Microglia, the innate immune cells of the central nervous system, have been genetically implicated in multiple neurodegenerative diseases. We previously mapped the genetic regulation of gene expression and mRNA splicing in human microglia, identifying several loci where common genetic variants in microglia-specific regulatory elements explain disease risk loci identified by GWAS. However, identifying genetic effects on splicing has been challenging due to the use of short sequencing reads to identify causal isoforms. Here we present the isoform-centric microglia genomic atlas (isoMiGA) which leverages the power of long-read RNA-seq to identify 35,879 novel microglia isoforms. We show that the novel microglia isoforms are involved in stimulation response and brain region specificity. We then quantified the expression of both known and novel isoforms in a multi-ethnic meta-analysis of 555 human microglia short-read RNA-seq samples from 391 donors, the largest to date, and found associations with genetic risk loci in Alzheimer's disease and Parkinson's disease. We nominate several loci that may act through complex changes in isoform and splice site usage.
Long-read RNA-seq atlas of novel microglia isoforms elucidates disease-associated genetic regulation of splicing.
新型小胶质细胞亚型的长读长 RNA-seq 图谱阐明了与疾病相关的剪接基因调控
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作者:Humphrey Jack, Brophy Erica, Kosoy Roman, Zeng Biao, Coccia Elena, Mattei Daniele, Ravi Ashvin, Efthymiou Anastasia G, Navarro Elisa, Muller Benjamin Z, Snijders Gijsje Jlj, Allan Amanda, Münch Alexandra, Kitata Reta Birhanu, Kleopoulos Steven P, Argyriou Stathis, Shao Zhiping, Francoeur Nancy, Tsai Chia-Feng, Gritsenko Marina A, Monroe Matthew E, Paurus Vanessa L, Weitz Karl K, Shi Tujin, Sebra Robert, Liu Tao, de Witte Lot D, Goate Alison M, Bennett David A, Haroutunian Vahram, Hoffman Gabriel E, Fullard John F, Roussos Panos, Raj Towfique
| 期刊: | medRxiv | 影响因子: | 0.000 |
| 时间: | 2023 | 起止号: | 2023 Dec 1 |
| doi: | 10.1101/2023.12.01.23299073 | 研究方向: | 细胞生物学 |
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