BCL6 repression of EP300 in human diffuse large B cell lymphoma cells provides a basis for rational combinatorial therapy
Leandro C. Cerchietti, … , Gabriela Chiosis, Ari Melnick
Leandro C. Cerchietti, … , Gabriela Chiosis, Ari Melnick
Published November 1, 2010
Citation Information: J Clin Invest. 2010;120(12):4569-4582. https://doi.org/10.1172/JCI42869.
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Research Article Oncology

BCL6 repression of EP300 in human diffuse large B cell lymphoma cells provides a basis for rational combinatorial therapy

Abstract

B cell lymphoma 6 (BCL6), which encodes a transcriptional repressor, is a critical oncogene in diffuse large B cell lymphomas (DLBCLs). Although a retro-inverted BCL6 peptide inhibitor (RI-BPI) was recently shown to potently kill DLBCL cells, the underlying mechanisms remain unclear. Here, we show that RI-BPI induces a particular gene expression signature in human DLBCL cell lines that included genes associated with the actions of histone deacetylase (HDAC) and Hsp90 inhibitors. BCL6 directly repressed the expression of p300 lysine acetyltransferase (EP300) and its cofactor HLA-B–associated transcript 3 (BAT3). RI-BPI induced expression of p300 and BAT3, resulting in acetylation of p300 targets including p53 and Hsp90. Induction of p300 and BAT3 was required for the antilymphoma effects of RI-BPI, since specific blockade of either protein rescued human DLBCL cell lines from the BCL6 inhibitor. Consistent with this, combination of RI-BPI with either an HDAC inhibitor (HDI) or an Hsp90 inhibitor potently suppressed or even eradicated established human DLBCL xenografts in mice. Furthermore, HDAC and Hsp90 inhibitors independently enhanced RI-BPI killing of primary human DLBCL cells in vitro. We also show that p300-inactivating mutations occur naturally in human DLBCL patients and may confer resistance to BCL6 inhibitors. Thus, BCL6 repression of EP300 provides a basis for rational targeted combinatorial therapy for patients with DLBCL.

Authors

Leandro C. Cerchietti, Katerina Hatzi, Eloisi Caldas-Lopes, Shao Ning Yang, Maria E. Figueroa, Ryan D. Morin, Martin Hirst, Lourdes Mendez, Rita Shaknovich, Philip A. Cole, Kapil Bhalla, Randy D. Gascoyne, Marco Marra, Gabriela Chiosis, Ari Melnick

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Figure 3

RI-BPI–induced cell death is rescued by p300 and BAT3 inhibition.

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RI-BPI–induced cell death is rescued by p300 and BAT3 inhibition. (A) A ...
(A) A panel of 7 BCL6-dependent DLBCL cell lines (OCI-Ly7, SU-DHL6, OCI-Ly1, Farage, OCI-Ly3, SU-DHL4, and OCI-Ly10) was exposed in triplicate to RI-BPI (10 μM) (dark gray bars), the p300-HAT inhibitor Lys-CoA (light gray bars), and the combination of both (black bars) for 48 hours (versus respective CPs). Cell viability (as percentage of CP-treated cells) is shown on the y axis. The experiment was carried out in triplicate with biological duplicates. (B) The BCL6-dependent SU-DHL4, SU-DHL6, and OCI-Ly3 cell lines were transfected with siRNA for BAT3 (siBAT3) or nontargeting sequence (siNT) and treated with RI-BPI (10 μM) or control. After 48 hours, viability was determined. Results are expressed as percentage of viable cells normalized to control (siNT). The experiment was carried out in 4 replicates with biological triplicates. Immunoblotting for BAT3 corresponding to the transfected cells is shown in Supplemental Figure 6. Data are presented as mean with 95% CI.