Abstract

<b>Rationale:</b> Monocytes belong to the mononuclear phagocyte system and are immune responders to tissue injury and infection. There were also reports of monocytes transforming to microglia-like cells. Here we explore the roles of monocytes in microglia ontogeny and the pathogenesis of neonatal cerebral hypoxic-ischemic (HI) brain injury in mice. <b>Methods:</b> We used three genetic methods to track the development of monocytes, including CX3CR1^GFP/+; CCR2^RFP/+ reporter mice, adoptive transfer of GFP⁺ monocytes, and fate-mapping with CCR2-CreER mice, in neonatal mouse brains with or without lipopolysaccharide (LPS, 0.3 mg/kg)-sensitized Vannucci HI. We also used genetic (CCR2^{RFP/ RFP}, CCR2 knockout) and pharmacological methods (RS102895, a CCR2 antagonist) to test the roles of monocytic influx in LPS/HI brain injury. <b>Results:</b> CCR2⁺ monocytes entered the late-embryonic brains via choroid plexus, but rapidly became CX3CR1⁺ amoeboid microglial cells (AMCs). The influx of CCR2⁺ monocytes declined after birth, but recurred after HI or LPS-sensitized HI (LPS/HI) brain injury, particularly in the hippocampus. The CCR2-CreER-based fate-mapping showed that CCR2⁺ monocytes became CD68⁺ TNFα⁺ macrophages within 4 d after LPS/HI, and maintained as TNFα⁺ MHCII⁺ macrophages or persisted as Tmem119⁺ Sall1⁺ P2RY12⁺ ramified microglia for at least five months after injury. Genetic deletion of the chemokine receptor CCR2 markedly diminished monocytic influx, the expression of pro- and anti-inflammatory cytokines, and brain damage. Post-LPS/HI application of RS102895 also reduced inflammatory responses and brain damage, leading to better cognitive functions. <b>Conclusion:</b> These results suggest that monocytes promote acute inflammatory responses and may become pathological microglia long after the neonatal LPS/HI insult. Further, blocking the influx of monocytes may be a potential therapy for neonatal brain injury.