Department of Internal Medicine, University of Texas Medical Branch, Galveston, TX, USA.
DNA Repair (Amst). 2012 Jun 1;11(6):570-8. doi: 10.1016/j.dnarep.2012.03.005. Epub 2012 Apr 10.
Human NEIL2, one of five oxidized base-specific DNA glycosylases, is unique in preferentially repairing oxidative damage in transcribed genes. Here we show that depletion of NEIL2 causes a 6-7-fold increase in spontaneous mutation frequency in the HPRT gene of the V79 Chinese hamster lung cell line. This prompted us to screen for NEIL2 variants in lung cancer patients' genomic DNA. We identified several polymorphic variants, among which R103Q and R257L were frequently observed in lung cancer patients. We then characterized these variants biochemically, and observed a modest decrease in DNA glycosylase activity relative to the wild type (WT) only with the R257L mutant protein. However, in reconstituted repair assays containing WT NEIL2 or its R257L and R103Q variants together with other DNA base excision repair (BER) proteins (PNKP, Polβ, Lig IIIα and XRCC1) or using NEIL2-FLAG immunocomplexes, an ~5-fold decrease in repair was observed with the R257L variant compared to WT or R103Q NEIL2, apparently due to the R257L mutant's lower affinity for other repair proteins, particularly Polβ. Notably, increased endogenous DNA damage was observed in NEIL2 variant (R257L)-expressing cells relative to WT cells. Taken together, our results suggest that the decreased DNA repair capacity of the R257L variant can induce mutations that lead to lung cancer development.
人类 NEIL2 是五种氧化碱基特异性 DNA 糖苷酶之一,其独特之处在于优先修复转录基因中的氧化损伤。在这里,我们发现 NEIL2 的耗竭会使 V79 中国仓鼠肺细胞系 HPRT 基因的自发突变频率增加 6-7 倍。这促使我们在肺癌患者的基因组 DNA 中筛选 NEIL2 变体。我们鉴定了几种多态性变体,其中 R103Q 和 R257L 在肺癌患者中经常观察到。然后,我们对这些变体进行了生化特性分析,发现只有 R257L 突变蛋白的 DNA 糖苷酶活性相对于野生型(WT)略有下降。然而,在包含 WT NEIL2 或其 R257L 和 R103Q 变体以及其他 DNA 碱基切除修复(BER)蛋白(PNKP、Polβ、Lig IIIα 和 XRCC1)的重建修复测定中,与 WT 或 R103Q NEIL2 相比,R257L 变体的修复活性下降了约 5 倍,这显然是由于 R257L 突变体与其他修复蛋白(尤其是 Polβ)的亲和力较低所致。值得注意的是,与 WT 细胞相比,表达 R257L 变体的细胞中观察到内源性 DNA 损伤增加。总之,我们的结果表明,R257L 变体降低的 DNA 修复能力可诱导导致肺癌发生的突变。