Acute kidney injury promotes development of papillary renal cell adenoma and carcinoma from renal progenitor cells

Peired, Anna Julie; Antonelli, Giulia; Angelotti, Maria Lucia; Allinovi, Marco; Guzzi, Francesco; Sisti, Alessandro; Semeraro, Roberto; Conte, Carolina; Mazzinghi, Benedetta; Nardi, S; Melica, Maria Elena; Chiara, Letizia De; Lazzeri, Elena; Lasagni, Laura; Lottini, Tiziano; Landini, Samuela; Giglio, Sabrina; Mari, Andrea; Maida, Fabrizio Di; Antonelli, Alessandro; Porpiglia, Francesco; Schiavina, Riccardo; Ficarra, Vincenzo; Facchiano, Davide; Gacci, Mauro; Serni, Sergio; Carini, Marco; Netto, George J.; Roperto, Rosa Maria; Magi, Alberto; Christiansen, Christian Fynbo; Rotondi, Mario; Liapis, Helen; Anders, Hans Joachim; Raspollini, Maria Rosaria; Romagnani, Paola

doi:10.1126/scitranslmed.aaw6003

Cited by 52 publications

(70 citation statements)

References 78 publications

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“…These molecules www.nature.com/scientificreports/ were overexpressed in FL clones along with ITGA5, GGT1, CDH6 and CA9 all previously shown to be highly expressed by clear cell RCC 24,[42][43][44][45] . Thus, intriguingly proximal clonal proliferation and behavior may be viewed as precursor cell lesion for RCC 46 . Oxidative phosphorylation, respiratory chain, mitochondrial matrix and envelope genes were also significantly elevated in FL clones.…”

Section: Discussionmentioning

confidence: 99%

Human kidney clonal proliferation disclose lineage-restricted precursor characteristics

Cohen-Zontag

Gershon

Harari‐Steinberg

et al. 2020

Sci Rep

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In-vivo single cell clonal analysis in the adult mouse kidney has previously shown lineage-restricted clonal proliferation within varying nephron segments as a mechanism responsible for cell replacement and local regeneration. To analyze ex-vivo clonal growth, we now preformed limiting dilution to generate genuine clonal cultures from one single human renal epithelial cell, which can give rise to up to 3.4 * 106 cells, and analyzed their characteristics using transcriptomics. A comparison between clonal cultures revealed restriction to either proximal or distal kidney sub-lineages with distinct cellular and molecular characteristics; rapidly amplifying de-differentiated clones and a stably proliferating cuboidal epithelial-appearing clones, respectively. Furthermore, each showed distinct molecular features including cell-cycle, epithelial-mesenchymal transition, oxidative phosphorylation, BMP signaling pathway and cell surface markers. In addition, analysis of clonal versus bulk cultures show early clones to be more quiescent, with elevated expression of renal developmental genes and overall reduction in renal identity markers, but with an overlapping expression of nephron segment identifiers and multiple identity. Thus, ex-vivo clonal growth mimics the in-vivo situation displaying lineage-restricted precursor characteristics of mature renal cells. These data suggest that for reconstruction of varying renal lineages with human adult kidney based organoid technology and kidney regeneration ex-vivo, use of multiple heterogeneous precursors is warranted.

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Section: Discussionmentioning

confidence: 99%

Human kidney clonal proliferation disclose lineage-restricted precursor characteristics

Cohen-Zontag

Gershon

Harari‐Steinberg

et al. 2020

Sci Rep

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“…These cells have a distinct morphology and expression profile and undergo expansion after acute kidney injury 19 . Furthermore, they have reported potential for tubular and podocyte regeneration [20][21][22][23] and have been implicated in the development of renal cell carcinoma 24 . However, the sparsity of these cells has hampered further characterization.…”

Section: Introductionmentioning

confidence: 99%

Single cell transcriptional and chromatin accessibility profiling redefine cellular heterogeneity in the adult human kidney

Wilson

Waikar

et al. 2020

Preprint

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The integration of single cell transcriptome and chromatin accessibility datasets enables a deeper understanding of cell heterogeneity. We performed single nucleus ATAC (snATAC-seq) and RNA (snRNA-seq) sequencing to generate paired, cell-type-specific chromatin accessibility and transcriptional profiles of the adult human kidney. We demonstrate that snATAC-seq is comparable to snRNA-seq in the assignment of cell identity and can further refine our understanding of functional heterogeneity in the nephron. The majority of differentially accessible chromatin regions are localized to promoters and a significant proportion are closely-associated with differentially expressed genes. Cell-type-specific enrichment of transcription factor binding motifs implicates the activation of NFκB that promotes VCAM1 expression and drives transition between a subpopulation of proximal tubule epithelial cells. These datasets can be visualized at this resource: http://humphreyslab.com/SingleCell/. Our multi-omics approach improves the ability to detect unique cell states within the kidney and redefines cellular heterogeneity in the proximal tubule and thick ascending limb.

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“…CD133+CD24+ cells are localized at the urinary pole of the Bowman capsule, as well as scattered along the tubular compartment of the nephron among differentiated tubular cells [ 6 ]. Some renal progenitors, including those localized in the Bowman capsule and a subset of the ones scattered along the tubule, also express CD106 (also called vascular cell adhesion molecule 1, VCAM1), while the majority of progenitors localized along the tubule do not [ 6 , 8 ]. These phenotypical differences reflect a diverse functional capacity; indeed, CD133+CD24+CD106- cells scattered along the tubules display functional features of tubular progenitors, while CD133+CD24+CD106+ parietal epithelial cells (PECs) are multipotent [ 6 ].…”

Section: Renal Progenitorsmentioning

confidence: 99%

Molecular Mechanisms of Renal Progenitor Regulation: How Many Pieces in the Puzzle?

Peired

Melica

Molli

et al. 2021

Cells

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Kidneys of mice, rats and humans possess progenitors that maintain daily homeostasis and take part in endogenous regenerative processes following injury, owing to their capacity to proliferate and differentiate. In the glomerular and tubular compartments of the nephron, consistent studies demonstrated that well-characterized, distinct populations of progenitor cells, localized in the parietal epithelium of Bowman capsule and scattered in the proximal and distal tubules, could generate segment-specific cells in physiological conditions and following tissue injury. However, defective or abnormal regenerative responses of these progenitors can contribute to pathologic conditions. The molecular characteristics of renal progenitors have been extensively studied, revealing that numerous classical and evolutionarily conserved pathways, such as Notch or Wnt/β-catenin, play a major role in cell regulation. Others, such as retinoic acid, renin-angiotensin-aldosterone system, TLR2 (Toll-like receptor 2) and leptin, are also important in this process. In this review, we summarize the plethora of molecular mechanisms directing renal progenitor responses during homeostasis and following kidney injury. Finally, we will explore how single-cell RNA sequencing could bring the characterization of renal progenitors to the next level, while knowing their molecular signature is gaining relevance in the clinic.

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Acute kidney injury promotes development of papillary renal cell adenoma and carcinoma from renal progenitor cells

Cited by 52 publications

References 78 publications

Human kidney clonal proliferation disclose lineage-restricted precursor characteristics

Human kidney clonal proliferation disclose lineage-restricted precursor characteristics

Single cell transcriptional and chromatin accessibility profiling redefine cellular heterogeneity in the adult human kidney

Molecular Mechanisms of Renal Progenitor Regulation: How Many Pieces in the Puzzle?

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