Genetics of complement proteins among Swedish newborns

Sammanfattning: Complement proteins play an important role in the body's immune processes and involve in the pathology of many diseases in human, such as major depressive disorder and schizophrenia. Understanding the genetics of those proteins is an important step toward unraveling their effects on psychiatric disorders.  The complement protein levels differ between neonates and adults. There are many studies investigating the genetic architecture of the complement proteins, but evidence about the genetics of neonatal complement proteins is scarce. In this study, I investigated the SNPs and haplotypes that are associated with the five complement proteins, C1q, C3, C4, CFB, and CFH among newborns. I also compared the effects of the identified SNPs among neonates and adults. This study uses 75 samples from Swedish newborns whose blood were primarily collected for Phenylketonuria screening. Genotype data and protein levels were measured from dried blood spots. To investigate the genetics of the complement proteins, I first conducted single SNPs association analyses. The single SNPs used in this study was derived from previous research of European adult samples and has been shown to be significantly associated with the target protein. Then, after imputing the SNPs for the MHC region, I conducted haplotype analysis in the MHC region for the five complement proteins. Finally, I compared the effects of the variants identified in the single SNPs association analysis with the effects that were reported for adult protein levels in previous studies. The results of single SNP association analysis showed that among the 14 SNPs that were associated with adult protein levels, SNP rs4151669 that associated with complement factor B (CFB) was significantly associated with the target protein in the neonatal population. Some SNPs (rs8283, rs4151669 and rs10737680) may have opposite effects in the two populations. This study found 86 haplotypes potentially associated with the complement proteins. Among them, the haplotype “H840” which located at chr6:32594217-32597172 was significantly associated with five complement proteins. This study provides evidence for the genetic component of the 5 complement protein levels among neonates. The results also suggested that the genetic influence of the complement protein among adult and neonatal population are different.