Published July 5, 2022 | Version v1
Journal article Open

Pyruvate Kinase M1 Suppresses Development and Progression of Prostate Adenocarcinoma

Creators

  • 1. Koch Institute for Integrative Cancer Research, Massachusetts Institute of Technology, Cambridge, Massachusetts
  • 2. Elucidata, Cambridge, Massachusetts
  • 3. Whitehead Institute, Cambridge, Massachusetts
  • 4. Weill Cornell Medical College, New York, New York
  • 5. Center for Cooperative Research in Biosciences (CIC bioGUNE), Derio, Spain
  • 6. Beth Israel Deaconess Medical Center, Boston, Massachusetts
  • 7. Dana-Farber Cancer Institute, Boston, Massachusetts
  • 8. National Center for Advancing Translational Sciences, NIH, Bethesda, Maryland

Description

Altered metabolism helps sustain cancer cell proliferation and survival. Most cancers, including prostate cancers, express the M2 splice isoform of pyruvate kinase (PKM2), which can support anabolic metabolism to support cell proliferation. However, Pkm2 expression is dispensable for the formation and growth of many cancers in vivo. Expression of pyruvate kinase isoform M1 (Pkm1) is restricted to relatively few tissues and has been reported to promote growth of select tumors, but the role of PKM1 in cancer has been less studied than PKM2. To test how differential expression of pyruvate kinase isoforms affects cancer initiation and progression, we generated mice harboring a conditional allele of Pkm1 and crossed these mice, or those with a Pkm2 conditional allele, with a Pten loss-driven prostate cancer model. Pkm1 loss led to increased PKM2 expression and accelerated prostate cancer development, whereas Pkm2 deletion led to increased PKM1 expression and suppressed tumor progression. Metabolic profiling revealed altered nucleotide levels in tumors with high PKM1 expression, and failure of these tumors to progress was associated with DNA replication stress and senescence. Consistent with these data, a small molecule pyruvate kinase activator that mimics a high activity PKM1-like state suppressed progression of established prostate tumors. Analysis of human specimens showed PKM2 expression is retained in most human prostate cancers. Overall, this study uncovers a role for pyruvate kinase isoforms in prostate cancer initiation and progression, and argues that pharmacologic pyruvate kinase activation may be beneficial for treating prostate cancer.

Notes

The authors thank the Swanson Biotechnology Center for tissue processing and members of the Vander Heiden Laboratory for thoughtful discussions. They also thank John Frangioni for assistance with FDG-PET studies and B. Bevis for help generating figures. S.M. Davidson was supported by an NSF Graduate Research Fellowship and T32GM007287. E. Freinkman acknowledges support from W81XWH-15-1-0337 from the Department of Defense. D.R. Schmidt acknowledges support by the Joint Center for Radiation Therapy Foundation and the Harvard University KL2/Catalyst Medical Research Investigator Training award (TR002542). C.J. Thomas acknowledges support from the Division of Preclinical Innovation, National Center for Advancing Translational Research and the Center for Cancer Research, NCI. L.C. Cantley acknowledges support from R35CA197588. M.G. Vander Heiden acknowledges support from the Ludwig Center at MIT, the Burroughs Wellcome Fund, the Damon Runyon Cancer Research Foundation, the MIT Center for Precision Cancer Medicine, a Stand Up To Cancer Innovative Research Grant (Grant Number SU2C-AACRIRG- 09-16), the Emerald Foundation, the NIH (P30CA1405141, R35CA242379, R01CA168653, K08CA136983, P50CA090381), and a faculty scholar award from the Howard Hughes Medical Institute. Stand Up To Cancer is a division of the Entertainment Industry Foundation. The indicated SU2C grant is administered by the American Association for Cancer Research, the scientific partner of SU2C.

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