| Literature DB >> 28109975 |
Júlia Plentz Portich1, Rafael Pereira Dos Santos2, Nathalia Kersting1, Karolina Brochado Jorge1, Pietro Rebelo Casagrande1, Gabriela Dos Santos Costa1, Jéssica Maria Gonçalves Dias Cionek1, Danielly Brufatto Olguins1, Marialva Sinigaglia3, Franciele Faccio Busatto4, Jenifer Saffi4, Sharbel Weidner Maluf5, Jiseh Fagundes Loss6, Algemir Lunardi Brunetto7, Rafael Roesler8, Caroline Brunetto de Farias9.
Abstract
Predicting the individual response to chemotherapy is a crucial challenge in cancer treatment. DNA damage caused by antitumor therapies evokes different repair mechanisms responses, such as Nucleotide Excision Repair (NER), whose components are being studied as prognosis biomarkers and target therapies. However, few reports have addressed DNA damages in pediatric Acute Lymphoid Leukemia (ALL). Hence, we conducted an observational follow-up study with pediatric patients to assess DNA damage (by Comet Assay) and gene expression from NER pathway during chemotherapy induction. Bone marrow samples from diagnosis, 15th(D15) and 35th (D35) days of the treatment were collected from 28 patients with ALL. There was no increase in damage index. However, there was a reduction of cells with low damages on D35 compared with diagnosis. NER pathway expression remained the same, however, in a single patient, a significant decrease was observed, maybe due to silencing or downregulation of repair pathways. DNA damage levels and repair may influence the clinical outcome, being involved in drug resistance and risk of relapse. In pediatric ALL, we analyzed for the first time DNA damage and repair behavior in BM samples. Monitoring patient's outcomes will help to access the implication of our findings in survival and relapse rates.Entities:
Keywords: Acute Lymphoid Leukemia; Comet assay; DNA damage; DNA repair; NER pathway
Mesh:
Year: 2017 PMID: 28109975 DOI: 10.1016/j.leukres.2017.01.013
Source DB: PubMed Journal: Leuk Res ISSN: 0145-2126 Impact factor: 3.156