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Genetic admixture predictors of fetal alcohol spectrum disorders (FASD) in a South African population. | LitMetric

Genetic admixture predictors of fetal alcohol spectrum disorders (FASD) in a South African population.

Gene

Department of Neurology and the Taub Institute for Research on Alzheimer's Disease and the Aging Brain, Columbia University Vagelos College of Physicians and Surgeons, Columbia University Irving Medical Center, New York, NY, USA. Electronic address:

Published: December 2024

AI Article Synopsis

  • Ancestrally admixed populations, like the South African Cape Coloured (SACC), are underrepresented in genetic studies of complex diseases, which typically focus on European-descent populations, leading to a lack of understanding of their unique genetic features.
  • The study examined the genetic admixture and its associations with fetal alcohol spectrum disorders (FASD) in the SACC population, using data from two longitudinal birth cohorts that looked at prenatal alcohol exposure effects on development.
  • Findings revealed a high prevalence of rare genetic variants and significant associations between ancestry profiles and FASD outcomes, suggesting that the SACC population could provide insights for identifying disease-associated genetic loci in FASD and potentially other conditions.

Article Abstract

Ancestrally admixed populations are underrepresented in genetic studies of complex diseases, which are still dominated by European-descent populations. This is relevant not only from a representation standpoint but also because of admixed populations' unique features, including being enriched for rare variants, for which effect sizes are disproportionately larger than common polymorphisms. Furthermore, results from these populations may be generalizable to other populations. The South African Cape Coloured (SACC) population is genetically admixed and has one of the highest prevalences of fetal alcohol spectrum disorders (FASD) worldwide. We profiled its admixture and examined associations between ancestry profiles and FASD outcomes using two longitudinal birth cohorts (N=308 mothers, 280 children) designed to examine effects of prenatal alcohol exposure on development. Participants were genotyped via MEGAex array to capture common and rare variants. Rare variants were overrepresented in our SACC cohorts, with numerous polymorphisms being monomorphic in other reference populations (e.g., ∼30,000 and ∼ 221,000 variants in gnomAD European and Asian populations, respectively). The cohorts showed global African (51 %; Bantu and San); European (26 %; Northern/Western); South Asian (18 %); and East Asian (5 %; largely Southern regions) ancestries. The cohorts exhibited high rates of homozygosity (6 %), with regions of homozygosity harboring more deleterious variants when lying within African local-ancestry genomic segments. Both maternal and child ancestry profiles were associated with higher FASD risk, and maternal and child ancestry-by-prenatal alcohol exposure interaction effects were seen on child cognition. Our findings indicate that the SACC population may be a valuable asset to identify novel disease-associated genetic loci for FASD and other diseases.

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Source
http://dx.doi.org/10.1016/j.gene.2024.148854DOI Listing

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