Single-cell long-read mRNA isoform regulation is pervasive across mammalian brain regions, cell types, and development.
Anoushka JoglekarWen HuBei ZhangOleksandr NarykovMark DiekhansJennifer BalaccoLishomwa C NdhlovuTeresa A MilnerOlivier FedrigoErich D JarvisGloria SheynkmanDmitry KorkinM Elizabeth RossHagen U TilgnerPublished in: bioRxiv : the preprint server for biology (2023)
RNA isoforms influence cell identity and function. Until recently, technological limitations prevented a genome-wide appraisal of isoform influence on cell identity in various parts of the brain. Using enhanced long-read single-cell isoform sequencing, we comprehensively analyze RNA isoforms in multiple mouse brain regions, cell subtypes, and developmental timepoints from postnatal day 14 (P14) to adult (P56). For 75% of genes, full-length isoform expression varies along one or more axes of phenotypic origin, underscoring the pervasiveness of isoform regulation across multiple scales. As expected, splicing varies strongly between cell types. However, certain gene classes including neurotransmitter release and reuptake as well as synapse turnover, harbor significant variability in the same cell type across anatomical regions, suggesting differences in network activity may influence cell-type identity. Glial brain-region specificity in isoform expression includes strong poly(A)-site regulation, whereas neurons have stronger TSS regulation. Furthermore, developmental patterns of cell-type specific splicing are especially pronounced in the murine adolescent transition from P21 to P28. The same cell type traced across development shows more isoform variability than across adult anatomical regions, indicating a coordinated modulation of functional programs dictating neural development. As most cell-type specific exons in P56 mouse hippocampus behave similarly in newly generated data from human hippocampi, these principles may be extrapolated to human brain. However, human brains have evolved additional cell-type specificity in splicing, suggesting gain-of-function isoforms. Taken together, we present a detailed single-cell atlas of full-length brain isoform regulation across development and anatomical regions, providing a previously unappreciated degree of isoform variability across multiple scales of the brain.
Keyphrases
- single cell
- rna seq
- genome wide
- high throughput
- white matter
- cell therapy
- resting state
- endothelial cells
- stem cells
- dna methylation
- preterm infants
- cerebral ischemia
- bone marrow
- functional connectivity
- brain injury
- long non coding rna
- subarachnoid hemorrhage
- bone mineral density
- single molecule
- neuropathic pain
- deep learning
- spinal cord injury
- big data
- blood brain barrier
- copy number