Tyrosine Kinase Activity and Transformation Potency of <i>bcr-abl</i> Oncogene Products

T G Lugo(Howard Hughes Medical Institute), Ann Marie Pendergast(Howard Hughes Medical Institute), Alexander J. Muller(Howard Hughes Medical Institute), Owen N. Witte(Howard Hughes Medical Institute)
Science
March 2, 1990
Cited by 1,302

Abstract

Oncogenic activation of the proto-oncogene c-abl in human leukemias occurs as a result of the addition of exons from the gene bcr and truncation of the first abl exon. Analysis of tyrosine kinase activity and quantitative measurement of transformation potency in a single-step assay indicate that variation in bcr exon contribution results in a functional difference between p210bcr-abl and p185bcr-abl proteins. Thus, foreign upstream sequences are important in the deregulation of the kinase activity of the abl product, and the extent of deregulation correlates with the pathological effects of the bcr-abl proteins.


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