عنوان به زبان ديگر :
Investigation of polymorphisms in non-coding region of human mitochondrial DNA in 31 Iranian Hypertrophic Cardiomyopathy (HCM) patients.
پديد آورندگان :
Montazeri Maryam نويسنده , Houshmand Massoud نويسنده , Shafa Shariat Panahi Mehdi نويسنده , Noohi Freidoon نويسنده , Givtaj Nozar نويسنده , Sanati Mohammad Hossein نويسنده , Zaklyazminskaya Elena V. نويسنده
چكيده لاتين :
The D-loop region is a hot spot for mitochondrial DNA (mtDNA) alterations, containing two hypervariable segments, HVS-I and HVS-II. In order to identify polymorphic sites and potential genetic background accounting for Hypertrophic CardioMyopathy (HCM) disease, the complete non-coding region of mtDNA from 31 unrelated HCM
patients and 45 normal controls were sequenced. The sequences were aligned upon the revised Cambridge Reference Sequence (rCRS) and any incompatibilities were recorded as numerical changes in homoPolymeric C Tract (PCT), single base substitutions, insertions and deletions (Indels). Nucleotide substitutions were found to make up the
majority of the mutations, rather than indels. We drew significantly high transition rate (81.8%) versus lower frequency of transversions (18.2%). 12 polymorphisms were identified in this study which had not been published in the MitoMap database. PCT changes at position 303-309 were detected in 83% of our samples. Our results suggest that an increased level of HVS-I and HVS-II substitutions may be an indicator
of mitochondrial DNA instability. Furthermore, mtDNA mutations may play an important role in pathogenesis of cardiac arrest which has remained unexplained for long.
