Brain expression profiles of two SCN1A antisense RNAs in children and adolescents with epilepsy

Author:

Schneider Marius Frederik12,Vogt Miriam3,Scheuermann Johanna1,Müller Veronika1,Fischer-Hentrich Antje H. L.4,Kremer Thomas5,Lugert Sebastian5,Metzger Friedrich6,Kudernatsch Manfred78,Kluger Gerhard89,Hartlieb Till89,Noachtar Soheyl10,Vollmar Christian1011,Kunz Mathias12,Tonn Jörg Christian12,Coras Roland13,Blümcke Ingmar13,Pace Claudia14,Heinen Florian15,Klein Christoph16,Potschka Heidrun14,Borggraefe Ingo11

Affiliation:

1. Division of Molecular Biology, Biomedical Center Munich, Ludwig Maximilians University , Munich , Germany

2. International Max Planck Research School (IMPRS) for Molecular Life Sciences , Planegg-Martinsried , Germany

3. ISAR Bioscience GmbH , Planegg , Germany

4. Munich Medical Research School, Ludwig Maximilians University , Munich , Germany

5. Roche Pharmaceutical Research and Early Development, Roche Innovation Center Basel , F Hoffmann-La Roche Ltd , Basel , Switzerland

6. Versameb AG , Hochbergerstrasse 60C, 4057 , Basel , Switzerland

7. Clinic for Neurosurgery , Schoen-Klinik Vogtareuth , Germany

8. Paracelsus Medical University , Salzburg , Austria

9. Neuropediatric Clinic and Clinic for Neurorehabilitation, Epilepsy Center for Children and Adolescents , Schoen-Klinik Vogtareuth , Germany

10. Department of Neurology, Comprehensive Epilepsy Center, University Hospital of Munich, Ludwig Maximilians University , Munich , Germany

11. Comprehensive Epilepsy Center, Division of Pediatric Neurology, Developmental Medicine and Social Pediatrics, Department of Pediatrics, University Hospital of Munich, Ludwig Maximilians University , Munich , Germany

12. Department of Neurosurgery, University Hospital of Munich, Ludwig Maximilians University , Munich , Germany

13. Department of Neuropathology, University Hospital Erlangen , Erlangen , Germany

14. Institute of Pharmacology, Toxicology, and Pharmacy, Ludwig Maximilians University , Munich , Germany

15. Division of Pediatric Neurology, Developmental Medicine and Social Pediatrics, Department of Pediatrics, University Hospital of Munich, Ludwig Maximilians University , Munich , Germany

16. Department of Pediatrics, University Hospital of Munich, Ludwig Maximilians University , Munich , Germany

Abstract

Abstract Objective Heterozygous mutations within the voltage-gated sodium channel α subunit (SCN1A) are responsible for the majority of cases of Dravet syndrome (DS), a severe developmental and epileptic encephalopathy. Development of novel therapeutic approaches is mandatory in order to directly target the molecular consequences of the genetic defect. The aim of the present study was to investigate whether cis-acting long non-coding RNAs (lncRNAs) of SCN1A are expressed in brain specimens of children and adolescent with epilepsy as these molecules comprise possible targets for precision-based therapy approaches. Methods We investigated SCN1A mRNA expression and expression of two SCN1A related antisense RNAs in brain tissues in different age groups of pediatric non-Dravet patients who underwent surgery for drug resistant epilepsy. The effect of different antisense oligonucleotides (ASOs) directed against SCN1A specific antisense RNAs on SCN1A expression was tested. Results The SCN1A related antisense RNAs SCN1A-dsAS (downstream antisense, RefSeq identifier: NR_110598) and SCN1A-usAS (upstream AS, SCN1A-AS, RefSeq identifier: NR_110260) were widely expressed in the brain of pediatric patients. Expression patterns revealed a negative correlation of SCN1A-dsAS and a positive correlation of lncRNA SCN1A-usAS with SCN1A mRNA expression. Transfection of SK-N-AS cells with an ASO targeted against SCN1A-dsAS was associated with a significant enhancement of SCN1A mRNA expression and reduction in SCN1A-dsAS transcripts. Conclusion These findings support the role of SCN1A-dsAS in the suppression of SCN1A mRNA generation. Considering the haploinsufficiency in genetic SCN1A related DS, SCN1A-dsAS is an interesting target candidate for the development of ASOs (AntagoNATs) based precision medicine therapeutic approaches aiming to enhance SCN1A expression in DS.

Publisher

Walter de Gruyter GmbH

Subject

General Neuroscience

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