Brain Sciences (Dec 2021)

Family-Based Whole-Exome Analysis of Specific Language Impairment (SLI) Identifies Rare Variants in <i>BUD13</i>, a Component of the Retention and Splicing (RES) Complex

  • Erin M. Andres,
  • Kathleen Kelsey Earnest,
  • Cuncong Zhong,
  • Mabel L. Rice,
  • Muhammad Hashim Raza

DOI
https://doi.org/10.3390/brainsci12010047
Journal volume & issue
Vol. 12, no. 1
p. 47

Abstract

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Specific language impairment (SLI) is a common neurodevelopmental disorder (NDD) that displays high heritability estimates. Genetic studies have identified several loci, but the molecular basis of SLI remains unclear. With the aim to better understand the genetic architecture of SLI, we performed whole-exome sequencing (WES) in a single family (ID: 489; n = 11). We identified co-segregating rare variants in three new genes: BUD13, APLP2, and NDRG2. To determine the significance of these genes in SLI, we Sanger sequenced all coding regions of each gene in unrelated individuals with SLI (n = 175). We observed 13 additional rare variants in 18 unrelated individuals. Variants in BUD13 reached genome-wide significance (p-value BUD13 is involved in SLI. Additionally, five BUD13 variants showed cohesive variant level evidence of likely pathogenicity. Bud13 is a component of the retention and splicing (RES) complex. Additional supportive evidence from studies of an animal model (loss-of-function mutations in BUD13 caused a profound neural phenotype) and individuals with an NDD phenotype (carrying a CNV spanning BUD13), indicates BUD13 could be a target for investigation of the neural basis of language.

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