CD33
髓系白血病
奥佐美星
白血病
嵌合抗原受体
髓样
癌症研究
免疫学
造血
医学
克隆(Java方法)
移植
川地34
干细胞
免疫疗法
生物
内科学
免疫系统
DNA
遗传学
作者
Saad S. Kenderian,Marco Ruella,Olga Shestova,Michael Klichinsky,Vania Aikawa,Jennifer J.D. Morrissette,John Scholler,Dawei Song,David Porter,Martin Carroll,Carl H. June,Saar Gill
出处
期刊:Leukemia
[Springer Nature]
日期:2015-02-27
卷期号:29 (8): 1637-1647
被引量:373
摘要
Patients with chemo-refractory acute myeloid leukemia (AML) have a dismal prognosis. Chimeric antigen receptor T (CART) cell therapy has produced exciting results in CD19+ malignancies and may overcome many of the limitations of conventional leukemia therapies. We developed CART cells to target CD33 (CART33) using the anti-CD33 single chain variable fragment used in gemtuzumab ozogamicin (clone My96) and tested the activity and toxicity of these cells. CART33 exhibited significant effector functions in vitro and resulted in eradication of leukemia and prolonged survival in AML xenografts. CART33 also resulted in human lineage cytopenias and reduction of myeloid progenitors in xenograft models of hematopoietic toxicity, suggesting that permanently expressed CD33-specific CART cells would have unacceptable toxicity. To enhance the viability of CART33 as an option for AML, we designed a transiently expressed mRNA anti-CD33 CAR. Gene transfer was carried out by electroporation into T cells and resulted in high-level expression with potent but self-limited activity against AML. Thus our preclinical studies show potent activity of CART33 and indicate that transient expression of anti-CD33 CAR by RNA modification could be used in patients to avoid long-term myelosuppression. CART33 therapy could be used alone or as part of a preparative regimen prior to allogeneic transplantation in refractory AML.
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