eLife (Jun 2021)

Dependency of human and murine LKB1-inactivated lung cancer on aberrant CRTC-CREB activation

  • Xin Zhou,
  • Jennifer W Li,
  • Zirong Chen,
  • Wei Ni,
  • Xuehui Li,
  • Rongqiang Yang,
  • Huangxuan Shen,
  • Jian Liu,
  • Francesco J DeMayo,
  • Jianrong Lu,
  • Frederic J Kaye,
  • Lizi Wu

DOI
https://doi.org/10.7554/eLife.66095
Journal volume & issue
Vol. 10

Abstract

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Lung cancer with loss-of-function of the LKB1 tumor suppressor is a common aggressive subgroup with no effective therapies. LKB1-deficiency induces constitutive activation of cAMP/CREB-mediated transcription by a family of three CREB-regulated transcription coactivators (CRTC1-3). However, the significance and mechanism of CRTC activation in promoting the aggressive phenotype of LKB1-null cancer remain poorly characterized. Here, we observed overlapping CRTC expression patterns and mild growth phenotypes of individual CRTC-knockouts in lung cancer, suggesting functional redundancy of CRTC1-3. We consequently designed a dominant-negative mutant (dnCRTC) to block all three CRTCs to bind and co-activate CREB. Expression of dnCRTC efficiently inhibited the aberrantly activated cAMP/CREB-mediated oncogenic transcriptional program induced by LKB1-deficiency, and specifically blocked the growth of human and murine LKB1-inactivated lung cancer. Collectively, this study provides direct proof for an essential role of the CRTC-CREB activation in promoting the malignant phenotypes of LKB1-null lung cancer and proposes the CRTC-CREB interaction interface as a novel therapeutic target.

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