Neural stem and progenitor cells support and protect adult hippocampal function via vascular endothelial growth factor secretion.

神经干细胞和祖细胞通过分泌血管内皮生长因子来支持和保护成年海马体的功能

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作者:Miller Lisa N, Walters Ashley E, Denninger Jiyeon K, Hanson Meretta A, Marshall Alec H, Johantges Aidan C, Hosawi Manal, Sebring Gwendolyn, Rieskamp Joshua D, Ding Tianli, Rindani Raina, Chen Kelly S, Goldberg Megan E, Senthilvelan Sakthi, Volk Abigail, Zhao Fangli, Askwith Candice, Wester Jason C, Kirby Elizabeth D
Adult neural stem and progenitor cells (NSPCs) reside in the dentate gyrus (DG) of the hippocampus throughout the lifespan of most mammalian species. In addition to generating new neurons, NSPCs may alter their niche via secretion of growth factors and cytokines. We recently showed that adult DG NSPCs secrete vascular endothelial growth factor (VEGF), which is critical for maintaining adult neurogenesis. Here, we asked whether NSPC-derived VEGF alters hippocampal function independent of adult neurogenesis. We found that loss of NSPC-derived VEGF acutely impaired hippocampal memory, caused neuronal hyperexcitability and exacerbated excitotoxic injury. Conversely, we observed that overexpression of VEGF reduced microglial response to excitotoxic injury. We also found that NSPCs generate substantial proportions of total DG VEGF and VEGF disperses widely throughout the DG, both of which help explain how this anatomically-restricted cell population could modulate function broadly. These findings suggest that NSPCs actively support and protect DG function via secreted VEGF, thereby providing a non-neurogenic functional dimension to endogenous NSPCs.

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