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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
is a complex and potentially fatal autoimmune disease, characterized by autoantibody production and multi-organ damage. By a genome-wide association study (320 patients and 1,500 controls) and subsequent replication altogether involving a total of 3,300 Asian
SLE
patients from Hong Kong, Mainland China, and Thailand, as well as 4,200 ethnically and geographically matched controls, genetic variants in ETS1 and
WDFY4
were found to be associated with
SLE
(ETS1: rs1128334, P = 2.33x10(-11), OR = 1.29;
WDFY4
: rs7097397, P = 8.15x10(-12), OR = 1.30). ETS1 encodes for a transcription factor known to be involved in a wide range of immune functions, including Th17 cell development and terminal differentiation of B lymphocytes. SNP rs1128334 is located in the 3'-UTR of ETS1, and allelic expression analysis from peripheral blood mononuclear cells showed significantly lower expression level from the risk allele.
WDFY4
is a conserved protein with unknown function, but is predominantly expressed in primary and secondary immune tissues, and rs7097397 in
WDFY4
changes an arginine residue to glutamine (R1816Q) in this protein. Our study also confirmed association of the HLA locus, STAT4, TNFSF4, BLK, BANK1, IRF5, and TNFAIP3 with
SLE
in Asians. These new genetic findings may help us to gain a better understanding of the disease and the functions of the genes involved.
...
PMID:Genome-wide association study in Asian populations identifies variants in ETS1 and WDFY4 associated with systemic lupus erythematosus. 2016 77
The genetic components in
systemic lupus erythematosus
(
SLE
) have long been established, however, it has been unclear for many years whether the same genetic risk factors for
SLE
are shared across different ethnic groups. Over the past few years, a number of genetic and genomic studies have been conducted in Asian populations to address this question. These studies have demonstrated that genetic heterogeneity does exist in
SLE
across different ethnic groups. With these studies, it has been established that a number of genes associated with
SLE
in Caucasians are also risk factors in Asians: HLA class II genes, STAT4, BANK1, BLK, IRF5, TNFSF4, ITGAM, etc., while there are also novel genetic risk factors identified by these studies in Asians, for instance, the ETS1 and
WDFY4
in Chinese. For the genomic studies, the interferon signature has been confirmed as a major
lupus
molecular phenotype in Asians the same as in Caucasians; microRNA expression profiling and its novel role in regulating the interferon pathway has been first revealed in Asians. Further understanding of the function of
lupus
disease genes and delineating the key molecular pathway(s) will enhance the development of novel therapeutic targets and biomarkers for individualized clinical management for
lupus
patients.
Lupus
2010 Oct
PMID:Current advances in lupus genetic and genomic studies in Asia. 2094 45
Two recent genome-wide association studies of East Asian populations revealed three genetic variants in
WDFY4
/LRRC18 associated with
systemic lupus erythematosus
(
SLE
). To identify the gene contributing to this disease susceptibility, we examined the mRNA expression of
WDFY4
and LRRC18 in patients with
SLE
and healthy controls.
WDFY4
was significantly downregulated in
SLE
patients as compared with controls. We used allelic expression and dual-luciferase assays to identify the functional variant. Transcriptional activity was lower for the rs877819A than -G allele. Electrophoretic mobility shift and supershift assays revealed that the transcription factor Yinyang1 (YY1) binds to rs877819, with lower affinity to the A allele, which explained the reduced transcriptional activity. This effect was further confirmed by YY1 small interfering RNA knockdown, overexpression and chromatin immunoprecipitation experiments. rs877819 in
WDFY4
might be the functional site associated with
SLE
by reduced binding of YY1 and downregulating
WDFY4
expression.
...
PMID:An intronic variant associated with systemic lupus erythematosus changes the binding affinity of Yinyang1 to downregulate WDFY4. 2297 72
Recent genome-wide association studies (GWASs) conducted in Asian populations have identified novel risk loci for
systemic lupus erythematosus
(
SLE
). Here, we genotyped 10 single-nucleotide polymorphisms (SNPs) in eight such loci and investigated their disease associations in three independent Caucasian
SLE
case-control cohorts recruited from Sweden, Finland and the United States. The disease associations of the SNPs in ETS1, IKZF1, LRRC18-
WDFY4
, RASGRP3, SLC15A4, TNIP1 and 16p11.2 were replicated, whereas no solid evidence of association was observed for the 7q11.23 locus in the Caucasian cohorts. SLC15A4 was significantly associated with renal involvement in
SLE
. The association of TNIP1 was more pronounced in
SLE
patients with renal and immunological disorder, which is corroborated by two previous studies in Asian cohorts. The effects of all the associated SNPs, either conferring risk for or being protective against
SLE
, were in the same direction in Caucasians and Asians. The magnitudes of the allelic effects for most of the SNPs were also comparable across different ethnic groups. On the contrary, remarkable differences in allele frequencies between Caucasian and Asian populations were observed for all associated SNPs. In conclusion, most of the novel
SLE
risk loci identified by GWASs in Asian populations were also associated with
SLE
in Caucasian populations. We observed both similarities and differences with respect to the effect sizes and risk allele frequencies across ethnicities.
...
PMID:Genes identified in Asian SLE GWASs are also associated with SLE in Caucasian populations. 2324 52
Studies attempting to functionally interpret complex-disease susceptibility loci by GWAS and eQTL integration have predominantly employed microarrays to quantify gene-expression. RNA-Seq has the potential to discover a more comprehensive set of eQTLs and illuminate the underlying molecular consequence. We examine the functional outcome of 39 variants associated with
Systemic Lupus Erythematosus
(
SLE
) through the integration of GWAS and eQTL data from the TwinsUK microarray and RNA-Seq cohort in lymphoblastoid cell lines. We use conditional analysis and a Bayesian colocalisation method to provide evidence of a shared causal-variant, then compare the ability of each quantification type to detect disease relevant eQTLs and eGenes. We discovered the greatest frequency of candidate-causal eQTLs using exon-level RNA-Seq, and identified novel
SLE
susceptibility genes (e.g. NADSYN1 and TCF7) that were concealed using microarrays, including four non-coding RNAs. Many of these eQTLs were found to influence the expression of several genes, supporting the notion that risk haplotypes may harbour multiple functional effects. Novel
SLE
associated splicing events were identified in the T-reg restricted transcription factor, IKZF2, and other candidate genes (e.g.
WDFY4
) through asQTL mapping using the Geuvadis cohort. We have significantly increased our understanding of the genetic control of gene-expression in
SLE
by maximising the leverage of RNA-Seq and performing integrative GWAS-eQTL analysis against gene, exon, and splice-junction quantifications. We conclude that to better understand the true functional consequence of regulatory variants, quantification by RNA-Seq should be performed at the exon-level as a minimum, and run in parallel with gene and splice-junction level quantification.
...
PMID:Mapping eQTLs with RNA-seq reveals novel susceptibility genes, non-coding RNAs and alternative-splicing events in systemic lupus erythematosus. 2806 64
Genome-wide association studies have recently illuminated that
WDFY4
is genetically associated with
systemic lupus erythematosus
(
SLE
) susceptibility in various ethnic groups. Despite strong genetic evidence suggesting a role of
WDFY4
in
SLE
pathogenesis, its functional relevance is largely unknown. In this study, we generated
Wdfy4
B lymphocyte conditional knockout (
Wdfy4
-CKO) mice and found that loss of
Wdfy4
led to a decrease in number of total B cells and several subpopulations of B cells in the periphery and a defect in the transition from the pro- to pre-B cell stage in bone marrow. Also,
Wdfy4
-CKO mice showed impaired Ab responses as compared with controls when challenged with Ag.
SLE
phenotypes were effectively alleviated in
Wdfy4
-CKO mice, with significantly diminished pristane-elicited production of autoantibodies and glomerulonephritis. Genetic silencing of
WDFY4
in B cells increased lipidation of LC3 independent of p62 and Beclin1, which are essential proteins of canonical autophagy. Our in vivo and in vitro data suggest that
WDFY4
facilitates noncanonical autophagic activity. Our findings provide a novel functional link underlying the mechanism of
SLE
in which
WDFY4
influences B cell fate via noncanonical autophagy.
...
PMID:WDFY4 Is Involved in Symptoms of Systemic Lupus Erythematosus by Modulating B Cell Fate via Noncanonical Autophagy. 3025 84
