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Publication : Autophagy deficiency in myeloid cells increases susceptibility to obesity-induced diabetes and experimental colitis.

First Author  Lee HY Year  2016
Journal  Autophagy Volume  12
Issue  8 Pages  1390-403
PubMed ID  27337687 Mgi Jnum  J:325823
Mgi Id  MGI:6873419 Doi  10.1080/15548627.2016.1184799
Citation  Lee HY, et al. (2016) Autophagy deficiency in myeloid cells increases susceptibility to obesity-induced diabetes and experimental colitis. Autophagy 12(8):1390-403
abstractText  Autophagy, which is critical for the proper turnover of organelles such as endoplasmic reticulum and mitochondria, affects diverse aspects of metabolism, and its dysregulation has been incriminated in various metabolic disorders. However, the role of autophagy of myeloid cells in adipose tissue inflammation and type 2 diabetes has not been addressed. We produced mice with myeloid cell-specific deletion of Atg7 (autophagy-related 7), an essential autophagy gene (Atg7 conditional knockout [cKO] mice). While Atg7 cKO mice were metabolically indistinguishable from control mice, they developed diabetes when bred to ob/w mice (Atg7 cKO-ob/ob mice), accompanied by increases in the crown-like structure, inflammatory cytokine expression and inflammasome activation in adipose tissue. Mphis (macrophages) from Atg7 cKO mice showed significantly higher interleukin 1 beta release and inflammasome activation in response to a palmitic acid plus lipopolysaccharide combination. Moreover, a decrease in the NAD(+):NADH ratio and increase in intracellular ROS content after treatment with palmitic acid in combination with lipopolysaccharide were more pronounced in Mphis from Atg7 cKO mice, suggesting that mitochondrial dysfunction in autophagy-deficient Mphis leads to an increase in lipid-induced inflammasome and metabolic deterioration in Atg7 cKO-ob/ob mice. Atg7 cKO mice were more susceptible to experimental colitis, accompanied by increased colonic cytokine expression, T helper 1 skewing and systemic bacterial invasion. These results suggest that autophagy of Mphis is important for the control of inflammasome activation in response to metabolic or extrinsic stress, and autophagy deficiency in Mphis may contribute to the progression of metabolic syndrome associated with lipid injury and colitis.
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