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Unveiling skin macrophage dynamics explains both tattoo persistence and strenuous removal

机译:揭露的皮肤巨噬细胞动力学解释了纹身的持久性和剧烈去除

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摘要

Here we describe a new mouse model that exploits the pattern of expression of the high-affinity IgG receptor (CD64) and allows diphtheria toxin (DT)–mediated ablation of tissue-resident macrophages and monocyte-derived cells. We found that the myeloid cells of the ear skin dermis are dominated by DT-sensitive, melanin-laden cells that have been missed in previous studies and correspond to macrophages that have ingested melanosomes from neighboring melanocytes. Those cells have been referred to as melanophages in humans. We also identified melanophages in melanocytic melanoma. Benefiting of our knowledge on melanophage dynamics, we determined the identity, origin, and dynamics of the skin myeloid cells that capture and retain tattoo pigment particles. We showed that they are exclusively made of dermal macrophages. Using the possibility to delete them, we further demonstrated that tattoo pigment particles can undergo successive cycles of capture–release–recapture without any tattoo vanishing. Therefore, congruent with dermal macrophage dynamics, long-term tattoo persistence likely relies on macrophage renewal rather than on macrophage longevity.
机译:在这里,我们描述了一种新的小鼠模型,该模型利用了高亲和力IgG受体(CD64)的表达模式,并允许白喉毒素(DT)介导的组织驻留巨噬细胞和单核细胞衍生细胞的消融。我们发现,耳部皮肤真皮的髓样细胞被DT敏感的,富含黑色素的细胞所占优势,这些细胞在以前的研究中已被遗漏,并且对应于从邻近的黑色素细胞中摄取了黑色素体的巨噬细胞。这些细胞在人类中被称为黑色素细胞。我们还确定了黑色素细胞黑色素瘤中的黑色素细胞。受益于我们对黑色素细胞动力学的了解,我们确定了捕获并保留纹身颜料颗粒的皮肤髓样细胞的身份,起源和动力学。我们证明它们仅由真皮巨噬细胞制成。利用删除它们的可能性,我们进一步证明了纹身颜料颗粒可以经历连续的捕获-释放-重新捕获周期,而不会消失任何纹身。因此,与皮肤巨噬细胞动力学一致,纹身的长期持久性可能取决于巨噬细胞的更新而不是巨噬细胞的寿命。

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