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坏死骨液体外抑制猪外周血单核细胞来源巨噬细胞的能量代谢。

Necrotic Bone Fluid Suppresses Energy Metabolism of Porcine PBMC-Derived Macrophages In Vitro.

作者信息

Deng Zhuo, Nguyen Chau P, Liu Yan, Kim Jaehyup, Mathews Thomas P, Ma Chi, Ren Yinshi, Xing Chao, Kim Harry K W

机构信息

Center of Excellence in Hip, Scottish Rite for Children, Dallas, TX 75219, USA.

Eugene McDermott Center for Human Growth and Development, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA.

出版信息

Cells. 2025 Aug 14;14(16):1258. doi: 10.3390/cells14161258.

Abstract

Legg-Calvé-Perthes disease is a juvenile ischemic osteonecrosis (ON) of the femoral head. A disruption of blood supply to the femoral head produces extensive cell death and necrotic debris. Macrophages are innate immune cells recruited to the necrotic bone to orchestrate the repair process. However, the role macrophages play in the ON repair process is still not elucidated. The purpose of this study was to determine the effect of artificial necrotic bone fluid (NBF) on porcine peripheral blood mononuclear cell (PBMC)-derived macrophages. Monocytes were positively selected by CD14 MicroBeads from pig PBMCs. After maturation, cells were treated with no stimulant (Con), LPS + IFNγ (M1), IL4 + IL13 (M2), or NBF. All culture supernatants and cells were harvested for ELISA, Western blot, FACS, RT-qPCR and bulk RNAseq. The Western blot and ELISA showed that only the M1 condition elevated the protein level of pro-inflammatory cytokines. The FACS results indicated that percentage of CD8086+ (M1 marker) cells was significantly lower in the M2 vs. other conditions, whereas the relative median fluorescence intensity of CD8086 was significantly higher in the M1 vs. other conditions. The NBF did not show any significant change compared to the Con. mRNA analysis showed significantly increased IL1β and IL8 expression in the M1 vs. Con scenario. TNFα expression was significantly decreased in the M2 vs. Con scenario. Interestingly, the NBF did not induce pro-inflammatory gene expression. For bulk RNAseq, the Gene Set Enrichment Analyses of the M1-stimulated cells revealed the enrichment of pro-inflammatory gene sets. For the M2, most of the enriched categories were related to the down-regulation of inflammation. For the NBF, the most enriched categories were related to the down-regulation of protein translation and mitochondrial metabolism. We further confirmed the suppressive effects of NBF on macrophage functions using Seahorse Cell Mito Stress Tests, C-glucose metabolic flux analysis, mitochondrial ROS detection via MitoSOX staining, and phagocytosis assay. Taken together, these results revealed that the artificial NBF down-regulates the overall cellular activity and energy metabolism of macrophages.

摘要

Legg-Calvé-Perthes病是一种股骨头的青少年缺血性骨坏死(ON)。股骨头血液供应中断会导致大量细胞死亡和坏死碎片。巨噬细胞是被招募到坏死骨中以协调修复过程的固有免疫细胞。然而,巨噬细胞在ON修复过程中所起的作用仍未阐明。本研究的目的是确定人工坏死骨液(NBF)对猪外周血单核细胞(PBMC)来源的巨噬细胞的影响。通过CD14微珠从猪PBMC中阳性选择单核细胞。成熟后,细胞分别用无刺激物(对照)、LPS + IFNγ(M1)、IL4 + IL13(M2)或NBF处理。收集所有培养上清液和细胞用于ELISA、蛋白质印迹、流式细胞术、RT-qPCR和批量RNA测序。蛋白质印迹和ELISA表明,只有M1条件下促炎细胞因子的蛋白质水平升高。流式细胞术结果表明,与其他条件相比,M2中CD8086+(M1标志物)细胞的百分比显著降低,而与其他条件相比,M1中CD8086的相对中位荧光强度显著更高。与对照相比,NBF未显示任何显著变化。mRNA分析表明,与对照情况相比,M1中IL1β和IL8表达显著增加。与对照情况相比,M2中TNFα表达显著降低。有趣的是,NBF未诱导促炎基因表达。对于批量RNA测序,M1刺激细胞的基因集富集分析显示促炎基因集富集。对于M2,大多数富集类别与炎症下调有关。对于NBF,最富集的类别与蛋白质翻译和线粒体代谢下调有关。我们使用海马细胞线粒体应激试验、C-葡萄糖代谢通量分析、通过MitoSOX染色检测线粒体ROS以及吞噬试验进一步证实了NBF对巨噬细胞功能的抑制作用。综上所述,这些结果表明人工NBF下调了巨噬细胞的整体细胞活性和能量代谢。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8473/12384577/cd9a32c977fd/cells-14-01258-g001.jpg

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