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Secondary microglia formation center in the human fetal brain

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Abstract Yolk sac-derived microglia migrate and populate the brain during development, constituting 10−15% of the total brain cells. The human brain is the largest and most complex brain with the highest cognitive capacity among all species. Therefore, the limitations of rodent brain studies in interpreting the human brain are evident. By co-immunostaining microglia in 50 µm fetal brain sections from 7.5 to 16 gestational weeks (gw) and combining high-resolution scanning, we identified a highly proliferative microglia aggregate (0.108−2.129 mm 2 ) that expanded in Down’s Syndrome fetal brain (4.168 mm 2 ) and was located near the ganglion eminence, in which Ki67 + microglia accounted for 23.4% of total microglia compared to 6.3% in other brain regions. The microglia in the aggregates lack phagocytic bulbs, membrane ruffles, and long/branching processes compared to microglia in other brain regions. Introducing human microglia into cortical organoids, but not macrophages, replicated proliferative microglial aggregates on the brain organoid surface and sufficiently penetrated deeper regions of the cortical organoids. Penetrating microglia display phagocytic capacity, enhance immunity, and accelerate the maturation of brain organoids. The large proliferative microglial aggregate may be a unique secondary microglial formation center in the human fetal brain to compensate for the enormous microglial demands during brain expansion.
Title: Secondary microglia formation center in the human fetal brain
Description:
Abstract Yolk sac-derived microglia migrate and populate the brain during development, constituting 10−15% of the total brain cells.
The human brain is the largest and most complex brain with the highest cognitive capacity among all species.
Therefore, the limitations of rodent brain studies in interpreting the human brain are evident.
By co-immunostaining microglia in 50 µm fetal brain sections from 7.
5 to 16 gestational weeks (gw) and combining high-resolution scanning, we identified a highly proliferative microglia aggregate (0.
108−2.
129 mm 2 ) that expanded in Down’s Syndrome fetal brain (4.
168 mm 2 ) and was located near the ganglion eminence, in which Ki67 + microglia accounted for 23.
4% of total microglia compared to 6.
3% in other brain regions.
The microglia in the aggregates lack phagocytic bulbs, membrane ruffles, and long/branching processes compared to microglia in other brain regions.
Introducing human microglia into cortical organoids, but not macrophages, replicated proliferative microglial aggregates on the brain organoid surface and sufficiently penetrated deeper regions of the cortical organoids.
Penetrating microglia display phagocytic capacity, enhance immunity, and accelerate the maturation of brain organoids.
The large proliferative microglial aggregate may be a unique secondary microglial formation center in the human fetal brain to compensate for the enormous microglial demands during brain expansion.

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