Therapeutic antagonists of microRNAs deplete leukemia-initiating cell activity

微小RNA的治疗性拮抗剂会降低白血病起始细胞的活性

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作者:Chinavenmeni S Velu, Aditya Chaubey, James D Phelan, Shane R Horman, Mark Wunderlich, Monica L Guzman, Anil G Jegga, Nancy J Zeleznik-Le, Jianjun Chen, James C Mulloy, Jose A Cancelas, Craig T Jordan, Bruce J Aronow, Guido Marcucci, Balkrishen Bhat, Brian Gebelein, H Leighton Grimes
期刊:Journal of Clinical Investigation影响因子:13.300
时间:2014起止号:2014 Jan;124(1):222-36.
doi:10.1172/JCI66005研究方向: 免疫、细胞生物学
疾病类型: 白血病细胞类型: 肿瘤细胞

Abstract

Acute myelogenous leukemia (AML) subtypes that result from oncogenic activation of homeobox (HOX) transcription factors are associated with poor prognosis. The HOXA9 transcription activator and growth factor independent 1 (GFI1) transcriptional repressor compete for occupancy at DNA-binding sites for the regulation of common target genes. We exploited this HOXA9 versus GFI1 antagonism to identify the genes encoding microRNA-21 and microRNA-196b as transcriptional targets of HOX-based leukemia oncoproteins. Therapeutic inhibition of microRNA-21 and microRNA-196b inhibited in vitro leukemic colony forming activity and depleted in vivo leukemia-initiating cell activity of HOX-based leukemias, which led to leukemia-free survival in a murine AML model and delayed disease onset in xenograft models. These data establish microRNA as functional effectors of endogenous HOXA9 and HOX-based leukemia oncoproteins, provide a concise in vivo platform to test RNA therapeutics, and suggest therapeutic value for microRNA antagonists in AML.

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