A PKM2 signature in the failing heart

Meredith L. Rees; Janani Subramaniam; Yuanteng Li; Dale J. Hamilton; O. Howard Frazier; Heinrich Taegtmeyer

doi:10.1016/j.bbrc.2015.02.122

A PKM2 signature in the failing heart

Meredith L. Rees, Janani Subramaniam, Yuanteng Li, Dale J. Hamilton, O. Howard Frazier, Heinrich Taegtmeyer

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

71 Scopus citations

Abstract

A salient feature of the failing heart is metabolic remodeling towards predominant glucose metabolism and activation of the fetal gene program. Sunitinib is a multitargeted receptor tyrosine kinase inhibitor used for the treatment of highly vascularized tumors. In diabetic patients, sunitinib significantly decreases blood glucose. However, a considerable proportion of sunitinib-treated patients develop cardiac dysfunction or failure. We asked whether sunitinib treatment results in shift towards glycolysis in the heart. Glucose uptake by the heart was increased fivefold in mice treated with sunitinib. Transcript analysis by qPCR revealed an induction of genes associated with glycolysis and reactivation of the fetal gene program. Additionally, we observed a shift in the enzyme pyruvate kinase from the adult M1 (PKM1) isoform to the fetal M2 (PKM2) isoform, a hallmark of the Warburg Effect. This novel observation led us to examine whether a similar shift occurs in human heart failure. Examination of tissue from patients with heart failure similarly displayed an induction of PKM2. Moreover, this phenomenon was partially reversed following mechanical unloading. We propose that pyruvate kinase isoform switching represents a novel feature of the fetal gene program in the failing heart.

Original language	English (US)
Pages (from-to)	430-436
Number of pages	7
Journal	Biochemical and Biophysical Research Communications
Volume	459
Issue number	3
DOIs	https://doi.org/10.1016/j.bbrc.2015.02.122
State	Published - Apr 10 2015

Keywords

Fetal gene program
Glycolysis
Heart failure
Hif1α
PKM2
Sunitinib

ASJC Scopus subject areas

Biophysics
Biochemistry
Molecular Biology
Cell Biology

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10.1016/j.bbrc.2015.02.122

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title = "A PKM2 signature in the failing heart",

abstract = "A salient feature of the failing heart is metabolic remodeling towards predominant glucose metabolism and activation of the fetal gene program. Sunitinib is a multitargeted receptor tyrosine kinase inhibitor used for the treatment of highly vascularized tumors. In diabetic patients, sunitinib significantly decreases blood glucose. However, a considerable proportion of sunitinib-treated patients develop cardiac dysfunction or failure. We asked whether sunitinib treatment results in shift towards glycolysis in the heart. Glucose uptake by the heart was increased fivefold in mice treated with sunitinib. Transcript analysis by qPCR revealed an induction of genes associated with glycolysis and reactivation of the fetal gene program. Additionally, we observed a shift in the enzyme pyruvate kinase from the adult M1 (PKM1) isoform to the fetal M2 (PKM2) isoform, a hallmark of the Warburg Effect. This novel observation led us to examine whether a similar shift occurs in human heart failure. Examination of tissue from patients with heart failure similarly displayed an induction of PKM2. Moreover, this phenomenon was partially reversed following mechanical unloading. We propose that pyruvate kinase isoform switching represents a novel feature of the fetal gene program in the failing heart.",

keywords = "Fetal gene program, Glycolysis, Heart failure, Hif1α, PKM2, Sunitinib",

author = "Rees, {Meredith L.} and Janani Subramaniam and Yuanteng Li and Hamilton, {Dale J.} and Frazier, {O. Howard} and Heinrich Taegtmeyer",

note = "Funding Information: We thank Dr. Mark Entman for his help with the manuscript preparation. We also thank Drs. Pradip Saha and Lawrence Chan of the Mouse Metabolism Core at Baylor College of Medicine for aiding with the hyperinsulinemic euglycemic clamp studies; Dr. Hernan Vasquez and Sylvia Carranza for collection of the failing human heart samples; Dr. Keith Youker for the collection of the non-failing human heart samples and Drs. Anren Song and Yang Xia for help with the Hif1α experiments. These studies were supported in part by a grant from the National Heart, Lung, and Blood Institute ( 5R01HL061483-10 ). M.L.R. received a predoctoral fellowship from the National Center for Advancing Translational Sciences of the National Institutes of Health under Award Numbers TL1TR000369 and UL1TR000371 . ",

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AU - Li, Yuanteng

AU - Hamilton, Dale J.

AU - Frazier, O. Howard

AU - Taegtmeyer, Heinrich

N1 - Funding Information: We thank Dr. Mark Entman for his help with the manuscript preparation. We also thank Drs. Pradip Saha and Lawrence Chan of the Mouse Metabolism Core at Baylor College of Medicine for aiding with the hyperinsulinemic euglycemic clamp studies; Dr. Hernan Vasquez and Sylvia Carranza for collection of the failing human heart samples; Dr. Keith Youker for the collection of the non-failing human heart samples and Drs. Anren Song and Yang Xia for help with the Hif1α experiments. These studies were supported in part by a grant from the National Heart, Lung, and Blood Institute ( 5R01HL061483-10 ). M.L.R. received a predoctoral fellowship from the National Center for Advancing Translational Sciences of the National Institutes of Health under Award Numbers TL1TR000369 and UL1TR000371 .

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AB - A salient feature of the failing heart is metabolic remodeling towards predominant glucose metabolism and activation of the fetal gene program. Sunitinib is a multitargeted receptor tyrosine kinase inhibitor used for the treatment of highly vascularized tumors. In diabetic patients, sunitinib significantly decreases blood glucose. However, a considerable proportion of sunitinib-treated patients develop cardiac dysfunction or failure. We asked whether sunitinib treatment results in shift towards glycolysis in the heart. Glucose uptake by the heart was increased fivefold in mice treated with sunitinib. Transcript analysis by qPCR revealed an induction of genes associated with glycolysis and reactivation of the fetal gene program. Additionally, we observed a shift in the enzyme pyruvate kinase from the adult M1 (PKM1) isoform to the fetal M2 (PKM2) isoform, a hallmark of the Warburg Effect. This novel observation led us to examine whether a similar shift occurs in human heart failure. Examination of tissue from patients with heart failure similarly displayed an induction of PKM2. Moreover, this phenomenon was partially reversed following mechanical unloading. We propose that pyruvate kinase isoform switching represents a novel feature of the fetal gene program in the failing heart.

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A PKM2 signature in the failing heart

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