Elevated levels of endogenous apoptotic DNA and IFN‐α in complement C4‐deficient mice: Implications for induction of systemic lupus erythematosus

Finke, Doreen; Randers, Katharina; Hoerster, Robert; Hennig, Holger; Zawatzky, Rainer; Marion, Tony N.; Brockmann, Christian; Klempt-Giessing, Katja; Jacobsen, Katja Kemp; Kirchner, Holger; Goerg, Siegfried

doi:10.1002/eji.200636719

Cited by 13 publications

(6 citation statements)

References 64 publications

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“…ITGAM (CD11b) expression was shown to increase DNA fragmentation, a prerequisite for apoptosis, and the level of fragmented DNA is increased in intravascular cells, which induces interferon α in SLE mice 9. CD11b also induces tumour necrosis factor α10 and modulates the innate immune mechanism11 in patients with SLE.…”

Section: Discussionmentioning

confidence: 99%

ITGAM coding variant (rs1143679) influences the risk of renal disease, discoid rash and immunological manifestations in patients with systemic lupus erythematosus with European ancestry

Kim-Howard

Maiti

Anaya

et al. 2009

Annals of the Rheumatic Diseases

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Purpose-We hypothesized that the coding variant (R77H), rs1143679, within ITGAM could predict specific clinical manifestations associated with lupus.Method-To assess genetic association, 2366 lupus cases and 2931 unaffected controls with European ancestry were analyzed. Lupus patients were coded by the presence or absence of individual ACR criteria. Logistic regression and Pearson chi-square tests were used to assess statistical significance.Results-First, for overall case-control analysis, we detected highly significant (p=2.22×10 −21 , OR=1.73) association. Second, using case-only analysis we detected significant association with renal criteria (p=0.0003), discoid rash (p=0.02), and immunologic criteria (p=0.04). Third, we compared them with healthy controls, the association became stronger for renal (p=4.69×10 −22 , OR=2.15), discoid (p=1.77×10 −14 , OR=2.03), and immunologic (p=3.49×10 −22 , OR = 1.86) criteria. Risk allele frequency increased from 10.6% (controls) to 17.0% (lupus), 20.4% (renal), 18.1% (immunologic), and 19.5% (discoid).Conclusion-These results demonstrated a strong association between the risk allele (A) at rs1143679 and renal disease, discoid rash, and immunological manifestations of lupus.

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Section: Discussionmentioning

confidence: 99%

ITGAM coding variant (rs1143679) influences the risk of renal disease, discoid rash and immunological manifestations in patients with systemic lupus erythematosus with European ancestry

Kim-Howard

Maiti

Anaya

et al. 2009

Annals of the Rheumatic Diseases

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“…Indeed, the binding of complement to apoptotic and necrotic cells can lead to opsonization and phagocytosis by macrophages, which can also affect the amounts of DNA that can enter the circulation. These proteins may also bind directly to DNA and therefore modulate its extracellular trafficking [30–38]. Among these humoral factors, complement appears to play an important role in determining disease susceptibility as exemplified by the development of lupus in humans with hereditary deficiency of C1q and C4 as well as the corresponding murine models.…”

Section: The Role Of Cell Death In the Generation Of Extracellular Dnamentioning

confidence: 99%

The Role of Extracellular DNA in Autoimmunity in SLE

Pisetsky

2009

Scand J Immunol

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Systemic lupus erythematosus (SLE) is a prototypic autoimmune disease characterized by the expression of antibodies to DNA. These antibodies form immune complexes that can stimulate cytokine production as well as deposit in the tissues to incite inflammation and damage. For the formation of immune complexes, the availability of extracellular DNA in an immunologically relevant form is essential. While apoptosis has been implicated as the source of this nuclear material in SLE, as shown with in vitro or in vivo systems, extracellular DNA can originate from apoptotic as well as necrotic cells. In experimental models, the release of DNA occurs with the administration of cells induced to die, in vitro as well as the administration of agents to induce cell death in situ. This release can be influenced by the presence of inflammatory cells such as macrophages that can interact with dead and dying cells to modulate the translocation of DNA from the inside to the outside of cells. In vivo, both glucocorticoids and oestrogens can modify the extent of DNA release from the administration of dead and dying cells. Together, these findings indicate that the generation of extracellular DNA in SLE can result from cell death and that steps in this process represent potential targets for new therapies.

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“…This could be a result of presentation of their cognate antigen in a tolerogenic environment, as it has been found that DCs induce immunity or tolerance depending solely upon their activation status . However, in the present study this explanation appears unlikely, given the established general proinflammatory environment in 564Igi mice , C4‐deficient mice , and 564Igi C4‐deficient mice in particular . Consequently, we speculate that it is an active dominant‐negative tolerance mechanism, mediated probably by forkhead box protein 3 (FoxP3) + regulatory T cells (T regs ).…”

Section: Discussionmentioning

confidence: 56%

B cell tolerance to epidermal ribonuclear-associated neo-autoantigenin vivo

Degn

Alicot

Carroll

2017

Clinical and Experimental Immunology

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Defining how self-antigens are perceived by the immune system is pivotal to understand how tolerance is maintained under homeostatic conditions. Clinically relevant, natural autoantigens targeted by autoantibodies, in e.g. systemic lupus erythematosus (SLE), commonly have an intrinsic ability to engage not only the B cell receptor (BCR), but also a co-stimulatory pathway in B cells, such as the Toll-like receptor (TLR)-7 pathway. Here we developed a novel mouse model displaying inducible expression of a fluorescent epidermal neo-autoantigen carrying an OT-II T cell epitope, B cell antigen and associated ribonucleic acids capable of stimulating TLR-7. The neo-autoantigen was expressed in skin, but did not drain in intact form into draining lymph nodes, even after ultraviolet B (UVB)-stimulated induction of apoptosis in the basal layer. Adoptively transferred autoreactive B cells were excluded follicularly and perished at the T-B border in the spleen, preventing their recirculation and encounter with antigen peripherally. This transitional check-point was bypassed by crossing the reporter to a BCR knock-in line on a C4-deficient background. Adoptively transferred OT-II T cells homed rapidly into cutaneous lymph nodes and up-regulated CD69. Surprisingly, however, tolerance was not broken, as the T cells subsequently down-regulated activation markers and contracted. Our results highlight how sequestration of intracellular and peripheral antigen, the transitional B cell tolerance check-point and T cell regulation co-operate to maintain immunological tolerance in vivo.

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Elevated levels of endogenous apoptotic DNA and IFN‐α in complement C4‐deficient mice: Implications for induction of systemic lupus erythematosus

Cited by 13 publications

References 64 publications

ITGAM coding variant (rs1143679) influences the risk of renal disease, discoid rash and immunological manifestations in patients with systemic lupus erythematosus with European ancestry

ITGAM coding variant (rs1143679) influences the risk of renal disease, discoid rash and immunological manifestations in patients with systemic lupus erythematosus with European ancestry

The Role of Extracellular DNA in Autoimmunity in SLE

B cell tolerance to epidermal ribonuclear-associated neo-autoantigenin vivo

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