| Literature DB >> 32204466 |
Federica Centofanti1, Massimo Santoro2, Mario Marini3,4, Virginia Veronica Visconti5, Anna Maria Rinaldi3,4, Monica Celi6, Giovanna D'Arcangelo3,4, Giuseppe Novelli5,7, Augusto Orlandi1, Virginia Tancredi3,4, Umberto Tarantino6,8, Annalisa Botta5.
Abstract
Osteoporosis (OP) is a multifactorial disease influenced by genetic, epigenetic, and environmental factors. One of the main causes of the bone homeostasis alteration is inflammation resulting in excessive bone resorption. Long non-coding RNAs (lncRNAs), have a crucial role in regulating many important biological processes in bone, including inflammation. We designed our study to identify lncRNAs misregulated in osteoblast primary cultures derived from OP patients (n = 4), and controls (CTRs, n = 4) with the aim of predicting possible RNA and/or protein targets implicated in this multifactorial disease. We focused on 84 lncRNAs regulating the expression of pro-inflammatory and anti-inflammatory genes and miRNAs. In silico analysis was utilized to predict the interaction of lncRNAs with miRNAs, mRNAs, and proteins targets. Six lncRNAs were significantly down-regulated in OP patients compared to controls: CEP83-AS1, RP11-84C13.1, CTC-487M23.5, GAS5, NCBP2-AS2, and SDCBP2-AS1. Bioinformatic analyses identified HDCA2, PTX3, and FGF2 proteins as downstream targets of CTC-487M23.5, GAS5, and RP11-84C13.1 lncRNAs mediated by the interaction with miRNAs implicated in OP pathogenesis, including miR-21-5p. Altogether, these data open a new regulatory mechanism of gene expression in bone homeostasis and could direct the development of future therapeutic approaches.Entities:
Keywords: bone homeostasis; epigenetics; inflammation; long non-coding RNAs; osteoblast; osteoporosis
Year: 2020 PMID: 32204466 DOI: 10.3390/biomedicines8030065
Source DB: PubMed Journal: Biomedicines ISSN: 2227-9059