Spatiotemporal immune zonation of the human kidney

Stewart, Benjamin; Ferdinand, John R.; Young, Matthew D.; Mitchell, Thomas J.; Loudon, Kevin; Riding, Alexandra; Richoz, Nathan; Frazer, Gordon L.; Staniforth, Joy; Braga, Felipe A. Vieira; Botting, Rachel A.; Popescu, Dorin-Mirel; Vento‐Tormo, Roser; Stephenson, Emily; Cagan, Alex; Farndon, Sarah J.; Polański, Krzysztof; Efremova, Mirjana; Green, Kile; Velasco-Herrera, Martín Del Castillo; Guzzo, Charlotte; Collord, Grace; Mamanova, Lira; Aho, Tevita; Armitage, James; Riddick, Antony C. P.; Mushtaq, Imran; Farrell, Stephen; Rampling, Dyanne; Nicholson, James C.; Filby, Andrew; Burge, Johanna; Lisgo, Steven; Lindsay, Susan; Bajénoff, Marc; Warren, Anne Y.; Stewart, Grant D.; Sebire, Neil J.; Coleman, Nicholas; Haniffa, Muzlifah; Teichmann, Sarah A.; Behjati, Sam; Clatworthy, Menna R.

doi:10.1126/science.aat5031

Cited by 299 publications

(322 citation statements)

References 68 publications

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“…Major cell types and subclusters were identified based on cell type-specific markers ( Fig. S2C, D, Dataset S1) (8)(9)(10). Each nephron segment performs unique reabsorptive and secretory functions to transform filtrate into urine, and this is reflected by segment-specific expression of all detected solute linked carriers, ATPases and channels ( Fig.…”

Section: Resultsmentioning

confidence: 99%

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Cell profiling of mouse acute kidney injury reveals conserved cellular responses to injury

Kirita

Uchimura

et al. 2020

Preprint

174

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After acute kidney injury (AKI), patients either recover or alternatively develop fibrosis and chronic kidney disease. Interactions between injured epithelia, stroma and inflammatory cells determine whether kidneys repair or undergo fibrosis, but the molecular events that drive these processes are poorly understood. Here, we use single nucleus RNA sequencing of a mouse model of AKI to characterize cell states during repair from acute injury. We identify a distinct proinflammatory and profibrotic proximal tubule cell state that fails to repair. Deconvolution of bulk RNA-seq datasets indicates that this "failed-repair proximal tubule cell" or FR-PTC, state can be detected in other models of kidney injury, increasing in the aging rat kidney and over time in human kidney allografts. We also describe dynamic intercellular communication networks and discern transcriptional pathways driving successful vs. failed repair. Our study provides a detailed description of cellular responses after injury and suggests that the FR-PTC state may represent a therapeutic target to improve repair. Significance StatementSingle nucleus RNA sequencing revealed gene expression changes during repair after acute kidney injury. We describe a small population of proximal tubule cells that fail to repair (FR-PTC). Since this subpopulation expresses abundant pro-inflammatory and profibrotic genes, it may represent a new therapeutic target to improve repair and reduce fibrosis after AKI.

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Section: Resultsmentioning

confidence: 99%

“…Recent scRNA-seq analyses have revealed unexpected stromal heterogeneity in both developing and adult kidney (8,9,23). With Harmony integration, we combined the stromal clusters from all timepoints to identify eight stromal cell subclusters (Fig.…”

Section: Stromal Cell Responses To Injurymentioning

confidence: 99%

Cell profiling of mouse acute kidney injury reveals conserved cellular responses to injury

Kirita

Uchimura

et al. 2020

Preprint

174

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“…Datasets were retrieved from published and unpublished datasets in multiple human tissues, including airways 26,27 , cornea (personal communication; Lako laboratory, Newcastle, UK), skeletal muscle (personal communication, Teichmann laboratory, Wellcome Sanger Institute and Zhang laboratory, Sun-Yat-Sen University, Guangzhou, China), ileum 28 , colon 29 , pancreas 30 , liver 31 , gallbladder (personal communication; Vallier laboratory, University of Cambridge, UK), heart (Teichmann laboratory, Hubner laboratory/Berlin, Seidmanns/Harvard and Noseda laboratory/Imperial College London, UK), kidney 32 , placenta/decidua 33 , testis 34 , prostate gland 35 , brain 36 , skin 37 , retina 38 , spleen 39 , esophagus 39 and fetal tissues 40,41 . Raw expression values were normalized and log transformed.…”

Section: Methodsmentioning

confidence: 99%

SARS-CoV-2 entry factors are highly expressed in nasal epithelial cells together with innate immune genes

Sungnak

Huang

Bécavin

et al. 2020

Nat Med

2,327

133

2,291

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“…We also compared the immune compartment of heart, skeletal muscle and adult kidney 79 by analyzing 40 206 cells and nuclei. Across the three tissues there was extensive overlap of lymphoid immune populations (B cells, CD4+ and CD8+ T cells, and NK/NKT cells).…”

Section: Cross-tissue Comparison Between Heart and Skeletal Musclementioning

confidence: 99%

Cells and gene expression programs in the adult human heart

Litviňuková

Talavera-López

Maatz

et al. 2020

Preprint

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SummaryCardiovascular disease is the leading cause of death worldwide. Advanced insights into disease mechanisms and strategies to improve therapeutic opportunities require deeper understanding of the molecular processes of the normal heart. Knowledge of the full repertoire of cardiac cells and their gene expression profiles is a fundamental first step in this endeavor. Here, using large-scale single cell and nuclei transcriptomic profiling together with state-of-the-art analytical techniques, we characterise the adult human heart cellular landscape covering six anatomical cardiac regions (left and right atria and ventricles, apex and interventricular septum). Our results highlight the cellular heterogeneity of cardiomyocytes, pericytes and fibroblasts, revealing distinct subsets in the atria and ventricles indicative of diverse developmental origins and specialized properties. Further we define the complexity of the cardiac vascular network which includes clusters of arterial, capillary, venous, lymphatic endothelial cells and an atrial-enriched population. By comparing cardiac cells to skeletal muscle and kidney, we identify cardiac tissue resident macrophage subsets with transcriptional signatures indicative of both inflammatory and reparative phenotypes. Further, inference of cell-cell interactions highlight a macrophage-fibroblast-cardiomyocyte network that differs between atria and ventricles, and compared to skeletal muscle. We expect this reference human cardiac cell atlas to advance mechanistic studies of heart homeostasis and disease.

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Spatiotemporal immune zonation of the human kidney

Cited by 299 publications

References 68 publications

Cell profiling of mouse acute kidney injury reveals conserved cellular responses to injury

Cell profiling of mouse acute kidney injury reveals conserved cellular responses to injury

SARS-CoV-2 entry factors are highly expressed in nasal epithelial cells together with innate immune genes

Cells and gene expression programs in the adult human heart

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