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Characterizing expression changes in noncoding RNAs during aging and heterochronic parabiosis across mouse tissues

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https://www.ncbi.nlm.nih.gov/sra/SRP406682
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Molecular mechanisms of organismal and cell aging remain incompletely understood. We, therefore, generated a body-wide map of noncoding RNA (ncRNA) expression in aging (16 organs at ten timepoints from 1 to 27 months) and rejuvenated mice. We found molecular aging trajectories are largely tissue-specific except for eight broadly deregulated microRNAs (miRNAs). Their individual abundance mirrors their presence in circulating plasma and extracellular vesicles (EVs) whereas tissue-specific ncRNAs were less present. For miR-29c-3p, we observe the largest correlation with aging in solid organs, plasma and EVs. In mice rejuvenated by heterochronic parabiosis, miR-29c-3p was the most prominent miRNA restored to similar levels found in young liver. miR-29c-3p targets the extracellular matrix and secretion pathways, known to be implicated in aging. We provide a map of organism-wide expression of ncRNAs with aging and rejuvenation and identify a set of broadly deregulated miRNAs, which may function as systemic regulators of aging via plasma and EVs. Overall design: This study contains the following two independent experimental setups, also denoted as experimental batches: 1. small non-coding RNAseq of all major organs of mice over the lifespan 2. small non-coding RNAseq of mice of a rejuvenation model (heterochronic parabiosis)
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2023-05-04
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