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Publication : Enhanced expression of the early retrotransposon in C3H mouse-derived myeloid leukemia cells.

First Author  Tanaka I Year  2001
Journal  Virology Volume  280
Issue  1 Pages  107-14
PubMed ID  11162824 Mgi Jnum  J:67518
Mgi Id  MGI:1930762 Doi  10.1006/viro.2000.0732
Citation  Tanaka I, et al. (2001) Enhanced expression of the early retrotransposon in C3H mouse-derived myeloid leukemia cells. Virology 280(1):107-14
abstractText  Cells of acute myeloid leukemia (AML) from C3H/He mice express an increased amount of RNA for an endogenous retrovirus-like retrotransposon, intracisternal A-particle element. We analyzed the transcription of other mouse retrotransposons in C3H-derived tumor cells and found that all the AML lines from different mice overexpress early-transposon (ETn) RNA. In contrast, only faint levels of ETn were detected in the cells from other tumors, including hepatoma and lymphoma. The polyadenylation sites of the ETn RNA in the AML cells varied. We also determined the binding site for the nuclear extract of the AML cells in the long terminal repeat sequence of ETn. The overexpression of ETn as a common phenotype of AML cells suggests that myeloid cells with this phenotype are the origin of all the AML cells or that the phenotype is acquired during leukemogenesis. Copyright 2001 Academic Press.
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