演題詳細

ポスター / Poster

ポスター 31 (Poster 31) :ATL:移植モガムリズマブ

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日程
2013年10月11日(金)
時間
16:50 - 17:50
会場
ポスター会場 / Poster (ロイトン札幌 3F ロイトンホールABCD)
座長・司会
今泉 芳孝 (Yoshitaka Imaizumi):1
1:長崎大学病院 血液内科
 
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Effects of anti-CCR4 antibodies for adult T-cell leukemia and a risk for viral infection

演題番号 : PS-1-231

江口 剛 (Go Eguchi):1、口分田 貴裕 (Takahiro Kumode):1、山口 晃史 (Terufumi Yamaguchi):1、松村 到 (Itaru Matsumura):2、前田 裕弘 (Yasuhiro Maeda):1

1:National Hospital Organization Osaka Minami Medical Center、2:Department of Hematology, Kinki University School of Medicine

 

The CC-chemokine receptor 4 (CCR4) is expressed in almost ATLL cells. Thus, anti-CCR4 antibodies can be used as a treatment strategy for ATLL. Mogamulizumab (MOG), which is a defucosylated anti-CCR4 monoclonal antibody, showed good results even in patients with recurrent ATLL in phase I or II studies. We treated 8 elderly patients with ATL who were resistant to chemotherapy using MOG monotherapy. All patients received 1.0 mg/kg of mogamulizumab (MOG) once per week for 8 weeks by intravenous infusion. In the present study, we observed CCR4-specific ADCC against CCR4-positive ATL cells. All patients showed CR with a marked decrease in the number of ATL cells. However, 2 patients contracted viral infection because of severe lymphopenia. One patient died because of severe cytomegalovirus infection despite adequate treatment. One patient had Stevens Johnson syndrome. These results suggested that MOG was effective in chemotherapy-resistant ATL patients. However, CCR4 is not only on ATL cells but also on endogenous Treg. The decrease in the number of Treg after MOG monotherapy has been expected to boost the antitumor activity and to be involved in the development of immune disorders, including autoimmune diseases. Furthermore, a decrease in CD4+ T cells led to viral infection. In conclusion, several treatments for prophylaxis of opportunistic infection, including CMV infection, should be recommended.

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