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iPS-cell-derived microglia promote brain organoid maturation via cholesterol transfer

Author

Listed:
  • Dong Shin Park

    (Technology and Research
    National University of Singapore)

  • Tatsuya Kozaki

    (Technology and Research)

  • Satish Kumar Tiwari

    (Technology and Research)

  • Marco Moreira

    (INSERM U1015, Gustave Roussy Cancer Campus)

  • Ahad Khalilnezhad

    (Technology and Research
    National University of Singapore)

  • Federico Torta

    (National University of Singapore
    National University of Singapore)

  • Nicolas Olivié

    (Institut de Biologie de l’Ecole Normale Supérieure (IBENS), Ecole Normale Supérieure, CNRS, INSERM, PSL Research University)

  • Chung Hwee Thiam

    (National University of Singapore)

  • Oniko Liani

    (Technology and Research)

  • Aymeric Silvin

    (Technology and Research
    INSERM U1015, Gustave Roussy Cancer Campus)

  • Wint Wint Phoo

    (Agency for Science, Technology and Research)

  • Liang Gao

    (National University of Singapore
    National University of Singapore)

  • Alexander Triebl

    (National University of Singapore
    National University of Singapore)

  • Wai Kin Tham

    (National University of Singapore)

  • Leticia Gonçalves

    (INSERM U1015, Gustave Roussy Cancer Campus)

  • Wan Ting Kong

    (Technology and Research
    INSERM U1015, Gustave Roussy Cancer Campus)

  • Sethi Raman

    (Technology and Research)

  • Xiao Meng Zhang

    (Technology and Research)

  • Garett Dunsmore

    (INSERM U1015, Gustave Roussy Cancer Campus)

  • Charles Antoine Dutertre

    (Technology and Research
    INSERM U1015, Gustave Roussy Cancer Campus)

  • Salanne Lee

    (Technology and Research)

  • Jia Min Ong

    (Technology and Research)

  • Akhila Balachander

    (Technology and Research)

  • Shabnam Khalilnezhad

    (Technology and Research
    SingHealth Duke-NUS Academic Medical Centre)

  • Josephine Lum

    (Technology and Research)

  • Kaibo Duan

    (Technology and Research)

  • Ze Ming Lim

    (Technology and Research)

  • Leonard Tan

    (Technology and Research)

  • Ivy Low

    (Technology and Research)

  • Kagistia Hana Utami

    (Technology and Research)

  • Xin Yi Yeo

    (Technology and Research)

  • Sylvaine Tommaso

    (Oncoprot Platform, TBM-Core US 005)

  • Jean-William Dupuy

    (University of Bordeaux)

  • Balazs Varga

    (University of Cambridge)

  • Ragnhildur Thora Karadottir

    (University of Cambridge)

  • Mufeeda Changaramvally Madathummal

    (Research Support Centre, Agency for Science, Technology and Research (A*STAR))

  • Isabelle Bonne

    (National University of Singapore)

  • Benoit Malleret

    (Technology and Research
    National University of Singapore
    Research Support Centre, Agency for Science, Technology and Research (A*STAR))

  • Zainab Yasin Binte

    (Technology and Research)

  • Ngan Wei Da

    (Technology and Research)

  • Yingrou Tan

    (Technology and Research)

  • Wei Jie Wong

    (Shanghai Jiao Tong University School of Medicine)

  • Jinqiu Zhang

    (Technology and Research)

  • Jinmiao Chen

    (Technology and Research)

  • Radoslaw M. Sobota

    (Agency for Science, Technology and Research)

  • Shanshan W. Howland

    (Technology and Research)

  • Lai Guan Ng

    (Technology and Research
    National University of Singapore
    Shanghai Jiao Tong University School of Medicine)

  • Frédéric Saltel

    (Oncoprot Platform, TBM-Core US 005)

  • David Castel

    (Université Paris-Saclay)

  • Jacques Grill

    (Université Paris-Saclay)

  • Veronique Minard

    (INSERM U1015, Gustave Roussy Cancer Campus)

  • Salvatore Albani

    (SingHealth Duke-NUS Academic Medical Centre)

  • Jerry K. Y. Chan

    (KK Women’s and Children’s Hospital)

  • Morgane Sonia Thion

    (Institut de Biologie de l’Ecole Normale Supérieure (IBENS), Ecole Normale Supérieure, CNRS, INSERM, PSL Research University)

  • Sang Yong Jung

    (Technology and Research
    CHA University)

  • Markus R. Wenk

    (National University of Singapore
    National University of Singapore)

  • Mahmoud A. Pouladi

    (Technology and Research
    University of British Columbia
    British Columbia Children’s Hospital Research Institute)

  • Claudia Pasqualini

    (INSERM U1015, Gustave Roussy Cancer Campus)

  • Veronique Angeli

    (National University of Singapore)

  • Olivier N. F. Cexus

    (National University of Singapore
    Technology and Research
    University of Surrey)

  • Florent Ginhoux

    (Technology and Research
    National University of Singapore
    INSERM U1015, Gustave Roussy Cancer Campus
    SingHealth Duke-NUS Academic Medical Centre)

Abstract

Microglia are specialized brain-resident macrophages that arise from primitive macrophages colonizing the embryonic brain1. Microglia contribute to multiple aspects of brain development, but their precise roles in the early human brain remain poorly understood owing to limited access to relevant tissues2–6. The generation of brain organoids from human induced pluripotent stem cells recapitulates some key features of human embryonic brain development7–10. However, current approaches do not incorporate microglia or address their role in organoid maturation11–21. Here we generated microglia-sufficient brain organoids by coculturing brain organoids with primitive-like macrophages generated from the same human induced pluripotent stem cells (iMac)22. In organoid cocultures, iMac differentiated into cells with microglia-like phenotypes and functions (iMicro) and modulated neuronal progenitor cell (NPC) differentiation, limiting NPC proliferation and promoting axonogenesis. Mechanistically, iMicro contained high levels of PLIN2+ lipid droplets that exported cholesterol and its esters, which were taken up by NPCs in the organoids. We also detected PLIN2+ lipid droplet-loaded microglia in mouse and human embryonic brains. Overall, our approach substantially advances current human brain organoid approaches by incorporating microglial cells, as illustrated by the discovery of a key pathway of lipid-mediated crosstalk between microglia and NPCs that leads to improved neurogenesis.

Suggested Citation

  • Dong Shin Park & Tatsuya Kozaki & Satish Kumar Tiwari & Marco Moreira & Ahad Khalilnezhad & Federico Torta & Nicolas Olivié & Chung Hwee Thiam & Oniko Liani & Aymeric Silvin & Wint Wint Phoo & Liang G, 2023. "iPS-cell-derived microglia promote brain organoid maturation via cholesterol transfer," Nature, Nature, vol. 623(7986), pages 397-405, November.
    • Handle: RePEc:nat:nature:v:623:y:2023:i:7986:d:10.1038_s41586-023-06713-1
    DOI: 10.1038/s41586-023-06713-1
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    Cited by:

    1. Jiayi Wang & Mengke Zhao & Meina Wang & Dong Fu & Lin Kang & Yu Xu & Liming Shen & Shilin Jin & Liang Wang & Jing Liu, 2024. "Human neural stem cell-derived artificial organelles to improve oxidative phosphorylation," Nature Communications, Nature, vol. 15(1), pages 1-24, December.

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