Ketones and lactate "fuel" tumor growth and metastasis: Evidence that epithelial cancer cells use oxidative mitochondrial metabolism

Gloria Bonuccelli; Aristotelis Tsirigos; Diana Whitaker-Menezes; Stephanos Pavlides; Richard G. Pestell; Barbara Chiavarina; Philippe G. Frank; Neal Flomenberg; Anthony Howell; Ubaldo E. Martinez-Outschoorn; Federica Sotgia; Michael P. Lisanti

doi:10.4161/cc.9.17.12731

Ketones and lactate "fuel" tumor growth and metastasis: Evidence that epithelial cancer cells use oxidative mitochondrial metabolism

Gloria Bonuccelli, Aristotelis Tsirigos, Diana Whitaker-Menezes, Stephanos Pavlides, Richard G. Pestell, Barbara Chiavarina, Philippe G. Frank, Neal Flomenberg, Anthony Howell, Ubaldo E. Martinez-Outschoorn, Federica Sotgia, Michael P. Lisanti

Research output: Contribution to journal › Article › peer-review

Abstract

Previously, we proposed a new model for understanding the "Warburg effect" in tumor metabolism. In this scheme, cancer-associated fibroblasts undergo aerobic glycolysis and the resulting energy-rich metabolites are then transferred to epithelial cancer cells, where they enter the TCA cycle, resulting in high ATP production via oxidative phosphorylation. We have termed this new paradigm "The Reverse Warburg Effect." Here, we directly evaluate whether the end-products of aerobic glycolysis (3-hydroxy-butyrate and L-lactate) can stimulate tumor growth and metastasis, using MDA-MB-231 breast cancer xenografts as a model system. More specifically, we show that administration of 3-hydroxy-butyrate (a ketone body) increases tumor growth by ∼2.5-fold, without any measurable increases in tumor vascularization/ angiogenesis. Both 3-hydroxy-butyrate and L-lactate functioned as chemo-attractants, stimulating the migration of epithelial cancer cells. Although L-lactate did not increase primary tumor growth, it stimulated the formation of lung metastases by ∼10-fold. Thus, we conclude that ketones and lactate fuel tumor growth and metastasis, providing functional evidence to support the "Reverse Warburg Effect." Moreover, we discuss the possibility that it may be unwise to use lactate-containing i.v. solutions (such as Lactated Ringer's or Hartmann's solution) in cancer patients, given the dramatic metastasis-promoting properties of L-lactate. Also, we provide evidence for the up-regulation of oxidative mitochondrial metabolism and the TCA cycle in human breast cancer cells in vivo, via an informatics analysis of the existing raw transcriptional profiles of epithelial breast cancer cells and adjacent stromal cells. Lastly, our findings may explain why diabetic patients have an increased incidence of cancer, due to increased ketone production, and a tendency towards autophagy/mitophagy in their adipose tissue. © 2010 Landes Bioscience.

Original language	English
Pages (from-to)	3506-3514
Number of pages	8
Journal	Cell Cycle
Volume	9
Issue number	17
DOIs	https://doi.org/10.4161/cc.9.17.12731
Publication status	Published - 1 Sept 2010

Keywords

3-hydroxybutyrate (ketone bodies)
Aerobic glycolysis
Cancer associated fibroblasts
L-lactate
Metastasis
Stroma
The Warburg effect
Tumor growth
Tumor microenvironment

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.4161/cc.9.17.12731

http://www.landesbioscience.com/journals/cc/BonuccelliCC9-17.pdf

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Bonuccelli, G., Tsirigos, A., Whitaker-Menezes, D., Pavlides, S., Pestell, R. G., Chiavarina, B., Frank, P. G., Flomenberg, N., Howell, A., Martinez-Outschoorn, U. E., Sotgia, F., & Lisanti, M. P. (2010). Ketones and lactate "fuel" tumor growth and metastasis: Evidence that epithelial cancer cells use oxidative mitochondrial metabolism. Cell Cycle, 9(17), 3506-3514. https://doi.org/10.4161/cc.9.17.12731

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abstract = "Previously, we proposed a new model for understanding the {"}Warburg effect{"} in tumor metabolism. In this scheme, cancer-associated fibroblasts undergo aerobic glycolysis and the resulting energy-rich metabolites are then transferred to epithelial cancer cells, where they enter the TCA cycle, resulting in high ATP production via oxidative phosphorylation. We have termed this new paradigm {"}The Reverse Warburg Effect.{"} Here, we directly evaluate whether the end-products of aerobic glycolysis (3-hydroxy-butyrate and L-lactate) can stimulate tumor growth and metastasis, using MDA-MB-231 breast cancer xenografts as a model system. More specifically, we show that administration of 3-hydroxy-butyrate (a ketone body) increases tumor growth by ∼2.5-fold, without any measurable increases in tumor vascularization/ angiogenesis. Both 3-hydroxy-butyrate and L-lactate functioned as chemo-attractants, stimulating the migration of epithelial cancer cells. Although L-lactate did not increase primary tumor growth, it stimulated the formation of lung metastases by ∼10-fold. Thus, we conclude that ketones and lactate fuel tumor growth and metastasis, providing functional evidence to support the {"}Reverse Warburg Effect.{"} Moreover, we discuss the possibility that it may be unwise to use lactate-containing i.v. solutions (such as Lactated Ringer's or Hartmann's solution) in cancer patients, given the dramatic metastasis-promoting properties of L-lactate. Also, we provide evidence for the up-regulation of oxidative mitochondrial metabolism and the TCA cycle in human breast cancer cells in vivo, via an informatics analysis of the existing raw transcriptional profiles of epithelial breast cancer cells and adjacent stromal cells. Lastly, our findings may explain why diabetic patients have an increased incidence of cancer, due to increased ketone production, and a tendency towards autophagy/mitophagy in their adipose tissue. {\textcopyright} 2010 Landes Bioscience.",

keywords = "3-hydroxybutyrate (ketone bodies), Aerobic glycolysis, Cancer associated fibroblasts, L-lactate, Metastasis, Stroma, The Warburg effect, Tumor growth, Tumor microenvironment",

author = "Gloria Bonuccelli and Aristotelis Tsirigos and Diana Whitaker-Menezes and Stephanos Pavlides and Pestell, {Richard G.} and Barbara Chiavarina and Frank, {Philippe G.} and Neal Flomenberg and Anthony Howell and Martinez-Outschoorn, {Ubaldo E.} and Federica Sotgia and Lisanti, {Michael P.}",

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year = "2010",

month = sep,

day = "1",

doi = "10.4161/cc.9.17.12731",

language = "English",

volume = "9",

pages = "3506--3514",

journal = "Cell Cycle",

issn = "1538-4101",

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Bonuccelli, G, Tsirigos, A, Whitaker-Menezes, D, Pavlides, S, Pestell, RG, Chiavarina, B, Frank, PG, Flomenberg, N, Howell, A, Martinez-Outschoorn, UE, Sotgia, F & Lisanti, MP 2010, 'Ketones and lactate "fuel" tumor growth and metastasis: Evidence that epithelial cancer cells use oxidative mitochondrial metabolism', Cell Cycle, vol. 9, no. 17, pp. 3506-3514. https://doi.org/10.4161/cc.9.17.12731

TY - JOUR

T1 - Ketones and lactate "fuel" tumor growth and metastasis: Evidence that epithelial cancer cells use oxidative mitochondrial metabolism

AU - Bonuccelli, Gloria

AU - Tsirigos, Aristotelis

AU - Whitaker-Menezes, Diana

AU - Pavlides, Stephanos

AU - Pestell, Richard G.

AU - Chiavarina, Barbara

AU - Frank, Philippe G.

AU - Flomenberg, Neal

AU - Howell, Anthony

AU - Martinez-Outschoorn, Ubaldo E.

AU - Sotgia, Federica

AU - Lisanti, Michael P.

N1 - P30-CA-56036, NCI NIH HHS, United StatesR01-AR-055660, NIAMS NIH HHS, United StatesR01-CA-080250, NCI NIH HHS, United StatesR01-CA-098779, NCI NIH HHS, United StatesR01-CA-107382, NCI NIH HHS, United StatesR01-CA-120876, NCI NIH HHS, United StatesR01-CA-70896, NCI NIH HHS, United StatesR01-CA-75503, NCI NIH HHS, United StatesR01-CA-86072, NCI NIH HHS, United States

PY - 2010/9/1

Y1 - 2010/9/1

N2 - Previously, we proposed a new model for understanding the "Warburg effect" in tumor metabolism. In this scheme, cancer-associated fibroblasts undergo aerobic glycolysis and the resulting energy-rich metabolites are then transferred to epithelial cancer cells, where they enter the TCA cycle, resulting in high ATP production via oxidative phosphorylation. We have termed this new paradigm "The Reverse Warburg Effect." Here, we directly evaluate whether the end-products of aerobic glycolysis (3-hydroxy-butyrate and L-lactate) can stimulate tumor growth and metastasis, using MDA-MB-231 breast cancer xenografts as a model system. More specifically, we show that administration of 3-hydroxy-butyrate (a ketone body) increases tumor growth by ∼2.5-fold, without any measurable increases in tumor vascularization/ angiogenesis. Both 3-hydroxy-butyrate and L-lactate functioned as chemo-attractants, stimulating the migration of epithelial cancer cells. Although L-lactate did not increase primary tumor growth, it stimulated the formation of lung metastases by ∼10-fold. Thus, we conclude that ketones and lactate fuel tumor growth and metastasis, providing functional evidence to support the "Reverse Warburg Effect." Moreover, we discuss the possibility that it may be unwise to use lactate-containing i.v. solutions (such as Lactated Ringer's or Hartmann's solution) in cancer patients, given the dramatic metastasis-promoting properties of L-lactate. Also, we provide evidence for the up-regulation of oxidative mitochondrial metabolism and the TCA cycle in human breast cancer cells in vivo, via an informatics analysis of the existing raw transcriptional profiles of epithelial breast cancer cells and adjacent stromal cells. Lastly, our findings may explain why diabetic patients have an increased incidence of cancer, due to increased ketone production, and a tendency towards autophagy/mitophagy in their adipose tissue. © 2010 Landes Bioscience.

AB - Previously, we proposed a new model for understanding the "Warburg effect" in tumor metabolism. In this scheme, cancer-associated fibroblasts undergo aerobic glycolysis and the resulting energy-rich metabolites are then transferred to epithelial cancer cells, where they enter the TCA cycle, resulting in high ATP production via oxidative phosphorylation. We have termed this new paradigm "The Reverse Warburg Effect." Here, we directly evaluate whether the end-products of aerobic glycolysis (3-hydroxy-butyrate and L-lactate) can stimulate tumor growth and metastasis, using MDA-MB-231 breast cancer xenografts as a model system. More specifically, we show that administration of 3-hydroxy-butyrate (a ketone body) increases tumor growth by ∼2.5-fold, without any measurable increases in tumor vascularization/ angiogenesis. Both 3-hydroxy-butyrate and L-lactate functioned as chemo-attractants, stimulating the migration of epithelial cancer cells. Although L-lactate did not increase primary tumor growth, it stimulated the formation of lung metastases by ∼10-fold. Thus, we conclude that ketones and lactate fuel tumor growth and metastasis, providing functional evidence to support the "Reverse Warburg Effect." Moreover, we discuss the possibility that it may be unwise to use lactate-containing i.v. solutions (such as Lactated Ringer's or Hartmann's solution) in cancer patients, given the dramatic metastasis-promoting properties of L-lactate. Also, we provide evidence for the up-regulation of oxidative mitochondrial metabolism and the TCA cycle in human breast cancer cells in vivo, via an informatics analysis of the existing raw transcriptional profiles of epithelial breast cancer cells and adjacent stromal cells. Lastly, our findings may explain why diabetic patients have an increased incidence of cancer, due to increased ketone production, and a tendency towards autophagy/mitophagy in their adipose tissue. © 2010 Landes Bioscience.

KW - 3-hydroxybutyrate (ketone bodies)

KW - Aerobic glycolysis

KW - Cancer associated fibroblasts

KW - L-lactate

KW - Metastasis

KW - Stroma

KW - The Warburg effect

KW - Tumor growth

KW - Tumor microenvironment

U2 - 10.4161/cc.9.17.12731

DO - 10.4161/cc.9.17.12731

M3 - Article

C2 - 20818174

SN - 1538-4101

VL - 9

SP - 3506

EP - 3514

JO - Cell Cycle

JF - Cell Cycle

IS - 17

ER -

Ketones and lactate "fuel" tumor growth and metastasis: Evidence that epithelial cancer cells use oxidative mitochondrial metabolism

Abstract

Keywords

UN SDGs

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