Cancer Science Institute of Singapore, National University of Singapore, Singapore, Singapore.
PLoS One. 2011 May 12;6(5):e19798. doi: 10.1371/journal.pone.0019798.
Combination with other small molecule drugs represents a promising strategy to improve therapeutic efficacy of FLT3 inhibitors in the clinic. We demonstrated that combining ABT-869, a FLT3 inhibitor, with SAHA, a HDAC inhibitor, led to synergistic killing of the AML cells with FLT3 mutations and suppression of colony formation. We identified a core gene signature that is uniquely induced by the combination treatment in 2 different leukemia cell lines. Among these, we showed that downregulation of PTP4A3 (PRL-3) played a role in this synergism. PRL-3 is downstream of FLT3 signaling and ectopic expression of PRL-3 conferred therapeutic resistance through upregulation of STAT (signal transducers and activators of transcription) pathway activity and anti-apoptotic Mcl-1 protein. PRL-3 interacts with HDAC4 and SAHA downregulates PRL-3 via a proteasome dependent pathway. In addition, PRL-3 protein was identified in 47% of AML cases, but was absent in myeloid cells in normal bone marrows. Our results suggest such combination therapies may significantly improve the therapeutic efficacy of FLT3 inhibitors. PRL-3 plays a potential pathological role in AML and it might be a useful therapeutic target in AML, and warrant clinical investigation.
联合其他小分子药物代表了一种很有前途的策略,可以提高 FLT3 抑制剂在临床上的治疗效果。我们证明,联合使用 FLT3 抑制剂 ABT-869 和 HDAC 抑制剂 SAHA 可以协同杀伤具有 FLT3 突变的 AML 细胞,并抑制集落形成。我们确定了一个核心基因特征,该特征在两种不同的白血病细胞系中由联合治疗独特诱导。在这些基因中,我们表明 PTP4A3(PRL-3)的下调在这种协同作用中起作用。PRL-3 是 FLT3 信号的下游,过表达 PRL-3 通过上调 STAT(信号转导和转录激活因子)途径活性和抗凋亡 Mcl-1 蛋白赋予治疗耐药性。PRL-3 与 HDAC4 相互作用,SAHA 通过蛋白酶体依赖途径下调 PRL-3。此外,在 47%的 AML 病例中鉴定出了 PRL-3 蛋白,但在正常骨髓中的髓样细胞中不存在。我们的研究结果表明,这种联合治疗策略可能显著提高 FLT3 抑制剂的治疗效果。PRL-3 在 AML 中发挥潜在的病理作用,它可能是 AML 中的一个有用的治疗靶点,值得临床研究。
Zotero 插件
