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直接靶向巨噬细胞的地塞米松可诱导促进红系细胞扩增的巨噬细胞微环境。

Dexamethasone targeted directly to macrophages induces macrophage niches that promote erythroid expansion.

作者信息

Falchi Mario, Varricchio Lilian, Martelli Fabrizio, Masiello Francesca, Federici Giulia, Zingariello Maria, Girelli Gabriella, Whitsett Carolyn, Petricoin Emanuel F, Moestrup Søren Kragh, Zeuner Ann, Migliaccio Anna Rita

机构信息

National AIDS Center, New York, NY, USA Tisch Cancer Institute, Mount Sinai School of Medicine, New York, NY, USA.

Tisch Cancer Institute, Mount Sinai School of Medicine, New York, NY, USA.

出版信息

Haematologica. 2015 Feb;100(2):178-87. doi: 10.3324/haematol.2014.114405. Epub 2014 Dec 22.

Abstract

Cultures of human CD34(pos) cells stimulated with erythroid growth factors plus dexamethasone, a model for stress erythropoiesis, generate numerous erythroid cells plus a few macrophages (approx. 3%; 3:1 positive and negative for CD169). Interactions occurring between erythroblasts and macrophages in these cultures and the biological effects associated with these interactions were documented by live phase-contrast videomicroscopy. Macrophages expressed high motility interacting with hundreds/thousands of erythroblasts per hour. CD169(pos) macrophages established multiple rapid 'loose' interactions with proerythroblasts leading to formation of transient erythroblastic island-like structures. By contrast, CD169(neg) macrophages established 'tight' interactions with mature erythroblasts and phagocytosed these cells. 'Loose' interactions of CD169(pos) macrophages were associated with proerythroblast cytokinesis (the M phase of the cell cycle) suggesting that these interactions may promote proerythroblast duplication. This hypothesis was tested by experiments that showed that as few as 103 macrophages significantly increased levels of 3-(4,5-dimethylthiazolyl-2)-2,5-diphenyltetrazolium bromide incorporation frequency in S/G2/M and cytokinesis expressed by proerythroblasts over 24 h of culture. These effects were observed also when macrophages were co-cultured with dexamethasone directly conjugated to a macrophage-specific CD163 antibody. In conclusion, in addition to promoting proerythroblast proliferation directly, dexamethasone stimulates expansion of these cells indirectly by stimulating maturation and cytokinesis supporting activity of macrophages.

摘要

用人红细胞生成素生长因子加地塞米松刺激人CD34阳性细胞所形成的培养物是应激性红细胞生成的模型,该培养物可产生大量红细胞及少量巨噬细胞(约3%;CD169阳性与阴性比例为3:1)。通过实时相差视频显微镜记录了这些培养物中幼红细胞与巨噬细胞之间的相互作用以及与这些相互作用相关的生物学效应。巨噬细胞表现出高运动性,每小时与数百/数千个幼红细胞相互作用。CD169阳性巨噬细胞与早幼红细胞建立多个快速“松散”的相互作用,导致形成短暂的类红细胞岛样结构。相比之下,CD169阴性巨噬细胞与成熟红细胞建立“紧密”相互作用并吞噬这些细胞。CD169阳性巨噬细胞的“松散”相互作用与早幼红细胞胞质分裂(细胞周期的M期)相关,提示这些相互作用可能促进早幼红细胞复制。通过实验对这一假设进行了验证,实验表明,在培养24小时期间,低至103个巨噬细胞就能显著提高早幼红细胞在S/G2/M期及胞质分裂期的3-(4,5-二甲基噻唑-2)-2,5-二苯基四氮唑溴盐掺入频率。当巨噬细胞与直接偶联巨噬细胞特异性CD163抗体的地塞米松共培养时,也观察到了这些效应。总之,地塞米松除了直接促进早幼红细胞增殖外,还通过刺激巨噬细胞的成熟和胞质分裂支持活性间接刺激这些细胞的扩增。

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A niche for every cell, for every function.每个细胞、每种功能都有一个特定的生态位。
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