Investigation of a nonsense mutation located in the complex KIV-2 copy number variation region of apolipoprotein(a) in 10,910 individuals.
Silvia Di MaioRebecca GrüneisGertraud StreiterClaudia LaminaManuel MaglioneSebastian SchoenherrDietmar ÖfnerBarbara ThorandAnnette PetersKai-Uwe EckardtAnna KöttgenFlorian KronenbergStefan CoassinPublished in: Genome medicine (2020)
We performed the largest epidemiological study on an LPA KIV-2 variant so far, showing that it is possible to assess LPA KIV-2 mutations on a large scale. Surprisingly, in all analyzed populations, R21X was located on the same haplotype as the splice mutation rs41272114, creating "double-null" LPA alleles. Despite being a nonsense variant, the R21X status does not provide additional information beyond the rs41272114 genotype. This has important implications for studies using LPA loss-of-function mutations as genetic instruments and emphasizes the complexity of LPA genetics.