2021
DOI: 10.1016/j.braindev.2021.06.010
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Neurodegeneration with brain iron accumulation: Characterization of clinical, radiological, and genetic features of pediatric patients from Southern India

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Cited by 6 publications
(2 citation statements)
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“…Indeed, according to such criteria, this variant is classified as a VUS, applying PM1 (mutational hot spot) and PM2 (absence in controls) at the supporting level. Upon discovering a positive family history and reexamining clinical and imaging data, we were able to manually flag two additional criteria at the supporting level, namely, PP1 (cosegregation into multiple family members) and PP4 (highly specific phenotype), yet, to strictly adhere to current guidelines, 8 we did not flag PP5 (reliable source reports the variant as pathogenic), although the same variant had formerly been reported in three unrelated patients with features in the spectrum of PLA2G6‐associated neurodegeneration 14‐17 . Thus, despite that this homozygous variant clearly appears as causative of the early‐onset dystonia‐parkinsonism phenotype shown by the patient, ACMG criteria still do not reach the sufficient strength to unequivocally classify the variant as pathogenic/likely pathogenic.…”
Section: Discussionmentioning
confidence: 99%
“…Indeed, according to such criteria, this variant is classified as a VUS, applying PM1 (mutational hot spot) and PM2 (absence in controls) at the supporting level. Upon discovering a positive family history and reexamining clinical and imaging data, we were able to manually flag two additional criteria at the supporting level, namely, PP1 (cosegregation into multiple family members) and PP4 (highly specific phenotype), yet, to strictly adhere to current guidelines, 8 we did not flag PP5 (reliable source reports the variant as pathogenic), although the same variant had formerly been reported in three unrelated patients with features in the spectrum of PLA2G6‐associated neurodegeneration 14‐17 . Thus, despite that this homozygous variant clearly appears as causative of the early‐onset dystonia‐parkinsonism phenotype shown by the patient, ACMG criteria still do not reach the sufficient strength to unequivocally classify the variant as pathogenic/likely pathogenic.…”
Section: Discussionmentioning
confidence: 99%
“…1,5,12 As highlighted in this case report, the application of next-generation sequencing (NGS) tests will improve diagnostic accuracy. 17 The differential diagnoses with similar clinical phenotype include multiple system atrophy, Machado Joseph's disease, Parkinson's plus syndrome and Wilson's disease. 1,13,18 We present here an adult Turkish patient with MPAN and a novel (c.101C>T;p.Ala34Val) disease-causing variant in the C19orf12 gene.…”
Section: Discussionmentioning
confidence: 99%