Variation analysis and gene annotation of eight MHC haplotypes: The MHC Haplotype Project

Horton, Roger W.; Gibson, Richard L.; Coggill, Penny; Miretti, Marcos Mateo; Allcock, Richard; Almeida, J. P.; Forbes, Simon; Gilbert, James; Halls, Karen; Harrow, Jennifer; Hart, Elizabeth A.; Howe, Kevin; Jackson, David; Palmer, Sophie; Roberts, A N; Sims, Sarah; Stewart, Claudia; Traherne, James A.; Trevanion, Stephen J.; Wilming, Laurens G.; Rogers, Jane; Jong, Pieter J. de; Elliott, John F.; Sawcer, Stephen; Todd, John A.; Trowsdale, John; Beck, Stephan

doi:10.1007/s00251-007-0262-2

Cited by 288 publications

(267 citation statements)

References 50 publications

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“…Otherwise, we have found that telomeric C4 genes of multimodular structures usually code for a C4A isotype protein, which is in agreement with previous assumptions deducted from sparse sequencing data 2 and results of the MHC Haplotype Project. 20 Here we also give evidence of the assumption that C4A genes are almost always long and that there is an approximately equal chance that a C4B gene belongs to the short or the long variant. 21 Former RCCX-related studies sometimes also detected dosage ratios of TNX and CYP21 active genes and pseudogenes.…”

Section: (L)-b(s)-b(s) and B(l)-a(s)-b(s)mentioning

confidence: 54%

Fine-tuned characterization of RCCX copy number variants and their relationship with extended MHC haplotypes

et al. 2012

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The human RCCX is a common multiallelic copy number variation locus whose number of segments varies between one and four in a chromosome. The monomodular form normally comprises four functional genes, but in duplicated RCCX segments generally only the gene-encoding complement component C4 produces a protein. C4 genes can code either for a C4A or a C4B isotype protein and exhibit dichotomous size variation. Distinct RCCX variants show association with numerous diseases; however, identification of the basis of these associations is often challenging, not least because the RCCX is localized in the major histocompatibility complex (MHC) region, a genomic area characterized by exceedingly long-range linkage disequilibrium. Here we present a detailed analysis on RCCX variants and their relationship with so-called 'ancestral' or 'conserved extended' MHC haplotypes in healthy Caucasians. In addition to former investigations, precise order and size of all C4A and C4B genes were determined even in trimodular RCCX structures. Considering C4 copy numbers, length, isotype specificity and CYP21A2 copy numbers, we have identified 15 distinct RCCX variants and described the RCCX structures involved in 29 repeatedly occurring MHC haplotypes. The findings should become a useful tool for future RCCX-and MHC-related disease association studies.

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Section: (L)-b(s)-b(s) and B(l)-a(s)-b(s)mentioning

confidence: 54%

Fine-tuned characterization of RCCX copy number variants and their relationship with extended MHC haplotypes

et al. 2012

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“…Many of the HLA alleles were first identified serologically and gave rise to a complex and often inconsistent nomenclature. Recent extensive efforts were made at mapping the serologic types to DNA sequences and the genetic architecture of the MHC is now much better understood (Allcock et al, 2002;Stewart et al, 2004;Miretti et al, 2005;de Bakker et al, 2006;Horton et al, 2008). As a consequence, the genetic basis of the serotypes has been defined and a consistent nomenclature has finally come into focus that will help advance further study of the MHC (http:/ /hla.alleles.org/).…”

Section: The Mhc and Ms Susceptibilitymentioning

confidence: 99%

Multiple sclerosis genetics

Cree

2014

Handbook of Clinical Neurology

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“…155 Similarly, several other class II loci including HLA-DRB1 and HLA-DQA1 are known to show haplotypic variation at splice sites, which may affect expression at a post-transcriptional level. 156 A growing number of reports highlight the role of DNA sequence variation in modulating alternative splicing, which can contribute to disease susceptibility. 157 The MHC class II region has already provided one of the clearest examples of a SNP modulating alternative splicing resulting in common disease through the work of Valentonyte et al (2005) 158 on genetic determinants of sarcoidosis, a chronic granulomatous condition.…”

Section: Mhc Class II Expression Polymorphism and Disease L Handunnementioning

confidence: 99%

Regulation of major histocompatibility complex class II gene expression, genetic variation and disease

et al. 2009

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Major histocompatibility complex (MHC) class II molecules are central to adaptive immune responses and maintenance of selftolerance. Since the early 1970s, the MHC class II region at chromosome 6p21 has been shown to be associated with a remarkable number of autoimmune, inflammatory and infectious diseases. Given that a full explanation for most MHC class II disease associations has not been reached through analysis of structural variation alone, in this review we examine the role of genetic variation in modulating gene expression. We describe the intricate architecture of the MHC class II regulatory system, indicating how its unique characteristics may relate to observed associations with disease. There is evidence that haplotypespecific variation involving proximal promoter sequences can alter the level of gene expression, potentially modifying the emergence and expression of key phenotypic traits. Although much emphasis has been placed on cis-regulatory elements, we also examine the role of more distant enhancer elements together with the evidence of dynamic inter-and intra-chromosomal interactions and epigenetic processes. The role of genetic variation in such mechanisms may hold profound implications for susceptibility to common disease.

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Variation analysis and gene annotation of eight MHC haplotypes: The MHC Haplotype Project

Cited by 288 publications

References 50 publications

Fine-tuned characterization of RCCX copy number variants and their relationship with extended MHC haplotypes

Fine-tuned characterization of RCCX copy number variants and their relationship with extended MHC haplotypes

Multiple sclerosis genetics

Regulation of major histocompatibility complex class II gene expression, genetic variation and disease

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