4.7 Article

Human Stem Cell-Derived Neurons Repair Circuits and Restore Neural Function

期刊

CELL STEM CELL
卷 28, 期 1, 页码 112-+

出版社

CELL PRESS
DOI: 10.1016/j.stem.2020.08.014

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资金

  1. National Key Research and Development Program of China [2018YFA0108000]
  2. Strategic Priority Research Program of the Chinese Academy of Sciences [XDA16010310]
  3. Shanghai Municipal Science and Technology Major Project [2018SHZDZX05]
  4. NIH-NINDS [NS096282, NS076352, NS086604]
  5. NIH-NIMH [MH099587, MH100031]
  6. Bleser Family Foundation
  7. Busta Foundation
  8. NICHD [U54 HD090256]
  9. National Medical Research Council of Singapore [MOH-000212, MOH-000207]
  10. National Natural Science Foundation of China [31771137, 31722024, 81974174, 31700887]
  11. Thousand Young Talents Program
  12. Shanghai Natural Science Foundation [17ZR1448500]
  13. Shanghai Rising-Star Program [17QA1400600]
  14. Shanghai Pujiang Program [17PJ1410200]

向作者/读者索取更多资源

The study demonstrates that human embryonic stem cell-derived neurons have the ability to repair specific circuits and restore functionality in the adult brain, leading to improvements in motor function.
Although cell transplantation can rescue motor defects in Parkinson's disease (PD) models, whether and how grafts functionally repair damaged neural circuitry in the adult brain is not known. We transplanted hESC-derived midbrain dopamine (mDA) or cortical glutamate neurons into the substantia nigra or striatum of a mouse PD model and found extensive graft integration with host circuitry. Axonal pathfinding toward the dorsal striatum was determined by the identity of the grafted neurons, and anatomical presynaptic inputs were largely dependent on graft location, whereas inhibitory versus excitatory input was dictated by the identity of grafted neurons. hESC-derived mDA neurons display A9 characteristics and restore functionality of the reconstructed nigrostriatal circuit to mediate improvements in motor function. These results indicate similarity in cell-type-specific pre- and post-synaptic integration between transplant-reconstructed circuit and endogenous neural networks, highlighting the capacity of hPSC-derived neuron subtypes for specific circuit repair and functional restoration in the adult brain.

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