A LIN28B-RAN-AURKA Signaling Network Promotes Neuroblastoma Tumorigenesis

Schnepp Robert W.; Khurana Priya; Attiyeh Edward F.; Raman Pichai; Chodosh Sara E.; Oldridge Derek A.; Gagliardi Maria E.; Conkrite Karina L.; Asgharzadeh Shahab; Seeger Robert C.; Madison Blair B.; Rustgi Anil K.; Maris John M.; Diskin Sharon J.

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A LIN28B-RAN-AURKA Signaling Network Promotes Neuroblastoma Tumorigenesis

机译：LIN28B-RAN-AURKA信号网络促进神经母细胞瘤的肿瘤发生

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A more complete understanding of aberrant oncogenic signaling in neuroblastoma, a malignancy of the developing sympathetic nervous system, is paramount to improving patient outcomes. Recently, we identified LIN28B as an oncogenic driver in high-risk neuroblastoma. Here, we identify the oncogene RAN as a LIN28B target and show regional gain of chromosome 12q24 as an additional somatic alteration resulting in increased RAN expression. We show that LIN28B influences RAN expression by promoting RAN Binding Protein 2 expression and by directly binding RAN mRNA. Further, we demonstrate a convergence of LIN28B and RAN signaling on Aurora kinase A activity. Collectively, these findings demonstrate that LIN28B-RAN-AURKA signaling drives neuroblastoma oncogenesis, suggesting that this pathway may be amenable to therapeutic targeting.

机译：对神经母细胞瘤（发展中的交感神经系统的恶性肿瘤）中异常致癌信号的更完整理解对于改善患者预后至关重要。最近，我们确定LIN28B为高危神经母细胞瘤的致癌驱动因子。在这里，我们将致癌基因RAN识别为LIN28B靶标，并显示了12q24染色体的区域增益，作为导致RAN表达增加的另一种体细胞变化。我们显示LIN28B通过促进RAN结合蛋白2表达和直接结合RAN mRNA来影响RAN表达。此外，我们证明了LIN28B和RAN信号对Aurora激酶A活性的收敛。总的来说，这些发现表明LIN28B-RAN-AURKA信号驱动神经母细胞瘤的发生，表明该途径可能适合治疗性靶向。

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《Cancer Cell》 |2015年第5期|共11页
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Schnepp Robert W.; Khurana Priya; Attiyeh Edward F.; Raman Pichai; Chodosh Sara E.; Oldridge Derek A.; Gagliardi Maria E.; Conkrite Karina L.; Asgharzadeh Shahab; Seeger Robert C.; Madison Blair B.; Rustgi Anil K.; Maris John M.; Diskin Sharon J.;
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正文语种 eng
中图分类肿瘤学;
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1. A LIN28B-RAN-AURKA Signaling Network Promotes Neuroblastoma Tumorigenesis [J] . Schnepp Robert W., Khurana Priya, Attiyeh Edward F., Cancer Cell . 2015,第5期

机译：LIN28B-RAN-AURKA信号网络促进神经母细胞瘤的肿瘤发生
2. The mitochondrial retrograde signaling regulates Wnt signaling to promote tumorigenesis in colon cancer [J] . Wen Yang-An, Xiong Xiaopeng, Scott Timothy, Cell death and differentiation . 2019,第10期

机译：线粒体逆行信号调节WNT信号传导，以促进结肠癌中的肿瘤内酯
3. Long noncoding RNA LINC01410 promotes the tumorigenesis of neuroblastoma cells by sponging microRNA‐506‐3p and modulating WEE1 [J] . Jie Mi, Yang Han, Jin Zhang, Cancer Medicine . 2020,第21期

机译：长度非编码RNA LINC01410通过海绵微润罗纳-506-3P促进神经母细胞瘤细胞的肿瘤鉴定，并调节WEE1
4. Tumor promoting mechanism of biomaterials: No involvement of mutation in cx43 gene in the tumorigenesis induced by polyurethanes in vitro [C] . Toshie Tsuchiya, Md. Abu Sayed, Akitada Nakamura Joint International Meeting of the Japanese Association for Animal Cell Technolog and and European Society for Animal Cell Technology . 1999

机译：生物材料的肿瘤促进机制：在体外聚氨酯诱导的CX43基因中突变中的突变缺失
5. Nuclear Factor-κB Promotes Urothelial Tumorigenesis and Cancer Progression via Cooperation with Androgen Receptor Signaling [D] . Inoue Satoshi, 井上聡 2019

机译：核因子-κB通过与雄激素受体信号传导协同促进尿路上皮肿瘤发生和癌症进展。
6. A LIN28B-RAN-AURKA Signaling Network Promotes Neuroblastoma Tumorigenesis [O] . Robert W. Schnepp, Priya Khurana, Edward F. Attiyeh, -1

机译：LIN28B-RAN-AURKA信号网络促进神经母细胞瘤的肿瘤发生
7. A LIN28B-RAN-AURKA Signaling Network Promotes Neuroblastoma Tumorigenesis [O] . Schnepp Robert W., Khurana Priya, Attiyeh Edward F., 2015

机译：LIN28B-RAN-AURKA信号网络促进神经母细胞瘤的肿瘤发生

A LIN28B-RAN-AURKA Signaling Network Promotes Neuroblastoma Tumorigenesis

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