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Query: UMLS:C0024141 (
systemic lupus erythematosus
)
44,322
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Recent evidence suggests that most of the rheumatic diseases are complex or multifactorial diseases with contributions from HLA and multiple non-HLA genes. Studies using candidate gene approach suggested that early components of the complement pathway, Fc receptor IIa, IIIa,
mannose-binding lectin
, IL-10 and TNFR2 might be potential non-HLA susceptibility genes to
systemic lupus erythematosus
, although substantial difference among populations are reported. Linkage analyses using affected sib pairs indicated several candidate regions on chromosome 1. A recently completed genome-wide linkage analysis of rheumatoid arthritis revealed a number of possible candidate regions in addition to HLA. Identification of the susceptibility genes will be accelerated along with technological advances and the accomplishment of human genome project, and will deepen our understanding of rheumatic diseases.
...
PMID:[Analysis of susceptibility genes to rheumatic diseases]. 1007 98
Three pathways are recognized in complement activation. The aim of our study is to elucidate immunohistologically which complement pathway is associated with complement activation in immunoglobulin A (IgA) glomerulonephritis (GN) and which IgA subclass is related to complement activation. Immunohistological staining was performed on renal biopsy specimens obtained from 36 patients with IgA GN, 10 patients with
systemic lupus erythematosus
(
SLE
), and 16 patients with other GNs using polyclonal antibodies of IgG, IgA, IgM, C1q, C3c, and C4 and monoclonal antibodies of IgA1, IgA2,
mannose-binding lectin
(
MBL
), and
MBL
-associated serine protease-1 (MASP-1). Mesangial deposits of both IgA1 and IgA2 were found in 19 of 36 patients with IgA GN. Mesangial deposits of C3c, C4,
MBL
, and MASP-1 also were detected in these 19 patients, and IgA2,
MBL
, and MASP-1 deposits were colocalized in the mesangium in these patients. The remaining 17 patients showed mesangial deposits of IgA1 alone. Twelve of these 17 patients showed mesangial deposits of C3c without C4,
MBL
, or MASP-1. No deposition of C1q was evident in patients with IgA GN. Three of 10 patients with
SLE
showed glomerular deposition of
MBL
and MASP-1 without glomerular deposition of IgA2. None of the patients with other GNs showed glomerular deposition of IgA1, IgA2,
MBL
, or MASP-1. There was no correlation in clinical or pathological indicators between IgA2-positive and IgA2-negative patients with IgA GN. In conclusion, alternative pathway-involved complement activation is associated with mesangial deposits of IgA1 alone in patients with IgA GN. In those with mesangial deposits of both IgA1 and IgA2, both the alternative and lectin pathways are involved in complement activation. We first report that mesangial deposits of IgA2 may activate the lectin pathway in patients with IgA GN.
...
PMID:Mesangial IgA2 deposits and lectin pathway-mediated complement activation in IgA glomerulonephritis. 1168 63
This study describes the importance of
mannose-binding lectin
(
MBL
) variant alleles for
systemic lupus erythematosus
(
SLE
) and accompanying infections in a population-based cohort.
MBL
alleles were determined in 99
SLE
patients recruited from a representative Danish region. Patients were classified according to the 1982 revised ACR criteria as definite
SLE
(D-SLE) (n = 77) fulfilling > or =4 criteria and incomplete
SLE
(I-SLE) (n = 22) with 0.99, respectively). A meta-analysis of eight previously published studies suggested that the presence of
MBL
variant alleles confer a 1.6 times overall increased risk for D-SLE (P < 0.00001).
MBL
variant allele carriers had higher disease activity (SLEDAI-index) in a 2-year follow-up period (P = 0.02) and had an increased risk of acquiring complicating infections in general (P = 0.03) and respiratory infections in particular (P = 0.0006). Only in
SLE
patients fulfilling > or =4 ACR criteria an increased frequency of
MBL
variant alleles was found.
MBL
variant alleles were also associated with increased risk of disease activity and of complicating infections indicating that the
MBL
gene is an
SLE
disease modifier locus.
...
PMID:Association of mannose-binding lectin gene variation with disease severity and infections in a population-based cohort of systemic lupus erythematosus patients. 1178 11
We have developed a method for quantitating
mannan-binding lectin
(
MBL
)-induced activation of the complement system (
MBL
-C4-AC) in human plasma. This method and an assay for
MBL
concentration were applied to plasma samples from healthy individuals and patients with
systemic lupus erythematosus
(
SLE
), Crohn's disease (CD) and colorectal cancer (CRC). The
MBL
concentration was measured by an enzyme-linked immunosorbent assay (ELISA) using monoclonal anti-
MBL
-antibodies and
MBL
-C4-AC by an ELISA using solid-phase mannan, incubating with plasma samples and quantitating the complement (C) activation by the use of antibodies against the C split-products C4b/C4c. The
MBL
concentration was nonsignificantly elevated in plasma from
SLE
-patients, whereas
MBL
-C4-AC was suppressed (P < 0.04). There was no correlation between
MBL
concentration and
MBL
-C4-AC in plasma from
SLE
-patients. In contrast, a significant correlation was found between the
MBL
concentration and
MBL
-C4-AC in plasma from healthy individuals. The C4 concentration was significantly reduced (P < 0.002) in plasma from the
SLE
patients and showed a significant correlation to
MBL
-C4-AC. The
MBL
-C4-AC assay was highly effective in discriminating the
SLE
patients from the other patient groups and healthy individuals.
...
PMID:Complement activation mediated by mannan-binding lectin in plasma from healthy individuals and from patients with SLE, Crohn's disease and colorectal cancer. Suppressed activation by SLE plasma. 1184 98
Infections are common in
systemic lupus erythematosus
(
SLE
), and remain a source of mortality. The types of infections (such as pneumonia, urinary tract infection, cellulitis, and sepsis) in
SLE
patients are similar to the general population and include the same pathogens (Gram-positive and Gram-negative).
SLE
patients may also develop opportunistic infections, especially when treated with immunosuppressive agents. As a high-risk population, identification and treatment of chronic infections such as tuberculosis, hepatitis B, or human immunodeficiency virus (HIV), are important prior to the institution of immunosuppression to prevent reactivation or exacerbation of the infection. A common caveat is to distinguish between a
lupus
flare and an acute infection; judicious use of corticosteroids and cytotoxic drugs is critical in limiting infectious complications. The risk factors associated with susceptibility to disease include severe flares, active renal disease, treatment with moderate or high doses of corticosteroids and/or immunosuppressive agents, and others. Genetic factors (complement deficiencies,
mannose-binding lectin
, Fcgamma III, granulocyte macrophage colony-stimulating factor [GM-CSF], osteopontin) may predispose certain
SLE
patients to develop infections. Parameters including C-reactive protein (CRP) and adhesion molecules may help to differentiate an infectious disease from an exacerbation of the disease. Finally, the mechanism of molecular mimicry by specific microbial agents may play a role in the induction of
SLE
.
...
PMID:SLE and infections. 1279 59
Mannose-binding lectin (MBL; also known as
mannan-binding lectin
) is an important component of innate immunity. MBL levels are mainly genetically determined. Low serum MBL levels and their cognate haplotypes have been associated with a wide range of infections. However, most subjects with MBL deficiency remain healthy. MBL deficiency is also associated with non-infectious diseases including
systemic lupus erythematosus
, rheumatoid arthritis, cystic fibrosis and common variable immunodeficiency. MBL deficiency may affect susceptibility to (e.g. meningococcal disease), or alter the natural history of (e.g. rheumatoid arthritis, cystic fibrosis), a disease. MBL (plasma-derived or recombinant) therapy has yet to be shown to be safe and effective. Potentially it may be useful in MBL-deficient patients to reduce susceptibility to, or enhance recovery from, bacterial infection or to alter the natural history of a disease (disease-modifying drug). In practise the place of MBL therapy may be as a disease-modifying drug to reduce the severity of rheumatoid arthritis and to preserve lung and liver function in cystic fibrosis. MBL therapy may also ameliorate various immunodeficiency syndromes. A potential hazard of MBL therapy is enhanced complement-mediated host damage. The place of MBL therapy will await results of randomized controlled clinical trials.
...
PMID:Clinical potential of mannose-binding lectin-replacement therapy. 1288 1
Immunosuppressive drugs have become the gold standard for the treatment of major organ involvement in
systemic lupus erythematosus
. The use of immunosuppressive therapy in
systemic lupus erythematosus
carries significant risks for infection. This article reviews infectious complications in
systemic lupus erythematosus
, focusing on effects of immunosuppressive therapy. Patients with
systemic lupus erythematosus
appear to carry an intrinsically increased risk for infection. Recent studies support this notion further by showing increased risk for serious infections in patients with
systemic lupus erythematosus
who had
mannose-binding lectin
deficiency associated with homozygous
mannose-binding lectin
variant alleles. Patients with
systemic lupus erythematosus
who were homozygous for
mannose-binding lectin
variant alleles had a fourfold increase in the incidence of infections, requiring hospitalization. In terms of extrinsic risk factors for infection, use of steroids and cyclophosphamide are the strongest risk factors. The effect of these drugs on infection is also dose dependent. The incidence of infectious complications in patients treated with mycophenolate mofetil, a newly used immunosuppressive drug in
systemic lupus erythematosus
, appears less frequent compared with cyclophosphamide. Herpes zoster is still the most common viral infection in patients with
systemic lupus erythematosus
treated with cyclophosphamide and mycophenolate mofetil. Overall data indicate that patients with
systemic lupus erythematosus
may have intrinsically increased risks for infection that are augmented by immunosuppressive therapies. Cyclophosphamide, in particular in combination with high-dose glucocorticoids, has the strongest effect in suppressing the immune responses against microorganisms. Careful monitoring of infectious complications is warranted in patients with
systemic lupus erythematosus
receiving immunosuppressive therapies, in particular those on high-dose glucocorticoids and cytotoxic drugs.
...
PMID:Infectious complications in SLE after immunosuppressive therapies. 1296 Apr 76
Deficiencies of early components of the classical complement pathway, particularly C1q, are strongly associated with susceptibility to
systemic lupus erythematosus
. Recent data link this predisposal to autoimmunity to an inappropriate clearance of apoptotic cells, which could lead to a loss of self-tolerance. In the present study, we demonstrate that opsonization of apoptotic cells with C1q and
mannose-binding lectin
allows and facilitates their uptake not only by macrophages but also by human immature dendritic cells (DCs). Both C1q and
mannose-binding lectin
enhance the uptake of apoptotic cells by DCs in a dose-dependent way. The uptake of C1q-opsonized apoptotic cells, but not nonopsonized apoptotic cells, by DCs stimulated the production of IL-6, IL-10, and TNF-alpha, without an effect on IL-12p70. We conclude that these recognition molecules of the complement system do not sequester apoptotic cells from DCs, but rather promote their uptake by immature DCs. Therefore, we propose that early complement components support safe clearance of cellular debris by facilitating phagocytosis and possibly by immunomodulatory mechanisms, thus preventing autoimmunity.
...
PMID:Opsonization with C1q and mannose-binding lectin targets apoptotic cells to dendritic cells. 1532 64
Dysfunction in various parts of immune defence, such as immune response, immune complex clearance, and inflammation, has an impact on pathogenesis in
systemic lupus erythematosus
(
SLE
). We hypothesised that combinations of common variants of genes involved in these immune functions are associated with susceptibility to
SLE
. The following variants were analysed: HLA DR3, HLA DQ2, C4AQ0, Fcgamma receptor IIa (FcgammaRIIa) genotype R/R, Fcgamma receptor IIIa (FcRgammaIIIa) genotype F/F,
mannan-binding lectin
(
MBL
) genotype conferring a low serum concentration of
MBL
(
MBL
-low), and interleukin-1 receptor antagonist (IL-1Ra) genotype 2/2. Polymorphisms were analysed in 143 Caucasian patients with
SLE
and 200 healthy controls. HLA DR3 in
SLE
patients was in 90% part of the haplotype HLA DR3-DQ2-C4AQ0, which was strongly associated with
SLE
(odds ratio [OR] 2.8, 95% CI 1.7-4.5). Analysis of combinations of gene variants revealed that the strong association with
SLE
for HLA DR3-DQ2-C4AQ0 remained after combination with FcgammaRIIa R/R, FcgammaRIIIa F/F, and
MBL
-low (OR>2). Furthermore, the combination of the FcgammaRIIa R/R and IL-1Ra 2/2 genotypes yielded a strong correlation with
SLE
(OR 11.8, 95% CI 1.5-95.4). This study demonstrates that certain combinations of gene variants may increase susceptibility to
SLE
, suggesting this approach for future studies. It also confirms earlier findings regarding the HLA DR3-DQ2-C4AQ0 haplotype.
...
PMID:Analysis of HLA DR, HLA DQ, C4A, FcgammaRIIa, FcgammaRIIIa, MBL, and IL-1Ra allelic variants in Caucasian systemic lupus erythematosus patients suggests an effect of the combined FcgammaRIIa R/R and IL-1Ra 2/2 genotypes on disease susceptibility. 1553 34
Viral and bacterial infections may serve as an environmental trigger for the development or exacerbation of
systemic lupus erythematosus
(
SLE
) in the genetically predetermined individual. In addition,
SLE
patients are more prone to develop common (pneumonia, urinary tract infection, cellulitis, sepsis), chronic (tuberculosis), and opportunistic infections possibly due to inherit genetic and immunologic defects (complement deficiencies,
mannose-binding lectin
[MBL] polymorphisms, elevated Fcgamma III and GM-CSF levels, osteopontion polymorphism), but also due to the broad spectrum immunosuppressive agents that are part of therapy for severe manifestations of the disease. Hence,
SLE
patients are considered a high-risk population, where identification and treatment of chronic infections such as tuberculosis, hepatitis B or human immunodeficiency virus, are important prior to the institution of immunosuppression so as to prevent reactivation or exacerbation of the infection. Infections in
SLE
patients remain a source of morbidity and mortality. A caveat often encountered is to distinguish between a
lupus
flare and an acute infection; in such cases parameters including elevated CRP (and adhesion molecules) may aid in the diagnosis of infection. Recent research has provided convincing evidence that EBV infection may play a major role not only in molecular mimicry but also in aberrations of B cells and apoptosis leading to a state of perpetual heightened immune response in
SLE
.
...
PMID:Infections and SLE. 1637 52
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