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Myeloid Slc2a1-Deficient Murine Model Revealed Macrophage Activation and Metabolic Phenotype Are Fueled by GLUT1
Alex J. Freemerman ,
Liyang Zhao ,
Ajeeth K. Pingili ,
Bin Teng ,
Alyssa J. Cozzo ,
Ashley M. Fuller ,
Amy R. Johnson ,
J. Justin Milner ,
Maili F. Lim ,
Joseph A. Galanko ,
Melinda A. Beck ,
James E. Bear ,
Jeremy D. Rotty ,
Lavanya Bezavada ,
Heather S. Smallwood ,
Michelle A. Puchowicz ,
Juan Liu ,
Jason W. Locasale ,
Douglas P. Lee ,
Brian J. Bennett ,
E. Dale Abel ,
Jeff C. Rathmell ,
Liza Makowski
February 04 2019
January 18 2019
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Abstract
<p class="first" id="d1348940e336">Macrophages (MΦs) are heterogeneous and metabolically
flexible, with metabolism strongly
affecting immune activation. A classic response to proinflammatory activation is increased
flux through glycolysis with a downregulation of oxidative metabolism, whereas alternative
activation is primarily oxidative, which begs the question of whether targeting glucose
metabolism is a viable approach to control MΦ activation. We created a murine model
of myeloid-specific glucose transporter GLUT1 (Slc2a1) deletion. Bone marrow-derived
MΦs (BMDM) from Slc2a1M-/- mice failed to uptake glucose and demonstrated reduced
glycolysis and pentose phosphate pathway activity. Activated BMDMs displayed elevated
metabolism of oleate and glutamine, yet maximal respiratory capacity was blunted in
MΦ lacking GLUT1, demonstrating an incomplete metabolic reprogramming. Slc2a1M-/-
BMDMs displayed a mixed inflammatory phenotype with reductions of the classically
activated pro- and anti-inflammatory markers, yet less oxidative stress. Slc2a1M-/-
BMDMs had reduced proinflammatory metabolites, whereas metabolites indicative of alternative
activation-such as ornithine and polyamines-were greatly elevated in the absence of
GLUT1. Adipose tissue MΦs of lean Slc2a1M-/- mice had increased alternative M2-like
activation marker mannose receptor CD206, yet lack of GLUT1 was not a critical mediator
in the development of obesity-associated metabolic dysregulation. However, Ldlr-/-
mice lacking myeloid GLUT1 developed unstable atherosclerotic lesions. Defective phagocytic
capacity in Slc2a1M-/- BMDMs may have contributed to unstable atheroma formation.
Together, our findings suggest that although lack of GLUT1 blunted glycolysis and
the pentose phosphate pathway, MΦ were metabolically flexible enough that inflammatory
cytokine release was not dramatically regulated, yet phagocytic defects hindered MΦ
function in chronic diseases.
</p>