Maternal KIR in Combination with Paternal HLA-C2 Regulate Human Birth Weight
2014; American Association of Immunologists; Volume: 192; Issue: 11 Linguagem: Inglês
10.4049/jimmunol.1400577
ISSN1550-6606
AutoresSusan E. Hiby, Richard Apps, Olympe Chazara, Lydia Farrell, Per Magnus, Lill Trogstad, Håkon K. Gjessing, Mary Carrington, Ashley Moffett,
Tópico(s)Reproductive Physiology in Livestock
ResumoAbstract Human birth weight is subject to stabilizing selection; babies born too small or too large are less likely to survive. Particular combinations of maternal/fetal immune system genes are associated with pregnancies where the babies are ≤5th birth weight centile, specifically an inhibitory maternal KIR AA genotype with a paternally derived fetal HLA-C2 ligand. We have now analyzed maternal KIR and fetal HLA-C combinations at the opposite end of the birth weight spectrum. Mother/baby pairs (n = 1316) were genotyped for maternal KIR as well as fetal and maternal HLA-C. Presence of a maternal-activating KIR2DS1 gene was associated with increased birth weight in linear or logistic regression analyses of all pregnancies >5th centile (p = 0.005, n = 1316). Effect of KIR2DS1 was most significant in pregnancies where its ligand, HLA-C2, was paternally but not maternally inherited by a fetus (p = 0.005, odds ratio = 2.65). Thus, maternal KIR are more frequently inhibitory with small babies but activating with big babies. At both extremes of birth weight, the KIR associations occur when their HLA-C2 ligand is paternally inherited by a fetus. We conclude that the two polymorphic immune gene systems, KIR and HLA-C, contribute to successful reproduction by maintaining birth weight between two extremes with a clear role for paternal HLA.
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