Khan Nahid Akhtar, Govindaraj Periyasamy, Jyothi Vuskamalla, Meena Angamuthu K, Thangaraj Kumarasamy
CSIR-Centre for Cellular and Molecular Biology, Hyderabad, India.
Mol Vis. 2013 Jun 11;19:1282-9. Print 2013.
Mitochondrial DNA (mtDNA) mutations are known to cause Leber hereditary optic neuropathy (LHON). However, the co-occurrence of double pathogenic mutations with different pathological significance in pedigrees is a rare event.
Detailed clinical investigation and complete mtDNA sequencing analysis was performed for two Indian families with LHON. The haplogroup was constructed based on evolutionarily important mtDNA variants.
We observed the existence of double pathogenic mutations (m.11778G>A and m.1555A>G) in two Indian LHON families, who are from different haplogroup backgrounds (M5a and U2e1), with different clinical penetrance of the disease (visual impairment). The m.11778G>A mutation in the MT-ND4 gene is associated primarily with LHON; whereas, m.1555A>G in the 12S rRNA gene has been reported with aminoglycoside-induced non-syndromic hearing loss.
The absence of hearing abnormality and widely varying clinical expression of LHON suggest additional nuclear modifier genes, environmental factors, and population heterogeneity might play an important role in the expression of visual impairment in these families.
已知线粒体DNA(mtDNA)突变会导致Leber遗传性视神经病变(LHON)。然而,在谱系中同时出现具有不同病理意义的双重致病突变是罕见事件。
对两个患有LHON的印度家庭进行了详细的临床调查和完整的mtDNA测序分析。基于具有进化重要性的mtDNA变异构建单倍群。
我们在两个来自不同单倍群背景(M5a和U2e1)的印度LHON家庭中观察到双重致病突变(m.11778G>A和m.1555A>G)的存在,这两个家庭的疾病临床外显率(视力损害)不同。MT-ND4基因中的m.11778G>A突变主要与LHON相关;而12S rRNA基因中的m.1555A>G突变与氨基糖苷类药物诱导的非综合征性听力损失有关。
这些家庭中不存在听力异常以及LHON广泛不同的临床表型表明,额外的核修饰基因、环境因素和人群异质性可能在这些家庭视力损害的表现中起重要作用。
