Compound heterozygous missense and deep intronic variants in NDUFAF6 unraveled by exome sequencing and mRNA analysis.

A Legati; Alan Robinson; Alessia Catania; Andrea Legati; Anna Ardissone; Anna Maria Pinto; Aurelio Reyes; Daniela Verrigni; Daniele Ghezzi; Daria Diodato; Davide Tonduti; DJ Pagliarini; E Ogawa; Eleonora Lamantea; Enrico Bertini; F Fang; HH Dahl; Isabella Moroni; L Bianciardi; M Kohda; M McKenzie; Massimo Zeviani; Rosalba Carrozzo; Valentina Imperatore

Compound heterozygous missense and deep intronic variants in NDUFAF6 unraveled by exome sequencing and mRNA analysis.

Authors: A Legati
Alan Robinson
Alessia Catania
Andrea Legati
Anna Ardissone
Anna Maria Pinto
Aurelio Reyes
Daniela Verrigni
Daniele Ghezzi
Daria Diodato
Davide Tonduti
DJ Pagliarini
E Ogawa
Eleonora Lamantea
Enrico Bertini
F Fang
HH Dahl
Isabella Moroni
L Bianciardi
M Kohda
M McKenzie
Massimo Zeviani
Rosalba Carrozzo
Valentina Imperatore
Publication date: 1 January 2018
Publisher: J Hum Genet
Doi

Abstract

Biallelic mutations in NDUFAF6 have been identified as responsible for cases of autosomal recessive Leigh syndrome associated with mitochondrial complex I deficiency. Here we report two siblings and two unrelated subjects with Leigh syndrome, in which we found the same compound heterozygous missense (c.532G>C:p.A178P) and deep intronic (c.420+784C>T) variants in NDUFAF6. We demonstrated that the identified intronic variant creates an alternative splice site, leading to the production of an aberrant transcript. A detailed analysis of whole-exome sequencing data together with the functional validation based on mRNA analysis may reveal pathogenic variants even in non-exonic regions