Human cortical neural progenitor cell transplantation holds significant potential in cortical stroke treatment by replacing lost cortical neurons and repairing damaged brain circuits. However, commonly utilized human cortical neural progenitors are limited in yield a substantial proportion of diverse cortical neurons and require an extended period to achieve functional maturation and synaptic integration, thereby potentially diminishing the optimal therapeutic benefits of cell transplantation for cortical stroke. Here, we generated forkhead box G1 (FOXG1)-positive forebrain progenitors from human inducible pluripotent stem cells, which can differentiate into diverse and balanced cortical neurons including upper- and deep-layer excitatory and inhibitory neurons, achieving early functional maturation simultaneously in vitro. Furthermore, these FOXG1 forebrain progenitor cells demonstrate robust cortical neuronal differentiation, rapid functional maturation and efficient synaptic integration after transplantation into the sensory cortex of stroke-injured adult rats. Notably, we have successfully utilized the non-invasive (18)F-SynVesT-1 PET imaging technique to assess alterations in synapse count before and after transplantation therapy of FOXG1 progenitors in vivo. Moreover, the transplanted FOXG1 progenitors improve sensory and motor function recovery following stroke. These findings provide systematic and compelling evidence for the suitability of these FOXG1 progenitors for neuronal replacement in ischemic cortical stroke.
Forebrain neural progenitors effectively integrate into host brain circuits and improve neural function after ischemic stroke.
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作者:He Xiao, Chen Jiadong, Zhong Yan, Cen Peili, Shen Li, Huang Fei, Wang Jing, Jin Chentao, Zhou Rui, Zhang Xiaohui, Wang Anxin, Fan Jing, Wu Shuang, Tu Mengjiao, Qin Xiyi, Luo Xiaoyun, Zhou Yu, Peng Jieqiao, Zhou Youyou, Civelek A Cahid, Tian Mei, Zhang Hong
期刊: | Nature Communications | 影响因子: | 15.700 |
时间: | 2025 | 起止号: | 2025 Jun 3; 16(1):5132 |
doi: | 10.1038/s41467-025-60187-5 |
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