Infiltrative classical monocyte-derived and SPP1 lipid-associated macrophages mediate inflammation and fibrosis in ANCA-associated glomerulonephritis.

IF 4.8 2区医学 Q1 TRANSPLANTATION

Nephrology Dialysis Transplantation Pub Date : 2025-06-30 DOI:10.1093/ndt/gfae292

Yosta Vegting, Aldo Jongejan, Annette E Neele, Nike Claessen, Gal Sela, Koen H M Prange, Jesper Kers, Joris J T H Roelofs, Joost W van der Heijden, Onno J de Boer, Ester B M Remmerswaal, Liffert Vogt, Frederike J Bemelman, Menno P J de Winther, Perry D Moerland, Marc L Hilhorst

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Abstract

Background: Kidney macrophage infiltration is a histological hallmark of vasculitic lesions and is strongly linked to disease activity in anti-neutrophil cytoplasmic antibodies (ANCA)-associated glomerulonephritis (AGN). The precise mechanisms by which kidney macrophages influence local inflammation and long-term damage remain largely unknown.

Methods: Here, we investigate kidney macrophage diversity using single-cell transcriptome analysis of 25 485 freshly retrieved unfrozen, high-quality kidney CD45+ immune cells from five AGN patients during active disease, a lupus nephritis and a nephrectomy control. Detailed subclustering of myeloid cells was performed to identify disease-specific macrophage subtypes. Next, transcriptome differences between macrophage subsets and disease serotypes were assessed. Findings were validated by immunostainings of an extended cohort of kidney biopsies and flow cytometric analysis of peripheral blood monocytes.

Results: Four main macrophage subsets were identified, including a classical monocyte-derived macrophage (MDM) subset expressing a chemotactic (CXCL2, CXCL3, CXCL8, CCL3) and pro-inflammatory (IL1β, TNF) set of markers and an osteopontin/SPP1+ lipid-associated macrophage (SPP1 LAMs) subtype exhibiting distinctive upregulation of fibrotic genesets. AGN samples revealed a markedly increased proportion of CD163+ macrophages, predominantly composed of classical MDMs, accompanied by resident-like C1Q macrophages, and SPP1 LAMs. An analogous trend was observed in the expansion of peripheral blood classical monocytes during active disease. The proteinase 3 (PR3)-AGN subtype exhibited heightened classical MDM and SPP1 LAM infiltration and markers of acute inflammation, while interferon signaling and markers of chronicity were reduced compared with myeloperoxidase-AGN.

Conclusions: Our findings highlight the expression of inflammatory and fibrotic genes by kidney macrophage subsets in AGN. Classical monocyte dysregulation might contribute to inflammation in the pathogenesis of AGN. Targeting these specific monocyte/macrophage subsets may potentially control the inflammatory cascade and attenuate resulting fibrosis in AGN and kidney disease in general.

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浸润性经典单核细胞来源和SPP1脂质相关巨噬细胞介导anca相关性肾小球肾炎的炎症和纤维化。

背景和假设：肾巨噬细胞浸润是血管病变的组织学标志，与抗中性粒细胞胞浆抗体（ANCA）相关性肾小球肾炎（AGN）的疾病活动性密切相关。肾巨噬细胞影响局部炎症和长期损伤的确切机制在很大程度上仍不清楚。方法：通过单细胞转录组分析，研究了来自5例活动性疾病、狼疮性肾炎和肾切除术对照组的AGN患者新鲜提取的25485个未冷冻的高质量肾CD45+免疫细胞的肾巨噬细胞多样性。对骨髓细胞进行详细的亚聚类，以确定疾病特异性巨噬细胞亚型。接下来，评估巨噬细胞亚群和疾病血清型之间的转录组差异。研究结果通过肾脏活检的免疫染色和外周血单核细胞的流式细胞术分析得到了验证。结果：确定了四个主要的巨噬细胞亚群，包括一个经典的单核细胞源性巨噬细胞（MDM）亚群，表达趋化（CXCL2、CXCL3、CXCL8、CCL3）和促炎（il - 1β、TNF）标记物，以及一个骨桥蛋白/SPP1+脂质相关巨噬细胞（SPP1 LAMs）亚型，表现出明显的纤维化基因上调。AGN样本显示CD163+巨噬细胞的比例显著增加，主要由经典MDMs组成，伴有常驻样C1Q巨噬细胞和SPP1 lam。在活动性疾病期间，外周血经典单核细胞的扩张也观察到类似的趋势。与髓过氧化物酶(MPO)-AGN相比，PR3 -AGN亚型表现出经典MDM和SPP1 LAM浸润和急性炎症标志物增加，而干扰素信号和慢性标志物减少。结论：我们的研究结果强调了AGN中肾巨噬细胞亚群中炎症和纤维化基因的表达。经典单核细胞失调可能在AGN的发病机制中参与炎症。针对这些特定的单核/巨噬细胞亚群可能潜在地控制炎症级联并减轻AGN和肾脏疾病中导致的纤维化。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Nephrology Dialysis Transplantation 医学-泌尿学与肾脏学

CiteScore

10.10

自引率

4.90%

发文量

1431

审稿时长

1.7 months

期刊介绍： Nephrology Dialysis Transplantation (ndt) is the leading nephrology journal in Europe and renowned worldwide, devoted to original clinical and laboratory research in nephrology, dialysis and transplantation. ndt is an official journal of the [ERA-EDTA](http://www.era-edta.org/) (European Renal Association-European Dialysis and Transplant Association). Published monthly, the journal provides an essential resource for researchers and clinicians throughout the world. All research articles in this journal have undergone peer review. Print ISSN: 0931-0509.