Advanced Science (Oct 2020)

SETD8C302R Mutation Revealed from Myofibroblastoma‐Discordant Monozygotic Twins Leads to p53/p21 Deficit and WEE1 Inhibitor Sensitivity

  • Miao Li,
  • Hongwu Wang,
  • Hongwei Liao,
  • Jiaxin Shen,
  • Yinfang Wu,
  • Yanping Wu,
  • Qingyu Weng,
  • Chen Zhu,
  • Xinwei Geng,
  • Fen Lan,
  • Yang Xia,
  • Bin Zhang,
  • Hang Zou,
  • Nan Zhang,
  • Yunzhi Zhou,
  • Zhihua Chen,
  • Huahao Shen,
  • Songmin Ying,
  • Wen Li

DOI
https://doi.org/10.1002/advs.202001041
Journal volume & issue
Vol. 7, no. 19
pp. n/a – n/a

Abstract

Read online

Abstract High‐throughput gene sequencing has identified various genetic variants as the culprits for some common hereditary cancers. However, the heritability of a substantial proportion of cancers remains unexplained, which may result from rare deleterious mutations hidden in a myriad of nonsense genetic variations. This poses a great challenge to the understanding of the pathology and thus the rational design of effective treatments for affected patients. Here, whole genome sequencing is employed in a representative case in which one monozygotic twin is discordant for lung inflammatory myofibroblastoma to disclose rare tumor‐related mutations. A missense single nucleotide variation rs61955126 T>C in the lysine methyltransferase SETD8 (accession: NM_020382, SETD8C302R) is exposed. It is shown that SETD8 is vital for genomic integrity by promoting faithful DNA replication, and its C302R mutation downregulates the p53/p21 pathway. Importantly, the SETD8C302R mutation significantly increases the sensitivity of cancer cells to WEE1 inhibition. Given that WEE1 inhibitors have shown great promise for clinical approval, these results impart a potential therapeutic approach using WEE1 inhibitor for cancer patients carrying the same mutation, and indicate that genome sequencing and genetic functional studies can be integrated into individualized therapies.

Keywords