Contribution of rare whole-genome sequencing variants to plasma protein levels and the missing heritability
Nature Communications, 2022
Kierczak M., Rafati N., Höglund J., Gourlé H., Lo Faro V., Schmitz D., Ek W., Gyllensten U., Enroth S., Ekman D., Nystedt B., Karlsson T., Johansson ?.
Disease area | Application area | Sample type | Products |
---|---|---|---|
Wider Proteomics Studies | Technical Evaluation | Plasma | Olink Target 96 |
Abstract
Despite the success of genome-wide association studies, much of the genetic contribution to complex traits remains unexplained. Here, we analyse high coverage whole-genome sequencing data, to evaluate the contribution of rare genetic variants to 414 plasma proteins. The frequency distribution of genetic variants is skewed towards the rare spectrum, and damaging variants are more often rare. We estimate that less than 4.3% of the narrow-sense heritability is expected to be explained by rare variants in our cohort. Using a gene-based approach, we identify Cis-associations for 237 of the proteins, which is slightly more compared to a GWAS (N = 213), and we identify 34 associated loci in Trans. Several associations are driven by rare variants, which have larger effects, on average. We therefore conclude that rare variants could be of importance for precision medicine applications, but have a more limited contribution to the missing heritability of complex diseases.