Developmental isoform diversity in the human neocortex informs neuropsychiatric risk mechanisms.

Ashok Patowary,Ashok Patowary,Ashok Patowary,Ashok Patowary,Bogdan Pasaniuc,Minsoo Kim,Connor Jops,Pan Zhang,Bogdan Pasaniuc,Xusheng Wang,Luis De La Torre-Ubieta,Bogdan Pasaniuc,Luis De La Torre-Ubieta,Bogdan Pasaniuc,Minsoo Kim,Chunyu Liu,Jingyi Jessica Li,Minsoo Kim,Daniel Vo,Celine K Vuong,Michael Margolis,Jingyi Jessica Li,Chunyu Liu,Kangcheng Hou,Michael J Gandal,Michael J Gandal,Pan Zhang,Celine K Vuong,Connor Jops,Xinzhou Ge,Celine K Vuong,Michael J Gandal,Jingyi Jessica Li,Naihua Gong,Michael J Gandal,Bogdan Pasaniuc,Jingyi Jessica Li,Pan Zhang,Daniel Vo,Michael J Gandal,Luis De La Torre-Ubieta,Xusheng Wang,Jingyi Jessica Li,Pan Zhang,Connor Jops,Daniel Vo

doi:10.1126/science.adh7688

Abstract

RNA splicing is highly prevalent in the brain and has strong links to neuropsychiatric disorders; yet, the role of cell type-specific splicing and transcript-isoform diversity during human brain development has not been systematically investigated. In this work, we leveraged single-molecule long-read sequencing to deeply profile the full-length transcriptome of the germinal zone and cortical plate regions of the developing human neocortex at tissue and single-cell resolution. We identified 214,516 distinct isoforms, of which 72.6% were novel (not previously annotated in Gencode version 33), and uncovered a substantial contribution of transcript-isoform diversity-regulated by RNA binding proteins-in defining cellular identity in the developing neocortex. We leveraged this comprehensive isoform-centric gene annotation to reprioritize thousands of rare de novo risk variants and elucidate genetic risk mechanisms for neuropsychiatric disorders.

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