SCL, A GENE FREQUENTLY ACTIVATED IN HUMAN T-CELL LEUKEMIA, DOES NOT INDUCE LYMPHOMAS IN TRANSGENIC MICE

Robb, L; Rasko, JEJ; Bath, ML; Strasser, A; Begley, CG

Author(s): Robb, L; Rasko, JEJ; Bath, ML; Strasser, A; Begley, CG;
Details: Publication Year 1995-01-05,Volume 10,Issue #1,Page 205-209
Journal Title: ONCOGENE
Publication Type: Journal Article
Abstract: The scl gene is implicated in human T cell acute lymphoblastic leukaemia (T-ALL) through its involvement in the t(1;14)(p32;q11) chromosomal translocation and, more frequently, as a result of a tumour-specific interstitial deletion on chromosome 1. The consequence of both these chromosomal alterations is overexpression of scl in the leukaemic cells. Despite the strong inference of a role in human T-ALL, scl has not yet been demonstrated to be causally involved in neoplastic transformation. We attempted to do this by generating transgenic mice in which scl expression was directed to the T cell lineage using the CD2 enhancer and the strong SR alpha viral promoter (CD2-scl mice). Three transgenic lines, an of which expressed the scl transgene at a high level, were bred and analysed. No alterations in T cell development were seen in the mice. Unexpectedly CD2-scl mice did not develop tumours, nor did the transgene enhance tumourigenesis by Moloney murine leukaemia virus. These findings throw into question the mechanism by which aberrant scl expression contributes to T cell leukaemogenesis.
Publisher: STOCKTON PRESS
Keywords: LOOP-HELIX GENE; ACUTE LYMPHOBLASTIC-LEUKEMIA; DNA-BINDING MOTIF; C-MYC; TAL-1 GENE; N-MYC; TRANSLOCATION; LOCUS; OVEREXPRESSION; HEMATOPOIESIS
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Creation Date: 1995-01-05 12:00:00