| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 3258920 | Clinical Immunology | 2006 | 8 Pages |
Nitric oxide (NO) production increases with age in the lupus-prone MRL/lpr mouse, paralleling disease activity. One mechanism for excess NO production in MRL/lpr mice may be a defect in down-regulatory mechanisms of the iNOS pathway. A potential modulator of NO is the nuclear hormone receptor peroxisome proliferation activated receptor gamma (PPARγ). We demonstrate that renal PPARγ protein expression was altered as disease progressed in MRL/lpr mice, which paralleled increased iNOS protein expression. Additionally, MRL/lpr-derived primary mesangial cells expressed less PPARγ than BALB/c mesangial cells and produced more NO in response to LPS and IFNγ. Furthermore, PPARγ activity was reduced in mesangial cells following exposure to inflammatory mediators. This activity was restored with the addition of a NOS enzyme inhibitor. These results indicate that the activation of inflammatory pathways may lead to reduced activity and expression of PPARγ, further exacerbating the disease state.
