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Accession IconSRP136021

Parabiosis and single-cell RNA-Sequencing reveal a limited contribution of monocytes to myofibroblasts in kidney fibrosis

Organism Icon Mus musculus
Sample Icon 384 Downloadable Samples
Technology Badge IconIllumina HiSeq 2500

Submitter Supplied Information

Description
Fibrosis is the common final pathway of virtually all chronic injury to the kidney. While it is well accepted that myofibroblasts are the scar-producing cells in the kidney, their cellular origin is still hotly debated. The relative contribution of proximal tubular epithelium and circulating cells including mesenchymal stem cells, macrophages and fibrocytes to the myofibroblast pool remains highly controversial. Using inducible genetic fate tracing of proximal tubular epithelium we confirm that proximal tubule does not contribute to the myofibroblast pool. However, in parabiosis models in which one parabiont is genetically labeled and the other is unlabeled and undergoes kidney fibrosis, we demonstrate that a small fraction of genetically labeled renal myofibroblasts derive from the circulation. Single cell RNA-Sequencing confirms this finding but indicates that these cells are circulating monocytes, express few extracellular matrix or other myofibroblast genes and do express many proinflammatory cytokines. We conclude that this small circulating myofibroblast progenitor population contributes to renal fibrosis by paracrine rather than direct mechanisms. Overall design: Single cell RNA-seq was performed on FACS-sorted PDGFRB+CD45- and PDGFRB+CD45+ cell populations
PubMed ID
Total Samples
384
Submitter’s Institution
No associated institution

Samples

Show of 384 Total Samples
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Additional Metadata
Cell31
8.000
mouse kidney
NA
Cell34
8.000
mouse kidney
NA
Cell6
8.000
mouse kidney
NA
Cell11
8.000
mouse kidney
NA
Cell13
8.000
mouse kidney
NA
Cell14
8.000
mouse kidney
NA
Cell15
8.000
mouse kidney
NA
Cell19
8.000
mouse kidney
NA
Cell21
8.000
mouse kidney
NA
Cell29
8.000
mouse kidney
NA
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