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Oxidative stress and antioxidant response in fibroblasts from Werner and Atypical Werner Syndromes

机译:Werner和非典型Werner综合征成纤维细胞的氧化应激和抗氧化反应

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摘要

Werner Syndrome (WS, ICD-10 E34.8, ORPHA902) and Atypical Werner Syndrome (AWS, ICD-10 E34.8, ORPHA79474) are very rare inherited syndromes characterized by premature aging. While approximately 90% of WS individuals have any of a range of mutations in the WRN gene, there exists a clinical subgroup in which the mutation occurs in the LMNA/C gene in heterozygosity. Although both syndromes exhibit an age-related pleiotropic phenotype, AWS manifests the onset of the disease during childhood, while major symptoms in WS appear between the ages of 20 and 30. To study the molecular mechanisms of progeroid diseases provides a useful insight into the normal aging process. Main changes found were the decrease in Cu/Zn and Mn SOD activities in the three cell lines. In AWS, both mRNA SOD and protein levels were also decreased. Catalase and glutathione peroxidases decrease, mainly in AWS. Glutaredoxin (Grx) and thioredoxin (Trx) protein expression was lower in the three progeroid cell lines. Grx and Trx were subjected to post-transcriptional regulation, because protein expression was reduced although mRNA levels were not greatly affected in WS.
机译:Werner综合征(WS,ICD-10 E34.8,ORPHA902)和非典型Werner综合征(AWS,ICD-10 E34.8,ORPHA79474)是非常罕见的以过早衰老为特征的遗传综合征。虽然大约90%的WS个体在WRN基因中具有任何范围的突变,但存在一个临床亚组,其中该突变发生在杂合性的LMNA / C基因中。尽管这两种综合症都表现出与年龄有关的多效性表型,但AWS在儿童时期就表现出该病的发作,而WS中的主要症状出现在20至30岁之间。研究早发型疾病的分子机制可为正常人的正常生活提供有用的见识。老龄化进程。发现的主要变化是三种细胞系中Cu / Zn和Mn SOD活性的降低。在AWS中,mRNA SOD和蛋白质水平均降低。过氧化氢酶和谷胱甘肽过氧化物酶减少,主要在AWS中。谷胱甘肽(Grx)和硫氧还蛋白(Trx)蛋白表达在三种早衰细胞系中较低。 Grx和Trx受到转录后调控,因为尽管WS中的mRNA水平没有受到很大的影响,但蛋白质表达降低了。

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