Development of Lupus-like Autoimmune Diseases by Disruption of the PD-1 Gene Encoding an ITIM Motif-Carrying Immunoreceptor

Nishimura, Hiroyuki; Nose, Masato; Hayashi, Hiroshi; Minato, Nagahiro; Honjo, Tasuku

doi:10.1016/s1074-7613(00)80089-8

Cited by 2,381 publications

(1,714 citation statements)

References 58 publications

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“…46 The PD-1 pathway has a crucial role in peripheral tolerance induction and maintenance as mice with deletion of PD-1 gene developed systemic autoimmunity. 47 Injection of PD-1 neutralizing monoclonal antibody into disease-resistant mice resulted in the majority (67%) of the mice developing EAE whereas none of the IgG controls developed disease. Although we failed to detect any significant changes in proportion of CD4 þ Foxp3 þ T cells, it remains to be determined whether antigen-specific Tregs were generated in this model.…”

Section: Discussionmentioning

confidence: 99%

Non-myeloablative transplantation of bone marrow expressing self-antigen establishes peripheral tolerance and completely prevents autoimmunity in mice

Hosseini

Chan

et al. 2011

Gene Ther

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Myeloablative transplantation of bone marrow (BM) engineered to express myelin oligodendrocyte glycoprotein (MOG) establishes central intrathymic tolerance and completely prevents MOG-induced experimental autoimmune encephalomyelitis (EAE) in mice. Here we asked whether non-myeloablative transplantation of MOG expressing BM (pMOG-bone marrow transplantation (BMT)) can also provide the same protection. Using stepwise reduction of irradiation doses, 275 cGy irradiation with pMOG-BMT protected 100% of mice from EAE development even with two subsequent re-challenge with MOG. Irradiation doses o275 cGy produced dose-dependent partial protection with significant disease protection still evident at 50 cGy. Splenocytes from 275 cGy recipients proliferated to MOG stimulation in vitro, indicating that MOG-reactive cells are present in the periphery but failed to induce disease. MOG-stimulated splenocytes produced little or no interleukin-17, interferon-g, granulocyte-monocyte colony stimulating factor and tumor necrosis factor-a compared with EAE control. Adoptive transfer of CD4 T cells from EAE-resistant mice into Rag2 À/À mice devoid of MOG expression resulted in MOG-induced EAE in B74% of mice. Treatment of EAE-resistant mice with anti-programmed death 1 (PD-1) monoclonal antibody-induced EAE in 67% of mice. We conclude that nonmyeloablative transplantation of self-antigen expressing BM induces robust peripheral tolerance that completely prevented EAE development. Our findings implicate clonal anergy and the PD-1 pathway in the maintenance of peripheral tolerance.

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Section: Discussionmentioning

confidence: 99%

Non-myeloablative transplantation of bone marrow expressing self-antigen establishes peripheral tolerance and completely prevents autoimmunity in mice

Hosseini

Chan

et al. 2011

Gene Ther

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“…Indeed, B6 mice deficient in Fc␥ receptor IIB (Fc␥RIIB) spontaneously develop circulating antichromatin and anti-dsDNA autoantibodies along with immune complex GN and pulmonary vasculitis, whereas Fc␥RIIB-deficient BALB/c mice do not (56). Moreover, B6 mice deficient in programmed death 1 (PD-1) develop a clinical phenotype highlighted by arthritis and GN (57), whereas BALB/c mice deficient in PD-1 develop no signs of arthritis or GN but do develop a lethal dilated cardiomyopathy (58). Thus, discrete immune disturbances elicit SLE-like features in B6 mice, but the identical immune disturbances do not do so in BALB/c mice.…”

Section: Discussionmentioning

confidence: 99%

BAFF overexpression and accelerated glomerular disease in mice with an incomplete genetic predisposition to systemic lupus erythematosus

Stohl¹,

Xu²,

Kim³

et al. 2005

Arthritis & Rheumatism

106

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Objective. To determine whether overexpression of BAFF can accelerate the development of systemic lupus erythematosus-associated end-organ disease in hosts with an underlying autoimmune diathesis.Methods. We introduced a BAFF transgene (Tg) into autoimmune-prone B6.Sle1 and B6.Nba2 mice and evaluated these mice for serologic autoimmunity and renal pathology.Results Conclusion. BAFF-driven effects on glomerular pathology may be mediated, at least in part, by autoantibodies with specificities other than chromatin and/or by autoantibody-independent means. There is an uncoupling of BAFF-driven precocious glomerular pathology from concomitant development of clinically apparent renal disease, strongly suggesting that BAFF overexpression works in concert with other factors to promote overt renal disease.Renal involvement in patients with systemic lupus erythematosus (SLE) is clinically apparent in ϳ50% of cases and leads to considerable morbidity. The vast majority of SLE patients with renal involvement develop increased proteinuria, sometimes to degrees great enough to adversely affect systemic fluid balance and hemodynamics (nephrotic syndrome). Glomerular disease is widely believed to be the major contributor to this increased proteinuria. Indeed, the World Health Organization (WHO) classification of lupus nephritis focuses almost entirely on glomerular lesions, with little attention to tubular, interstitial, or vascular lesions. Accordingly, factors which promote glomerular disease in SLE may be vital to the pathogenesis of lupus nephritis.

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“…The in vivo functions of PD-1, PD-L1, and PD-L2 have been of interest because PD-1 -/-mice progressively develop autoimmune diseases [12,13]. Since previous studies have shown that PD-L2 expression may be regulated in some cell types by Th2 cytokines or Th2 cells [21], and because asthma is believed to be a Th2-driven disease [23][24][25][26][27][28][29][30][31][32], it was of interest to examine whether PD-L2 can play a role in immune regulation in this context.…”

Section: Discussionmentioning

confidence: 99%

“…PD-1 has an immunoreceptor tyrosine-based inhibitory motif in its cytoplasmic domain [9][10][11]. Depending on background strain, PD-1 -/-mice develop increased rates of glomerulonephritis, lupus-like arthritis [12], or autoimmune cardiomyopathy [13]. This provides direct evidence for PD-1 as a negative regulator of immune responses in vivo [13].…”

Section: Introductionmentioning

confidence: 99%

Paradoxical role of programmed death‐1 ligand 2 in Th2 immune responses in vitro and in a mouse asthma model in vivo

et al. 2004

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Programmed death-1 ligand 2 (PD-L2) is a ligand for programmed death-1 (PD-1), a receptor that plays an inhibitory role in T cell activation. Since previous studies have shown upregulation of PD-L2 expression by Th2 cytokines, and asthma is driven by a Th2 response, we hypothesized that PD-L2 might be involved in regulation of the immune response in this disease. We have found that lungs from asthmatic mice had sustained up-regulation of PD-1 and PD-L2, with PD-L2 primarily on dendritic cells. Although addition of PD-L2-Fc in vitro led to decreased T cell proliferation and cytokine production, administration of PD-L2-Fc in vivo in a mouse asthma model resulted in elevated serum IgE levels, increased eosinophilic and lymphocytic infiltration into bronchoalveolar lavage fluid, higher number of cells in the draining lymph nodes, and production of IL-5 and IL-13 from these cells. Although PD-1 was expressed on regulatory T cells, PD-L2-Fc did not affect regulatory T cell activity in vitro. This study provides in vivo evidence of an exacerbated inflammatory response following PD-L2-Fc administration and indicates a potential role for this molecule in Th2-mediated diseases such as asthma.

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Development of Lupus-like Autoimmune Diseases by Disruption of the PD-1 Gene Encoding an ITIM Motif-Carrying Immunoreceptor

Cited by 2,381 publications

References 58 publications

Non-myeloablative transplantation of bone marrow expressing self-antigen establishes peripheral tolerance and completely prevents autoimmunity in mice

Non-myeloablative transplantation of bone marrow expressing self-antigen establishes peripheral tolerance and completely prevents autoimmunity in mice

BAFF overexpression and accelerated glomerular disease in mice with an incomplete genetic predisposition to systemic lupus erythematosus

Paradoxical role of programmed death‐1 ligand 2 in Th2 immune responses in vitro and in a mouse asthma model in vivo

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