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Specification of neural circuit architecture shaped by context-dependent patterned LAR-RPTP microexons

Author

Listed:
  • Kyung Ah Han

    (Daegu Gyeongbuk Institute of Science and Technology (DGIST)
    Center for Synapse Diversity and Specificity, DGIST)

  • Taek-Han Yoon

    (Daegu Gyeongbuk Institute of Science and Technology (DGIST))

  • Jinhu Kim

    (Daegu Gyeongbuk Institute of Science and Technology (DGIST))

  • Jusung Lee

    (DGIST)

  • Ju Yeon Lee

    (Korea Basic Science Institute, Research Center for Bioconvergence Analysis)

  • Gyubin Jang

    (Daegu Gyeongbuk Institute of Science and Technology (DGIST)
    Center for Synapse Diversity and Specificity, DGIST)

  • Ji Won Um

    (Daegu Gyeongbuk Institute of Science and Technology (DGIST)
    Center for Synapse Diversity and Specificity, DGIST)

  • Jong Kyoung Kim

    (DGIST
    Pohang University of Science and Technology (POSTECH))

  • Jaewon Ko

    (Daegu Gyeongbuk Institute of Science and Technology (DGIST)
    Center for Synapse Diversity and Specificity, DGIST)

Abstract

LAR-RPTPs are evolutionarily conserved presynaptic cell-adhesion molecules that orchestrate multifarious synaptic adhesion pathways. Extensive alternative splicing of LAR-RPTP mRNAs may produce innumerable LAR-RPTP isoforms that act as regulatory “codes” for determining the identity and strength of specific synapse signaling. However, no direct evidence for this hypothesis exists. Here, using targeted RNA sequencing, we detected LAR-RPTP mRNAs in diverse cell types across adult male mouse brain areas. We found pronounced cell-type–specific patterns of two microexons, meA and meB, in Ptprd mRNAs. Moreover, diverse neural circuits targeting the same neuronal populations were dictated by the expression of different Ptprd variants with distinct inclusion patterns of microexons. Furthermore, conditional ablation of Ptprd meA+ variants at presynaptic loci of distinct hippocampal circuits impaired distinct modes of synaptic transmission and objection-location memory. Activity-triggered alterations of the presynaptic Ptprd meA code in subicular neurons mediates NMDA receptor-mediated postsynaptic responses in CA1 neurons and objection-location memory. Our data provide the evidence of cell-type- and/or circuit-specific expression patterns in vivo and physiological functions of LAR-RPTP microexons that are dynamically regulated.

Suggested Citation

  • Kyung Ah Han & Taek-Han Yoon & Jinhu Kim & Jusung Lee & Ju Yeon Lee & Gyubin Jang & Ji Won Um & Jong Kyoung Kim & Jaewon Ko, 2024. "Specification of neural circuit architecture shaped by context-dependent patterned LAR-RPTP microexons," Nature Communications, Nature, vol. 15(1), pages 1-21, December.
    • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-45695-0
    DOI: 10.1038/s41467-024-45695-0
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    References listed on IDEAS

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    1. Shuo Li & Sumana Raychaudhuri & Stephen Alexander Lee & Marisa M. Brockmann & Jing Wang & Grant Kusick & Christine Prater & Sarah Syed & Hanieh Falahati & Raul Ramos & Tomas M. Bartol & Eric Hosy & Sh, 2021. "Asynchronous release sites align with NMDA receptors in mouse hippocampal synapses," Nature Communications, Nature, vol. 12(1), pages 1-13, December.
    2. Marina Reixachs-Solé & Jorge Ruiz-Orera & M. Mar Albà & Eduardo Eyras, 2020. "Ribosome profiling at isoform level reveals evolutionary conserved impacts of differential splicing on the proteome," Nature Communications, Nature, vol. 11(1), pages 1-12, December.
    3. Alberto Parras & Héctor Anta & María Santos-Galindo & Vivek Swarup & Ainara Elorza & José L. Nieto-González & Sara Picó & Ivó H. Hernández & Juan I. Díaz-Hernández & Eulàlia Belloc & Annie Rodolosse &, 2018. "Autism-like phenotype and risk gene mRNA deadenylation by CPEB4 mis-splicing," Nature, Nature, vol. 560(7719), pages 441-446, August.
    4. Ji Won Um & Kee Hun Kim & Beom Seok Park & Yeonsoo Choi & Doyoun Kim & Cha Yeon Kim & Soo Jin Kim & Minhye Kim & Ji Seung Ko & Seong-Gyu Lee & Gayoung Choii & Jungyong Nam & Won Do Heo & Eunjoon Kim &, 2014. "Structural basis for LAR-RPTP/Slitrk complex-mediated synaptic adhesion," Nature Communications, Nature, vol. 5(1), pages 1-16, December.
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