Transformation properties of the E2a-Pbx1 chimeric oncoprotein: fusion with E2a is essential, but the Pbx1 homeodomain is dispensable.

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Mol Cell Biol. 1994 December; 14(12): 8304-8314

Transformation properties of the E2a-Pbx1 chimeric oncoprotein: fusion with E2a is essential, but the Pbx1 homeodomain is dispensable.

K Monica, D P LeBrun, D A Dedera, R Brown and M L Cleary

Department of Pathology, Stanford University Medical Center, California 94305.

ABSTRACT

The t(1;19) chromosomal translocation in acute lymphoblasticleukemias creates chimeric E2a-Pbx1 oncoproteins that can actas DNA-binding activators of transcription. A structural analysisof the functional domains of E2a-Pbx1 showed that portions ofboth E2a and Pbx1 were essential for transformation of NIH 3T3cells and transcriptional activation of synthetic reporter genescontaining PBX1 consensus binding sites. Hyperexpression ofwild-type or experimentally truncated Pbx1 proteins was insufficientfor transformation, consistent with their inability to activatetranscription. When fused with E2a, the Pbx-related proteinsPbx2 and Pbx3 were also transformation competent, demonstratingthat all known members of this highly similar subfamily of homeodomainproteins have latent oncogenic potential. The oncogenic contributionsof E2a to the chimeras were localized to transactivation motifsAD1 and AD2, as their mutation significantly impaired transformation.Either the homeodomain or Pbx1 amino acids flanking this regioncould mediate transformation when fused to E2a. However, thehomeodomain was not essential for transformation, since a mutantE2a-Pbx1 protein (E2a-Pbx delta HD) lacking the homeodomainefficiently transformed fibroblasts and induced malignant lymphomasin transgenic mice. Thus, transformation mediated by the chimericoncoprotein E2a-Pbx1 is absolutely dependent on motifs acquiredfrom E2a but the Pbx1 homeodomain is optional. The latter findingsuggests that E2a-Pbx1 may interact with cellular proteins thatassist or mediate alterations in gene expression responsiblefor oncogenesis even in the absence of homeodomain-DNA interactions.

Mol Cell Biol. 1994 December; 14(12): 8304-8314

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