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HLA-G genetic diversity and evolutive aspects in worldwide populations.

Erick da Cruz CastelliBibiana S de AlmeidaYara C N MunizNayane S B SilvaMarília R S PassosAndreia S SouzaAbigail E PageMark DybleDaniel SmithGabriela AguiletaJaume BertranpetitAndrea B MiglianoYeda A O DuarteMarília O ScliarJaqueline WangMaria Rita Passos-BuenoMichel S NaslavskyMayana ZatzCelso Teixeira Mendes-JuniorEduardo A Donadi
Published in: Scientific reports (2021)
HLA-G is a promiscuous immune checkpoint molecule. The HLA-G gene presents substantial nucleotide variability in its regulatory regions. However, it encodes a limited number of proteins compared to classical HLA class I genes. We characterized the HLA-G genetic variability in 4640 individuals from 88 different population samples across the globe by using a state-of-the-art method to characterize polymorphisms and haplotypes from high-coverage next-generation sequencing data. We also provide insights regarding the HLA-G genetic diversity and a resource for future studies evaluating HLA-G polymorphisms in different populations and association studies. Despite the great haplotype variability, we demonstrated that: (1) most of the HLA-G polymorphisms are in introns and regulatory sequences, and these are the sites with evidence of balancing selection, (2) linkage disequilibrium is high throughout the gene, extending up to HLA-A, (3) there are few proteins frequently observed in worldwide populations, with lack of variation in residues associated with major HLA-G biological properties (dimer formation, interaction with leukocyte receptors). These observations corroborate the role of HLA-G as an immune checkpoint molecule rather than as an antigen-presenting molecule. Understanding HLA-G variability across populations is relevant for disease association and functional studies.
Keyphrases
  • genetic diversity
  • genome wide
  • dna methylation
  • gene expression
  • case report
  • hepatitis c virus
  • human immunodeficiency virus
  • hiv infected
  • big data