Abstract
The genetic influence in epilepsy, characterized by unprovoked and recurrent seizures, is through variants in genes critical to brain development and function. We have carried out variant calling in Mesial Temporal Lobe Epilepsy (MTLE) patients by mapping the RNA-Seq data available at SRA, NCBI, USA onto human genome assembly hg-19. We have identified 1,75,641 SNVs in patient samples. These SNVs are distributed over 14700 genes of which 655 are already known to be associated with epilepsy. Large number of variants occur in the 3’-UTR, which is one of the regions involved in the regulation of protein translation through binding of miRNAs and RNA-binding proteins (RBP). We have focused on studying the structure-function relationship of the 3’-UTR SNVs that are common to at-least 10 of the 35 patient samples. For the first time we find SNVs exclusively in the 3’-UTR of FGF12, FAR1, NAPB, SLC1A3, SLC12A6, GRIN2A, CACNB4 and FBXO28 genes. Structural modelling reveals that the variant 3’-UTR segments possess altered secondary and tertiary structures which could affect mRNA stability and binding of RBPs to form proper ribonucleoprotein (RNP) complexes. Secondly, these SNVs have either created or destroyed miRNA-binding sites, and molecular modeling reveals that, where binding sites are created, the additional miRNAs bind strongly to 3’-UTR of only variant mRNAs. These two factors affect protein production thereby creating an imbalance in the amounts of select proteins in the cell. We suggest that in the absence of missense and nonsense variants, protein-activity imbalances associated with MTLE patients can be caused through 3’-UTR variants in relevant genes by the mechanisms mentioned above. 3’-UTR SNV has already been identified as causative variant in the neurological disorder, Tourette syndrome. Inhibition of these miRNA-mRNA bindings could be a novel way of treating drug-resistant MTLE patients. We also suggest that joint occurrence of these SNVs could serve as markers for MTLE. We find, in the present study, SNV-mediated destruction of miRNA binding site in the 3’-UTR of the gene encoding glutamate receptor subunit, and, interestingly, overexpression of one of this receptor subunit is also associated with Febrile Seizures.
Highlights
Epilepsy is amongst the most common neurological disorders, affecting up to 1% of the population of all ages [1]
We find a probable linkage between Febrile seizures and Mesial Temporal Lobe Epilepsy (MTLE) through genetic signals for over-expression of glutamate receptor subunits in both
The SRA Ids of the RNA-Seq data and statistics of mapping to hg-19 are given in S1 Table
Summary
Epilepsy is amongst the most common neurological disorders, affecting up to 1% of the population of all ages [1]. Though epilepsy can have both genetic and acquired causes, in about 60% of cases, the cause is not known [2,3,4]. The target gene luciferase assay (reporting gene technology), developed only recently, reveals that variants in the non-coding regions significantly influence epilepsy and other neurological disorders [7,8,9,10]. In a comparative study of 237 ion channel genes from neurologically normal individuals (n = 139) and idiopathic generalized epilepsy patients (n = 152) [11], 1.4% SNVs were found in the 3’-UTR regions. It is suggested that excess suppression of target mRNAs by miRNA binding in the 3’UTR region disturbs the balance between neuronal excitation and neuronal inhibition thereby leading to epileptic seizures [12]
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