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Comprehensive whole-genome sequence analyses provide insights into the genomic architecture of cerebral palsy.

Darcy L FehlingsMehdi ZarreiWorrawat EngchuanNeal SondheimerBhooma ThiruvahindrapuramJeffrey R MacDonaldEdward J HigginbothamRitesh ThapaTarannum BehlimSabrina AimolaLauren SwitzerPamela NgJohn WeiPrakroothi S DanthiGiovanna PellecchiaSylvia LamoureuxKaren HoSergio L PereiraJill de RijkeWilson W L SungAlireza MowjoodiJennifer L HoweThomas NalpathamkalamRoozbeh ManshaeiSiavash GhaffariJoseph WhitneyRohan V PatelOmar HamdanRulan ShaathBrett TrostShannon KnightsDawa SamdupAnna McCormickCarolyn HuntAdam KirtonAnne KawamuraRonit MestermanJan Willem GorterNomazulu DlaminiDaniele MericoMurto HilaliKyle HirschfeldKritika GroverNelson X BautistaKara HanChristian R MarshallRyan K C YuenPadmaja SubbaraoMeghan B AzadStuart E TurveyPiush MandhaneTheo J MoraesElinor SimonsGeorge MaxwellMichael ShevellGregory CostainJacques L MichaudFadi F HamdanJulie GauthierKévin UguenDimitri J StavropoulosRichard F WintleMaryam OskouiStephen W Scherer
Published in: Nature genetics (2024)
We performed whole-genome sequencing (WGS) in 327 children with cerebral palsy (CP) and their biological parents. We classified 37 of 327 (11.3%) children as having pathogenic/likely pathogenic (P/LP) variants and 58 of 327 (17.7%) as having variants of uncertain significance. Multiple classes of P/LP variants included single-nucleotide variants (SNVs)/indels (6.7%), copy number variations (3.4%) and mitochondrial mutations (1.5%). The COL4A1 gene had the most P/LP SNVs. We also analyzed two pediatric control cohorts (n = 203 trios and n = 89 sib-pair families) to provide a baseline for de novo mutation rates and genetic burden analyses, the latter of which demonstrated associations between de novo deleterious variants and genes related to the nervous system. An enrichment analysis revealed previously undescribed plausible candidate CP genes (SMOC1, KDM5B, BCL11A and CYP51A1). A multifactorial CP risk profile and substantial presence of P/LP variants combine to support WGS in the diagnostic work-up across all CP and related phenotypes.
Keyphrases
  • copy number
  • mitochondrial dna
  • genome wide
  • dna methylation
  • cerebral palsy
  • children with cerebral palsy
  • oxidative stress
  • gene expression
  • genome wide identification
  • transcription factor
  • single cell