Multiple approaches for massively parallel sequencing of HCoV-19 (SARS-CoV-2) genomes directly from clinical samples

  1. Minfeng Xiao
  2. Xiaoqing Liu
  3. Jingkai Ji
  4. Min Li
  5. Jiandong Li
  6. Lin Yang
  7. Wanying Sun
  8. Peidi Ren
  9. Guifang Yang
  10. Jincun Zhao
  11. Tianzhu Liang
  12. Huahui Ren
  13. Tian Chen
  14. Huanzi Zhong
  15. Wenchen Song
  16. Yanqun Wang
  17. Ziqing Deng
  18. Yanping Zhao
  19. Zhihua Ou
  20. Daxi Wang
  21. Jielun Cai
  22. Xinyi Cheng
  23. Taiqing Feng
  24. Honglong Wu
  25. Yanping Gong
  26. Huanming Yang
  27. Jian Wang
  28. Xun Xu
  29. Shida Zhu
  30. Fang Chen
  31. Yanyan Zhang
  32. Weijun Chen
  33. Yimin Li
  34. Junhua Li
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Abstract

COVID-19 has caused a major epidemic worldwide, however, much is yet to be known about the epidemiology and evolution of the virus. One reason is that the challenges underneath sequencing HCoV-19 directly from clinical samples have not been completely tackled. Here we illustrate the application of amplicon and hybrid capture (capture)-based sequencing, as well as ultra-high-throughput metatranscriptomic (meta) sequencing in retrieving complete genomes, inter-individual and intra-individual variations of HCoV-19 from clinical samples covering a range of sample types and viral load. We also examine and compare the bias, sensitivity, accuracy, and other characteristics of these approaches in a comprehensive manner. This is, to date, the first work systematically implements amplicon and capture approaches in sequencing HCoV-19, as well as the first comparative study across methods. Our work offers practical solutions for genome sequencing and analyses of HCoV-19 and other emerging viruses.

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