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Data from Pyruvate Kinase Inhibits Proliferation during Postnatal Cerebellar Neurogenesis and Suppresses Medulloblastoma Formation

Posted on 2023-03-31 - 00:21
Abstract

Aerobic glycolysis supports proliferation through unresolved mechanisms. We have previously shown that aerobic glycolysis is required for the regulated proliferation of cerebellar granule neuron progenitors (CGNP) and for the growth of CGNP-derived medulloblastoma. Blocking the initiation of glycolysis via deletion of hexokinase-2 (Hk2) disrupts CGNP proliferation and restricts medulloblastoma growth. Here, we assessed whether disrupting pyruvate kinase-M (Pkm), an enzyme that acts in the terminal steps of glycolysis, would alter CGNP metabolism, proliferation, and tumorigenesis. We observed a dichotomous pattern of PKM expression, in which postmitotic neurons throughout the brain expressed the constitutively active PKM1 isoform, while neural progenitors and medulloblastomas exclusively expressed the less active PKM2. Isoform-specific Pkm2 deletion in CGNPs blocked all Pkm expression. Pkm2-deleted CGNPs showed reduced lactate production and increased SHH-driven proliferation. 13C-flux analysis showed that Pkm2 deletion reduced the flow of glucose carbons into lactate and glutamate without markedly increasing glucose-to-ribose flux. Pkm2 deletion accelerated tumor formation in medulloblastoma-prone ND2:SmoA1 mice, indicating the disrupting PKM releases CGNPs from a tumor-suppressive effect. These findings show that distal and proximal disruptions of glycolysis have opposite effects on proliferation, and that efforts to block the oncogenic effect of aerobic glycolysis must target reactions upstream of PKM. Cancer Res; 77(12); 3217–30. ©2017 AACR.

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FUNDING

UNC CGBID Histology Core

UNC Tissue Pathology Laboratory Core

National Institute of Neurological Disorders and Stroke

American Institute for Cancer Research

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AUTHORS (18)

  • Katherine Tech
    Andrey P. Tikunov
    Hamza Farooq
    A. Sorana Morrissy
    Jessica Meidinger
    Taylor Fish
    Sarah C. Green
    Hedi Liu
    Yisu Li
    Andrew J. Mungall
    Richard A. Moore
    Yussanne Ma
    Steven J.M. Jones
    Marco A. Marra
    Matthew G. Vander Heiden
    Michael D. Taylor
    Jeffrey M. Macdonald
    Timothy R. Gershon
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