Critical role for a single leucine residue in leukemia induction by E2A-PBX1

Bayly, R; Murase, T; Hyndman, BD; Savage, R; Nurmohamed, S; Munro, K; Casselman, R; Smith, SP; LeBrun, DP

Journal article

Critical role for a single leucine residue in leukemia induction by E2A-PBX1

Abstract:: In roughly 5% of cases of acute lymphoblastic leukemia, a chromosomal translocation leads to expression of the oncogenic protein E2A-PBX1. The N-terminal portion of E2A-PBX1, encoded by the E2A gene, is identical in sequence to the corresponding portion of the E proteins E12/E47 and includes transcriptional activation domains. The C terminus consists of most of the HOX interacting transcription factor PBX1, including its DNA-binding homeodomain. Structure-function correlative experiments have suggested that oncogenesis by E2A-PBX1 requires an activation domain, called AD1, at the extreme N terminus. We recently demonstrated that a potentially helical portion of AD1 interacts directly with the transcriptional coactivator protein cyclic AMP response element-binding protein (CBP) and that this interaction is essential in the immortalization of primary bone marrow cells in tissue culture. Here we show that a conserved LXXLL motif within AD1 is required in the interaction between E2A-PBX1 and the KIX domain of CBP. We show by circular dichroism spectroscopy that the LXXLL-containing portion of AD1 undergoes a helical transition upon interacting with the KIX domain and that amino acid substitutions that prevent helix formation prevent both the KIX interaction and cell immortalization by E2A-PBX1. Perhaps most strikingly, substitution of a single, conserved leucine residue (L20) within the LXXLL motif impairs leukemia induction in mice after transplantation with E2A-PBX1-expressing bone marrow. The KIX domain of CBP mediates well-characterized interactions with several transcription factors of relevance to leukemia induction. Circumstantial evidence suggests that the side chain of L20 might interact with a deep hydrophobic pocket in the KIX domain. Therefore, our results serve to identify a potential new drug target.

Publication status:: Published

Peer review status:: Peer reviewed

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APA Style

Bayly, R., Murase, T., Hyndman, B. D., Savage, R., Nurmohamed, S., Munro, K., Casselman, R., Smith, S. P., & LeBrun, D. P. (2006). Critical role for a single leucine residue in leukemia induction by E2A-PBX1. Molecular and Cellular Biology, 26(17), 6442–6452.

MLA Style

Bayly, R, et al. “Critical Role for a Single Leucine Residue in Leukemia Induction by E2A-PBX1.” Molecular and Cellular Biology, vol. 26, no. 17, 2006, pp. 6442–52.

Chicago Style

Bayly, R, T Murase, BD Hyndman, et al. 2006. “Critical Role for a Single Leucine Residue in Leukemia Induction by E2A-PBX1.” Molecular and Cellular Biology 26 (17): 6442–52.
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