Requirement of toll‐like receptor 7 for pristane‐induced production of autoantibodies and development of murine lupus nephritis

Savarese, Emina; Steinberg, Christian; Pawar, Rahul D.; Reindl, Wolfgang; Akira, Shizuo; Anders, Hans‐Joachim; Krug, Anne

doi:10.1002/art.23407

Cited by 127 publications

(118 citation statements)

References 29 publications

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“…STING-deficient MRL/lpr mice develop a dramatically accelerated disease profile characterized by the expansion and activation of both the lymphoid and myeloid compartments, increased numbers of type I IFN-producing cells, elevated autoantibody titers, and a shorter lifespan. Similar to our findings in the MRL/lpr model, STING deficiency exacerbated TMPD-induced inflammation, a condition also associated with type I IFNs and TLR-activated Ly6C hi monocytes (24,26). Nonautoimmune-prone STING-deficient mice do not exhibit any evidence of systemic autoimmunity.…”

Section: Discussionsupporting

confidence: 88%

“…These features include a type I IFN signature, ANAs, and glomerulonephritis (24,25). Importantly, TMPD-induced autoimmunity is dependent upon TLR7 and type I IFNs (26). Pristane injection of C57/Bl6 mice results in an early and persistent peritoneal inflammation and the recruitment of TLR7 hi Ly6C hi monocytes, a potential source of type I IFNs, in this model (25).…”

Section: Sting Deficiency Results In the Increased Expression Of Ifn-mentioning

confidence: 84%

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Suppression of systemic autoimmunity by the innate immune adaptor STING

Sharma

Campbell

Chan

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

147

139

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Cytosolic DNA-sensing pathways that signal via Stimulator of interferon genes (STING) mediate immunity to pathogens and also promote autoimmune pathology in DNaseII- and DNaseIII-deficient mice. In contrast, we report here that STING potently suppresses inflammation in a model of systemic lupus erythematosus (SLE). Lymphoid hypertrophy, autoantibody production, serum cytokine levels, and other indicators of immune activation were markedly increased in STING-deficient autoimmune-prone mice compared with STING-sufficient littermates. As a result, STING-deficient autoimmune-prone mice had significantly shorter lifespans than controls. Importantly, Toll-like receptor (TLR)-dependent systemic inflammation during 2,6,10,14-tetramethylpentadecane (TMPD)-mediated peritonitis was similarly aggravated in STING-deficient mice. Mechanistically, STING-deficient macrophages failed to express negative regulators of immune activation and thus were hyperresponsive to TLR ligands, producing abnormally high levels of proinflammatory cytokines. This hyperreactivity corresponds to dramatically elevated numbers of inflammatory macrophages and granulocytes in vivo. Collectively these findings reveal an unexpected negative regulatory role for STING, having important implications for STING-directed therapies.

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Section: Discussionsupporting

confidence: 88%

Section: Sting Deficiency Results In the Increased Expression Of Ifn-mentioning

confidence: 84%

Suppression of systemic autoimmunity by the innate immune adaptor STING

Sharma

Campbell

Chan

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

147

139

View full text Add to dashboard Cite

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“…In addition, Christensen, et al [6] showed that lupus nephritis takes a significantly milder course in Tlr7-deficient MRLlpr/lpr mice. This was confirmed in pristane-induced lupus nephritis in C57BL/6 mice [8]. Both studies also observed a significant reduction in the plasma levels of IgG2a/2c isotype antibodies in Tlr7-deficient mice mice [6,8].…”

Section: See Accompanying Article By Fairhurst Et Almentioning

confidence: 53%

“…Both studies also observed a significant reduction in the plasma levels of IgG2a/2c isotype antibodies in Tlr7-deficient mice mice [6,8]. Lack of Tlr7 in MRLlpr/lpr mice was associated with a general reduction in immune activation affecting the proliferation and activation of splenic B and T lymphocytes [6], which was not observed in pristane-induced lupus in C57BL/6 mice [8].…”

Section: See Accompanying Article By Fairhurst Et Almentioning

confidence: 85%

“…In all three models studied so far, the MRLlpr/lpr mice and the 564 immunoglobulin transgenic mice, which develop lupus spontaneously, as well as the pristaneinduced lupus model, production of class switched autoantibodies recognizing the RNA-containing antigens snRNP, Sm, and ssRNA was specifically abrogated in the absence of Tlr7 [6][7][8]. In contrast the production of anti-chromatin and anti-dsDNA antibodies was found to be independent of Tlr7 in these models [6,8]. These results demonstrate an essential and specific function of Tlr7 for the generation of high affinity RNA-reactive autoantibodies in murine lupus.…”

Section: See Accompanying Article By Fairhurst Et Almentioning

confidence: 97%

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Molecular mimicry in innate immunity? The viral RNA recognition receptor TLR7 accelerates murine lupus

2008

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Toll-like receptors (TLR), such as TLR7, were first described as innate pathogen recognition receptors that trigger appropriate antimircrobial immune responses upon exposure to pathogen-associated molecules, e.g. viral ssRNA. In parallel to ongoing studies on TLRbiology, mounting experimental evidence suggests that endogenous RNA-related autoantigens may also activate dendritic cells (DC) and B cells through TLR7. TLR7-mediated DC activation, autoantibody secretion, lymphoproliferation, and autoimmune tissue injury, are frequently observed in various murine models of systemic lupus and lupus nephritis. A paper in the current issue of the European Journal of Immunology, provide striking experimental evidence for this concept; the authors show that the Y chromosome-linked autoimmune accelerating (Yaa) translocation from the X-chromosome, consisting of 16 genes including Tlr7, largely mediates the autoimmune phenotype via the duplication of Tlr7. This finding highlights the need to address the significance of TLR7 in human lupus in terms of both genetic risk and as a therapeutic option.

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Chemically Induced Autoimmunity

Schiraldi

Monestier

2009

Endogenous Toxins

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Requirement of toll‐like receptor 7 for pristane‐induced production of autoantibodies and development of murine lupus nephritis

Cited by 127 publications

References 29 publications

Suppression of systemic autoimmunity by the innate immune adaptor STING

Suppression of systemic autoimmunity by the innate immune adaptor STING

Molecular mimicry in innate immunity? The viral RNA recognition receptor TLR7 accelerates murine lupus

Chemically Induced Autoimmunity

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