PLoS ONE (Mar 2010)

Array-based FMR1 sequencing and deletion analysis in patients with a fragile X syndrome-like phenotype.

  • Stephen C Collins,
  • Brad Coffee,
  • Paul J Benke,
  • Elizabeth Berry-Kravis,
  • Fred Gilbert,
  • Ben Oostra,
  • Dicky Halley,
  • Michael E Zwick,
  • David J Cutler,
  • Stephen T Warren

DOI
https://doi.org/10.1371/journal.pone.0009476
Journal volume & issue
Vol. 5, no. 3
p. e9476

Abstract

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Fragile X syndrome (FXS) is caused by loss of function mutations in the FMR1 gene. Trinucleotide CGG-repeat expansions, resulting in FMR1 gene silencing, are the most common mutations observed at this locus. Even though the repeat expansion mutation is a functional null mutation, few conventional mutations have been identified at this locus, largely due to the clinical laboratory focus on the repeat tract.To more thoroughly evaluate the frequency of conventional mutations in FXS-like patients, we used an array-based method to sequence FMR1 in 51 unrelated males exhibiting several features characteristic of FXS but with normal CGG-repeat tracts of FMR1. One patient was identified with a deletion in FMR1, but none of the patients were found to have other conventional mutations.These data suggest that missense mutations in FMR1 are not a common cause of the FXS phenotype in patients who have normal-length CGG-repeat tracts. However, screening for small deletions of FMR1 may be of clinically utility.