BCL6 confers KRAS-mutant non–small-cell lung cancer resistance to BET inhibitors
Jiawei Guo, … , Mingyao Liu, Xiufeng Pang
Jiawei Guo, … , Mingyao Liu, Xiufeng Pang
Published January 4, 2021
Citation Information: J Clin Invest. 2021;131(1):e133090. https://doi.org/10.1172/JCI133090.
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BCL6 confers KRAS-mutant non–small-cell lung cancer resistance to BET inhibitors

Abstract

The bromodomain and extra-terminal domain (BET) proteins are promising therapeutic targets to treat refractory solid tumors; however, inherent resistance remains a major challenge in the clinic. Recently, the emerging role of the oncoprotein B cell lymphoma 6 (BCL6) in tumorigenesis and stress response has been unveiled. Here, we demonstrate that BCL6 was upregulated upon BET inhibition in KRAS-mutant cancers, including non–small-cell lung cancer (NSCLC). We further found that BRD3, not BRD2 or BRD4, directly interacted with BCL6 and maintained the negative autoregulatory circuit of BCL6. Disrupting this negative autoregulation by BET inhibitors (BETi) resulted in a striking increase in BCL6 transcription, which further activated the mTOR signaling pathway through repression of the tumor suppressor death-associated protein kinase 2. Importantly, pharmacological inhibition of either BCL6 or mTOR improved the tumor response and enhanced the sensitivity of KRAS-mutant NSCLC to BETi in both in vitro and in vivo settings. Overall, our findings identify a mechanism of BRD3-mediated BCL6 autoregulation and further develop an effective combinatorial strategy to circumvent BETi resistance in KRAS-driven NSCLC.

Authors

Jiawei Guo, Yanan Liu, Jing Lv, Bin Zou, Zhi Chen, Kun Li, Juanjuan Feng, Zhenyu Cai, Lai Wei, Mingyao Liu, Xiufeng Pang

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Figure 2

BCL6 is required for the therapeutic efficacy of BETi.

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BCL6 is required for the therapeutic efficacy of BETi. (A) Efficacy of B...
(A) Efficacy of BCL6 overexpression in A549 cells by immunoblot analysis. (B and C) BCL6 overexpression (BCL6OE) impaired the inhibitory effects of OTX015 on A549 cells, as indicated by (B) growth curves and (C) relative cell viability of cultured colonies. (D) Efficacy of BCL6 overexpression in H23 cells by immunoblot analysis. (E and F) BCL6 overexpression impaired the inhibitory effects of OTX015 on H23 cells, as indicated by the (E) growth curves and (F) relative viability of the cultured colonies. (G) BCL6 silencing potentiated OTX015 efficacy in H441 cells. Left: Representative images of colony formation assays. Right: Relative viability of the cultured colonies. siNC, siRNA negative control. (H) BI3802 enhanced the efficacy of OTX015 in A549 cells. A549 cells were treated with concentration gradients of OTX015 with or without BI3802 for 48 hours. Shown are cell viability curves and immunoblot analysis of BCL6 expression. Results in C, F and G are representative of 3 independent experiments. Data represent the mean ± SEM of biological triplicates. ***P < 0.001, by unpaired, 2-tailed Student’s t test.