DNA repair gene expressions are related to bone marrow cellularity in myelodysplastic syndrome

Ribeiro Jr., Howard L.; Maia, Allan Rodrigo S.; Oliveira, Roberta Taiane G. de; Costa, Marília Braga; Farias, Izabelle Rocha; Borges, Daniela de Paula; Sousa, Juliana Cordeiro de; Magalhães, Silvia Maria M.; Pinheiro, Ronald F.

Please use this identifier to cite or link to this item: http://repositorio.ufc.br/handle/riufc/24918

Type:	Artigo de Periódico
Title:	DNA repair gene expressions are related to bone marrow cellularity in myelodysplastic syndrome
Authors:	Ribeiro Jr., Howard L. Maia, Allan Rodrigo S. Oliveira, Roberta Taiane G. de Costa, Marília Braga Farias, Izabelle Rocha Borges, Daniela de Paula Sousa, Juliana Cordeiro de Magalhães, Silvia Maria M. Pinheiro, Ronald F.
Keywords:	DNA;Genes
Issue Date:	Aug-2017
Publisher:	Journal of Clinical Pathology
Citation:	RIBEIRO Jr., H. L. et al. DNA repair gene expressions are related to bone marrow cellularity in myelodysplastic syndrome, p. 1-11, aug. 2017.
Abstract:	Objective To evaluate the expression of genes related to nuclear excision (ERCC8, XPA and XPC), homologous recombination and non-homologous end-joining (ATM, BRCA1, BRCA2 and LIG4) repair mechanisms, using quantitative PCR methodologies, and it relation with bone marrow cellularity in myelodysplastic syndrome (MDS). Methods and results A total of 51 adult de novo patients with MDS (3 refractory anaemia (RA), 11 refractory anaemia with ringed sideroblasts (RARS), 28 refractory cytopenia with multilineage dysplasia (RCMD), 3 refractory anaemia with excess blasts type I (RAEB-I), 5 refractory anaemia with excess blasts type II (RAEB-II), and 1 chronic myelomonocytic leukaemia (CMML) were evaluated. For karyotype, 16.2% patients were defined as very low prognosis, 59.5% low risk, 8.1% intermediate risk, 5.4% high risk and 10.8% very high risk. For bone marrow cellularity, 17.6%, 17.6% and 64.7% presented as hypocellular, normocellular and hypercellular, respectively. Patients with hypocellular MDS had significantly decreased expression of ATM (p=0.000), BRCA1 (p=0.014), BRCA2 (p=0.003), LIG4 (p=0.004) and ERCC8 (p=0.000) than those with normocellular/hypercellular bone marrow, whereas XPA (p=0.049) and XPC (p=0.000) genes were increased. In patients with hypoplastic MDS, a low expression of ATM (p=0.0268), LIG4 (p=0.0199) and ERCC8 (p=0.0493) was significantly associated with the presence of chromosomal abnormalities. We detected positive correlations between BRCA1 and BRCA2 (r=0.416; p=0.007), ATM and LIG4 (r=0.472; p=0.001), LIG4 and BRCA1 (r=0.333; p=0.026), LIG4 and BRCA2 (r=0.334; p=0.025), ATM and XPA (r=0.377; p=0.008), ATM and XPC (r=0.287; p=0.046), LIG4 and XPC (r=0.371; p=0.007) and XPA and XPC genes (r=0.895; p=0.0000). We also found among all patients evaluated that correlation with LIG4 occurred most often. Conclusions These correlations demonstrate the important intrinsic relations between single and double DNA strand breaks genes in MDS, emphasising that these genes are related to MDS pathogenesis.
URI:	http://www.repositorio.ufc.br/handle/riufc/24918
ISSN:	0021-9746 1472-4146 (on line)
Appears in Collections:	DMC - Artigos publicados em revistas científicas

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