AI Article Synopsis

  • The study explores the complex process of RNA expression and splicing during early human embryo development, utilizing both long- and short-read RNA sequencing on 73 embryos.
  • It identifies over 110,000 new RNA isoforms from known genes and nearly 18,000 isoforms from unannotated genes, revealing a rich landscape of non-coding RNA and associations with transposable elements.
  • The findings highlight significant complexity in the human embryo transcriptome, suggesting a need for refined exploration of embryonic development in future research.

Article Abstract

Human preimplantation development involves extensive remodeling of RNA expression and splicing. However, its transcriptome has been compiled using short-read sequencing data, which fails to capture most full-length mRNAs. Here, we generate an isoform-resolved transcriptome of early human development by performing long- and short-read RNA sequencing on 73 embryos spanning the zygote to blastocyst stages. We identify 110,212 unannotated isoforms transcribed from known genes, including highly conserved protein-coding loci and key developmental regulators. We further identify 17,964 isoforms from 5,239 unannotated genes, which are largely non-coding, primate-specific, and highly associated with transposable elements. These isoforms are widely supported by the integration of published multi-omics datasets, including single-cell 8CLC and blastoid studies. Alternative splicing and gene co-expression network analyses further reveal that embryonic genome activation is associated with splicing disruption and transient upregulation of gene modules. Together, these findings show that the human embryo transcriptome is far more complex than currently known, and will act as a valuable resource to empower future studies exploring development.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10616205PMC
http://dx.doi.org/10.1038/s41467-023-42558-yDOI Listing

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