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人巨噬细胞中类二十烷酸和其他氧化脂质的形成。

Formation of eicosanoids and other oxylipins in human macrophages.

作者信息

Radmark Olof

机构信息

Department of Medical Biochemistry and Biophysics, Division of Physiological Chemistry II, Karolinska Institutet, Stockholm, Sweden.

出版信息

Biochem Pharmacol. 2022 Oct;204:115210. doi: 10.1016/j.bcp.2022.115210. Epub 2022 Aug 13.

Abstract

In this review it is attempted to summarize current studies about formation of eicosanoids and other oxylipins in different human macrophages. There are several reports on M1 and M2 cells, also other phenotypes have been described. The eicosanoids formed in the largest amounts are the COX products TxB and PGE. Thus shortlived bioactive TxA is a dominating product both in M1- and in M2-lineages, one exception seems to be M cells. 5-LOX products are produced in both M1 and M2 macrophages, as well as in not fully polarized cells of both lineages. M as well as M2 macrophages produced LTC more readily compared to M1 lineage cells. In M cells LTB is a major eicosanoid, in line with high expression of LTA hydrolase. Recent reports described increased formation of leukotrienes in macrophages subjected to trained immunity with inflammatory transcriptional reprogramming. Also in macrophages derived from monocytes collected from post-COVID-19 patients. 15-LOX-1 is strongly upregulated in CD206 M2 cells (M2a), differentiated in presence of IL-4. These macrophages also express 15-LOX-2. In incubations with pathogenic E. coli as well as other stimuli 15(S)-HETE and 17(S)-HDHA were major oxylipins formed. Also, the SPM precursor 5,15-diHETE and the SPM RvD5 were produced in considerable amounts, while other SPMs were less abundant. In M2 macrophages incubated with E. coli or S. aureus the cytosolic 15-LOX-1 enzyme accumulated to punctuate structures in a Ca dependent manner with a relatively slow time course, leading to formation of mediators from endogenous substrate. Chalcones, flavone-like anti-inflammatory natural products, induced translocation of 15-LOX-1 in M2 cells, with high formation of 15-LOX derived oxylipins.

摘要

在本综述中,我们试图总结目前关于不同人类巨噬细胞中类二十烷酸和其他氧化脂质形成的研究。关于M1和M2细胞有几份报告,也描述了其他表型。形成量最大的类二十烷酸是COX产物TxB和PGE。因此,寿命短暂的生物活性TxA是M1和M2谱系中的主要产物,一个例外似乎是M细胞。5-LOX产物在M1和M2巨噬细胞以及两个谱系未完全极化的细胞中均有产生。与M1谱系细胞相比,M和M2巨噬细胞更易产生LTC。在M细胞中,LTB是主要的类二十烷酸,这与LTA水解酶的高表达一致。最近的报告描述了经过训练免疫和炎症转录重编程的巨噬细胞中白三烯形成增加。在从COVID-19康复患者收集的单核细胞衍生的巨噬细胞中也是如此。15-LOX-1在存在IL-4的情况下分化的CD206 M2细胞(M2a)中强烈上调。这些巨噬细胞也表达15-LOX-2。在用致病性大肠杆菌以及其他刺激物孵育时,15(S)-HETE和17(S)-HDHA是形成的主要氧化脂质。此外,SPM前体5,15-二HETE和SPM RvD5大量产生,而其他SPM则较少。在用大肠杆菌或金黄色葡萄球菌孵育的M2巨噬细胞中,胞质15-LOX-1酶以钙依赖的方式积累成点状结构,时间进程相对较慢,导致从内源性底物形成介质。查耳酮,一种黄酮类抗炎天然产物,诱导M2细胞中15-LOX-1的易位,形成大量15-LOX衍生的氧化脂质。

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