De Biase Irene, Rasmussen Astrid, Monticelli Antonella, Al-Mahdawi Sahar, Pook Mark, Cocozza Sergio, Bidichandani Sanjay I
Department of Biochemistry and Molecular Biology, University of Oklahoma Health Sciences Center, Oklahoma City, OK 73104, USA.
Genomics. 2007 Jul;90(1):1-5. doi: 10.1016/j.ygeno.2007.04.001. Epub 2007 May 10.
Friedreich ataxia (FRDA) patients are homozygous for expanded GAA triplet-repeat alleles in the FXN gene. Primary neurodegeneration involving the dorsal root ganglia (DRG) results in progressive ataxia. While it is known that DRG are inherently sensitive to frataxin deficiency, recent observations also indicate that they show age-dependent, further expansion of the GAA triplet-repeat mutation. Whether somatic instability is progressive has not been systematically investigated in FRDA patients. "Small-pool" PCR analysis of approximately 2300 individual molecules from tissues of an 18-week fetus homozygous for expanded alleles revealed very low levels of instability compared with adult-derived tissues (4.2% versus 30.6%, p<0.0001). Mutation load in blood samples from multiple patients and carriers increased significantly with age, ranging from 7.5% at 18-weeks gestation to 78.7% at 49 years of age (R=0.91; p=0.0001). Therefore, somatic instability in FRDA occurs mostly after early embryonic development and progresses throughout life, lending further support to the role of postnatal somatic instability in disease pathogenesis.
弗里德赖希共济失调(FRDA)患者在FXN基因中存在GAA三联体重复等位基因扩增的纯合子状态。涉及背根神经节(DRG)的原发性神经变性会导致进行性共济失调。虽然已知DRG对frataxin缺乏固有敏感性,但最近的观察结果还表明,它们表现出年龄依赖性的GAA三联体重复突变进一步扩增。FRDA患者中体细胞不稳定性是否呈进行性尚未得到系统研究。对一名18周龄胎儿组织中约2300个个体分子进行“小池”PCR分析,该胎儿为扩增等位基因纯合子,结果显示与成人来源组织相比,其不稳定性水平极低(4.2%对30.6%,p<0.0001)。多名患者和携带者血液样本中的突变负荷随年龄显著增加,从妊娠18周时的7.5%到49岁时的78.7%(R=0.91;p=0.0001)。因此,FRDA中的体细胞不稳定性大多发生在胚胎早期发育之后,并在一生中持续进展,这进一步支持了出生后体细胞不稳定性在疾病发病机制中的作用。
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