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The Ews-ERG Fusion Protein Can Initiate Neoplasia from Lineage-Committed Haematopoietic Cells

机译:Ews-ERG融合蛋白可以从血统的造血细胞中引发肿瘤

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摘要

The EWS-ERG fusion protein is found in human sarcomas with the chromosomal translocation t(21;22)(q22;q12), where the translocation is considered to be an initiating event in sarcoma formation within uncommitted mesenchymal cells, probably long-lived progenitors capable of self renewal. The fusion protein may not therefore have an oncogenic capability beyond these progenitors. To assess whether EWS-ERG can be a tumour initiator in cells other than mesenchymal cells, we have analysed Ews-ERG fusion protein function in a cellular environment not typical of that found in human cancers, namely, committed lymphoid cells. We have used Ews-ERG invertor mice having an inverted ERG cDNA cassette flanked by loxP sites knocked in the Ews intron 8, crossed with mice expressing Cre recombinase under the control of the Rag1 gene to give conditional, lymphoid-specific expression of the fusion protein. Clonal T cell neoplasias arose in these mice. This conditional Ews gene fusion model of tumourigenesis shows that Ews-ERG can cause haematopoietic tumours and the precursor cells are committed cells. Thus, Ews-ERG can function in cells that do not have to be pluripotent progenitors or mesenchymal cells.
机译:EWS-ERG融合蛋白在具有染色体易位t(21; 22)(q22; q12)的人肉瘤中发现,其中该易位被认为是未定型间充质细胞(可能是长寿祖细胞)中肉瘤形成的起始事件能够自我更新。因此,融合蛋白可能不具有这些祖细胞以外的致癌能力。为了评估EWS-ERG是否可以是除间充质细胞以外的其他细胞中的肿瘤引发剂,我们分析了Ews-ERG融合蛋白在人类癌症所不常见的细胞环境中的功能,即定型淋巴样细胞。我们使用的Ews-ERG转化子小鼠具有一个反向ERG cDNA盒,其侧翼是敲入Ews内含子8的loxP位点,与在Rag1基因控制下表达Cre重组酶的小鼠杂交,以有条件地,淋巴样表达融合蛋白。在这些小鼠中出现了克隆性T细胞瘤形成。该有条件的Ews基因融合基因融合模型表明,Ews-ERG可引起造血系统肿瘤,其前体细胞是定型细胞。因此,Ews-ERG可以在不一定是多能祖细胞或间充质细胞的细胞中发挥功能。

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