Frontiers in Medicine (Jul 2022)

Whole-Genome Sequencing Identified KCNJ12 and SLC25A5 Mutations in Port-Wine Stains

  • Kai Chen,
  • Kai Chen,
  • Yan-Yan Hu,
  • Lin-Lin Wang,
  • Yun Xia,
  • Qian Jiang,
  • Lan Sun,
  • Shan-Shan Qian,
  • Shan-Shan Qian,
  • Jin-Zhao Wu,
  • Jin-Zhao Wu,
  • Liu-Qing Chen,
  • Liu-Qing Chen,
  • Dong-Sheng Li,
  • Dong-Sheng Li

DOI
https://doi.org/10.3389/fmed.2022.905902
Journal volume & issue
Vol. 9

Abstract

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Port-wine stains (PWSs) are a congenital capillary malformed disorder and are caused by a number of somatic mutations that disrupt vascular development. However, the underlying genetic mutations in the pathogenesis of PWS have not yet been fully elucidated. To understand PWS genetic variations and investigate novel genetic mutations, we extracted genomic DNA from four sporadic PWS patients and then performed whole-genome sequencing (WGS). Using Sorting Intolerant from Tolerant (SIFT), PolyPhen2, Mutation Assessor, MetaSVM to identify candidate genetic mutations and whole-exome sequencing (WES) to confirm the identified variants. We found a previously reported G protein subunit alpha q (GNAQ) mutation c.548G > A, p.Arg183Gln in one case, whereas no such mutation was found in the other three samples. Moreover, six novel somatic mutations in three genes, including KCNJ12, SLC25A5, POTEE, were found in these four samples. Importantly, WES also verified the KCNJ12 (c.433G > A, p.Gly145Ser) and SLC25A5 (c.413G > A, p.Arg138His) mutations in other five sporadic PWS patients, with the frequency of 60% (3 of 5) and 40% (2 of 5), respectively. Thus, we reveal in this study two novel somatic mutations, KCNJ12 and SLC25A5, in the sporadic PWS patients for the first time. These findings highlight the genetic polymorphism of PWS and provide potential clinical prediction targets for this disease.

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