Department of Microbiology and Molecular Genetics, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, United States of America.
PLoS Genet. 2010 Mar 5;6(3):e1000871. doi: 10.1371/journal.pgen.1000871.
Xeroderma pigmentosum (XP) is caused by defects in the nucleotide excision repair (NER) pathway. NER removes helix-distorting DNA lesions, such as UV-induced photodimers, from the genome. Patients suffering from XP exhibit exquisite sun sensitivity, high incidence of skin cancer, and in some cases neurodegeneration. The severity of XP varies tremendously depending upon which NER gene is mutated and how severely the mutation affects DNA repair capacity. XPF-ERCC1 is a structure-specific endonuclease essential for incising the damaged strand of DNA in NER. Missense mutations in XPF can result not only in XP, but also XPF-ERCC1 (XFE) progeroid syndrome, a disease of accelerated aging. In an attempt to determine how mutations in XPF can lead to such diverse symptoms, the effects of a progeria-causing mutation (XPF(R153P)) were compared to an XP-causing mutation (XPF(R799W)) in vitro and in vivo. Recombinant XPF harboring either mutation was purified in a complex with ERCC1 and tested for its ability to incise a stem-loop structure in vitro. Both mutant complexes nicked the substrate indicating that neither mutation obviates catalytic activity of the nuclease. Surprisingly, differential immunostaining and fractionation of cells from an XFE progeroid patient revealed that XPF-ERCC1 is abundant in the cytoplasm. This was confirmed by fluorescent detection of XPF(R153P)-YFP expressed in Xpf mutant cells. In addition, microinjection of XPF(R153P)-ERCC1 into the nucleus of XPF-deficient human cells restored nucleotide excision repair of UV-induced DNA damage. Intriguingly, in all XPF mutant cell lines examined, XPF-ERCC1 was detected in the cytoplasm of a fraction of cells. This demonstrates that at least part of the DNA repair defect and symptoms associated with mutations in XPF are due to mislocalization of XPF-ERCC1 into the cytoplasm of cells, likely due to protein misfolding. Analysis of these patient cells therefore reveals a novel mechanism to potentially regulate a cell's capacity for DNA repair: by manipulating nuclear localization of XPF-ERCC1.
着色性干皮病 (XP) 是由核苷酸切除修复 (NER) 途径的缺陷引起的。NER 从基因组中去除螺旋扭曲的 DNA 损伤,如紫外线诱导的光二聚体。患有 XP 的患者表现出极度的阳光敏感性、皮肤癌高发,在某些情况下还会出现神经退行性变。XP 的严重程度差异很大,具体取决于突变的 NER 基因以及突变对 DNA 修复能力的影响程度。XPF-ERCC1 是一种结构特异性内切酶,对于 NER 中损伤链的切割至关重要。XPF 的错义突变不仅会导致 XP,还会导致 XPF-ERCC1 (XFE) 早老症综合征,这是一种加速衰老的疾病。为了确定 XPF 中的突变如何导致如此多样化的症状,我们将导致早老症的突变 (XPF(R153P)) 的影响与导致 XP 的突变 (XPF(R799W)) 进行了比较,分别在体外和体内进行了研究。用 ERCC1 纯化携带任一种突变的重组 XPF,并测试其在体外切割茎环结构的能力。两种突变体复合物均切开了底物,表明这两种突变都没有消除核酸酶的催化活性。令人惊讶的是,来自 XFE 早老症患者的细胞的差异免疫染色和分离揭示了 XPF-ERCC1 在细胞质中含量丰富。这通过在 Xpf 突变细胞中表达的 XPF(R153P)-YFP 的荧光检测得到了证实。此外,将 XPF(R153P)-ERCC1 微注射到 XPF 缺陷的人类细胞的核内,恢复了紫外线诱导的 DNA 损伤的核苷酸切除修复。有趣的是,在所有检查的 XPF 突变细胞系中,细胞质中都检测到 XPF-ERCC1。这表明,与 XPF 突变相关的至少部分 DNA 修复缺陷和症状是由于 XPF-ERCC1 错误定位到细胞的细胞质中,可能是由于蛋白质错误折叠所致。因此,对这些患者细胞的分析揭示了一种潜在的调节细胞 DNA 修复能力的新机制:通过操纵 XPF-ERCC1 的核定位。
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