Identification of six novel mutations in BCKDHA gene for classic form of maple syrup urine disease in Iranian patients and their in silico analysis

In this study, two sets of multiplex polymorphic STR (short tandem repeat) markers linked to the above genes were used to aid in homozygosity mapping in order to find probable pathogenic change(s) in the studied families. The families who showed homozygote haplotype for the BCKDHA gene were subsequently sequenced. Our findings showed that exons 2, 4 and 6 contain most of the mutations which are novel. The changes include two single nucleotide deletion (i.e. c. 143delT and c.702delT), one gross deletion covering the whole exon four c.(375±1_376-1)_(884±1_885-1), two splice site changes (c.1167±1G≥T, c. 288±1G≥A), and one point mutation (c.731G≥A). Computational approaches were used to analyze these two novel mutations in terms of their impact on protein structure. Computational structural modeling indicated that these mutations might affect structural stability and multimeric assembly of branched-chain α-keto acid dehydrogenase complex (BCKDC).
Source: Mutation Research Fundamental and Molecular Mechanisms of Mutagenesis - Category: Cytology Source Type: research