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YAP and TAZ modulate cell phenotype in a subset of small cell lung cancer

机译:YAP和TAZ调节小细胞肺癌子集中的细胞表型

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摘要

Small cell lung cancer (SCLC) is a highly aggressive and metastatic malignancy that shows rapid development of chemoresistance and a high rate of recurrence. Recent genome and transcriptome studies have provided the whole landscape of genomic alterations and gene expression changes in SCLC. In light of the inter-individual heterogeneity of SCLC, subtyping of SCLC might be helpful for prediction of therapeutic response and prognosis. Based on the transcriptome data of SCLC cell lines, we undertook transcriptional network-defined SCLC classification and identified a unique SCLC subgroup characterized by relatively high expression of Hippo pathway regulators Yes-associated protein (YAP) and transcriptional coactivator with PDZ-binding motif (TAZ) (YAP/TAZ subgroup). The YAP/TAZ subgroup displayed adherent cell morphology, lower expression of achaete-scute complex homolog 1 (ASCL1) and neuroendocrine markers, and higher expression of laminin and integrin. YAP knockdown caused cell morphological alteration reminiscent of floating growth pattern in many SCLC cell lines, and microarray analyses revealed a subset of genes regulated by YAP, including Ajuba LIM protein (AJUBA). AJUBA also contributed to cell morphology regulation. Of clinical importance, SCLC cell lines of the YAP/TAZ subgroup showed unique patterns of drug sensitivity. Our findings shed light on a subtype of SCLC with YAP and TAZ expression, and delineate molecular networks underlying the heterogeneity of SCLC.
机译:小细胞肺癌(SCLC)是一种高度侵袭性和转移性恶性肿瘤,表现出化学耐药性的快速发展和高复发率。最近的基因组和转录组研究提供了SCLC中基因组改变和基因表达变化的整体情况。鉴于SCLC个体间的异质性,SCLC的亚型可能有助于预测治疗反应和预后。根据SCLC细胞系的转录组数据,我们进行了转录网络定义的SCLC分类,并确定了一个独特的SCLC亚组,其特征是相对较高的Hippo途径调节因子Yes相关蛋白(YAP)和具有PDZ结合基序的转录共激活因子(TAZ) )(YAP / TAZ子组)。 YAP / TAZ亚组显示出贴壁细胞形态,achaete-scute复杂同源物1(ASCL1)和神经内分泌标记物的较低表达,以及层粘连蛋白和整联蛋白的较高表达。 YAP敲低导致细胞形态变化,使人联想到许多SCLC细胞系中的漂浮生长模式,微阵列分析显示了受YAP调控的基因子集,包括Ajuba LIM蛋白(AJUBA)。 AJUBA还有助于细胞形态调节。在临床上,YAP / TAZ亚组的SCLC细胞系显示出独特的药物敏感性模式。我们的发现揭示了具有YAP和TAZ表达的SCLC的亚型,并描绘了SCLC异质性的分子网络。

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