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FLT3配体对携带FLT3内部串联重复突变的小鼠模型的生存及疾病表型的影响。

Effect of FLT3 ligand on survival and disease phenotype in murine models harboring a FLT3 internal tandem duplication mutation.

作者信息

Bailey Emily J, Duffield Amy S, Greenblatt Sarah M, Aplan Peter D, Small Donald

机构信息

Department of Pediatric Oncology, Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.

出版信息

Comp Med. 2013 Jun;63(3):218-26.

Abstract

Many of the mutations contributing to leukemogenesis in acute myeloid leukemia have been identified. A common activating mutation is an internal tandem duplication (ITD) mutation in the FLT3 gene that is found in approximately 25% of patients and confers a poor prognosis. FLT3 inhibitors have been developed and have some efficacy, but patients often relapse. Levels of FLT3 ligand (FL) are significantly elevated in patients during chemotherapy and may be an important component contributing to relapse. We used a mouse model to investigate the possible effect of FL expression on leukemogenesis involving FLT3-ITD mutations in an in vivo system. FLT3(ITD/ITD) FL(-/-) (knockout) mice had a statistically significant increase in survival compared with FLT3(ITD/ITD) FL(+/+) (wildtype) mice, most of which developed a fatal myeloproliferative neoplasm. These findings suggest that FL levels may have prognostic significance in human patients. We also studied the effect of FL expression on survival in a FLT3-ITD NUP98-HOX13 (NHD13) fusion mouse model. These mice develop an aggressive leukemia with short latency. We asked whether FL expression played a similar role in this context. The NUP98-HOX13 FLT3(ITD/wt) FL(-/-) mice did not have a survival advantage, compared with NUP98-HOX13 FLT3(ITD/wt) FL(+/+) mice (normal FL levels). The loss of the survival advantage of the FL knockout group in the NUP98-HOX13 model suggests that adding a second mutation changes the effect of FL expression in the context of more aggressive disease.

摘要

急性髓系白血病中许多导致白血病发生的突变已被确定。一种常见的激活突变是FLT3基因的内部串联重复(ITD)突变,约25%的患者存在该突变,其预后较差。FLT3抑制剂已被研发出来并具有一定疗效,但患者常出现复发。化疗期间患者体内的FLT3配体(FL)水平显著升高,这可能是导致复发的一个重要因素。我们使用小鼠模型在体内系统中研究FL表达对涉及FLT3-ITD突变的白血病发生的可能影响。与FLT3(ITD/ITD) FL(+/+)(野生型)小鼠相比,FLT3(ITD/ITD) FL(-/-)(敲除)小鼠的生存率有统计学意义的显著提高,大多数野生型小鼠会发展为致命的骨髓增殖性肿瘤。这些发现表明,FL水平在人类患者中可能具有预后意义。我们还研究了FL表达对FLT3-ITD NUP98-HOX13(NHD13)融合小鼠模型生存率的影响。这些小鼠会迅速发展为侵袭性白血病。我们探讨在这种情况下FL表达是否发挥类似作用。与NUP98-HOX13 FLT3(ITD/wt) FL(+/+)小鼠(正常FL水平)相比,NUP98-HOX13 FLT3(ITD/wt) FL(-/-)小鼠没有生存优势。在NUP98-HOX13模型中FL敲除组失去生存优势,这表明添加第二个突变会改变FL表达在更侵袭性疾病背景下的作用。

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