Tyrosine Phosphorylation Inhibits PKM2 to Promote the Warburg Effect and Tumor Growth

Hitosugi, Taro; Kang, Sumin; Heiden, Matthew G. Vander; Chung, Tae‐Wook; Elf, Shannon; Lythgoe, Katherine; Dong, Suchuan; Lonial, Sagar; Wang, Xu; Chen, Georgia Z.; Xie, Jingui; Gu, Ting; Polakiewicz, Roberto D.; Roesel, Johannes; Boggon, Titus J.; Khuri, Fadlo R.; Gilliland, D. Gary; Cantley, Lewis C.; Kaufman, Jonathan L.; Chen, Jing

doi:10.1126/scisignal.2000431

Cited by 673 publications

(758 citation statements)

References 24 publications

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“…So, inhibition of expression of PKM2 may also affect the proliferation of other cells. The superiority of PKM2 compared with PKM1 might be that it can balance energy supply and glycolytic phospho-metabolite pools by switching between two quaternary conformations (12)(13)(14)(15)(16)(17)(18). As is mentioned above, PKM2 can exist as an active tetrameric and an inactive dimeric form.…”

Section: Discussionmentioning

confidence: 99%

“…Studies have shown that most PKM2 exists mainly as a dimeric form in tumor cells. Some viral oncoproteins like HPV-16E7 and pp60v-Src kinase (12,13) as well as cellular phosphotyrosine signaling (14,15) can induce the dimerization of PKM2, but the Ras oncogene induces the tetramerization of PKM2 (16,17). Recently, Kosugi et al (18) found that PKM2 activity is also regulated by direct binding of oncoprotein MUC1-C. Another important metabolic regulator of PKM2 is fructose 1,6-bisphosphate.…”

Section: Introductionmentioning

confidence: 99%

“…High level of this glycolytic intermediate reflects sufficient amounts of phosphor-metabolites and induces reassociation of the dimeric form of PKM2 to the highly active tetrameric form, thus shifting tumor metabolism from synthesis of cell building blocks to energy regeneration (12). So it is believed that PKM2 plays a key role in the channeling of glucose carbons either into catabolic or into anabolic pathways [14,15]. But not all of the tumors express PKM2 only; there might be different expressing patterns and roles of PKM2 in different tumors (19,20).…”

Section: Introductionmentioning

confidence: 99%

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Pyruvate kinase type M2 is upregulated in colorectal cancer and promotes proliferation and migration of colon cancer cells

Zhou

Sun

et al. 2012

IUBMB Life

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SummaryPyruvate kinase type M2 (PKM2) has been reported to be involved in aerobic glycolysis and cell growth in various tumors. However, the expression pattern of PKM2 in colorectal cancer (CRC) and the correlation between PKM2 expression and CRC remains unclear. The aim of this study is to investigate PKM2 expression and its possible role in CRC. We found that expression of PKM2 was increased in CRC and the increased PKM2 expression was associated with later stage and lymph metastasis of the tumors. Knockdown of PKM2 suppressed the aerobic glycolysis and decreased lactate production of colon cancer RKO cells. Knockdown of PKM2 repressed proliferation and migration of the cells. Inhibition of PKM2 suppressed xenograft tumor growth of RKO cells in vivo. These results suggest that the expression of PKM2 plays a critical role in development of CRC, and it may provide a growth advantage for colon cancer cells. Thus, PKM2 might be a potential therapeutic target for CRC.2012 IUBMB IUBMB Life, 64(9): 775-782, 2012

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Pyruvate kinase type M2 is upregulated in colorectal cancer and promotes proliferation and migration of colon cancer cells

Zhou

Sun

et al. 2012

IUBMB Life

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“…I Mor et al phosphorylation of tyrosine residues and proteinprotein interactions, are inhibitory (Hitosugi et al, 2009;Mazurek, 2011). The M2 isoform is expressed during embryonic development and is turned off in adult somatic cells (Hitosugi et al, 2009;Mazurek, 2011).…”

Section: Dapk Regulates Cell Metabolism Through Pkm2mentioning

confidence: 99%

“…The M2 isoform is expressed during embryonic development and is turned off in adult somatic cells (Hitosugi et al, 2009;Mazurek, 2011). A switch in the alternative splicing pattern leads to re-expression of the PKM2 during cancerous transformation and as a consequence, this isoform is almost ubiquitously expressed in tumors and proliferating cell lines (Clower et al, 2010;David et al, 2010).…”

Section: Dapk Regulates Cell Metabolism Through Pkm2mentioning

confidence: 99%

Death-associated protein kinase increases glycolytic rate through binding and activation of pyruvate kinase

et al. 2011

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Death-associated protein kinase (DAPk), a multi-domain serine/threonine kinase, regulates numerous cell death mechanisms and harbors tumor suppressor functions. In this study, we report that DAPk directly binds and functionally activates pyruvate kinase M2 (PKM2), a key glycolytic enzyme, which contributes to the regulation of cancer cell metabolism. PKM2 was identified as a novel binding partner of DAPk by a yeast two-hybrid screen. This interaction was validated in vitro by enzyme-linked immunosorbent assay using purified proteins and in vivo by co-immunoprecipitation of the two endogenous proteins from cells. In vitro interaction with full-length DAPk resulted in a significant increase in the activity of PKM2. Conversely, a fragment of DAPk harboring only the functional kinase domain (KD) could neither bind PKM2 in cells nor activate it in vitro. Indeed, DAPk failed to phosphorylate PKM2. Notably, transfection of cells, with a truncated DAPk lacking the KD, elevated endogenous PKM2 activity, suggesting that PKM2 activation by DAPk occurs independently of its kinase activity. DAPk-transfected cells displayed changes in glycolytic activity, as reflected by elevated lactate production, whereas glucose uptake remained unaltered. A mild reduction in cell proliferation was detected as well in these transfected cells. Altogether, this work identifies a new role for DAPk as a metabolic regulator, suggesting the concept of direct interactions between a tumor suppressor and a key glycolytic enzyme to limit cell growth. Moreover, the work documents a unique function of DAPk that is independent of its catalytic activity and a novel mechanism to activate PKM2 by protein-protein interaction.

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Cancer‐associated mutations in human pyruvate kinase M2 impair enzyme activity

et al. 2019

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Mammalian pyruvate kinase catalyzes the final step of glycolysis, and its M2 isoform (PKM2) is widely expressed in proliferative tissues. Mutations in PKM2 are found in some human cancers; however, the effects of these mutations on enzyme activity and regulation are unknown. Here, we characterized five cancer‐associated PKM2 mutations, occurring at various locations on the enzyme, with respect to substrate kinetics and activation by the allosteric activator fructose‐1,6‐bisphosphate (FBP). The mutants exhibit reduced maximal velocity, reduced substrate affinity, and/or altered activation by FBP. The kinetic parameters of five additional PKM2 mutants that have been used to study enzyme function or regulation also demonstrate the deleterious effects of mutations on PKM2 function. Our findings indicate that PKM2 is sensitive to many amino acid changes and support the hypothesis that decreased PKM2 activity is selected for in rapidly proliferating cells.

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Tyrosine Phosphorylation Inhibits PKM2 to Promote the Warburg Effect and Tumor Growth

Cited by 673 publications

References 24 publications

Pyruvate kinase type M2 is upregulated in colorectal cancer and promotes proliferation and migration of colon cancer cells

Pyruvate kinase type M2 is upregulated in colorectal cancer and promotes proliferation and migration of colon cancer cells

Death-associated protein kinase increases glycolytic rate through binding and activation of pyruvate kinase

Cancer‐associated mutations in human pyruvate kinase M2 impair enzyme activity

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