2002
DOI: 10.1016/s0198-8859(02)00377-4
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Linkage disequilibrium and age estimates of a deletion polymorphism (1597ΔC) in HLA-G suggest non-neutral evolution

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Cited by 58 publications
(44 citation statements)
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“…The deletion of nucleotide 1597 in exon 3 does not cause a total failure of the protein to perform its function, rather it changes its morphology to resemble a class II MHC molecule rather than a class I molecule, to which it is evolutionarily related. Aldrich et al (2002) hypothesize that the 1597⌬C is a recent mutation and has achieved a high frequency due to the action of positive selection. If the mutation is recent, one expects that it would be in strong disequilibrium with flanking markers, whereas no such association would exist with older mutations that occur at the same frequency.…”
Section: Linkage Disequilibriummentioning
confidence: 99%
“…The deletion of nucleotide 1597 in exon 3 does not cause a total failure of the protein to perform its function, rather it changes its morphology to resemble a class II MHC molecule rather than a class I molecule, to which it is evolutionarily related. Aldrich et al (2002) hypothesize that the 1597⌬C is a recent mutation and has achieved a high frequency due to the action of positive selection. If the mutation is recent, one expects that it would be in strong disequilibrium with flanking markers, whereas no such association would exist with older mutations that occur at the same frequency.…”
Section: Linkage Disequilibriummentioning
confidence: 99%
“…First, assuming neutrality and an infinite allele model, mean allele age and an MLE of allele age and its approximate confidence interval were estimated from the observed allele frequencies in the sample following Griffiths (2003) and Slatkin and Rannala (2000). Allele age estimates were also obtained using the approach outlined in Aldrich et al (2002) and Toomajian et al (2003). The basic idea is to estimate an allele's age by the decay of ancestral haplotype sharing (DHS, McPeek and Strahs, 1999).…”
Section: Dna Sequence Analysismentioning
confidence: 99%
“…Given the putative role of HLA-G in placental development, it has been proposed that the G*0105N allele is maintained in high frequency in some populations by non-neutral evolutionary forces [10]. The highest frequencies of G*0105N in geographic areas with a historically high pathogen load suggest that intrauterine pathogens may act as selective agents, increasing survival of heterozygous fetuses carrying the G*0105N allele in infected pregnancies (balancing selection).…”
Section: Introductionmentioning
confidence: 99%
“…The highest frequencies of G*0105N in geographic areas with a historically high pathogen load suggest that intrauterine pathogens may act as selective agents, increasing survival of heterozygous fetuses carrying the G*0105N allele in infected pregnancies (balancing selection). In this case, the reduced HLA-G1 expression in G*0105N heterozygous placentas may result in an overall increase in the number of T cells available in the uterus and reverse the inhibition of NK cells, improving the intrauterine defense against infections [10,18]. The survival of healthy individuals homozygous for the G*0105N allele [7,18,19] that do not express the G1, G4, and G5 soluble isoforms suggest that such isoforms are not essential for fetal survival in uncomplicated pregnancies [10,20].…”
Section: Introductionmentioning
confidence: 99%
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