the ews-erg fusion protein can initiate neoplasia from lineage-committed haematopoietic cells从lineage-committed ews-erg融合蛋白可以启动肿瘤造血的细胞.pdfVIP
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the ews-erg fusion protein can initiate neoplasia from lineage-committed haematopoietic cells从lineage-committed ews-erg融合蛋白可以启动肿瘤造血的细胞
Open access, freely available online PLoS BIOLOGY
The Ews-ERG Fusion Protein Can Initiate
Neoplasia from Lineage-Committed
Haematopoietic Cells
Rosalind Codrington, Richard Pannell, Alan Forster, Lesley F. Drynan, Angelika Daser, Nati Lobato, Markus Metzler,
*
Terence H. Rabbitts
MRC Laboratory of Molecular Biology, Cambridge, United Kingdom
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.
Citation: Codrington R, Pannell R, Forster A, Drynan LF, Daser A, et al. (2005) The Ews-ERG fusion protein can initiate neoplasia from lineage-committed haematopoietic cells.
PLoS Biol 3(8): e242.
Introduction
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