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狼疮肾炎患者肾脏中丰富且与 T 细胞相邻的新型炎症树突状细胞。

A Novel Inflammatory Dendritic Cell That Is Abundant and Contiguous to T Cells in the Kidneys of Patients With Lupus Nephritis.

机构信息

Division of Nephrology, The Ohio State University Wexner Medical Center, Columbus, OH, United States.

Nephrology Unit, Hospital Fernandez, Buenos Aires, Argentina.

出版信息

Front Immunol. 2021 Feb 17;12:621039. doi: 10.3389/fimmu.2021.621039. eCollection 2021.

Abstract

The mechanisms that promote local inflammatory injury during lupus nephritis (LN) flare are largely unknown. Understanding the key immune cells that drive intrarenal inflammation will advance our knowledge of disease pathogenesis and inform the development of new therapeutics for LN management. In this study, we analyzed kidney biopsies from patients with proliferative LN and identified a novel inflammatory dendritic cell (infDC) population that is highly expressed in the LN kidney, but minimally present in healthy human kidneys. During an agnostic evaluation of immune transcript expression in the kidneys of patients with proliferative LN, the most abundantly overexpressed transcript from isolated glomeruli was , which encodes the Fc receptor gamma chain (FcRγ). To identify the cell types expressing FcRγ that infiltrate the kidney in LN, studies were done on kidney biopsies from patients with active LN using confocal immunofluorescence (IF) microscopy. This showed that FcRγ is abundantly present in the periglomerular (PG) region of the kidney and to a lesser extent in the tubulointerstitium (TI). Further investigation of the surface markers of these cells showed that they were FcRγ, MHC II, CD11c, CD163, CD5, DC-SIGN, CD64, CD14, CD16, SIRPα, CD206, CD68, CD123, CD3, and CD11b, suggesting the cells were infDCs. Quantification of the infDCs showed an average 10-fold higher level of infDCs in the LN kidney compared to the healthy kidneys. Importantly, IF identified CD3 T cells to be adjacent to these infDCs in the PG space of the LN kidney, whereas both cell types are minimally present in the healthy kidney. Thus, we have identified a previously undescribed DC in lupus kidneys that may interact with intrarenal T cells and play a role in the pathogenesis of kidney injury during LN flare.

摘要

在狼疮肾炎 (LN) 发作期间,促进局部炎症损伤的机制在很大程度上尚不清楚。了解驱动肾内炎症的关键免疫细胞将增进我们对疾病发病机制的认识,并为 LN 管理的新疗法的开发提供信息。在这项研究中,我们分析了患有增生性 LN 的患者的肾脏活检,并鉴定了一种新型炎症树突状细胞 (infDC) 群体,该群体在 LN 肾脏中高度表达,但在健康人肾脏中很少表达。在对增生性 LN 患者肾脏免疫转录物表达进行的盲目评估中,从分离的肾小球中过度表达的最多的转录物是 ,其编码 Fc 受体γ链 (FcRγ)。为了鉴定在 LN 中浸润肾脏的表达 FcRγ 的细胞类型,使用共聚焦免疫荧光 (IF) 显微镜对患有活动性 LN 的患者的肾脏活检进行了研究。这表明 FcRγ 在肾脏的肾小球旁 (PG) 区域大量存在,在肾小管间质 (TI) 中则较少。对这些细胞表面标志物的进一步研究表明,它们是 FcRγ、MHC II、CD11c、CD163、CD5、DC-SIGN、CD64、CD14、CD16、SIRPα、CD206、CD68、CD123、CD3 和 CD11b,提示这些细胞是 infDC。对 infDC 的定量分析显示,LN 肾脏中的 infDC 水平比健康肾脏高 10 倍。重要的是,IF 鉴定出 CD3 T 细胞与 LN 肾脏 PG 空间中的这些 infDC 相邻,而这两种细胞在健康肾脏中很少存在。因此,我们在狼疮肾脏中鉴定出了一种以前未描述的 DC,它可能与肾内 T 细胞相互作用,并在 LN 发作期间肾脏损伤的发病机制中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a692/7919935/09e2ad5f113e/fimmu-12-621039-g0001.jpg

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