Department of Oncology, University of Alberta, Cross Cancer Institute, 11560 University Ave., Edmonton, AB, T6G 1Z2, Canada.
Department of Biochemistry, University of Alberta, Medical Sciences Building, Edmonton, AB, T6G 2H7, Canada.
Sci Rep. 2022 Mar 30;12(1):5386. doi: 10.1038/s41598-022-09097-w.
Polynucleotide Kinase-Phosphatase (PNKP) is a bifunctional enzyme that possesses both DNA 3'-phosphatase and DNA 5'-kinase activities, which are required for processing termini of single- and double-strand breaks generated by reactive oxygen species (ROS), ionizing radiation and topoisomerase I poisons. Even though PNKP is central to DNA repair, there have been no reports linking PNKP mutations in a Microcephaly, Seizures, and Developmental Delay (MSCZ) patient to cancer. Here, we characterized the biochemical significance of 2 germ-line point mutations in the PNKP gene of a 3-year old male with MSCZ who presented with a high-grade brain tumor (glioblastoma multiforme) within the cerebellum. Functional and biochemical studies demonstrated these PNKP mutations significantly diminished DNA kinase/phosphatase activities, altered its cellular distribution, caused defective repair of DNA single/double stranded breaks, and were associated with a higher propensity for oncogenic transformation. Our findings indicate that specific PNKP mutations may contribute to tumor initiation within susceptible cells in the CNS by limiting DNA damage repair and increasing rates of spontaneous mutations resulting in pediatric glioma associated driver mutations such as ATRX and TP53.
多核苷酸激酶-磷酸酶(PNKP)是一种具有 DNA 3'-磷酸酶和 DNA 5'-激酶活性的双功能酶,这些活性对于处理活性氧(ROS)、电离辐射和拓扑异构酶 I 毒物产生的单链和双链断裂的末端至关重要。尽管 PNKP 是 DNA 修复的核心,但目前尚无报道将 PNKP 突变与 Microcephaly、Seizures 和 Developmental Delay(MSCZ)患者的癌症联系起来。在这里,我们对一名 3 岁男性 MSCZ 患者的 PNKP 基因中的 2 个种系点突变进行了生化特征分析,该患者小脑内存在高级别脑肿瘤(多形性胶质母细胞瘤)。功能和生化研究表明,这些 PNKP 突变显著降低了 DNA 激酶/磷酸酶活性,改变了其细胞分布,导致 DNA 单链/双链断裂的修复缺陷,并与更高的致癌转化倾向相关。我们的研究结果表明,特定的 PNKP 突变可能通过限制 DNA 损伤修复并增加自发突变的频率,从而导致与儿童胶质母细胞瘤相关的驱动突变,如 ATRX 和 TP53,从而在易感细胞中促进肿瘤的起始。
