Simultaneous miRNA and mRNA transcriptome profiling of human myoblasts reveals a novel set of myogenic differentiation-associated miRNAs and their target genes

Dmitriev, Petr; Barat, Ana; Polesskaya, Anna; O’Connell, Mary J.; Thomas, Robert; Dessen, Philippe; Walsh, Thomas A.; Lazar, Vladimir; Turki, Ahmed; Carnac, Gilles; Laoudj-Chenivesse, Dalila; Lipinski, Marc; Vassetzky, Yegor S.

doi:10.1186/1471-2164-14-265

Cited by 79 publications

(79 citation statements)

References 117 publications

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“…The level of expression of miRNA targets in a system is relevant for increasing the success rate in the target prediction [10]. By selecting just the mRNAs that were overexpressed in the transition in situ to metastatic cells, we take into consideration the specific cellular context allowing a more precise prediction.…”

Section: Discussionmentioning

confidence: 99%

“…To perform microarray data analysis we used R language and the Limma package on Bioconductor software essentially as described in [10]. Data were background corrected using AgiMicroRNA algorithm and normalized between arrays by the quantile method in order to compensate for systematic technical differences between probe affinity and arrays.…”

Section: Methodsmentioning

confidence: 99%

“…To increase the accuracy in miR-205-5p in silico target prediction we used as approach a combined miRNA and mRNA transcriptome profiling [10]. First, the mRNAs that had the expression increased more than two fold in 21T cells during the transition in situ to metastatic tumor (21MT1 vs 21NT) were selected from a published database [8].…”

Section: Methodsmentioning

confidence: 99%

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The microRNA-205-5p is correlated to metastatic potential of 21T series: A breast cancer progression model

et al. 2017

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MicroRNA is a class of noncoding RNAs able to base pair with complementary messenger RNA sequences, inhibiting their expression. These regulatory molecules play important roles in key cellular processes including cell proliferation, differentiation and response to DNA damage; changes in miRNA expression are a common feature of human cancers. To gain insights into the mechanisms involved in breast cancer progression we conducted a microRNA global expression analysis on a 21T series of cell lines obtained from the same patient during different stages of breast cancer progression. These stages are represented by cell lines derived from normal epithelial (H16N2), atypical ductal hyperplasia (21PT), primary in situ ductal carcinoma (21NT) and pleural effusion of a lung metastasis (21MT-1 and 21MT-2). In a global microRNA expression analysis, miR-205-5p was the only miRNA to display an important downregulation in the metastatic cell lines (21MT-1; 21MT-2) when compared to the non-invasive cells (21PT and 21NT). The lower amounts of miR-205-5p found also correlated with high histological grades biopsies and with higher invasion rates in a Boyden chamber assay. This work pinpoints miR-205-5p as a potential player in breast tumor invasiveness.

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Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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The microRNA-205-5p is correlated to metastatic potential of 21T series: A breast cancer progression model

et al. 2017

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“…The data shown in Fig. 15a suggest that myostatin propeptide may stimulate myogenesis by upregulating miR-23b, as miR-23b is known as a myogenic miRNA (Dmitriev et al, 2013). The myostatin propeptide also upregulates let-7e, and the let-7 group of miRNAs are known to suppress cell proliferation.…”

Section: Year 4 Addendum (May 2014-november 2014)mentioning

confidence: 95%

Novel Therapeutic Strategy for the Prevention of Bone Fractures

Hamrick¹

2015

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“…miR23a, 30b, 98, 101, 148b, 206, 145, 199a and let-7 have in silico-predicted targets that are involved in the insulin signalling pathway), it is difficult to determine which of the suggested miRNAs are false positive and which are the true positive. Data from animal studies, muscular disease models, exercise experiments and ageing research by other groups also support, to various extent, the involvement of miR-206, miR-23a, miR23b, miR-30b and miR-98 in muscle atrophy (Drummond et al 2008, Granjon et al 2009, Jeng et al 2009, McCarthy et al 2009, Williams et al 2009, Nakasa et al 2010, Nielsen et al 2010, Wada et al 2011, Liu et al 2012, Dmitriev et al 2013. Recently, a study analysing the expression of miRNA in different mouse models of muscle atrophy showed that each model has a different signature of miRNA changes and, more importantly, that there is a temporal change in miRNA expression (Soares et al 2014).…”

mentioning

confidence: 95%