Casein kinase 1α–dependent feedback loop controls autophagy in RAS-driven cancers
Jit Kong Cheong, … , Andrew Thorburn, David M. Virshup
Jit Kong Cheong, … , Andrew Thorburn, David M. Virshup
Published March 23, 2015
Citation Information: J Clin Invest. 2015;125(4):1401-1418. https://doi.org/10.1172/JCI78018.
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Research Article Oncology

Casein kinase 1α–dependent feedback loop controls autophagy in RAS-driven cancers

Abstract

Activating mutations in the RAS oncogene are common in cancer but are difficult to therapeutically target. RAS activation promotes autophagy, a highly regulated catabolic process that metabolically buffers cells in response to diverse stresses. Here we report that casein kinase 1α (CK1α), a ubiquitously expressed serine/threonine kinase, is a key negative regulator of oncogenic RAS–induced autophagy. Depletion or pharmacologic inhibition of CK1α enhanced autophagic flux in oncogenic RAS–driven human fibroblasts and multiple cancer cell lines. FOXO3A, a master longevity mediator that transcriptionally regulates diverse autophagy genes, was a critical target of CK1α, as depletion of CK1α reduced levels of phosphorylated FOXO3A and increased expression of FOXO3A-responsive genes. Oncogenic RAS increased CK1α protein abundance via activation of the PI3K/AKT/mTOR pathway. In turn, elevated levels of CK1α increased phosphorylation of nuclear FOXO3A, thereby inhibiting transactivation of genes critical for RAS-induced autophagy. In both RAS-driven cancer cells and murine xenograft models, pharmacologic CK1α inactivation synergized with lysosomotropic agents to inhibit growth and promote tumor cell death. Together, our results identify a kinase feedback loop that influences RAS-dependent autophagy and suggest that targeting CK1α-regulated autophagy offers a potential therapeutic opportunity to treat oncogenic RAS–driven cancers.

Authors

Jit Kong Cheong, Fuquan Zhang, Pei Jou Chua, Boon Huat Bay, Andrew Thorburn, David M. Virshup

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Figure 9

CK1α inhibition synergizes with autophagy inhibition to arrest growth of RAS-driven human cancers.

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CK1α inhibition synergizes with autophagy inhibition to arrest growth of...
(A) D4476:CQ delays HCT-116 tumor xenograft growth. BALB/c athymic nude mice with HCT-116 tumor xenografts were treated with the indicated compounds by daily i.p. injection (n = 6 mice; total of 12 xenografts per treatment group). (B) D4476:CQ results in smaller HCT-116 tumor xenografts. Representative images of tumor xenografts in B and their respective tumor weights are expressed in a scatter plot (mean ± SD). Two-way ANOVA was used to analyze statistical significance in B; **P < 0.01; P < 0.0001.