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Full-length transcriptome reconstruction reveals a large diversity of RNA and protein isoforms in rat hippocampus

Author

Listed:
  • Xi Wang

    (Max Delbrück Center for Molecular Medicine
    German Cancer Research Center)

  • Xintian You

    (Max Delbrück Center for Molecular Medicine
    Max Planck Institute for Molecular Genetics)

  • Julian D. Langer

    (Max Planck Institute for Brain Research)

  • Jingyi Hou

    (Max Delbrück Center for Molecular Medicine)

  • Fiona Rupprecht

    (Max Planck Institute for Brain Research)

  • Irena Vlatkovic

    (Max Planck Institute for Brain Research)

  • Claudia Quedenau

    (Max Delbrück Center for Molecular Medicine)

  • Georgi Tushev

    (Max Planck Institute for Brain Research)

  • Irina Epstein

    (Max Planck Institute for Brain Research)

  • Bernhard Schaefke

    (Southern University of Science and Technology
    Southern University of Science and Technology)

  • Wei Sun

    (Southern University of Science and Technology)

  • Liang Fang

    (Southern University of Science and Technology
    Southern University of Science and Technology)

  • Guipeng Li

    (Southern University of Science and Technology
    Southern University of Science and Technology)

  • Yuhui Hu

    (Southern University of Science and Technology)

  • Erin M. Schuman

    (Max Planck Institute for Brain Research)

  • Wei Chen

    (Southern University of Science and Technology
    Southern University of Science and Technology)

Abstract

Gene annotation is a critical resource in genomics research. Many computational approaches have been developed to assemble transcriptomes based on high-throughput short-read sequencing, however, only with limited accuracy. Here, we combine next-generation and third-generation sequencing to reconstruct a full-length transcriptome in the rat hippocampus, which is further validated using independent 5´ and 3´-end profiling approaches. In total, we detect 28,268 full-length transcripts (FLTs), covering 6,380 RefSeq genes and 849 unannotated loci. Based on these FLTs, we discover co-occurring alternative RNA processing events. Integrating with polysome profiling and ribosome footprinting data, we predict isoform-specific translational status and reconstruct an open reading frame (ORF)-eome. Notably, a high proportion of the predicted ORFs are validated by mass spectrometry-based proteomics. Moreover, we identify isoforms with subcellular localization pattern in neurons. Collectively, our data advance our knowledge of RNA and protein isoform diversity in the rat brain and provide a rich resource for functional studies.

Suggested Citation

  • Xi Wang & Xintian You & Julian D. Langer & Jingyi Hou & Fiona Rupprecht & Irena Vlatkovic & Claudia Quedenau & Georgi Tushev & Irina Epstein & Bernhard Schaefke & Wei Sun & Liang Fang & Guipeng Li & Y, 2019. "Full-length transcriptome reconstruction reveals a large diversity of RNA and protein isoforms in rat hippocampus," Nature Communications, Nature, vol. 10(1), pages 1-15, December.
    • Handle: RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-13037-0
    DOI: 10.1038/s41467-019-13037-0
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    Cited by:

    1. Huihui Liu & Hongchao Liu & Longhao Wang & Lei Song & Guixian Jiang & Qing Lu & Tao Yang & Hu Peng & Ruijie Cai & Xingle Zhao & Ting Zhao & Hao Wu, 2023. "Cochlear transcript diversity and its role in auditory functions implied by an otoferlin short isoform," Nature Communications, Nature, vol. 14(1), pages 1-19, December.

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