首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Mutation in the DNA-binding domain of the EWS-Oct-4 oncogene results in dominant negative activity that interferes with EWS-Oct-4-mediated transactivation.
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Mutation in the DNA-binding domain of the EWS-Oct-4 oncogene results in dominant negative activity that interferes with EWS-Oct-4-mediated transactivation.

机译:EWS-OCT-4癌基因的DNA结合结构域中的突变导致显性的阴性活性干扰EWS-OCT-4介导的转移激活。

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摘要

The EWS-Oct-4 protein is a chimeric molecule in which the amino terminal domain (NTD) of the EWS becomes fused to the carboxy terminal domain (CTD) of the Oct-4 transcription factor. It was identified in human bone and soft-tissue tumors associated with t(6;22)(p21;q12). Using in vitro and in vivo systems, we found that the EWS-Oct-4 protein self-associates. The major domains required for self-association mapped to the EWS NTD (amino acids 70-163) and the POU DNA-binding domain. EWS-Oct-4 protein also associated with EWS-Oct-4 (V351P), which contains a mutation in the POU DNA-binding domain. Using electrophoretic mobility shift assays, we found that the EWS-Oct-4 (V351P) mutant interfered with wild-type EWS-Oct-4 DNA-binding activity. In addition, we found that EWS-Oct-4-mediated transcriptional activation was inhibited by EWS-Oct-4 (V351P) protein in vivo. Thus, this mutation in the POU DNA-binding domain results in a dominant negative protein. These findings suggest that the biological functions of the EWS-Oct-4 oncogene can be modulated by the dominant negative mutant EWS-Oct-4 (V351P).
机译:EWS-OCT-4蛋白是嵌合分子,其中EWS的氨基末端结构域(NTD)与OCT-4转录因子的羧基末端结构域(CTD)融合。它是在与T(6; 22)相关的人骨和软组织肿瘤中鉴定(P21; Q12)。在体外和体内系统中使用,我们发现EWS-OCT-4蛋白质自我联系。自我关联所需的主要结构域映射到EWS NTD(氨基酸70-163)和POU DNA结合结构域。 EWS-OCT-4蛋白也与EWS-OCT-4(V351P)相关,其含有POU DNA结合结构域中的突变。使用电泳迁移率移位测定,我们发现EWS-OCT-4(V351P)突变体干扰了野生型EWS-OCT-44DNA结合活性。此外,我们发现EWS-OCT-4-介导的转录激活受到体内EWS-OCT-4(V351P)蛋白抑制的。因此,POU DNA结合结构域的这种突变导致显性阴性蛋白质。这些发现表明EWS-OCT-4癌基因的生物功能可以由显性负突变体EWS-OCT-10-10-4(V351P)调节。

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