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Publication : Cell-intrinsic lysosomal lipolysis is essential for alternative activation of macrophages.

First Author  Huang SC Year  2014
Journal  Nat Immunol Volume  15
Issue  9 Pages  846-55
PubMed ID  25086775 Mgi Jnum  J:259371
Mgi Id  MGI:6142764 Doi  10.1038/ni.2956
Citation  Huang SC, et al. (2014) Cell-intrinsic lysosomal lipolysis is essential for alternative activation of macrophages. Nat Immunol 15(9):846-55
abstractText  Alternative (M2) activation of macrophages driven via the alpha-chain of the receptor for interleukin 4 (IL-4Ralpha) is important for immunity to parasites, wound healing, the prevention of atherosclerosis and metabolic homeostasis. M2 polarization is dependent on fatty acid oxidation (FAO), but the source of the fatty acids that support this metabolic program has not been clear. We found that the uptake of triacylglycerol substrates via the scavenger receptor CD36 and their subsequent lipolysis by lysosomal acid lipase (LAL) was important for the engagement of elevated oxidative phosphorylation, enhanced spare respiratory capacity (SRC), prolonged survival and expression of genes that together define M2 activation. Inhibition of lipolysis suppressed M2 activation during infection with a parasitic helminth and blocked protective responses to this pathogen. Our findings delineate a critical role for cell-intrinsic lysosomal lipolysis in M2 activation.
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