| Literature DB >> 28928972 |
Carolina Leite1, Lucas Delmonico2, Gilda Alves2, Romario José Gomes2, Mariana Rodrigues Martino2, Aline Rodrigues da Silva2, Aline Dos Santos Moreira3, Maria Christina Maioli1, Luciano Rios Scherrer4, Elenice Ferreira Bastos5, Roberto Irineu6, Maria Helena Ornellas2.
Abstract
Myelodysplastic syndrome (MDS) is a heterogeneous group of clonal bone marrow disorders characterized by ineffective hematopoiesis, different degrees of cellular dysplasia, and increased risk of progression to acute myeloid leukemia. International Prognostic Scoring System is the gold standard for MDS classification; however, patients exhibiting different clinical behaviors often coexist in the same group, indicating that the currently available scoring systems are insufficient. The genes that have recently been identified as mutated in MDS, including additional sex combs like 1, transcriptional regulator (ASXL1), tumor protein p53 (TP53), and KRAS proto-oncogene and GTPase (KRAS)/NRAS proto-oncogene, GTPase (NRAS), may contribute to a more comprehensive classification, as well as to the prognosis and progression of the disease. In the present study, the mutations in the ASXL1, TP53 and NRAS/KRAS genes in 50 patients were evaluated by sequencing genomic bone marrow DNA. Nine patients (18%) presented with at least one type of mutation. Mutations in TP53 were the most frequent in six patients (12%), followed by ASXL1 in two patients (4%) and NRAS in one patient (2%). The nine mutations were detected in patients with low- and high-risk MDS. The screening of mutations in MDS cases contributes to the application of personalized medicine.Entities:
Keywords: GTPase; GTPase/NRAS proto-oncogene; additional sex combs like 1; myelodysplastic syndrome; transcriptional regulator; tumor protein p53, and KRAS proto-oncogene
Year: 2017 PMID: 28928972 PMCID: PMC5590036 DOI: 10.3892/br.2017.965
Source DB: PubMed Journal: Biomed Rep ISSN: 2049-9434