| Literature DB >> 29685658 |
Lance H Rodan1, Marissa Hauptman2, Alissa M D'Gama3, Anita E Qualls4, Siqi Cao5, Karin Tuschl6, Fatma Al-Jasmi7, Jozef Hertecant7, Susan J Hayflick8, Marianne Wessling-Resnick9, Edward T Yang10, Gerard T Berry3, Andrea Gropman11, Alan D Woolf2, Pankaj B Agrawal5.
Abstract
Congenital disorders of manganese metabolism are rare occurrences in children, and medical management of these disorders is complex and challenging. Homozygous exonic mutations in the manganese transporter SLC39A14 have recently been associated with a pediatric-onset neurodegenerative disorder characterized by brain manganese accumulation and clinical signs of manganese neurotoxicity, including parkinsonism-dystonia. We performed whole exome sequencing on DNA samples from two unrelated female children from the United Arab Emirates with progressive movement disorder and brain mineralization, identified a novel homozygous intronic mutation in SLC39A14 in both children, and demonstrated that the mutation leads to aberrant splicing. Both children had consistently elevated serum manganese levels and were diagnosed with SLC39A14-associated manganism. Over a four-year period, we utilized a multidisciplinary management approach for Patient 1 combining decreased manganese dietary intake and chelation with symptomatic management of dystonia. Our treatment strategy appeared to slow disease progression, but did not lead to a cure or reversal of already established deficits. Clinicians should consider testing for noncoding mutations in the diagnosis of congenital disorders of manganese metabolism and utilizing multidisciplinary approaches in the management of these disorders.Entities:
Keywords: Congenital manganism; Manganese toxicity; SLC39A14
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Year: 2018 PMID: 29685658 PMCID: PMC5976541 DOI: 10.1016/j.ymgme.2018.04.002
Source DB: PubMed Journal: Mol Genet Metab ISSN: 1096-7192 Impact factor: 4.797