Age-dependent variation of genotypes in MHC II transactivator gene (CIITA) in controls and association to type 1 diabetes

Gyllenberg, Alexandra; Asad, Samina; Piehl, Fredrik; Swanberg, Maria; Padyukov, Leonid; Yserloo, Brian Van; Rutledge, Elizabeth A.; McNeney, Brad; Graham, Jinko; Orho‐Melander, Marju; Lindholm, Eero; Graff, Caroline; Forsell, Charlotte; Åkesson, Karin; Landin‐Olsson, Mona; Carlsson, Annelie; Forsander, Gun; Ivarsson, Sten; Larsson, Helena; Lindblad, Bengt; Ludvigsson, Johnny; Marcus, Claude; Lernmark, Åke; Alfredsson, Lars; Olsson, Tomas; Kockum, Ingrid

doi:10.1038/gene.2012.44

Cited by 25 publications

(22 citation statements)

References 49 publications

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“…CIITA has been implicated in immune function through association with autoimmune diseases or very recently with leprosy (Liu et al 2015). The gene complex including CIITA and neighboring DEXI/CLEC16A has been shown to be associated with multiple autoimmune diseases (Bronson et al 2011; Gyllenberg et al 2012, 2014; Leikfoss et al 2015). DOCK2 is predominantly expressed in hematopoietic cells, regulates migration and activation of neutrophils through Rac activation (Nishikimi et al 2013) and is associated with early-onset invasive infections (Dobbs et al 2015).…”

Section: Discussionmentioning

confidence: 99%

Genome-wide Analysis in Brazilians Reveals Highly Differentiated Native American Genome Regions

et al. 2017

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Despite its population, geographic size, and emerging economic importance, disproportionately little genome-scale research exists into genetic factors that predispose Brazilians to disease, or the population genetics of risk. After identification of suitable proxy populations and careful analysis of tri-continental admixture in 1,538 North-Eastern Brazilians to estimate individual ancestry and ancestral allele frequencies, we computed 400,000 genome-wide locus-specific branch length (LSBL) Fst statistics of Brazilian Amerindian ancestry compared to European and African; and a similar set of differentiation statistics for their Amerindian component compared with the closest Asian 1000 Genomes population (surprisingly, Bengalis in Bangladesh). After ranking SNPs by these statistics, we identified the top 10 highly differentiated SNPs in five genome regions in the LSBL tests of Brazilian Amerindian ancestry compared to European and African; and the top 10 SNPs in eight regions comparing their Amerindian component to the closest Asian 1000 Genomes population. We found SNPs within or proximal to the genes CIITA (rs6498115), SMC6 (rs1834619), and KLHL29 (rs2288697) were most differentiated in the Amerindian-specific branch, while SNPs in the genes ADAMTS9 (rs7631391), DOCK2 (rs77594147), SLC28A1 (rs28649017), ARHGAP5 (rs7151991), and CIITA (rs45601437) were most highly differentiated in the Asian comparison. These genes are known to influence immune function, metabolic and anthropometry traits, and embryonic development. These analyses have identified candidate genes for selection within Amerindian ancestry, and by comparison of the two analyses, those for which the differentiation may have arisen during the migration from Asia to the Americas.

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Section: Discussionmentioning

confidence: 99%

Genome-wide Analysis in Brazilians Reveals Highly Differentiated Native American Genome Regions

et al. 2017

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“…GWAS and patient exome sequencing studies have linked SNPs in CIITA to celiac disease (238, 239), susceptibility to myocardial infarction (240), rheumatoid arthritis (240–242), multiple sclerosis (240, 242), primary adrenal insufficiency (243), SLE (244), and type 1 diabetes (245, 246), although these results have not always been replicated in subsequent studies (247–249). Gyllenberg et al suggested that age-dependent variation in the gene encoding CIITA could be responsible for false associations in GWAS (250).…”

Section: Non-inflammasome-forming Nlrsmentioning

confidence: 99%

Functions of NOD-Like Receptors in Human Diseases

Zhong¹,

Kinio²,

Saleh³

2013

Front. Immunol.

257

215

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Nucleotide-binding and oligomerization domain NOD-like receptors (NLRs) are highly conserved cytosolic pattern recognition receptors that perform critical functions in surveying the intracellular environment for the presence of infection, noxious substances, and metabolic perturbations. Sensing of these danger signals by NLRs leads to their oligomerization into large macromolecular scaffolds and the rapid deployment of effector signaling cascades to restore homeostasis. While some NLRs operate by recruiting and activating inflammatory caspases into inflammasomes, others trigger inflammation via alternative routes including the nuclear factor-κB, mitogen-activated protein kinase, and regulatory factor pathways. The critical role of NLRs in development and physiology is demonstrated by their clear implications in human diseases. Mutations in the genes encoding NLRP3 or NLRP12 lead to hereditary periodic fever syndromes, while mutations in CARD15 that encodes NOD2 are linked to Crohn’s disease or Blau’s syndrome. Genome-wide association studies (GWASs) have identified a number of risk alleles encompassing NLR genes in a host of diseases including allergic rhinitis, multiple sclerosis, inflammatory bowel disease, asthma, multi-bacillary leprosy, vitiligo, early-onset menopause, and bone density loss in elderly women. Animal models have allowed the characterization of underlying effector mechanisms in a number of cases. In this review, we highlight the functions of NLRs in health and disease and discuss how the characterization of their molecular mechanisms provides new insights into therapeutic strategies for the management of inflammatory pathologies.

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“…41 Chromosomal translocation of CIITA has been linked to primary mediastinal B-cell lymphoma and classical Hodgkin lymphoma. 42 Genetic variations in the CIITA gene have also been associated with several autoimmune disorders in humans, including RA, 13,15,16 MS, 13,17,18 myocardial infarction, 13 T1D, 19 coeliac disease 20 and systemic lupus erythematosus. 20,21 Different SNPs have been associated with these diseases, including rs3087456 in the type III promoter of CIITA, an intronic SNP rs8048002, and rs4774, which is a missense mutation resulting in an amino acid change from glycine to alanine.…”

Section: Discussionmentioning

confidence: 99%

“…13 It was later shown in the congenic strains in rats that the C2ta polymorphisms alter susceptibility to experimental autoimmune encephalomyelitis (EAE), a chronic relapsing model of MS. 14 The experimental findings in rats prompted further investigation of C2TA in humans and it was demonstrated that a single nucleotide polymorphism in the 5 0 flanking region of type III promoter of C2TA is associated with susceptibility to RA, MS and myocardial infarction. 13 C2TA disease association has since then been shown in different patient cohorts in not only RA 15,16 and MS, 17,18 but also T1D, 19 coeliac disease 20 and systemic lupus erythematosus, 21,22 although disease associations could not be reproduced in some populations. [23][24][25] In this study, we generated a C2ta congenic mouse strain to investigate the effect of an allelic variant of C2ta promoter on MHC-II expression in different antigen-presenting cells (APCs).…”

Section: M M U N O L O G Y O R I G I N a L A R T I C L Ementioning

confidence: 99%

“…The experimental findings in rats prompted further investigation of C2TA in humans and it was demonstrated that a single nucleotide polymorphism in the 5′ flanking region of type III promoter of C2TA is associated with susceptibility to RA, MS and myocardial infarction . C2TA disease association has since then been shown in different patient cohorts in not only RA and MS, but also T1D, coeliac disease and systemic lupus erythematosus, although disease associations could not be reproduced in some populations …”

Section: Introductionmentioning

confidence: 99%

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Effects of C2ta genetic polymorphisms on MHC class II expression and autoimmune diseases

et al. 2016

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Antigen presentation by the MHC-II to CD4 T cells is important in adaptive immune responses. The class II transactivator (CIITA in human and C2TA in mouse) is the master regulator of MHC-II gene expression. It coordinates the transcription factors necessary for the transcription of MHC-II molecules. In humans, genetic variations in CIITA have been associated with differential expression of MHC-II and susceptibility to autoimmune diseases. Here we made use of a C2ta congenic mouse strain (expressing MHC-II haplotype H-2 ) to investigate the effect of the natural genetic polymorphisms in type I promoter of C2ta on MHC-II expression and function. We demonstrate that an allelic variant in the type I promoter of C2ta resulted in an increased expression of MHC-II on macrophages (72-151% higher mean florescence intensity) and conventional dendritic cells (13-65% higher mean florescence intensity) in both spleen and peripheral blood. The increase in MHC-II expression resulted in an increase in antigen presentation to T cells in vitro and increased T-cell activation. The differential MHC-II expression in B6Q.C2ta, however, did not alter the disease development in models of rheumatoid arthritis (collagen-induced arthritis and human glucose-6-phosphate-isomerase -peptide-induced arthritis), or multiple sclerosis (MOG protein-induced and MOG peptide-induced experimental autoimmune encephalomyelitis). This is the first study to address the role of an allelic variant in type I promoter of C2ta in MHC-II expression and autoimmune diseases; and shows that C2ta polymorphisms regulate MHC-II expression and T-cell responses but do not necessarily have a strong impact on autoimmune diseases.

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Age-dependent variation of genotypes in MHC II transactivator gene (CIITA) in controls and association to type 1 diabetes

Cited by 25 publications

References 49 publications

Genome-wide Analysis in Brazilians Reveals Highly Differentiated Native American Genome Regions

Genome-wide Analysis in Brazilians Reveals Highly Differentiated Native American Genome Regions

Functions of NOD-Like Receptors in Human Diseases

Effects of C2ta genetic polymorphisms on MHC class II expression and autoimmune diseases

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