Otros
DNA repair genes in astrocytoma tumorigenesis, progression and therapy resistance
Fecha
2020-01-01Registro en:
Genetics and Molecular Biology, v. 43, n. 1, 2020.
1678-4685
1415-4757
10.1590/1678-4685-gmb-2019-0066
S1415-47572020000200306
2-s2.0-85077278668
S1415-47572020000200306.pdf
Autor
National Institutes of Health
Universidade de São Paulo (USP)
Universidade Estadual Paulista (Unesp)
Centro de Terapia Celular (CEPID-FAPESP)
Institución
Resumen
Glioblastoma (GBM) is the most common and malignant type of primary brain tumor, showing rapid development and resistance to therapies. On average, patients survive 14.6 months after diagnosis and less than 5% survive five years or more. Several pieces of evidence have suggested that the DNA damage signaling and repair activities are directly correlated with GBM phenotype and exhibit opposite functions in cancer establishment and progression. The functions of these pathways appear to present a dual role in tumorigenesis and cancer progression. Activation and/or overexpression of ATRX, ATM and RAD51 genes were extensively characterized as barriers for GBM initiation, but paradoxically the exacerbated activity of these genes was further associated with cancer progression to more aggressive stages. Excessive amounts of other DNA repair proteins, namely HJURP, EXO1, NEIL3, BRCA2, and BRIP, have also been connected to proliferative competence, resistance and poor prognosis. This scenario suggests that these networks help tumor cells to manage replicative stress and treatment-induced damage, diminishing genome instability and conferring therapy resistance. Finally, in this review we address promising new drugs and therapeutic approaches with potential to improve patient survival. However, despite all technological advances, the prognosis is still dismal and further research is needed to dissect such complex mechanisms.