Duplication, mutation and recombination of the human orphan gene KIR2DS3 contribute to the diversity of KIR haplotypes

Ordóñez, David; Meenagh, Ashley; Gómez‐Lozano, Natalia; Castaño, J; Middleton, Derek; Vilches, Carlos

doi:10.1038/gene.2008.34

Cited by 42 publications

(59 citation statements)

References 34 publications

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“…The reason for this is that without determining copy number or defining alleles, ascertainment of the gene arrangements on these haplotypes can be obscured by variation in KIR gene content of the partnering chromosome, even with pedigrees to track gene transmission . Six of the uncommon gene combinations (haplotypes 12, 13, 14, 15, 18, and 33) appeared to match recombinant haplotypes reported previously by us and others (Gomez-Lozano et al 2003, 2005Martin et al 2003;Ordonez et al 2008Ordonez et al , 2011Traherne et al 2010). Using published methods for detecting hybrid genes (e.g., 2DL5/3DP1 [3DP1*004], 2DS2/2DS3 [2DS2*005], and 2DL3/2DP1) and specific alleles associated with these recombinant haplotypes, we were able to Gene copy number varies from zero to three copies on a single haplotype.…”

Section: Many Kir Haplotypes Exhibit Novel Structural Variationmentioning

confidence: 49%

“…For example, the haplotype motif tA01 may have either form of 2DS4 (2DS4f or 2DS4v), and tB01 may have either variant of 2DS3S5 (2DS3 or 2DS5). T and C suffixes for 2DL5 (2DL5A or 2DL5B) and 2DS3S5 indicate the telomeric and centromeric versions of the genes, respectively (Gomez-Lozano et al 2002;Ordonez et al 2008;Pyo et al 2010). For simplicity, 2DS1 and 2DS4 are shown at the same site because they showed a mutually exclusive relationship.…”

Section: Disease Analyses Can Be Simplified But Current Kir Typing Imentioning

confidence: 99%

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Copy number variation leads to considerable diversity for B but not A haplotypes of the human KIR genes encoding NK cell receptors

et al. 2012

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The KIR complex appears to be evolving rapidly in humans, and more than 50 different haplotypes have been described, ranging from four to 14 KIR loci. Previously it has been suggested that most KIR haplotypes consist of framework genes, present in all individuals, which bracket a variable number of other genes. We used a new technique to type 793 families from the United Kingdom and United States for both the presence/absence of all individual KIR genes as well as copy number and found that KIR haplotypes are even more complex. It is striking that all KIR loci are subject to copy number variation (CNV), including the so-called framework genes, but CNV is much more frequent in KIR B haplotypes than KIR A haplotypes. These two basic KIR haplotype groups, A and B, appear to be following different evolutionary trajectories. Despite the great diversity, there are 11 common haplotypes, derived by reciprocal recombination near KIR2DL4, which collectively account for 94% of KIR haplotypes determined in Caucasian samples. These haplotypes could be derived from combinations of just three centromeic and two telomeric motifs, simplifying disease analysis for these haplotypes. The remaining 6% of haplotypes displayed novel examples of expansion and contraction of numbers of loci. Conventional KIR typing misses much of this additional complexity, with important implications for studying the genetics of disease association with KIR that can now be explored by CNV analysis.

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Section: Many Kir Haplotypes Exhibit Novel Structural Variationmentioning

confidence: 49%

Section: Disease Analyses Can Be Simplified But Current Kir Typing Imentioning

confidence: 99%

Copy number variation leads to considerable diversity for B but not A haplotypes of the human KIR genes encoding NK cell receptors

et al. 2012

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“…To rule out this possibility and, also, to map KIR2DS2*005 in the unusual haplotype, we studied its arrangement through analysis of the genes flanking KIR2DS2*005. Using a KIR-gene walking approach, 11 we found KIR2DS2*005 downstream of KIR3DL3, the normal arrangement of these two genes. On the contrary, we found that KIR2DS2 was followed not by KIR2DL2 as it happens in most haplotypes, but by the KIR2DP1 pseudogene, from which KIR2DS2 is normally separated by three KIR genes (Figure 1).…”

Section: Resultsmentioning

confidence: 99%

“…Genetic features of KIR2DS2*005 In a previous study on KIR-B haplotypes, we identified a healthy Caucasoid woman carrying KIR2DS2*005, 11 an uncommon allele with a hybrid primary structure. KIR-gene segregation in her sibling revealed that KIR2DS2*005 was inherited in a KIR haplotype that lacked a KIR2DL2 gene (Figure 1), whereas its central and telomeric regions were characteristic of B haplotypes (KIR 3DP1-2DL4-3DS1-2DL5A*001-2DS5-2DS1-3DL2).…”

Section: Resultsmentioning

confidence: 99%

“…Generic KIR typing, allelic KIR2DL5 and KIR2DS3 typing, and long-range PCR for initial KIR2DS2*005 identification were done as described. 11,19,20 A new PCR-SSP method for specific detection of KIR2DS2*005 was designed: genomic DNA was amplified using 0.2 U of BioTaq DNA polymerase (Bioline, London, UK), and primers Fi6a þ 3019b (forward, The KIR genes flanking KIR2DS2*005 in donor C180F2 genomic DNA were determined using KIR-gene walking protocols similar to those we have reported previously DNA sequencing. All PCR products were submitted to direct nucleotide sequencing with no cloning step.…”

Section: Genetic Analysesmentioning

confidence: 99%

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Molecular characterisation of KIR2DS2*005, a fusion gene associated with a shortened KIR haplotype

et al. 2011

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KIR2DS2 is an activating homologue of KIR2DL2, an inhibitory killer-cell immunoglobulin-like receptor (KIR) that surveys expression of major histocompatibility complex-C allotypes bearing a C1 epitope. We have studied here its allele KIR2DS2 *005, which shows a hybrid structure-it is identical to other KIR2DS2 alleles in the ectodomain, but has transmembrane and cytoplasmic regions identical to those of KIR2DS3*001, a short-tailed KIR of uncertain expression and function. Our results reveal that KIR2DS2 *005 is a fusion gene-the product of an unequal crossing over by which the genes KIR2DS2 and KIR2DS3 recombined within a 400 base pair region of complete identity in intron 6. Also resulting from that recombination was a shortened KIR haplotype of the B group, in which three genes commonly linked to KIR2DS2 (KIR2DL2, KIR2DL5B and KIR2DS3) are deleted. Population studies indicate that KIR2DS2 *005 is still associated to such haplotype, and it can be found in approximately 1.2% of Caucasoids. Using a combination of two monoclonal antibodies, we also demonstrate that KIR2DS2 *005 encodes a molecule expressed on the surface of natural killer-and T-lymphocytes.

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Overview of the Killer Cell Immunoglobulin-Like Receptor System

Rajalingam

2012

Methods in Molecular Biology

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Natural killer (NK) cells are more than simple killers and have been implicated in control and clearance of malignant and virally infected cells, regulation of adaptive immune responses, rejection of bone marrow transplants, and autoimmunity and the maintenance of pregnancy. Human NK cells largely use a family of germ-line encoded killer cell immunoglobulin-like receptors (KIR) to respond to the perturbations from self-HLA class I molecules present on infected, malignant, or HLA-disparate fetal or allogenic transplants. Genes encoding KIR receptors and HLA class I ligands are located on different chromosomes, and both feature extraordinary diversity in the number and type of genes. The independent segregation of KIR and HLA gene families produce diversity in the number and type of KIR-HLA gene combinations inherited in individuals, which may determine their immunity and susceptibility to diseases. This chapter provides an overview of NK cells and their unprecedented phenotypic and functional diversity within and between individuals.

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Duplication, mutation and recombination of the human orphan gene KIR2DS3 contribute to the diversity of KIR haplotypes

Cited by 42 publications

References 34 publications

Copy number variation leads to considerable diversity for B but not A haplotypes of the human KIR genes encoding NK cell receptors

Copy number variation leads to considerable diversity for B but not A haplotypes of the human KIR genes encoding NK cell receptors

Molecular characterisation of KIR2DS2*005, a fusion gene associated with a shortened KIR haplotype

Overview of the Killer Cell Immunoglobulin-Like Receptor System

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