| Literature DB >> 33562297 |
Barbara Marengo1, Alessandra Pulliero2, Maria Valeria Corrias3, Riccardo Leardi4, Emanuele Farinini4, Gilberto Fronza5, Paola Menichini5, Paola Monti5, Lorenzo Monteleone1, Giulia Elda Valenti1, Andrea Speciale5, Patrizia Perri3, Francesca Madia6, Alberto Izzotti1,5, Cinzia Domenicotti1.
Abstract
Neuroblastoma (NB) accounts for about 8-10% of pediatric cancers, and the main causes of death are the presence of metastases and the acquisition of chemoresistance. Metastatic NB is characterized by MYCN amplification that correlates with changes in the expression of miRNAs, which are small non-coding RNA sequences, playing a crucial role in NB development and chemoresistance. In the present study, miRNA expression was analyzed in two human MYCN-amplified NB cell lines, one sensitive (HTLA-230) and one resistant to Etoposide (ER-HTLA), by microarray and RT-qPCR techniques. These analyses showed that miRNA-15a, -16-1, -19b, -218, and -338 were down-regulated in ER-HTLA cells. In order to validate the presence of this down-regulation in vivo, the expression of these miRNAs was analyzed in primary tumors, metastases, and bone marrow of therapy responder and non-responder pediatric patients. Principal component analysis data showed that the expression of miRNA-19b, -218, and -338 influenced metastases, and that the expression levels of all miRNAs analyzed were higher in therapy responders in respect to non-responders. Collectively, these findings suggest that these miRNAs might be involved in the regulation of the drug response, and could be employed for therapeutic purposes.Entities:
Keywords: MYCN amplification; chemoresistance; metastases; miRNA; neuroblastoma
Year: 2021 PMID: 33562297 PMCID: PMC7916079 DOI: 10.3390/jpm11020107
Source DB: PubMed Journal: J Pers Med ISSN: 2075-4426