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皮肤的紫外线照射增强了骨髓来源的树突状细胞的糖酵解通量,并降低了其迁移能力。

UV Irradiation of Skin Enhances Glycolytic Flux and Reduces Migration Capabilities in Bone Marrow-Differentiated Dendritic Cells.

机构信息

Telethon Kids Institute, University of Western Australia, West Perth, Western Australia, Australia.

School of Biomedical Sciences, Curtin Health Innovation Research Institute Biosciences, Curtin University, Perth, Western Australia, Australia.

出版信息

Am J Pathol. 2017 Sep;187(9):2046-2059. doi: 10.1016/j.ajpath.2017.06.003. Epub 2017 Jul 11.

DOI:10.1016/j.ajpath.2017.06.003
PMID:28708972
Abstract

A systemic immunosuppression follows UV irradiation of the skin of humans and mice. In this study, dendritic cells (DCs) differentiating from the bone marrow (BM) of UV-irradiated mice had a reduced ability to migrate toward the chemokine (C-C motif) ligand 21. Fewer DCs also accumulated in the peritoneal cavity of UV-chimeric mice (ie, mice transplanted with BM from UV-irradiated mice) after injection of an inflammatory stimulus into that site. We hypothesized that different metabolic states underpin altered DC motility. Compared with DCs from the BM of nonirradiated mice, those from UV-irradiated mice produced more lactate, consumed more glucose, and had greater glycolytic flux in a bioenergetics stress test. Greater expression of 3-hydroxyanthranilate 3,4-dioxygenase was identified as a potential contributor to increased glycolysis. Inhibition of 3-hydroxyanthranilate 3,4-dioxygenase by 6-chloro-dl-tryptophan prevented both increased lactate production and reduced migration toward chemokine (C-C motif) ligand 21 by DCs differentiated from BM of UV-irradiated mice. UV-induced prostaglandin E has been implicated as an intermediary in the effects of UV radiation on BM cells. DCs differentiating from BM cells pulsed in vitro for 2 hours with dimethyl prostaglandin E were functionally similar to those from the BM of UV-irradiated mice. Reduced migration of DCs to lymph nodes associated with increased glycolytic flux may contribute to their reduced ability to initiate new immune responses in UV-irradiated mice.

摘要

人类和小鼠皮肤经紫外线(UV)照射后会出现全身性免疫抑制。在这项研究中,从经 UV 照射的小鼠骨髓中分化而来的树突状细胞(DC)向趋化因子(C-C 基序)配体 21 迁移的能力降低。在将炎症刺激物注射到该部位后,在 UV 嵌合小鼠(即接受来自经 UV 照射的小鼠的骨髓移植的小鼠)的腹腔中,也积累了较少的 DC。我们假设不同的代谢状态是导致 DC 迁移能力改变的基础。与来自未照射小鼠骨髓的 DC 相比,来自经 UV 照射的小鼠骨髓的 DC 在生物能量应激测试中产生更多的乳酸、消耗更多的葡萄糖,并且具有更高的糖酵解通量。发现 3-羟基犬尿氨酸 3,4-加双氧酶的更高表达是导致糖酵解增加的潜在原因。6-氯-dl-色氨酸抑制 3-羟基犬尿氨酸 3,4-加双氧酶可防止由经 UV 照射的小鼠骨髓分化而来的 DC 增加乳酸产生和减少向趋化因子(C-C 基序)配体 21 的迁移。已经提出,紫外线诱导的前列腺素 E 是紫外线辐射对骨髓细胞影响的中间产物。在体外用二甲基前列腺素 E 脉冲孵育 2 小时的骨髓细胞分化而来的 DC 与来自经 UV 照射的小鼠骨髓的 DC 具有相似的功能。与增加的糖酵解通量相关的向淋巴结的 DC 迁移减少可能导致它们在经 UV 照射的小鼠中启动新的免疫反应的能力降低。

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2
More Than Effects in Skin: Ultraviolet Radiation-Induced Changes in Immune Cells in Human Blood.不止于皮肤:紫外线辐射诱导人血中免疫细胞的变化。
Front Immunol. 2021 Jun 10;12:694086. doi: 10.3389/fimmu.2021.694086. eCollection 2021.
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