Long-read transcript sequencing identifies differential isoform expression in the entorhinal cortex in a transgenic model of tau pathology.
Szi Kay LeungRosemary A BamfordAaron R JeffriesIsabel CastanhoBarry A ChiozaChristine S FlaxmanKaren MooreEmma L DempsterJoshua HarveyJonathan T BrownZeshan AhmedPaul O'NeillSarah J RichardsonEilis J HannonJonathan S MillPublished in: Nature communications (2024)
Increasing evidence suggests that alternative splicing plays an important role in Alzheimer's disease (AD) pathology. We used long-read sequencing in combination with a novel bioinformatics tool (FICLE) to profile transcript diversity in the entorhinal cortex of female transgenic (TG) mice harboring a mutant form of human tau. Our analyses revealed hundreds of novel isoforms and identified differentially expressed transcripts - including specific isoforms of Apoe, App, Cd33, Clu, Fyn and Trem2 - associated with the development of tau pathology in TG mice. Subsequent profiling of the human cortex from AD individuals and controls revealed similar patterns of transcript diversity, including the upregulation of the dominant TREM2 isoform in AD paralleling the increased expression of the homologous transcript in TG mice. Our results highlight the importance of differential transcript usage, even in the absence of gene-level expression alterations, as a mechanism underpinning gene regulation in the development of AD neuropathology.
Keyphrases
- single cell
- rna seq
- poor prognosis
- endothelial cells
- high fat diet induced
- functional connectivity
- cerebrospinal fluid
- wild type
- binding protein
- long non coding rna
- cognitive decline
- single molecule
- genome wide
- induced pluripotent stem cells
- dna damage
- cell proliferation
- high fat diet
- type diabetes
- gene expression
- copy number
- signaling pathway
- metabolic syndrome
- insulin resistance
- oxidative stress
- mild cognitive impairment
- transcription factor