Author
Listed:
- Filippos Kottakis
(Cancer Center, Massachusetts General Hospital
Center for Regenerative Medicine, Massachusetts General Hospital
Harvard Medical School)
- Brandon N. Nicolay
(Cancer Center, Massachusetts General Hospital
Harvard Medical School)
- Ahlima Roumane
(Cancer Center, Massachusetts General Hospital
Center for Regenerative Medicine, Massachusetts General Hospital
Harvard Medical School)
- Rahul Karnik
(Broad Institute of MIT and Harvard
Harvard Stem Cell Institute
Harvard University)
- Hongcang Gu
(Broad Institute of MIT and Harvard
Harvard Stem Cell Institute
Harvard University)
- Julia M. Nagle
(Cancer Center, Massachusetts General Hospital
Center for Regenerative Medicine, Massachusetts General Hospital
Harvard Medical School)
- Myriam Boukhali
(Cancer Center, Massachusetts General Hospital
Harvard Medical School)
- Michele C. Hayward
(UNC, Lineberger Comprehensive Cancer Center, Chapel Hill)
- Yvonne Y. Li
(Brigham and Women’s Hospital and Harvard Medical School
Dana Farber Cancer Institute)
- Ting Chen
(Brigham and Women’s Hospital and Harvard Medical School
Dana Farber Cancer Institute
Belfer Institute for Applied Cancer Science, Dana Farber Cancer Institute)
- Marc Liesa
(Evans Center for Interdisciplinary Research, Mitochondria ARC, Boston University School of Medicine
Diabetes and Hypertension, UCLA David Geffen School of Medicine)
- Peter S. Hammerman
(Brigham and Women’s Hospital and Harvard Medical School
Dana Farber Cancer Institute
Cancer Program, Broad Institute of Harvard and MIT)
- Kwok Kin Wong
(Brigham and Women’s Hospital and Harvard Medical School
Dana Farber Cancer Institute
Belfer Institute for Applied Cancer Science, Dana Farber Cancer Institute)
- D. Neil Hayes
(UNC, Lineberger Comprehensive Cancer Center, Chapel Hill)
- Orian S. Shirihai
(Evans Center for Interdisciplinary Research, Mitochondria ARC, Boston University School of Medicine
Diabetes and Hypertension, UCLA David Geffen School of Medicine)
- Nicholas J. Dyson
(Cancer Center, Massachusetts General Hospital
Harvard Medical School)
- Wilhelm Haas
(Cancer Center, Massachusetts General Hospital
Harvard Medical School)
- Alexander Meissner
(Broad Institute of MIT and Harvard
Harvard Stem Cell Institute
Harvard University)
- Nabeel Bardeesy
(Cancer Center, Massachusetts General Hospital
Center for Regenerative Medicine, Massachusetts General Hospital
Harvard Medical School)
Abstract
Intermediary metabolism generates substrates for chromatin modification, enabling the potential coupling of metabolic and epigenetic states. Here we identify a network linking metabolic and epigenetic alterations that is central to oncogenic transformation downstream of the liver kinase B1 (LKB1, also known as STK11) tumour suppressor, an integrator of nutrient availability, metabolism and growth. By developing genetically engineered mouse models and primary pancreatic epithelial cells, and employing transcriptional, proteomics, and metabolic analyses, we find that oncogenic cooperation between LKB1 loss and KRAS activation is fuelled by pronounced mTOR-dependent induction of the serine–glycine–one-carbon pathway coupled to S-adenosylmethionine generation. At the same time, DNA methyltransferases are upregulated, leading to elevation in DNA methylation with particular enrichment at retrotransposon elements associated with their transcriptional silencing. Correspondingly, LKB1 deficiency sensitizes cells and tumours to inhibition of serine biosynthesis and DNA methylation. Thus, we define a hypermetabolic state that incites changes in the epigenetic landscape to support tumorigenic growth of LKB1-mutant cells, while resulting in potential therapeutic vulnerabilities.
Suggested Citation
Filippos Kottakis & Brandon N. Nicolay & Ahlima Roumane & Rahul Karnik & Hongcang Gu & Julia M. Nagle & Myriam Boukhali & Michele C. Hayward & Yvonne Y. Li & Ting Chen & Marc Liesa & Peter S. Hammerma, 2016.
"LKB1 loss links serine metabolism to DNA methylation and tumorigenesis,"
Nature, Nature, vol. 539(7629), pages 390-395, November.
Handle:
RePEc:nat:nature:v:539:y:2016:i:7629:d:10.1038_nature20132
DOI: 10.1038/nature20132
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