Blood Cancer J. 2011 Jun;1(6):e21. doi: 10.1038/bcj.2011.19. Epub 2011 Jun 3.
Nucleophosmin-anaplastic lymphoma kinase (NPM-ALK) is a tyrosine kinase oncogene responsible for the pathogenesis of the majority of human ALK-positive lymphomas. We recently reported that it activated the Rac1 GTPase in anaplastic large-cell lymphoma (ALCL), leading to Rac-dependent formation of active invadopodia required for invasiveness. Herein, we went further into the study of this pathway and used the inhibitor of Rac, NSC23766, to validate its potential as a molecular target in ALCL in vitro and in vivo in a xenograft model and in a conditional model of NPM-ALK transgenic mice. Our data demonstrate that Rac regulates important effectors of NPM-ALK-induced transformation such as Erk1/2, p38 and Akt. Moreover, inhibition of Rac signaling abrogates NPM-ALK-elicited disease progression and metastasis in mice, highlighting the potential of small GTPases and their regulators as additional therapic targets in lymphomas.
核仁磷酸蛋白-间变性淋巴瘤激酶(NPM-ALK)是一种酪氨酸激酶癌基因,负责大多数人类 ALK 阳性淋巴瘤的发病机制。我们最近报道,它在间变性大细胞淋巴瘤(ALCL)中激活 Rac1 GTPase,导致 Rac 依赖性活性侵袭伪足的形成,这是侵袭所必需的。在此基础上,我们进一步研究了这一途径,并使用 Rac 抑制剂 NSC23766,在体外和异种移植模型以及 NPM-ALK 转基因小鼠的条件模型中验证了其作为 ALCL 的潜在分子靶点的作用。我们的数据表明,Rac 调节 NPM-ALK 诱导的转化的重要效应物,如 Erk1/2、p38 和 Akt。此外,抑制 Rac 信号转导可消除 NPM-ALK 引起的小鼠疾病进展和转移,突出了小 GTPases 及其调节剂作为淋巴瘤的额外治疗靶点的潜力。
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