Beta-thalassemia, one of the most common single-gene disorders, is the result of reduced or absent production of beta-globin chains. Patients with beta-thalassemia show weak genotype-phenotype correlations. Mitochondrial DNA polymorphisms are a potential source for different physiological and pathological characteristics and have been found to be associated as genetic modifiers with various pathophysiologies, including cancers and neurodegenerative diseases. A group of 35 patients with beta-thalassemia was investigated for the presence of mtDNA D-loop polymorphisms in comparison with 504 normal controls. We found four mtDNA D-loop polymorphisms at nucleotides 16,069C>T, 16,189T>C, 16,319G>A, and 16,519T>C that showed significant differences between patients and normal subjects. There is no strong proof for the association of these polymorphisms with beta-thalassemia. It is hypothesized that iron overload or its effects on sequestration of calcium or zinc can lead to oxidative stress and ROS production inside the mitochondria. Therefore, possible accompanying of mtDNA polymorphisms with beta-thalassemia disease may complicate the genotype-phenotype correlation and could affect the clinical outcomes in the patients.

• 出版日期2016