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Transcriptome analysis using RNA sequencing of the hippocampus of aged LPAR2-/- versus wildtype control mice

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干细胞与再生医学数据中心2022-02-20 更新2024-03-06 收录
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http://data.iscr.ac.cn/Article?id=24b17a125f4fd66bb7c074791b7e32fd
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We assessed the effect of a deletion of the lysophosphatidic acid receptor, LPAR2 in mice on gene regulation in the hippocampus of aged mice by comparing RNA-seq expression profiles. Presynaptic LPAR2 fortifies the release of glutamate, hence increases neuronal excitability and baseline activity. LPAR2 deficiency prevents an age-associated hyperexcitability and decline of hippocampal long-term-potentiation and improves repose and attention in behaving animals. RNAseq was performed to assess if these protective features manifested at the expressional level of pro-longevity or pro-aging genes. A total number of 18126 genes was reliably detected, and 16420 passed the filtering criteria of >3 valid samples per group. GSEA gene set enrichment analysis was used for gene ranking and identication of top up- and downregulated genes and evaluation of their functions based on P-value, Q-value, fold change and abundance. Among the top downregulated genes were several typical neuronal activity markers including Fos, Fosb, Egr2 suggesting that indeed neuronal baseline activity was lower in LPAR2-/- hippocampus.
提供机构:
University Hospital Frankfurt
创建时间:
2022-02-20
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