3.9 Article

Association of soluble HLA-G plasma levels with HLA-G alleles

期刊

TISSUE ANTIGENS
卷 57, 期 1, 页码 15-21

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MUNKSGAARD INT PUBL LTD
DOI: 10.1034/j.1399-0039.2001.057001015.x

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soluble HLA-G; HLA-G polymorphism; low sHLA-G secretor allele; high sHLA-G secretor allele

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Soluble HLA-G (sHLA-G) molecules are found in the peripheral blood of healthy females and males, in cord blood and in amniotic fluids and discussed to be a mediator in maternal-fetal tolerance. In this study we investigated whether there are allele-specific differences in expression of sHLA-G molecules. For this, the sHLA-G plasma concentrations of 94 healthy unrelated individuals were measured by ELISA and correlated to their HLA-G genotypes, as determined by sequence analysis of exon 2 and 3 of the HLA-G gene. Mean sHLA-G levels in individuals with the most common HLA-G alleles G*01011 (27.0+/-2.1 SEM ng/ml, n=66), G*01012 (28.4+/-3.2 SEM ng/ml, n=34) were very similar. In contrast, individuals carrying the HLA-G*01013 (8.1+/-1.7 SEM ng/ml, n=17) or the null allele HLA-G*0105N (8.2+/-3.2 SEM ng/ml, n=7) presented significantly (P-c=0.001 and P-c<0.01, resp.) reduced sHLA-G levels. Furthermore, individuals with the HLA-G*01041 allele had significantly (P-c=0.004) increased sHLA-G levels (42.5+/-4.6 SEM ng/ml, n=14). These results demonstrate that the generation of sHLA-G molecules is associated to certain HLA-G alleles and imply that sHLA-G levels are under genetic control. As low and high sHLA-G plasma levels did not segregate with HLA haplotypes including the HLA-G*01013 or *01041 allele, additional mechanisms may be involved in the regulation of the individual sHLA-G levels. Nevertheless, the existence of low and high secretor HLA-G alleles further suggests different levels of functionality in immune regulation.

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