Role of Nucleic Acid–Sensing TLRs in Diverse Autoantibody Specificities and Anti-Nuclear Antibody–Producing B Cells

Koh, Yi Ting; Scatizzi, John C.; Gahan, Jennifer D.; Lawson, Brian R.; Baccalà, Roberto; Pollard, K. Michael; Beutler, Bruce; Theofilopoulos, Argyrios N.; Kono, Dwight H.

doi:10.4049/jimmunol.1202986

Cited by 40 publications

(38 citation statements)

References 64 publications

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“…B cell MyD88 was needed to generate all antinuclear antibodies and a part of rheumatoid factor, whereas the contribution of dendritic cell MyD88 was less relevant. These data are in line with a study using Unc93b1(3d) lupusprone mice that lack signalling of all nucleic acidspecific TLRs in B cells [14]. Interestingly, lupus nephritis entirely depends on B cell MyD88, whereas dendritic cell MyD88 triggers dermatitis [13 As another interesting aspect, targeted TLR7 over-expression in B cells alone is sufficient to specifically trigger RNA autoantibody production followed by aggravated SLE [15].…”

Section: Cell Death and Dead Cell Clearancesupporting

confidence: 75%

Lupus nephritis

Lorenz

Desai

Anders

2014

Current Opinion in Nephrology and Hypertension

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Section: Cell Death and Dead Cell Clearancesupporting

confidence: 75%

Lupus nephritis

Lorenz

Desai

Anders

2014

Current Opinion in Nephrology and Hypertension

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“…This model addresses the potential epistatic interaction between TLRs and the lupus associated SLAM family genes in breaking the GC tolerance checkpoint. Recent studies have shown that the deficiency of nucleic acid sensing TLR signaling due to mutations in Unc93b1 is sufficient to interfere with the generation of ANAs (65, 66). Additionally, other pathogenic non-nuclear autoAb specificities including anti-cardiolipin, anti-RBC and anti-MPO, commonly found in SLE patients are also reduced by Unc93b1 mutations (65, 66).…”

Section: Discussionmentioning

confidence: 99%

“…Recent studies have shown that the deficiency of nucleic acid sensing TLR signaling due to mutations in Unc93b1 is sufficient to interfere with the generation of ANAs (65, 66). Additionally, other pathogenic non-nuclear autoAb specificities including anti-cardiolipin, anti-RBC and anti-MPO, commonly found in SLE patients are also reduced by Unc93b1 mutations (65, 66). Our work extends their observation and defines TLR7 as the key nucleic acid sensing TLR for the production of nuclear and non-nuclear antigen specific autoAbs.…”

Section: Discussionmentioning

confidence: 99%

B Cell–Intrinsic TLR7 Signaling Is Essential for the Development of Spontaneous Germinal Centers

Soni

Wong

Domeier

et al. 2014

The Journal of Immunology

138

146

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Spontaneous germinal center (Spt-GC) B cells and follicular helper T cells (Tfh) generate high affinity autoantibodies involved in the development of systemic lupus erythematosus (SLE). Toll like receptors (TLRs) play a pivotal role in SLE pathogenesis. While previous studies have focused on the B cell intrinsic role of TLR-MyD88 signaling on immune activation, autoantibody repertoire and systemic inflammation, a thorough investigation of the mechanisms by which TLRs control the formation of Spt-GCs remains unclear. Using non-autoimmune C57BL/6 (B6) mice deficient in MyD88, TLR2, 3, 4, 7 or 9, we identified B cell-intrinsic TLR7 signaling as a prerequisite to Spt-GC formation without the confounding effects of autoimmune susceptibility genes and the overexpression of TLRs. TLR7 deficiency also rendered autoimmune B6.Sle1b mice unable to form Spt-GCs, leading to markedly decreased autoantibodies. Conversely, B6.yaa and B6.Sle1b.yaa mice expressing an extra copy of TLR7 and B6.Sle1b mice treated with a TLR7 agonist had increased Spt-GCs and Tfh. Further, TLR7/ MyD88 deficiency led to compromised B cell proliferation and survival after B cell stimulation both in vitro and in vivo. In contrast, TLR9 inhibited Spt-GC development. Our findings demonstrate an absolute requirement of TLR7 and a negative regulatory function for TLR9 in Spt-GC formation under non-autoimmune and autoimmune conditions. Our data suggest that, under non-autoimmune conditions, Spt-GCs initiated by TLR7 produce protective antibodies. However, in the presence of autoimmune susceptibility genes, TLR7 dependent Spt-GCs produce pathogenic autoantibodies. Thus, a single copy of TLR7 in B cells is the minimal requirement for breaking the GC-tolerance checkpoint.

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“…The concept is that RNA and DNA–associated autoantigens are bound by the BCR and transported to a TLR-compartment where TLR detection of DNA or RNA provides a second signal promoting B cell activation. Intriguingly, a recent paper demonstrated the surprising finding in UNC-93B deficient lupus-prone mice that the development of non-nuclear autoantibody specificities, including anti-red blood cell and in other contexts anti-MPO, was dependent on TLR signaling in B cells [26]. One possible explanation for the dependence of non-nuclear antibodies on nucleic acid-TLR signaling is that they act as auto-antigens only when associated with nucleic acids, for example on apoptotic cells or neutrophil extracellular traps.…”

Section: The B Cell- Innate Immune System Interfacementioning

confidence: 99%

New insights into B cell biology in systemic lupus erythematosus and Sjögren's syndrome

Bird

Meednu

Anolik

2015

Current Opinion in Rheumatology

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Purpose of review Our understanding of the physiological and pathogenic functions of B cells in systemic lupus erythematosus (SLE) and Sjogren’s syndrome (pSS) continues to expand. In this review, we discuss novel insights published in the last 18 months into the roles of B cells in systemic autoimmunity. Recent findings Data has continued to expand the diverse mechanisms by which innate immune signals including toll like receptors (TLR) may regulate the B cell compartment. Localized B cells and long-lived plasma cells have been identified as playing an important role in target tissue including the development of ectopic lymphoid structures in kidney and salivary gland. In addition to pathogenic roles for B cells, there is mounting evidence for regulatory B cell subsets that play a protective role and new insights into the signals that regulate their development. Summary The past few years have provided insights into the multiple paths by which innate immune signals can lead to B cell activation in SLE and pSS and the increasingly diverse ways in which B cells contribute to disease expression. Further understanding the imbalance between protective and pathogenic functions for B cells in disease including in understudied target tissue should yield new treatment approaches.

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Role of Nucleic Acid–Sensing TLRs in Diverse Autoantibody Specificities and Anti-Nuclear Antibody–Producing B Cells

Cited by 40 publications

References 64 publications

Lupus nephritis

Lupus nephritis

B Cell–Intrinsic TLR7 Signaling Is Essential for the Development of Spontaneous Germinal Centers

New insights into B cell biology in systemic lupus erythematosus and Sjögren's syndrome

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