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Identification of the Wallenda JNKKK as an Alk suppressor reveals increased competitiveness of Alk-expressing cells

机译:作为ALK抑制剂的瓦伦达JNKKK的鉴定揭示了ALK表达细胞的竞争力增加

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Anaplastic lymphoma kinase (Alk) is a receptor tyrosine kinase of the insulin receptor super-family that functions as oncogenic driver in a range of human cancers such as neuroblastoma. In order to investigate mechanisms underlying Alk oncogenic signaling, we conducted a genetic suppressor screen in Drosophila melanogaster. Our screen identified multiple loci important for Alk signaling, including members of Ras/Raf/ERK-, Pi3K-, and STAT-pathways as well as tailless (tll) and foxo whose orthologues NR2E1/TLX and FOXO3 are transcription factors implicated in human neuroblastoma. Many of the identified suppressors were also able to modulate signaling output from activated oncogenic variants of human ALK, suggesting that our screen identified targets likely relevant in a wide range of contexts. Interestingly, two misexpression alleles of wallenda (wnd, encoding a leucine zipper bearing kinase similar to human DLK and LZK) were among the strongest suppressors. We show that Alk expression leads to a growth advantage and induces cell death in surrounding cells. Our results suggest that Alk activity conveys a competitive advantage to cells, which can be reversed by over-expression of the JNK kinase kinase Wnd.
机译:气相生线淋巴瘤激酶(ALK)是胰岛素受体超级家族的受体酪氨酸激酶,其用作一系列人类癌症如神经母细胞瘤的致癌钳。为了研究碱性致癌信号传导的机制,我们在果蝇Melanogaster中进行了遗传抑制筛查。我们的屏幕确定了对ALK信号传导的多个基因座,包括RAS / RAF / ERK-,PI3K和统计途径以及尾部(TLL)和FOXO的成员,其直向导卵剂NR2E1 / TLX和FOXO3是涉及人类神经母细胞瘤的转录因子。许多所识别的抑制剂还能够调节来自人ALK的活化的致癌变体的信号传导输出,这表明我们的筛选在广泛的背景下识别可能相关的目标。有趣的是,Wallenda的两位Misexpression等位基因(Wnd,编码与人DLK和LZK类似的亮氨酸拉链轴承激酶)是最强的抑制剂。我们表明,烷表达导致生长优势并在周围细胞中诱导细胞死亡。我们的研究结果表明,ALK活性对细胞传达了竞争优势,这可以通过过于表达JNK激酶激酶Wnd而逆转。

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