Transcriptomic profiling of TK2 deficient human skeletal muscle suggests a role for the p53 signalling pathway and identifies growth and differentiation factor-15 as a potential novel biomarker for mitochondrial myopathies

Susana G. Kalko,Sonia Paco,Cristina Jou,Maria Angels Rodríguez,Marija Meznaric,Mihael Rogac,Maja Jekovec-Vrhovsek,Monica Sciacco,Maurizio Moggio,Gigliola Fagiolari,Boel De Paepe,Linda De Meirleir,Isidre Ferrer,Manel Roig-Quilis,Francina Munell,Julio Montoya,Ester López-Gallardo,Eduardo Ruiz Pesini,Rafael Artuch,Raquel Montero,Ferran Torner,Andrés Nascimento,Carlos Ortez,Jaume Colomer,Cecilia Jimenez-Mallebrera

Transcriptomic profiling of TK2 deficient human skeletal muscle suggests a role for the p53 signalling pathway and identifies growth and differentiation factor-15 as a potential novel biomarker for mitochondrial myopathies

2014

Background Mutations in the gene encoding thymidine kinase 2 (TK2) result in the myopathic form of mitochondrial DNA depletion syndrome which is a mitochondrial encephalomyopathy presenting in children. In order to unveil some of the mechanisms involved in this pathology and to identify potential biomarkers and therapeutic targets we have investigated the gene expression profile of human skeletal muscle deficient for TK2 using cDNA microarrays.

Keywords:

Mitochondrial encephalomyopathy
Gene expression profiling
DNA microarray
Genetics
Mitochondrial DNA depletion syndrome
Skeletal muscle
Mitochondrial myopathy
Mitochondrial DNA
Bioinformatics
Biology
Thymidine kinase

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