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. 2023 Jul 27;14(8):1536.
doi: 10.3390/genes14081536.

Leigh Syndrome Spectrum: A Portuguese Population Cohort in an Evolutionary Genetic Era

Manuela Schubert Baldo  1 Célia Nogueira  1   2 Cristina Pereira  1   2 Patrícia Janeiro  3 Sara Ferreira  4 Charles M Lourenço  5 Anabela Bandeira  6 Esmeralda Martins  6   7 Marina Magalhães  8 Esmeralda Rodrigues  9 Helena Santos  10 Ana Cristina Ferreira  11 Laura Vilarinho  1   2
Affiliations

Leigh Syndrome Spectrum: A Portuguese Population Cohort in an Evolutionary Genetic Era

Manuela Schubert Baldo et al. Genes (Basel). .

Abstract

Mitochondrial diseases are the most common inherited inborn error of metabolism resulting in deficient ATP generation, due to failure in homeostasis and proper bioenergetics. The most frequent mitochondrial disease manifestation in children is Leigh syndrome (LS), encompassing clinical, neuroradiological, biochemical, and molecular features. It typically affects infants but occurs anytime in life. Considering recent updates, LS clinical presentation has been stretched, and is now named LS spectrum (LSS), including classical LS and Leigh-like presentations. Apart from clinical diagnosis challenges, the molecular characterization also progressed from Sanger techniques to NGS (next-generation sequencing), encompassing analysis of nuclear (nDNA) and mitochondrial DNA (mtDNA). This upgrade resumed steps and favored diagnosis. Hereby, our paper presents molecular and clinical data on a Portuguese cohort of 40 positive cases of LSS. A total of 28 patients presented mutation in mtDNA and 12 in nDNA, with novel mutations identified in a heterogeneous group of genes. The present results contribute to the better knowledge of the molecular basis of LS and expand the clinical spectrum associated with this syndrome.

Keywords: NGS; clinical spectrum; leigh syndrome; mitochondrial disorders; mutational spectrum.

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Conflict of interest statement

The authors declare no conflict of interest.

Figures

Figure 1
Figure 1
Mitochondrial and nuclear genes with mutations in our cohort, implicated in LSS.
See this image and copyright information in PMC

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