2016
DOI: 10.1136/jmedgenet-2016-104212
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Compound heterozygosity for severe and hypomorphicNDUFS2mutations cause non-syndromic LHON-like optic neuropathy

Abstract: BackgroundNon-syndromic hereditary optic neuropathy (HON) has been ascribed to mutations in mitochondrial fusion/fission dynamics genes, nuclear and mitochondrial DNA-encoded respiratory enzyme genes or nuclear genes of poorly known mitochondrial function. However, the disease causing gene remains unknown in many families. The objective of the present study was to identify the molecular cause of non-syndromic LHON-like disease in siblings born to non-consanguineous parents of French origin.MethodsWe used a com… Show more

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Cited by 48 publications
(40 citation statements)
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References 35 publications
(29 reference statements)
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“…In summary, of the five NUBPL missense variants that were functionally assessed in Y. lipolytica , four (L104P, D105Y, L193F and G285C) were found to be deleterious to complex I and one (G138D) was found to exhibit a mild defect. Along with other studies ( 18 , 21 , 35 , 36 ), these results reconfirm the utility of Y. lipolytica as a model for human mitochondrial disorders. However, care must be taken in over-interpreting the results, as some effects seen in Y. lipolytica have not been found in humans.…”
Section: Discussionsupporting
confidence: 84%
“…In summary, of the five NUBPL missense variants that were functionally assessed in Y. lipolytica , four (L104P, D105Y, L193F and G285C) were found to be deleterious to complex I and one (G138D) was found to exhibit a mild defect. Along with other studies ( 18 , 21 , 35 , 36 ), these results reconfirm the utility of Y. lipolytica as a model for human mitochondrial disorders. However, care must be taken in over-interpreting the results, as some effects seen in Y. lipolytica have not been found in humans.…”
Section: Discussionsupporting
confidence: 84%
“…In summary four of the six mutations (L104P, D105Y, L193F and G285C) were classed as pathogenic and one (G138D) was classed as potentially pathogenic. Along with other studies (17,20,33,34) these results reconfirm the utility of Y. lipolytica as a model for human mitochondrial disorders. However, care must be taken in over-interpreting the results as some effects seen in Y. lipolytica have not been found in humans.…”
Section: Discussionsupporting
confidence: 81%
“…Yarrowia lipolytica has an ortholog of NDUFA8; truncation mutants are, as expected, inviable (Dr Mark Blenner, personal communication). As has been done for another nuclear encoded assembly factor gene in Yarrowia lipolytica (Gerber et al, 2017), hypomorphic NDUFA8 missense mutants are being generated now in collaboration with a lab at Clemson University so that the piericidin A suppressors described herein will be tested for their ability to rescue the growth defects of this mutant. Once validated in yeast and patient derived cells (fibroblasts, followed by iPSCs), piericidin A suppressors can be further validated in complex I deficient worms (Polyak et al, 2018), flies (Cabirol-Pol et al, 2018) and zebrafish (Pinho et al, 2013).…”
Section: Discussionmentioning
confidence: 99%