2009
DOI: 10.1016/j.humimm.2009.02.001
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CR1 levels and gene polymorphisms exhibit differential association with falciparum malaria in regions of varying disease endemicity

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Cited by 37 publications
(53 citation statements)
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“…15 This allele has been associated with a multifold reduction of the level of CR1 in multiple studies of subjects with European ancestry, [15][16][17][18] and also in South Asian and East Asian population groups. 19,20 Previous studies in Europeans have also found that this haplotype also contains the rs3738467 T allele (Gln981His), an allele that is associated with decreased CR1 in European, East Asian and Papua New Guineans. 15,19,21 Other studies have also identified additional amino acid variants, including the Ile1574Val (rs669117 G allele), as part of this haplotype.…”
Section: Introductionmentioning
confidence: 97%
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“…15 This allele has been associated with a multifold reduction of the level of CR1 in multiple studies of subjects with European ancestry, [15][16][17][18] and also in South Asian and East Asian population groups. 19,20 Previous studies in Europeans have also found that this haplotype also contains the rs3738467 T allele (Gln981His), an allele that is associated with decreased CR1 in European, East Asian and Papua New Guineans. 15,19,21 Other studies have also identified additional amino acid variants, including the Ile1574Val (rs669117 G allele), as part of this haplotype.…”
Section: Introductionmentioning
confidence: 97%
“…21,23 Importantly, the rs2274567 G allele that is within the dominant Sardinian haplotype has been found at much higher frequency in malaria endemic than in non-endemic regions of India. 20 Recently, Tham et al 14 have provided strong evidence that CR1 is the host erythrocyte receptor for the reticulocyte-binding-like homolog protein PfRh4, a major P. falciparum ligand that is essential for sialic-acidindependent invasion. Moreover, the exon 22 polymorphism (rs2274567 G allele) is associated with a decreased sialic-acid-independent malarial invasion of erythrocytes.…”
Section: Introductionmentioning
confidence: 99%
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“…Another study (Cockburn et al 2004) in Caucasians provided evidence that heterozygotes for the CR1 low-expression allele (HL) are significantly protected from severe malaria, while homozygotes LL have reduced risk compared with HH homozygotes; however, this did not reach statistical significance. A recent study (Sinha et al 2009) analyzed CR1 polymorphisms in Indian populations living in endemic and non-endemic malaria areas. Results showed that of the three CR1 SNPs analyzed, only exon 22 and intron 27 SNPs were found to be associated with susceptibility to malaria.…”
Section: Malariamentioning
confidence: 99%
“…The soluble form of CR1 differs from the surface form only in the cytoplasmic part of the protein at the C-terminus, removed through the proteolytic cleavage of the transmembrane protein [76]. Research has associated CR1 to a number of diseases such as autoimmune disorders [77], systemic lupus erythematosus [78][79][80][81], rheumatoid arthritis [81,82], malaria [83], atopic dermatitis [84], HIV infection [85]. Expression of CR1 has been shown to be regulated by cytokines and immune complexes in diseases (reviewed by Khera and Das, 2009 [73, 86]).…”
Section: Cr1mentioning
confidence: 99%