| Literature DB >> 30528883 |
Joseph J Chin1, Babak Behnam1, Mariska Davids1, Prashant Sharma1, Wadih M Zein2, Camille Wang1, Xenia Chepa-Lotrea1, William Brian Gallantine3, Camilo Toro4, David R Adams4, Cynthia J Tifft4, William A Gahl4, May Christine V Malicdan5.
Abstract
CLN6 is a transmembrane protein located in the endoplasmic reticulum that is involved in lysosomal acidification. Mutations in CLN6 cause late-infantile neuronal ceroid lipofuscinosis (LINCL), and teenage and adult onset NCL without visual impairment. Here we describe two pediatric patients with LINCL from unrelated families who were evaluated at the National Institutes of Health. Both children exhibited typical phenotypes associated with LINCL except that they lacked the expected visual impairment. Whole exome sequencing identified novel biallelic mutations in CLN6, i.e., c.218-220dupGGT (p.Trp73dup) and c.296A > G (p.Lys99Arg) in Proband 1 and homozygous c.723G > T (p.Met241Ile) in Proband 2. Expression analysis in dermal fibroblasts showed a small increase in CLN6 protein levels. Electron micrographs of these fibroblasts demonstrated large numbers of small membrane-bound vesicles, in addition to lipofuscin deposits. LysoTracker™ Red intensity was increased in fibroblasts from both patients. This study supports a role for CLN6 in lysosomal homeostasis, and highlights the importance of considering CLN6 mutations in the diagnosis of Batten Disease even in patients with normal vision.Entities:
Keywords: Batten disease; Lysosomal Storage Disorders; Neuronal Ceroid Lipofuscinosis
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Year: 2018 PMID: 30528883 DOI: 10.1016/j.ymgme.2018.12.001
Source DB: PubMed Journal: Mol Genet Metab ISSN: 1096-7192 Impact factor: 4.797