Therapy-induced selective loss of leukemia-initiating activity in murine adult T cell leukemia

治疗诱导的小鼠成年T细胞白血病白血病起始活性选择性丧失

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作者：El Hajj,Hiba,El-Sabban,Marwan,Hasegawa,Hideki,Zaatari,Ghazi,Ablain,Julien,Saab,Shahrazad T,Janin,Anne,Mahfouz,Rami,Nasr,Rihab,Kfoury,Youmna,Nicot,Christophe,Hermine,Olivier,Hall,William,de Thé,Hugues,Bazarbachi,Ali

期刊：	Journal of Experimental Medicine	影响因子：	10.600
时间：	2010	起止号：	2010 Dec 20;207(13):2785-92
doi：	10.1084/jem.20101095	研究方向：	细胞生物学、免疫/内分泌
疾病类型：	白血病	细胞类型：	T细胞

Abstract

Chronic HTLV-I (human T cell lymphotropic virus type I) infection may cause adult T cell leukemia/lymphoma (ATL), a disease with dismal long-term prognosis. The HTLV-I transactivator, Tax, initiates ATL in transgenic mice. In this study, we demonstrate that an As(2)O(3) and IFN-α combination, known to trigger Tax proteolysis, cures Tax-driven ATL in mice. Unexpectedly, this combination therapy abrogated initial leukemia engraftment into secondary recipients, whereas the primary tumor bulk still grew in the primary hosts, only to ultimately abate later on. This loss of initial transplantability required proteasome function. A similar regimen recently yielded unprecedented disease control in human ATL. Our demonstration that this drug combination targeting Tax stability abrogates tumor cell immortality but not short-term growth may foretell a favorable long-term efficiency of this regimen in patients.

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