Microglial cells, the innate immune cells of the brain, are derived from yolk sac precursor cells, begin to colonize the telencephalon at the onset of cortical neurogenesis, and occupy specific layers including the telencephalic proliferative zones. Microglia are an intrinsic component of cortical germinal zones, establish extensive contacts with neural precursor cells (NPCs) and developing cortical vessels, and regulate the size of the NPC pool through mechanisms that include phagocytosis. Microglia exhibit notable differences in number and distribution in the prenatal neocortex between rat and Old World nonhuman primate telencephalon, suggesting that microglia exhibit distinct properties across vertebrate species. To begin addressing this subject we quantified the number of microglia and NPCs in proliferative zones of the fetal human, rhesus monkey, ferret, and rat, and the pre-hatch chick and turtle telencephalon. We show that the ratio of NPCs to microglia varies significantly across species. Few microglia populate the pre-hatch chick telencephalon, but the number of microglia approaches that of NPCs in fetal human and non-human primate telencephalon. These data demonstrate that microglia are in a position to perform similar functions in a number of vertebrate species, but more heavily colonize proliferative zones of fetal human and rhesus monkey telencephalon.
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