Molecular Genetics & Genomic Medicine (Jul 2019)

Targeted gene panel sequencing for the rapid diagnosis of acutely ill infants

  • Luca Brunelli,
  • Sabrina M. Jenkins,
  • James M. Gudgeon,
  • Steven B. Bleyl,
  • Christine E. Miller,
  • Tatiana Tvrdik,
  • Shale A. Dames,
  • Betsy Ostrander,
  • Josue A. F. Daboub,
  • Brandon A. Zielinski,
  • Erin K. Zinkhan,
  • Hunter R. Underhill,
  • Theodore Wilson,
  • Joshua L. Bonkowsky,
  • Christian C. Yost,
  • Lorenzo D. Botto,
  • Justin Jenkins,
  • Theodore J. Pysher,
  • Pinar Bayrak‐Toydemir,
  • Rong Mao

DOI
https://doi.org/10.1002/mgg3.796
Journal volume & issue
Vol. 7, no. 7
pp. n/a – n/a

Abstract

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Abstract Background Exome/genome sequencing (ES/GS) have been recently used in neonatal and pediatric/cardiac intensive care units (NICU and PICU/CICU) to diagnose and care for acutely ill infants, but the effectiveness of targeted gene panels for these purposes remains unknown. Methods RapSeq, a newly developed panel targeting 4,503 disease‐causing genes, was employed on selected patients in our NICU/PICU/CICU. Twenty trios were sequenced from October 2015 to March 2017. We assessed diagnostic yield, turnaround times, and clinical consequences. Results A diagnosis was made in 10/20 neonates (50%); eight had de novo variants (ASXL1, CHD, FBN1, KMT2D, FANCB, FLNA, PAX3), one was a compound heterozygote for CHAT, and one had a maternally inherited GNAS variant. Preliminary reports were generated by 9.6 days (mean); final reports after Sanger sequencing at 16.3 days (mean). In all positive infants, the diagnosis changed management. In a case with congenital myasthenia, diagnosis and treatment occurred at 17 days versus 7 months in a historical control. Conclusions This study shows that a gene panel that includes the majority of known disease‐causing genes can rapidly identify a diagnosis in a large number of tested infants. Due to simpler deployment and interpretation and lower costs, this approach might represent an alternative to ES/GS in the NICU/PICU/CICU.

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