Department of Internal Medicine, University of Michigan, Ann Arbor, 48109-0644, USA.
Circ Res. 2010 Aug 6;107(3):388-97. doi: 10.1161/CIRCRESAHA.110.218651. Epub 2010 Jun 17.
Adhesive interactions between endothelial cells and leukocytes affect leukocyte trafficking in adipose tissue. The role of P-selectin glycoprotein ligand-1 (Psgl-1) in this process is unclear.
The goal of this study was to determine the effect of Psgl-1 deficiency on adhesive properties of the endothelium and on leukocyte recruitment into obese adipose depots.
A genetic model of obesity was generated to study the effects of Psgl-1 deficiency on leukocyte trafficking. Leukocyte-endothelial interactions were increased in obese leptin receptor mutant mice (Lepr(db/db),Psgl-1(+/+)) but not obese Psgl-1-deficient mice (Lepr(db/db),Psgl-1(-/-)), when compared with lean mice (Lepr(+/+),Psgl-1(+/+)). This effect of Psgl-1 deficiency was due to indirect effects of Psgl-1, because Psgl-1(+/+) adoptively transferred leukocytes did not exhibit enhanced rolling in Lepr (db/db),Psgl-1(-/-) mice. Additionally, circulating levels of P-selectin, E-selectin, monocyte chemoattractant protein-1, and macrophage content of visceral adipose tissue were reduced in Lepr(db/db),Psgl-1(-/-) compared with Lepr(db/db),Psgl-1(+/+) mice. Reduced leukocyte-endothelial interactions and macrophage content of visceral adipose tissue due to Psgl-1 deficiency was also observed in a diet-induced obese mouse model. Psgl-1(-/-) mice were resistant to the endothelial effects of exogenous IL-1beta, suggesting that defective cytokine signaling contributes to the effect of Psgl-1 deficiency on leukocyte-endothelial interactions. Mice deficient in the IL-1 receptor also had reduced levels of circulating P-selectin, similar to those observed in Psgl-1(-/-) mice.
Deficiency of Psgl-1 is associated with reduced IL-1 receptor-mediated adhesive properties of the endothelium and is protective against visceral fat inflammation in obese mice.
内皮细胞与白细胞之间的黏附相互作用会影响白细胞在脂肪组织中的迁移。P-选择素糖蛋白配体-1(Psgl-1)在此过程中的作用尚不清楚。
本研究旨在确定 Psgl-1 缺乏对内皮细胞黏附特性以及肥胖脂肪组织中白细胞募集的影响。
构建了肥胖的遗传模型,以研究 Psgl-1 缺乏对白细胞迁移的影响。与瘦鼠(Lepr(+/+),Psgl-1(+/+))相比,肥胖瘦素受体突变小鼠(Lepr(db/db),Psgl-1(+/+))的白细胞-内皮细胞相互作用增加,但肥胖 Psgl-1 缺陷小鼠(Lepr(db/db),Psgl-1(-/-))则不然。Psgl-1 缺乏的这种作用归因于 Psgl-1 的间接作用,因为 Psgl-1(+/+)过继转移的白细胞在 Lepr(db/db),Psgl-1(-/-)小鼠中没有表现出增强的滚动。此外,与 Lepr(db/db),Psgl-1(+/+)小鼠相比,Lepr(db/db),Psgl-1(-/-)小鼠的循环 P-选择素、E-选择素、单核细胞趋化蛋白-1和内脏脂肪组织中巨噬细胞含量降低。由于 Psgl-1 缺乏,在饮食诱导的肥胖小鼠模型中也观察到白细胞-内皮细胞相互作用和内脏脂肪组织中巨噬细胞含量减少。Psgl-1(-/-) 小鼠对内源 IL-1β的内皮作用具有抗性,表明细胞因子信号转导缺陷导致 Psgl-1 缺乏对白细胞-内皮细胞相互作用的影响。IL-1 受体缺陷小鼠的循环 P-选择素水平也降低,与 Psgl-1(-/-)小鼠相似。
Psgl-1 缺乏与 IL-1 受体介导的内皮黏附特性降低有关,并可防止肥胖小鼠的内脏脂肪炎症。