Systematic characterization of seed overlap microRNA cotargeting associated with lupus pathogenesis (small RNA-seq)
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https://www.ncbi.nlm.nih.gov/sra/SRP396593
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Background: Combinatorial gene regulation by multiple microRNAs (miRNAs) is widespread, and closely spaced target sites often act cooperatively to achieve stronger repression (âneighborhoodâ miRNA cotargeting). While miRNA cotarget sites are suggested to be more conserved and implicated in developmental control, the pathological significance of miRNA cotargeting remains elusive. Results: Here, we report pathogenic impacts of combinatorial miRNA regulation on inflammation in systemic lupus erythematosus (SLE). In the SLE mouse model, we identified downregulation of two miRNAs, miR-128 and miR-148a, by TLR7 stimulation in plasmacytoid dendritic cells. Functional analyses using human cell lines demonstrated that miR-128 and miR-148a additively target KLF4 via extensively overlapping target sites (âseed overlapâ miRNA cotargeting) and suppress the inflammatory responses. At the transcriptome level, âseed overlapâ miRNA cotargeting increases susceptibility to downregulation by two miRNAs, consistent with additive but not cooperative recruitment of two miRNAs. Systematic characterization further revealed that extensive âseed overlapâ is a prevalent feature among broadly conserved miRNAs. Highly conserved target sites of broadly conserved miRNAs are largely divided into two classesâthose conserved among eutherian mammals and from human to Coelacanth, and the latter, including KLF4-cotargeting sites, has a stronger association with both âseed overlapâ and âneighborhoodâ miRNA cotargeting. Furthermore, a deeply conserved miRNA target class has a higher probability of haplo-insufficient genes. Conclusions: Our study collectively suggests the complexity of distinct modes of miRNA cotargeting and importance of their perturbations in human diseases. Overall design: Small RNA sequencing (small RNA-seq) in pDCs from the IMQ-induced SLE mouse model.
创建时间:
2022-12-02



