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Long-lived self-renewing bone marrow-derived macrophages displace embryo-derived cells to inhabit adult serous cavities

机译:寿命长的自我更新的骨髓来源的巨噬细胞置换胚胎来源的细胞以栖息于成人浆液腔中

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摘要

Peritoneal macrophages are one of the most studied macrophage populations in the body, yet the composition, developmental origin and mechanisms governing the maintenance of this compartment are controversial. Here we show resident F4/80hiGATA6+ macrophages are long-lived, undergo non-stochastic self-renewal and retain cells of embryonic origin for at least 4 months in mice. However, Ly6C+ monocytes constitutively enter the peritoneal cavity in a CCR2-dependent manner, where they mature into short-lived F4/80loMHCII+ cells that act, in part, as precursors of F4/80hiGATA6+ macrophages. Notably, monocyte-derived F4/80hi macrophages eventually displace the embryonic population with age in a process that is highly gender dependent and not due to proliferative exhaustion of the incumbent embryonic population, despite the greater proliferative activity of newly recruited cells. Furthermore, although monocyte-derived cells acquire key characteristics of the embryonic population, expression of Tim4 was impaired, leading to cumulative changes in the population with age.
机译:腹膜巨噬细胞是机体中研究最多的巨噬细胞群体之一,但其组成,发育起源和控制该区室维持的机制仍存在争议。在这里,我们显示了居民F4 / 80 hi GATA6 + 巨噬细胞寿命长,经历了非随机自我更新并在小鼠中保留了至少4个月的胚胎来源细胞。然而,Ly6C + 单核细胞以依赖CCR2的方式组成性进入腹膜腔,在那里它们成熟为短命的F4 / 80 lo MHCII + 细胞,部分充当F4 / 80 hi GATA6 + 巨噬细胞的前体。值得注意的是,单核细胞衍生的F4 / 80 hi 巨噬细胞最终会随着年龄的增长而置换胚胎种群,这一过程高度依赖性别,而不是由于现存胚胎种群的增殖衰竭所致,尽管新招募的细胞。此外,尽管单核细胞衍生的细胞获得了胚胎种群的关键特征,但Tim4的表达受损,导致种群随年龄的累积变化。

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