B-cell extrinsic CR1/CR2 promotes natural antibody production and tolerance induction of anti-αGAL–producing B-1 cells

Shimizu, Ichiro; Kawahara, Toshiyasu; Haspot, Fabienne; Bardwell, Philip D.; Carroll, Michael; Sykes, Megan

doi:10.1182/blood-2006-02-002386

Cited by 21 publications

(14 citation statements)

References 64 publications

(98 reference statements)

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“…mice. However, MyD88 signaling is not only involved in the TLR9-dependent development of anti-nucleosome IgG2c and IgG2b autoantibodies but also in cell maturation via other TLRs (e.g., TLR7) (7-12, 14, 15, 17, 40, 41 analyzed by CD5 expression at day 7. that B-1b cells have a tolerogenic function, but underlying mechanisms have been unknown (44,45 Taken together, our data suggest that the tolerogenic function of MyD88-dependent TLR9 signaling is mediated by the production of self-reactive serum IgM Abs by peritoneal B-1b cells, which protects from uncontrolled accumulation of Th17 cells and severe autoimmunity. These findings provide new insight in the tolerogenic function of TLR9, B-1b cells, and self-reactive IgM to control autoimmunity and have implications for the development of TLR ligand-dependent therapies and B cell depletion protocols as a treatment for autoimmunity.…”

Section: Monoclonal Self-reactive Igm Abs Reduce Th17 Cell Accumulatimentioning

confidence: 79%

TLR9 in Peritoneal B-1b Cells Is Essential for Production of Protective Self-Reactive IgM To Control Th17 Cells and Severe Autoimmunity

Stoehr

Schoen

Mertes

et al. 2011

The Journal of Immunology

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The role of TLR9 in the development of the autoimmune disease systemic lupus erythematosus is controversial. In different mouse models of the disease, loss of TLR9 abolishes the generation of anti-nucleosome IgG autoantibodies but at the same time exacerbates lupus disease. However, the TLR9-dependent tolerance mechanism is unknown. In this study, we show that loss of TLR9 is associated with low peritoneal B-1b cell numbers and low levels of protective self-reactive IgM serum autoantibodies in lupus-prone FcγRIIB-deficient mice leading to the uncontrolled accumulation of proinflammatory CD4+ cells and exacerbated autoimmunity. TLR7 signaling was not able to compensate for the loss of TLR9 signaling in peritoneal B-1b cells to induce IgM Abs. Transfer of TLR9-expressing peritoneal B-1b cells from FcγRIIB-deficient mice or of recombinant monoclonal self-reactive IgM Abs was sufficient to reduce the frequency of proinflammatory Th17 cells and lupus disease in FcγRIIB/TLR9 double-deficient mice. Taken together, these data provide evidence for a TLR9-dependent tolerance mechanism of peritoneal B-1b cells generating protective self-reactive IgM in lupus-prone mice to control Th17 cell development and severe autoimmunity.

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Section: Monoclonal Self-reactive Igm Abs Reduce Th17 Cell Accumulatimentioning

confidence: 79%

TLR9 in Peritoneal B-1b Cells Is Essential for Production of Protective Self-Reactive IgM To Control Th17 Cells and Severe Autoimmunity

Stoehr

Schoen

Mertes

et al. 2011

The Journal of Immunology

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“…On a FACSVantage (Becton Dickinson, San Jose, CA), CD21 neg CD23 neg B1b and CD21 high CD23 low MZB cells were sorted, 15,19 collected, and resuspended in PBS for intravenous injection. Purity of selected cell populations was more than 90%.…”

Section: Cell Isolation Proceduresmentioning

confidence: 99%

“…Accordingly, xenografts transplanted on day 2 or 14 were accepted indefinitely (Table 1; groups F,G) without IgM xenoantibody production (not shown). In contrast, xenografting at week 4 after TBI, when MZB cells had recovered, again resulted in acute vascular rejection (Table 1; group H) accompanied with high IgM xenoantibody levels (not shown).In order to confirm that MZB cells and not B1b lymphocytes were responsible for rapidly induced IgM xenoantibody production, MACS-enriched CD19 ϩ B cells from BALB/c nude spleens were purified using fluorescence-activated cell sorter (FACS) sorting into CD21 high CD23 low MZB cells and CD21 neg CD23 neg B1b cells 15,19 (Figure 3A). CB17 severe combined immunodeficiency (SCID) mice were given 2 to 5 ϫ 10 6 subset B cells intravenously on day 0, and 200 L whole hamster blood on day 7.…”

mentioning

confidence: 99%

Rapidly induced, T-cell–independent xenoantibody production is mediated by marginal zone B cells and requires help from NK cells

Yan

Lin

et al. 2007

Blood

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Xenoantibody production directed at a wide variety of T lymphocyte-dependent and T lymphocyte-independent xenoantigens remains the major immunologic obstacle for successful xenotransplantation. The B lymphocyte subpopulations and their helper factors, involved in T-cellindependent xenoantibody production are only partially understood, and their identification will contribute to the clinical applicability of xenotransplantation. Here we show, using models involving T-celldeficient athymic recipient mice, that rapidly induced, T-cell-independent xenoantibody production is mediated by marginal zone B lymphocytes and requires help from natural killer ( IntroductionSuccessful xenotransplantation may alleviate the ever-increasing need for donor organs, but severe immunologic barriers, of which xenoreactive antibodies represent the most important 1, still hamper (pre)clinical application. Pigs are now generally considered the most suitable organ donors for clinical xenotransplantation, 1 but transplantation of pig organs into nonhuman primates, currently constituting the best validated preclinical model, leads to xenograft rejection within a few hours. This hyperacute rejection is mediated by pre-existing, so-called "natural antibodies," which are directed at a specific Gal␣1,3Gal␤1,4GlcNAc (Gal) oligosaccharide, that is present on (especially endothelial) proteins of most lower animal species, but not of nonhuman primates or man. [2][3][4] Anti-Gal natural antibodies can rapidly activate the complement system of the recipient, leading to hyperacute rejection. 5 Several procedures have been explored in recent years to solve the problem of hyperacute rejection. 6,7 The most appealing ones were the development of genetically modified donor pig strains that either expressed transgenes of human complement regulatory proteins, able to interfere with complement activation, 8 or that lacked the ␣1,3-galactosyltransferase gene to synthesise ␣Gal. 9,10 The latter pig strain seemed particularly attractive, as Gal antigens had been found to be also strongly involved in acute vascular xenograft rejection, a second type of xenograft rejection that develops within a few days in situations where hyperacute rejection is prevented. 7,11 It was hoped, therefore, that elimination of Gal epitopes would prevent both hyperacute rejection and acute vascular rejection.A number of recent reports on the transplantation of ␣1,3-galactosyltransferase-ko pig kidney or heart grafts in nonhuman primates have shown that loss of Gal expression in donor pig organs could indeed prevent hyperacute rejection, but that T-celldependent IgG xenoantibodies were induced against non-Gal xenoantigens, unless a treatment regimen was used that resulted in specific T-cell xenotolerance. [12][13][14] In the latter case, long-term functional renal xenograft survival was obtained, but after a few months, mild focal thrombotic microangiopathy was observed, suggesting that additional modifications to the treatment regimen are needed to permit the development of the kin...

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“…The resulting activation of helper T lymphocytes enables the B cells to complete their activation process, ultimately resulting in proliferation, isotype switching, and the generation of plasma cells and high-affinity anti-aGal antibodies (Tanemura et al 2000). Finally, there are reports of follicular dendritic cells expressing complement receptors 1 and 2 being involved in the presentation of immune complexes to aGal-reactive B cells and being needed for antigen-specific antiaGal response (Shimizu et al 2007). At this stage, thanks to the many approaches pursued with a view to removing preexisting anti-aGal antibodies and controlling their effector functions, HAR of a solid organ xenograft has become a rare event.…”

Section: Antibody-mediated Xenograft Rejectionmentioning

confidence: 99%

Immunological Challenges and Therapies in Xenotransplantation

Vadori

2014

Cold Spring Harbor Perspectives in Medicine

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B-cell extrinsic CR1/CR2 promotes natural antibody production and tolerance induction of anti-αGAL–producing B-1 cells

Cited by 21 publications

References 64 publications

TLR9 in Peritoneal B-1b Cells Is Essential for Production of Protective Self-Reactive IgM To Control Th17 Cells and Severe Autoimmunity

TLR9 in Peritoneal B-1b Cells Is Essential for Production of Protective Self-Reactive IgM To Control Th17 Cells and Severe Autoimmunity

Rapidly induced, T-cell–independent xenoantibody production is mediated by marginal zone B cells and requires help from NK cells

Immunological Challenges and Therapies in Xenotransplantation

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