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Query: UMLS:C0024141 (
systemic lupus erythematosus
)
44,322
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Systemic lupus erythematosus
(
SLE
) is a chronic, multisystem autoimmune disease characterized by the differentiation of short- and long-lived immunoglobulin secreting plasma cells that secrete pathogenic autoantibodies. Ectopic germinal centers and plasma cells secreting autoantibodies have been observed in lupus nephritis kidneys. Candidate genetic susceptibility loci for
SLE
include genes that affect differentiation and survival of plasma cells, such as those that influence activation, proliferation, cytokine and chemokine secretion/responsiveness, and apoptosis of the T and B cells that are involved in humoral immunity generated in germinal centers, as well as genes that are involved in presentation and clearance of apoptotic material and autoantigens by antigen presenting cells and other phagocytes. Emerging data have demonstrated that B lymphocytes are active participants in humoral immune responses that lead to T-dependent and T-independent differentiation of immunoglobulin-secreting plasma cells by homotypic
CD154
-CD40 interactions as well as continued stimulation by B cell activating factor through B cell maturation antigen, B cell activating factor receptor and transmembrane activater.
...
PMID:B cell abnormalities in systemic lupus erythematosus. 1518 Aug 94
CD40 ligand (
CD40L
, also known as
CD154
or
gp39
) is a member of the tumor necrosis superfamily of transmembrane proteins. The interaction of
CD40L
on activated T cells with its receptor, CD40 on B cells, is necessary for normal immune function, including B cell differentiation, germinal center formation, and antibody isotype switching. Abnormal expression of
CD40L
in patients with
systemic lupus erythematosus
(
SLE
) may contribute to autoantibody production and disease pathogenesis. Although murine models of monoclonal antibodies directed against
CD40L
initially showed promise, human trials either have failed to demonstrate efficacy or have been associated with adverse events. This review will summarize in vitro and murine model data and human clinical trials involving anti-
CD40L
monoclonal antibody.
Lupus
2004
PMID:The role of CD40 ligand in systemic lupus erythematosus. 1523 Feb 96
The CD40-
CD40L
system has pleiotropic effects in a variety of cells and biological processes including immune response, thrombosis and atherogenesis. Within the immune system, these molecules represent a critical link between its humoral and cellular arms. As a result of these attributes and based on preclinical data in animals, anti-
CD40L
antibodies were tested in a variety of immunologic diseases including idiopathic thrombocytopenic purpura, psoriasis, Crohn's disease,
systemic lupus erythematosus
and transplantation. Phase I/II studies in humans with lupus nephritis demonstrated reduction of anti-double-stranded DNA (anti-dsDNA) antibodies but not of protective antibodies. Reduction of anti-DNA was associated with increased serum complement levels and reduced glomerular inflammation. As a result of thrombotic effects, observed even in patients negative for anti-cardiolipin antibodies, there is a temporary halt on further human studies. The reasons for the prothrombotic effects are not clear at present but may represent effects on platelets and/or the endothelium. In view of the significant immunomodulatory effects of anti-
CD40L
treatment in patients with lupus nephritis, the increasing realization of the importance of premature atherosclerosis in
lupus
and an increasing amount of data supporting a role for the CD40-
CD40L
interactions in this process, inhibition of this pathway deserves further exploration in
lupus
.
Lupus
2004
PMID:Lessons learned from anti-CD40L treatment in systemic lupus erythematosus patients. 1523 Feb 98
Blockade of the
CD154
-CD40 co-stimulatory pathway with anti-
CD154
mAbs has shown impressive efficacy in models of autoimmunity and allotransplantation. Clinical benefit was also demonstrated in
systemic lupus erythematosus
(
SLE
) and idiopathic thrombocytopenia patients with the humanized anti-
CD154
mAb, 5C8 (hu5C8). However, thromboembolic complications that occurred during the course of the hu5C8 clinical trials have proven to be a major setback to the field and safe alternative therapeutics targeting the
CD154
-CD40 pathway are of great interest. Recently, effector mechanisms have been shown to play a part in anti-
CD154
mAb-induced transplant acceptance in murine models, while this issue remains unresolved for humoral-mediated models. Herein, aglycosyl anti-
CD154
mAbs with reduced binding to FcgammaR and complement were used as a novel means to test the role of effector mechanisms in non-human primate and murine models not amenable to gene knockout technology. While aglycosyl hu5C8 mAb was relatively ineffective in rhesus renal and islet allotransplantation, it inhibited primary and secondary humoral responses to a protein immunogen in cynomolgus monkeys. Moreover, an aglycosyl, chimeric MR1 mAb (muMR1) prolonged survival and inhibited pathogenic auto-antibody production in a murine model of
SLE
. Thus, the mechanisms required for efficacy of anti-
CD154
mAbs depend on the nature of the immune challenge.
...
PMID:The contribution of Fc effector mechanisms in the efficacy of anti-CD154 immunotherapy depends on the nature of the immune challenge. 1546 14
Costimulation between T cells and APC is required for productive immune responses. A number of receptor/ligand pairs have been shown to mediate costimulation, including CD28/B7 molecules (CD80 and CD86), CD40/CD40 ligand (
CD40L
,
CD154
), and LFA-1 (CD18)/ICAM-1 (CD54). T-B cell costimulation also plays a significant role in autoimmune diseases such as
systemic lupus erythematosus
. Murine HgCl2-induced autoimmunity (mHgIA) is a T cell-dependent systemic autoimmune disease that shares a number of common pathogenic mechanisms with idiopathic
lupus
. In this report, the significance of costimulation in mHgIA is examined by attempting to induce disease in mice deficient in either
CD40L
, CD28, or ICAM-1. Unlike absence of ICAM-1, homozygous deficiencies in either
CD40L
or CD28 significantly reduced the development of mHgIA.
CD40L
displayed a gene dosage effect as heterozygous mice also showed reduction of autoantibody responses and immunopathology. Markers of T cell activation such as CD44 and CTLA-4 were associated with disease expression in wild-type and ICAM-1-deficient mice but not in
CD40L
- or CD28-deficient mice. Absence of CTLA-4 expression in
CD40L
-/- mice suggests that signaling via both CD28 and
CD40L
is important for T cell activation and subsequent autoimmunity in mHgIA. Attempts to circumvent the absence of
CD40L
by increasing CD28 signaling via agonistic Ab failed to elicit CTLA-4 expression. These findings indicate that breaking of self-tolerance in mHgIA requires signaling via both the CD28/B7 and CD40/
CD40L
pathways.
...
PMID:Costimulation requirements of induced murine systemic autoimmune disease. 1549 42
The immunological hallmark of
SLE
is B cell hyperactivity.
CD154
(CD40-L) is normally expressed in activated T cells, and plays an important role in T-B interactions. Its expression is increased in
SLE
T cells. Additionally, its expression on B cells leads to the development of
SLE
-like disease in a transgenic model. IL-10 is a key cytokine in the disturbed
SLE
immune system. The aim of this work was to explore the relation between IL-10 and
CD154
expression in
SLE
B cells. We studied 11
SLE
patients and 10 healthy volunteers. Mononuclear cells were isolated from peripheral blood and cultured in the presence or absence of Cowan I Strain Staphylococcus (CSS). Surface
CD154
and intracytoplasmic IL-10 expression were quantified with flow cytometry. In basal conditions,
CD154
expression was not different in patients and controls. B cell stimulation did not cause a significant increase in
CD154
expression in control B cells. However, its expression increased 2 times in B cells obtained from
SLE
patients. IL-10 expression was confined to
CD154
(+) cells. Our results show that IL-10 production is intimately linked to
CD154
expression in B cells, and that the IL-10(+)
CD154
(+) B cell subset increases abnormally when
SLE
-derived cells are stimulated with CSS.
...
PMID:IL-10 production in B cells is confined to CD154+ cells in patients with systemic lupus erythematosus. 1557 32
Many tissue injuries and immune mediated pathologies such as graft allo-rejections were found to involve CD40-CD40 ligand (
CD40L
,
CD154
) signaling pathway. The disruption of this pathway in many animal models led to the improvement of graft survival in these models. CD40-
CD154
interactions were also shown to play a significant role in the maintenance of autoimmunity, and the production of auto-antibodies in
systemic lupus erythematosus
(
SLE
). High-level expression of
CD154
has been detected on T cells from patients with active
SLE
, rheumatoid arthritis (RA) and other autoimmune diseases, indicating that such cells could account for the high-level expression of immune accessory molecules on B cells of patients with active disease. An increased serum level of soluble
CD154
was also reported in
SLE
, RA, and Sjogren's disease in correlation with the relevant auto-antibodies and with the clinical disease activity. Anti-
CD154
antibody therapy prevents auto-antibody production and renal immune complex deposition in lupus nephritis, indicating that disruption of this pathway could be a beneficial treatment in
SLE
. However, the etiology of the higher than expected number of thromboembolic events in anti-
CD154
treated
SLE
patients should be investigated and preventive measures should be considered.
...
PMID:The role of CD40-CD154 interactions in autoimmunity and the benefit of disrupting this pathway. 1562 72
Systemic lupus erythematosus
(
SLE
) is a prototypic autoimmune disease that is caused by genetic and environmental factors. The tumour necrosis factor (TNF) superfamily of genes play a central role in immune regulation and have been proposed to be involved in the development of
SLE
. TNFRSF5 (CD40) falls on 20q11-13, a region linked with
SLE
in three independent genome-wide studies. TNFSF5 (
CD40L
) falls on Xq26 and is the ligand for TNFRSF5. Seven single-nucleotide polymorphisms (SNPs) in CD40 and eight SNPs in
CD40L
were looked at for linkage disequilibrium (LD) and haplotype analysis in European-Caucasians. Limited haplotype diversity was observed across CD40 and
CD40L
, and >97% of the diversity was captured. We also examined the association of SNPs and haplotypes in CD40 and
CD40L
with
SLE
in European-Caucasians. There was no evidence of association for CD40 or
CD40L
in 408 European-Caucasian families with
SLE
from UK. Haplotype tagging SNPs (htSNPs) are made known, which will facilitate analysis for susceptibility in other autoimmune diseases and risk for infectious disease.
...
PMID:Haplotype structure of TNFRSF5-TNFSF5 (CD40-CD40L) and association analysis in systemic lupus erythematosus. 1565 13
CD40 and
CD154
belong to the tumor necrosis factor (TNF) receptor superfamily and the TNF superfamily, respectively. Evidence is accumulating that indicates the importance of this receptor-ligand pair in the immunopathogenesis of autoimmune diseases. The CD40-
CD154
interaction influences antigen presentation, tolerance, autoantibody production and tissue damage, all of which are relevant to the development and perpetuation of autoimmune diseases. Among the collagen diseases, the CD40-
CD154
interaction has been intensively investigated in
systemic lupus erythematosus
(
SLE
) and rheumatoid arthritis (RA). In this article, both basic and clinical research suggesting the involvement of the CD40-
CD154
interaction in
SLE
, RA, inflammatory myopathies, systemic sclerosis and antiphospholipid syndrome are reviewed. The results of clinical trials from CD40-
CD154
blockade are also analyzed. CD40-
CD154
blockade in animal models of autoimmune diseases has been reported to be a promising novel therapeutic approach and, thus, has attracted great attention from pharmaceutical companies. However, the development of CD40-
CD154
blockers with both significant clinical efficacy and safety has not been successful and research advances in this field are eagerly awaited.
...
PMID:[Involvement of CD40-CD154 interaction in immunopathogenesis of collagen diseases and its application to a novel therapeutic strategy]. 1567 91
In systemic, humoral autoimmune diseases such as
systemic lupus erythematosus
, a pathogenic hyperactivation of T- and B-lymphocytes results in the elaboration of high-titer, high-affinity autoantibodies that mediate end organ damage. Although several T-dependent and -independent cell-surface molecules and cytokines, such as
CD154
and the interferons, have been proposed to play key roles in disease, they have remained insufficient to explain fully the pathophysiology of these syndromes and have so far failed to yield premium therapeutic targets. Recent genome-based approaches to autoimmunity, however, have revealed novel pathogenic targets, including genes that negatively regulate T- and/or B-cell effector differentiation, as well as genes that specifically regulate T-cell-B-cell collaboration. It is hoped that continued investigation of such pathogenic targets will yield novel and specific therapeutic agents for the treatment of human autoimmune conditions.
...
PMID:Target identification and validation in systemic autoimmunity. 1610 71
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