLs and background mucosa using an esophageal cancer panel. Each mutation was checked whether it was oncogenic or not concerning OncoKB. In LVLs, TP53 was the most dominant mutation (80%). Furthermore, 72% of TP53 mutations was putative drivers. In background mucosa, NOTCH1 was the most dominant mutation (88%) and TP53 was the second most dominant mutation (48%). Furthermore, 73% of TP53 mutations and 8% of NOTCH1 mutations were putative drivers. Putative driver mutations of TP53 had significantly higher allele frequency (AF) in SCC than in IN and hyperplasia. Conversely, putative driver mutations of NOTCH1 did not have a significant accumulation of AF in the progression of carcinogenesis. Furthermore, in SCC, AF of TP53 mutations was significantly higher in LVLs than in background mucosa, but not in IN and hyperplasia. Regarding NOTCH1, a significant difference was not observed between LVLs and background mucosa in each group. The background mucosa in patients with LVLs already had putative driver mutations such as TP53 and NOTCH1. Of these two genes, TP53 mutation could be the main target gene of carcinogenesis in esophageal SCC.
  • 類家 裕太郎, 鈴木 佐和子, 青野 和人, 五十嵐 活志, 石渡 一樹, 内藤 久美子, 石田 晶子, 出口 ハンナ, 藤本 真徳, 小出 尚史, 山崎 有人, 笹野 公伸, 新井 誠人, 西村 基, 坂本 信一, 市川 智彦, 横手 幸太郎
    日本内分泌学会雑誌 97(1) 347-347 2021年4月  
  • Hiroaki Ochiiwa, Guzhanuer Ailiken, Masataka Yokoyama, Kazuyuki Yamagata, Hidekazu Nagano, Chihoko Yoshimura, Hiromi Muraoka, Keiji Ishida, Tomonori Haruma, Akitoshi Nakayama, Naoko Hashimoto, Kazutaka Murata, Motoi Nishimura, Yusuke Kawashima, Osamu Ohara, Shuichi Ohkubo, Tomoaki Tanaka
    ONCOGENE 40(7) 1217-1230 2021年2月  査読有り
    TAS4464, a potent, selective small molecule NEDD8-activating enzyme (NAE) inhibitor, leads to inactivation of cullin-RING E3 ubiquitin ligases (CRLs) and consequent accumulations of its substrate proteins. Here, we investigated the antitumor properties and action mechanism of TAS4464 in acute myeloid leukemia (AML). TAS4464 induced apoptotic cell death in various AML cell lines. TAS4464 treatments resulted in the activation of both the caspase-9-mediated intrinsic apoptotic pathway and caspase-8-mediated extrinsic apoptotic pathway in AML cells; combined treatment with inhibitors of these caspases markedly diminished TAS4464-induced apoptosis. In each apoptotic pathway, TAS4464 induced the mRNA transcription of the intrinsic proapoptotic factor NOXA and decreased that of the extrinsic antiapoptotic factor c-FLIP. RNA-sequencing analysis showed that the signaling pathway of the CRL substrate c-Myc was enriched after TAS4464 treatment. Chromatin immunoprecipitation (ChIP) assay revealed that TAS4464-induced c-Myc bound to the PMAIP1 (encoding NOXA) and CFLAR (encoding c-FLIP) promoter regions, and siRNA-mediated c-Myc knockdown neutralized both TAS4464-mediated NOXA induction and c-FLIP downregulation. TAS4464 activated both caspase-8 and caspase-9 along with an increase in NOXA and a decrease in c-FLIP, resulting in complete tumor remission in a human AML xenograft model. These findings suggest that NAE inhibition leads to anti-AML activity via a novel c-Myc-dependent apoptosis induction mechanism.
  • 宮林 諒, 内藤 久美子, 五十嵐 活志, 類家 裕太郎, 石渡 一樹, 石田 晶子, 出口 ハンナ, 藤本 真徳, 志賀 明菜, 鈴木 佐和子, 小出 尚史, 西村 基, 横手 幸太郎
    日本内分泌学会雑誌 96(3) 677-677 2021年1月  
  • クリス・ダイ, 澤井 恵, 相羽 良寿, 曽根原 弘樹, 西村 基, 川崎 健治, 竹内 公一, 松下 一之
    日本臨床検査医学会誌 69(1) 25-37 2021年1月  
  • 大庭 千尋, 藤井 克則, 市川 智彦, 宇津野 恵美, 澤田 大輔, 塩浜 直, 西村 基, 松下 一之, 澤井 摂, 小俣 卓, 下条 直樹
    脳と発達 53(1) 74-74 2021年1月  
  • 大庭 千尋, 藤井 克則, 市川 智彦, 宇津野 恵美, 澤田 大輔, 塩浜 直, 西村 基, 松下 一之, 澤井 摂, 小俣 卓, 下条 直樹
    脳と発達 53(1) 74-74 2021年1月  
  • 西村 基, 村田 正太, 石毛 崇之, 宮部 安規子, 北村 浩一, 根川 真実, 藤川 樹, 古家 若葉, 梅谷 友輔, 堀田 恵海, 吉田 俊彦, 川崎 健治, 松下 一之
    日本臨床微生物学会雑誌 31(Suppl.1) 232-232 2020年12月  
  • 西村 基, 村田 正太, 石毛 崇之, 宮部 安規子, 北村 浩一, 根川 真実, 藤川 樹, 古家 若葉, 梅谷 友輔, 堀田 恵海, 吉田 俊彦, 川崎 健治, 松下 一之
    日本臨床微生物学会雑誌 31(Suppl.1) 232-232 2020年12月  
  • 高倉 大暉, 塚越 彩乃, 瀧 由樹, 河野 貴史, 番 典子, 西村 基, 田中 知明, 山本 恭平
    日本内分泌学会雑誌 96(2) 554-554 2020年10月  
  • 石毛 崇之, 川崎 健治, 宇津野 恵美, 澤井 摂, 西村 基, 野村 文夫, 松下 一之
    臨床化学 49(Suppl.1) 195-195 2020年10月  
  • 新井 誠人, 北村 浩一, 加野 将之, 太和田 暁之, 西村 基, 楯 真一, 藤木 亮二, 金田 篤志, 松下 一之, 加藤 直也, 松原 久裕, 滝口 裕一
    日本癌治療学会学術集会抄録集 58回 O62-6 2020年10月  
  • 樋口 誠一郎, 高 躍, 姚 躍, 大和 梓, 橋本 直子, 永野 秀和, 中山 哲俊, 西村 基, 山形 一行, 横山 真隆, 藤井 陽一, 小川 誠司, 田中 知明
    日本内分泌学会雑誌 96(1) 283-283 2020年8月  

MISC

 175

共同研究・競争的資金等の研究課題

 17