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Publication : CCR2(+) monocytes replenish border-associated macrophages in the diseased mouse brain.

First Author  Wang L Year  2024
Journal  Cell Rep Volume  43
Issue  4 Pages  114120
PubMed ID  38625796 Mgi Jnum  J:348960
Mgi Id  MGI:7627877 Doi  10.1016/j.celrep.2024.114120
Citation  Wang L, et al. (2024) CCR2(+) monocytes replenish border-associated macrophages in the diseased mouse brain. Cell Rep 43(4):114120
abstractText  Border-associated macrophages (BAMs) are tissue-resident macrophages that reside at the border of the central nervous system (CNS). Since BAMs originate from yolk sac progenitors that do not persist after birth, the means by which this population of cells is maintained is not well understood. Using two-photon microscopy and multiple lineage-tracing strategies, we determine that CCR2(+) monocytes are significant contributors to BAM populations following disruptions of CNS homeostasis in adult mice. After BAM depletion, while the residual BAMs possess partial self-repopulation capability, the CCR2(+) monocytes are a critical source of the repopulated BAMs. In addition, we demonstrate the existence of CCR2(+) monocyte-derived long-lived BAMs in a brain compression model and in a sepsis model after the initial disruption of homeostasis. Our study reveals that the short-lived CCR2(+) monocytes transform into long-lived BAM-like cells at the CNS border and subsequently contribute to BAM populations.
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