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      Novel nonsense mutation in UNC80 in a Turkish patient further validates the sociable skill and severe gastrointestinal problems as part of disease spectrum

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          Abstract

          NALCN channelosome complex contributes to maintaining resting membrane potential. The complex has four domains including two intracellular domains (UNC79 and UNC80), one transmembrane domain (NALCN) and one extracellular domain (FAM155A). Mutations in UNC80 were previously linked to infantile hypotonia with psychomotor retardation and characteristics facies 2. A 6‐year‐old male with neurodevelopmental disorder was referred for clinical exome sequencing. Sanger sequencing was conducted for variant confirmation and segregation analysis. The index had severe to profound neurodevelopmental delay, progressive failure to thrive, severe constipation and reflux, and sociable skills. Trio exome sequencing identified a homozygous c.6495G > A change causing p.Trp2165Ter in UNC80 in the proband. The variant was novel and predicted to be deleterious. We reported a novel nonsense mutation in UNC80. Our case also established the association between, and sociable skills and severe gastrointestinal problems.

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          NMD factors UPF2 and UPF3 bridge UPF1 to the exon junction complex and stimulate its RNA helicase activity.

          Hala Chamieh, Lionel Ballut, Fabien Bonneau (2008)
          Nonsense-mediated mRNA decay (NMD) eliminates mRNAs containing a premature translation termination codon through the recruitment of the conserved NMD factors UPF1, UPF2 and UPF3. In humans, a dynamic assembly pathway allows UPF1 to join UPF2 and UPF3 recruited to the mRNA by the exon-junction complex (EJC). Here we show that the recombinant EJC core is sufficient to reconstitute, with the three UPF proteins, a stable heptameric complex on RNA. The EJC proteins MAGOH, Y14 and eIF4AIII provide a composite binding site for UPF3b that serves as a bridge to UPF2 and UPF1. In the UPF trimeric complex, UPF2 and UPF3b cooperatively stimulate both ATPase and RNA helicase activities of UPF1. This work demonstrates that the EJC core is sufficient to stably anchor the UPF proteins to mRNA and provides insights into the regulation of its central effector, UPF1.
          Article 0 comments Cited 121 times – based on 0 reviews     Review now
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            The neuronal channel NALCN contributes resting sodium permeability and is required for normal respiratory rhythm.

            Boxun Lu, Yanhua Su, Jin Liu (2007)
            Sodium plays a key role in determining the basal excitability of the nervous systems through the resting "leak" Na(+) permeabilities, but the molecular identities of the TTX- and Cs(+)-resistant Na(+) leak conductance are totally unknown. Here we show that this conductance is formed by the protein NALCN, a substantially uncharacterized member of the sodium/calcium channel family. Unlike any of the other 20 family members, NALCN forms a voltage-independent, nonselective cation channel. NALCN mutant mice have a severely disrupted respiratory rhythm and die within 24 hours of birth. Brain stem-spinal cord recordings reveal reduced neuronal firing. The TTX- and Cs(+)-resistant background Na(+) leak current is absent in the mutant hippocampal neurons. The resting membrane potentials of the mutant neurons are relatively insensitive to changes in extracellular Na(+) concentration. Thus, NALCN, a nonselective cation channel, forms the background Na(+) leak conductance and controls neuronal excitability.
            Article 0 comments Cited 108 times – based on 0 reviews     Review now
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              Extracellular calcium controls background current and neuronal excitability via an UNC79-UNC80-NALCN cation channel complex.

              Haikun Wang, Dejian Ren, Qi Zhang (2010)
              In contrast to its extensively studied intracellular roles, the molecular mechanisms by which extracellular Ca(2+) regulates the basal excitability of neurons are unclear. One mechanism is believed to be through Ca(2+)'s interaction with the negative charges on the cell membrane (the charge screening effect). Here we show that, in cultured hippocampal neurons, lowering [Ca(2+)](e) activates a NALCN channel-dependent Na(+)-leak current (I(L-Na)). The coupling between [Ca(2+)](e) and NALCN requires a Ca(2+)-sensing G protein-coupled receptor, an activation of G-proteins, an UNC80 protein that bridges NALCN to a large novel protein UNC79 in the same complex, and the last amino acid of NALCN's intracellular tail. In neurons from nalcn and unc79 knockout mice, I(L-Na) is insensitive to changes in [Ca(2+)](e), and reducing [Ca(2+)](e) fails to elicit the excitatory effects seen in the wild-type. Therefore, extracellular Ca(2+) influences neuronal excitability through the UNC79-UNC80-NALCN complex in a G protein-dependent fashion. Copyright © 2010 Elsevier Inc. All rights reserved.
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                Author and article information

                Contributors
                Fatih M. Kelesoglu: (View ORCID Profile)
                Journal
                Title: American Journal of Medical Genetics Part A
                Abbreviated Title: American J of Med Genetics Pt A
                Publisher: Wiley
                ISSN (Print): 1552-4825
                ISSN (Electronic): 1552-4833
                Publication date Created: July 2023
                Publication date (Electronic): April 17 2023
                Publication date (Print): July 2023
                Volume: 191
                Issue: 7
                Pages: 1959-1962
                Affiliations
                [1 ] Pediatrician Lossburg Baden‐Wurttemberg Germany
                [2 ] Kolan International Hospital, Division of Pediatrics Istanbul Turkey
                [3 ] School of Medicine University of Pamukkale Pamukkale Turkey
                [4 ] School of Medicine University of Istanbul Istanbul Turkey
                Article
                DOI: 10.1002/ajmg.a.63213
                SO-VID: e4552cfe-64d9-4128-9f09-9fb20e4f4418
                Copyright © © 2023
                License:

                http://onlinelibrary.wiley.com/termsAndConditions#vor

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