Mutations of the DNA repair gene PNKP in a patient with microcephaly, seizures, and developmental delay (MCSZ) presenting with a high-grade brain tumor

Author:

Jiang Bingcheng,Murray Cameron,Cole Bonnie L.,Glover J. N. Mark,Chan Gordon K.,Deschenes Jean,Mani Rajam S.,Subedi Sudip,Nerva John D.,Wang Anthony C.,Lockwood Christina M.,Mefford Heather C.,Leary Sarah E. S.,Ojemann Jeffery G.,Weinfeld Michael,Ene Chibawanye I.

Abstract

AbstractPolynucleotide 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.

Funder

The Canadian Institutes of Health Research

National Institute of Neurological Disorders and Stroke, National Institutes of Health

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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