Novel homozygous missense mutation in NT5C2 underlying hereditary spastic paraplegia SPG45.

Rachel StraussbergAlexandros OnoufriadisOsnat KonenYasmin ZouabiLior CohenJohn Y W LeeChao-Kai HsuMichael A SimpsonJohn A McGrath

Published in: American journal of medical genetics. Part A (2017)

SPG45 is a rare form of autosomal recessive spastic paraplegia associated with mental retardation. Detailed phenotyping and mutation analysis was undertaken in three individuals with SPG45 from a consanguineous family of Arab Muslim origin. Using whole-exome sequencing, we identified a novel homozygous missense mutation in NT5C2 (c.1379T>C; p.Leu460Pro). Our data expand the molecular basis of SPG45, adding the first missense mutation to the current database of nonsense, frameshift, and splice site mutations. NT5C2 mutations seem to have a broad clinical spectrum and should be sought in patients manifesting either as uncomplicated or complicated HSP.

Keyphrases

intellectual disability
end stage renal disease
ejection fraction
newly diagnosed
cerebral palsy
mental health
chronic kidney disease
high throughput
autism spectrum disorder
heat shock protein
emergency department
patient reported outcomes
big data
deep learning
single cell
data analysis
adverse drug