Autophagy-Dependent Generation of Free Fatty Acids Is Critical for Normal Neutrophil Differentiation

自噬依赖的游离脂肪酸生成对正常中性粒细胞分化至关重要

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作者:Thomas Riffelmacher ,Alexander Clarke ,Felix C Richter ,Amanda Stranks ,Sumeet Pandey ,Sara Danielli ,Philip Hublitz ,Zhanru Yu ,Errin Johnson ,Tobias Schwerd ,James McCullagh ,Holm Uhlig ,Sten Eirik W Jacobsen ,Anna Katharina Simon

Abstract

Neutrophils are critical and short-lived mediators of innate immunity that require constant replenishment. Their differentiation in the bone marrow requires extensive cytoplasmic and nuclear remodeling, but the processes governing these energy-consuming changes are unknown. While previous studies show that autophagy is required for differentiation of other blood cell lineages, its function during granulopoiesis has remained elusive. Here, we have shown that metabolism and autophagy are developmentally programmed and essential for neutrophil differentiation in vivo. Atg7-deficient neutrophil precursors had increased glycolytic activity but impaired mitochondrial respiration, decreased ATP production, and accumulated lipid droplets. Inhibiting autophagy-mediated lipid degradation or fatty acid oxidation alone was sufficient to cause defective differentiation, while administration of fatty acids or pyruvate for mitochondrial respiration rescued differentiation in autophagy-deficient neutrophil precursors. Together, we show that autophagy-mediated lipolysis provides free fatty acids to support a mitochondrial respiration pathway essential to neutrophil differentiation.

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