Sequencing XMET genes to promote genotype-guided risk assessment and precision medicine

  • Yaqiong Jin
  • , Geng Chen
  • , Wenming Xiao
  • , Huixiao Hong
  • , Joshua Xu
  • , Yongli Guo
  • , Wenzhong Xiao
  • , Tieliu Shi
  • , Leming Shi
  • , Weida Tong
  • , Baitang Ning*
  • *Corresponding author for this work

Research output: Contribution to journalReview articlepeer-review

5 Scopus citations

Abstract

High-throughput next generation sequencing (NGS) is a shotgun approach applied in a parallel fashion by which the genome is fragmented and sequenced through small pieces and then analyzed either by aligning to a known reference genome or by de novo assembly without reference genome. This technology has led researchers to conduct an explosion of sequencing related projects in multidisciplinary fields of science. However, due to the limitations of sequencing-based chemistry, length of sequencing reads and the complexity of genes, it is difficult to determine the sequences of some portions of the human genome, leaving gaps in genomic data that frustrate further analysis. Particularly, some complex genes are difficult to be accurately sequenced or mapped because they contain high GC-content and/or low complexity regions, and complicated pseudogenes, such as the genes encoding xenobiotic metabolizing enzymes and transporters (XMETs). The genetic variants in XMET genes are critical to predicate inter-individual variability in drug efficacy, drug safety and susceptibility to environmental toxicity. We summarized and discussed challenges, wet-lab methods, and bioinformatics algorithms in sequencing “complex” XMET genes, which may provide insightful information in the application of NGS technology for implementation in toxicogenomics and pharmacogenomics.

Original languageEnglish
Pages (from-to)895-904
Number of pages10
JournalScience China Life Sciences
Volume62
Issue number7
DOIs
StatePublished - 1 Jul 2019

Keywords

  • next generation sequencing
  • pharmacogenomics
  • precision medicine
  • toxicogenomics
  • xenobiotic metabolizing enzymes and transporters

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