Bim suppresses the development of SLE by limiting myeloid inflammatory responses.
FuNien TsaiPhilip J HomanHemant AgrawalAlexander V MisharinHiam Abdala-ValenciaG Kenneth HainesSalina DominguezChristina L BloomfieldRana SaberAnthony ChangChandra MohanJack HutchesonAnne DavidsonG R Scott BudingerPhilippe BouilletAndrea DorfleutnerChristian StehlikDeborah R WinterCarla M CudaHarris R PerlmanPublished in: The Journal of experimental medicine (2017)
The Bcl-2 family is considered the guardian of the mitochondrial apoptotic pathway. We demonstrate that Bim acts as a molecular rheostat by controlling macrophage function not only in lymphoid organs but also in end organs, thereby preventing the break in tolerance. Mice lacking Bim in myeloid cells (LysMCreBimfl/fl) develop a systemic lupus erythematosus (SLE)-like disease that mirrors aged Bim-/- mice, including loss of marginal zone macrophages, splenomegaly, lymphadenopathy, autoantibodies (including anti-DNA IgG), and a type I interferon signature. LysMCreBimfl/fl mice exhibit increased mortality attributed to glomerulonephritis (GN). Moreover, the toll-like receptor signaling adaptor protein TRIF (TIR-domain-containing adapter-inducing interferon-β) is essential for GN, but not systemic autoimmunity in LysMCreBimfl/fl mice. Bim-deleted kidney macrophages exhibit a novel transcriptional lupus signature that is conserved within the gene expression profiles from whole kidney biopsies of patients with SLE. Collectively, these data suggest that the Bim may be a novel therapeutic target in the treatment of SLE.
Keyphrases
- systemic lupus erythematosus
- disease activity
- toll like receptor
- high fat diet induced
- dendritic cells
- rheumatoid arthritis
- acute myeloid leukemia
- inflammatory response
- gene expression
- insulin resistance
- type diabetes
- adipose tissue
- wild type
- nuclear factor
- skeletal muscle
- metabolic syndrome
- genome wide
- risk factors
- single molecule
- cardiovascular disease
- cell proliferation
- machine learning
- drug induced