Perilipin 1 (Plin1) deficiency promotes inflammatory responses in lean adipose tissue through lipid dysregulation

Perilipin 1 (Plin1) 缺乏会通过脂质失调促进瘦脂肪组织中的炎症反应

阅读：10

作者：Jee Hyung Sohn, Yun Kyung Lee, Ji Seul Han, Yong Geun Jeon, Jong In Kim, Sung Sik Choe, Su Jung Kim, Hyun Ju Yoo, Jae Bum Kim

期刊：

Journal of Biological Chemistry

影响因子：

4.000

时间：

2018

起止号：

2018 Sep 7;293(36):13974-13988.

doi：

10.1074/jbc.RA118.003541

研究方向：

免疫

Abstract

Lipid droplets are specialized cellular organelles that contain neutral lipid metabolites and play dynamic roles in energy homeostasis. Perilipin 1 (Plin1), one of the major lipid droplet-binding proteins, is highly expressed in adipocytes. In mice, Plin1 deficiency impairs peripheral insulin sensitivity, accompanied with reduced fat mass. However, the mechanisms underlying insulin resistance in lean Plin1 knockout (Plin1-/-) mice are largely unknown. The current study demonstrates that Plin1 deficiency promotes inflammatory responses and lipolysis in adipose tissue, resulting in insulin resistance. M1-type adipose tissue macrophages (ATMs) were higher in Plin1-/- than in Plin1+/+ mice on normal chow diet. Moreover, using lipidomics analysis, we discovered that Plin1-/- adipocytes promoted secretion of pro-inflammatory lipid metabolites such as prostaglandins, which potentiated monocyte migration. In lean Plin1-/- mice, insulin resistance was relieved by macrophage depletion with clodronate, implying that elevated pro-inflammatory ATMs might be attributable for insulin resistance under Plin1 deficiency. Together, these data suggest that Plin1 is required to restrain fat loss and pro-inflammatory responses in adipose tissue by reducing futile lipolysis to maintain metabolic homeostasis.

Perilipin 1 (Plin1) deficiency promotes inflammatory responses in lean adipose tissue through lipid dysregulation

Perilipin 1 (Plin1) 缺乏会通过脂质失调促进瘦脂肪组织中的炎症反应

Abstract

特别声明