TY - JOUR
T1 - A MT-TL1 variant identified by whole exome sequencing in an individual with intellectual disability, epilepsy, and spastic tetraparesis
AU - Solve-RD SNV-indel working group
AU - Solve-RD DITF-ITHACA
AU - de Boer, Elke
AU - Ockeloen, Charlotte W.
AU - Matalonga, Leslie
AU - Horvath, Rita
AU - Cohen, Enzo
AU - Cuesta, Isabel
AU - Danis, Daniel
AU - Denommé-Pichon, Anne Sophie
AU - Duffourd, Yannis
AU - Gilissen, Christian
AU - Johari, Mridul
AU - Laurie, Steven
AU - Li, Shuang
AU - Matalonga, Leslie
AU - Nelson, Isabelle
AU - Peters, Sophia
AU - Paramonov, Ida
AU - Prasanth, Sivakumar
AU - Sablauskas, Karolis
AU - Savarese, Marco
AU - Steyaert, Wouter
AU - Töpf, Ana
AU - van der Velde, Joeri K.
AU - Vitobello, Antonio
AU - Rodenburg, Richard J.
AU - Coenen, Marieke J.H.
AU - Janssen, Mirian
AU - Henssen, Dylan
AU - Gilissen, Christian
AU - Steyaert, Wouter
AU - Paramonov, Ida
AU - Banka, Siddharth
AU - Benetti, Elisa
AU - Casari, Giorgio
AU - Ciolfi, Andrea
AU - Clayton-Smith, Jill
AU - Dallapiccola, Bruno
AU - de Boer, Elke
AU - Faivre, Laurence
AU - Haack, Tobias B.
AU - Hammarsjö, Anna
AU - Havlovicova, Marketa
AU - Hoischen, Alexander
AU - Hugon, Anne
AU - Jackson, Adam
AU - Kleefstra, Tjitske
AU - Lindstrand, Anna
AU - López-Martín, Estrella
AU - Macek, Milan
AU - Nigro, Vicenzo
N1 - Publisher Copyright:
© 2021, The Author(s).
PY - 2021/9
Y1 - 2021/9
N2 - The genetic etiology of intellectual disability remains elusive in almost half of all affected individuals. Within the Solve-RD consortium, systematic re-analysis of whole exome sequencing (WES) data from unresolved cases with (syndromic) intellectual disability (n = 1,472 probands) was performed. This re-analysis included variant calling of mitochondrial DNA (mtDNA) variants, although mtDNA is not specifically targeted in WES. We identified a functionally relevant mtDNA variant in MT-TL1 (NC_012920.1:m.3291T > C; NC_012920.1:n.62T > C), at a heteroplasmy level of 22% in whole blood, in a 23-year-old male with severe intellectual disability, epilepsy, episodic headaches with emesis, spastic tetraparesis, brain abnormalities, and feeding difficulties. Targeted validation in blood and urine supported pathogenicity, with heteroplasmy levels of 23% and 58% in index, and 4% and 17% in mother, respectively. Interestingly, not all phenotypic features observed in the index have been previously linked to this MT-TL1 variant, suggesting either broadening of the m.3291T > C-associated phenotype, or presence of a co-occurring disorder. Hence, our case highlights the importance of underappreciated mtDNA variants identifiable from WES data, especially for cases with atypical mitochondrial phenotypes and their relatives in the maternal line.
AB - The genetic etiology of intellectual disability remains elusive in almost half of all affected individuals. Within the Solve-RD consortium, systematic re-analysis of whole exome sequencing (WES) data from unresolved cases with (syndromic) intellectual disability (n = 1,472 probands) was performed. This re-analysis included variant calling of mitochondrial DNA (mtDNA) variants, although mtDNA is not specifically targeted in WES. We identified a functionally relevant mtDNA variant in MT-TL1 (NC_012920.1:m.3291T > C; NC_012920.1:n.62T > C), at a heteroplasmy level of 22% in whole blood, in a 23-year-old male with severe intellectual disability, epilepsy, episodic headaches with emesis, spastic tetraparesis, brain abnormalities, and feeding difficulties. Targeted validation in blood and urine supported pathogenicity, with heteroplasmy levels of 23% and 58% in index, and 4% and 17% in mother, respectively. Interestingly, not all phenotypic features observed in the index have been previously linked to this MT-TL1 variant, suggesting either broadening of the m.3291T > C-associated phenotype, or presence of a co-occurring disorder. Hence, our case highlights the importance of underappreciated mtDNA variants identifiable from WES data, especially for cases with atypical mitochondrial phenotypes and their relatives in the maternal line.
UR - http://www.scopus.com/inward/record.url?scp=85107553844&partnerID=8YFLogxK
U2 - 10.1038/s41431-021-00900-2
DO - 10.1038/s41431-021-00900-2
M3 - Article
C2 - 34075211
AN - SCOPUS:85107553844
SN - 1018-4813
VL - 29
SP - 1359
EP - 1368
JO - European Journal of Human Genetics
JF - European Journal of Human Genetics
IS - 9
ER -