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Integrated microRNA-mRNA analyses reveal OPLL specific microRNA regulatory network using high-throughput sequencing

机译:集成的microRNA-mRNA分析使用高通量测序显示OPLL特定的MicroRNA调节网络

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Ossification of the posterior longitudinal ligament (OPLL) is a genetic disorder which involves pathological heterotopic ossification of the spinal ligaments. Although studies have identified several genes that correlated with OPLL, the underlying regulation network is far from clear. Through small RNA sequencing, we compared the microRNA expressions of primary posterior longitudinal ligament cells form OPLL patients with normal patients (PLL) and identified 218 dysregulated miRNAs (FDR??0.01). Furthermore, assessing the miRNA profiling data of multiple cell types, we found these dysregulated miRNAs were mostly OPLL specific. In order to decipher the regulation network of these OPLL specific miRNAs, we integrated mRNA expression profiling data with miRNA sequencing data. Through computational approaches, we showed the pivotal roles of these OPLL specific miRNAs in heterotopic ossification of longitudinal ligament by discovering highly correlated miRNA/mRNA pairs that associated with skeletal system development, collagen fibril organization, and extracellular matrix organization. The results of which provide strong evidence that the miRNA regulatory networks we established may indeed play vital roles in OPLL onset and progression. To date, this is the first systematic analysis of the micronome in OPLL, and thus may provide valuable resources in finding novel treatment and diagnostic targets of OPLL.
机译:后纵韧带(OP11)的骨化是一种遗传性疾病,涉及脊髓韧带的病理异位骨化。尽管研究已经确定了几个与OPLL相关的基因,但潜在的调节网络远非清晰。通过小的RNA测序,我们将初级后纵韧带细胞的MicroRNA表达与正常患者(PLL)形成opl1患者,并鉴定了218个疑虑的miRNA(FDR?<0.01)。此外,评估多种细胞类型的miRNA分析数据,我们发现这些失去了麦芽系统主要是OPLL特定的。为了破译这些OPLL特异性miRNA的调节网络,我们通过miRNA测序数据集成mRNA表达分析数据。通过计算方法,通过发现与骨骼系统发育,胶原素原纤维组织和细胞外基质组织相关的高度相关的miRNA / mRNA对,展示了这些OPLS特异性miRNA在纵向韧带的异位骨化中的枢转作用。结果提供了强有力的证据表明我们建立的MiRNA监管网络可能确实在OPLL发作和进展中起到重要作用。迄今为止,这是OPLL中微米体的第一次系统分析,因此可以提供有价值的资源来查找OPLL的新型处理和诊断目标。

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