Single-cell profiling reveals kidney CD163+dendritic cell participation in human lupus nephritis

Author:

Chen Wei,Jin Bei,Cheng Cheng,Peng Huajing,Zhang Xinxin,Tan Weiping,Tang Ruihan,Lian Xingji,Diao Hui,Luo Ning,Li Xiaoyan,Fan Jinjin,Shi Jian,Yin Changjun,Wang Ji,Peng Sui,Yu Li,Li Jun,Wu Rui-Qi,Kuang Dong-Ming,Shi Guo-Ping,Zhou Yi,Wang Fang,Jiang XiaoyunORCID

Abstract

ObjectivesThe current work aimed to provide a comprehensive single-cell landscape of lupus nephritis (LN) kidneys, including immune and non-immune cells, identify disease-associated cell populations and unravel their participation within the kidney microenvironment.MethodsSingle-cell RNA and T cell receptor sequencing were performed on renal biopsy tissues from 40 patients with LN and 6 healthy donors as controls. Matched peripheral blood samples from seven LN patients were also sequenced. Multiplex immunohistochemical analysis was performed on an independent cohort of 60 patients and validated using flow cytometric characterisation of human kidney tissues and in vitro assays.ResultsWe uncovered a notable enrichment of CD163+dendritic cells (DC3s) in LN kidneys, which exhibited a positive correlation with the severity of LN. In contrast to their counterparts in blood, DC3s in LN kidney displayed activated and highly proinflammatory phenotype. DC3s showed strong interactions with CD4+T cells, contributing to intrarenal T cell clonal expansion, activation of CD4+effector T cell and polarisation towards Th1/Th17. Injured proximal tubular epithelial cells (iPTECs) may orchestrate DC3 activation, adhesion and recruitment within the LN kidneys. In cultures, blood DC3s treated with iPTECs acquired distinct capabilities to polarise Th1/Th17 cells. Remarkably, the enumeration of kidney DC3s might be a potential biomarker for induction treatment response in LN patients.ConclusionThe intricate interplay involving DC3s, T cells and tubular epithelial cells within kidneys may substantially contribute to LN pathogenesis. The enumeration of renal DC3 holds potential as a valuable stratification feature for guiding LN patient treatment decisions in clinical practice.

Funder

National Institute of Neurological Disorders and Stroke

Key Laboratory of National Health Commission, and Key Laboratory of Nephrology,

National Natural Science Foundation of China

Sun Yat-Sen University Clinical Research 5010 Program

Clinical Research 2030 Project of the First Affiliated Hospital, Sun Yat-Sen University

National Key Research and Development Program of China

National Heart, Lung, and Blood Institute

Publisher

BMJ

Subject

General Biochemistry, Genetics and Molecular Biology,Immunology,Immunology and Allergy,Rheumatology

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