FCGR3A-158 polymorphism influences the biological response to infliximab in Crohn’s disease through affecting the ADCC activity
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  • 作者:Rintaro Moroi (1) (3)
    Katsuya Endo (1)
    Yoshitaka Kinouchi (1)
    Hisashi Shiga (1)
    Yoichi Kakuta (1)
    Masatake Kuroha (1)
    Yoshitake Kanazawa (1)
    Yosuke Shimodaira (1)
    Takahiko Horiuchi (2)
    Seiichi Takahashi (1)
    Tooru Shimosegawa (1)
  • 关键词:Infliximab ; Crohn’s disease ; FCGR3A ; Polymorphism ; ADCC
  • 刊名:Immunogenetics
  • 出版年:2013
  • 出版时间:April 2013
  • 年:2013
  • 卷:65
  • 期:4
  • 页码:265-271
  • 全文大小:222KB
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  • 作者单位:Rintaro Moroi (1) (3)
    Katsuya Endo (1)
    Yoshitaka Kinouchi (1)
    Hisashi Shiga (1)
    Yoichi Kakuta (1)
    Masatake Kuroha (1)
    Yoshitake Kanazawa (1)
    Yosuke Shimodaira (1)
    Takahiko Horiuchi (2)
    Seiichi Takahashi (1)
    Tooru Shimosegawa (1)

    1. Division of Gastroenterology, Tohoku University Graduate School of Medicine, Aoba-ku, Sendai, Japan
    3. 1-1, Seiryo, Aoba-ku, Sendai, Miyagi, Japan
    2. Department of Medicine and Biosystemic Science, Kyushu University Faculty of Medicine, Kyushu, Japan
  • ISSN:1432-1211
文摘
An association between FCGR3A-158?V/F polymorphism and biological responses to infliximab has been reported in Crohn’s disease (CD) in Western countries. However, little is known about the mechanism by which gene polymorphism affects the responses to infliximab. The aims of this study were to confirm the association in Japanese CD patients and to reveal the effect of gene polymorphism on biological responses to infliximab. Japanese CD patients were examined retrospectively at weeks 8 and 30. Clinical and biological responses were assessed by the Crohn’s disease activity index and C-reactive protein levels, respectively. The infliximab-binding affinity of natural killer (NK) cells from FCGR3A-158?V/V, V/F and F/F donors was examined. Infliximab-mediated antibody-dependent cell-mediated cytotoxicity (ADCC) activities were also determined using transmembrane TNF-α-expressing Jurkat T cells as target cells and peripheral blood mononuclear cells (PBMCs) from V/V, V/F and F/F donors as effector cells. Biological responses at week 8 were statistically higher in V/V patients, whereas no significant differences were observed in either clinical responses at weeks 8 and 30 or biological responses at week 30 among the three genotypes. NK cells and PBMCs from V/V patients also showed higher infliximab-binding affinity and infliximab-mediated ADCC activity, respectively. Our results suggest that FCGR3A-158 polymorphism is a predicting factor of biological responses to infliximab in the early phases. FCGR3A-158 polymorphism was also found to affect the infliximab-binding affinity of NK cells and infliximab-mediated ADCC activity in vitro, suggesting that an effect on ADCC activity influences biological responses to infliximab in CD patients.

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