Human fetal kidney organoids model early human nephrogenesis and Notch-driven cell fate

Michael Namestnikov; Osnat Cohen-Zontag; Dorit Omer; Yehudit Gnatek; Sanja Goldberg; Thomas Vincent; Swati Singh; Yair Shiber; Tal Rafaeli Yehudai; Hadas Volkov; Dani Folkman Genet; Achia Urbach; Sylvie Polak-Charcon; Igor Grinberg; Naomi Pode-Shakked; Boaz Weisz; Zvi Vaknin; Benjamin S. Freedman; Benjamin Dekel

doi:10.1038/s44318-025-00504-2

Human fetal kidney organoids model early human nephrogenesis and Notch-driven cell fate

Michael Namestnikov
, Osnat Cohen-Zontag
, Dorit Omer
, Yehudit Gnatek
, Sanja Goldberg
, Thomas Vincent
, Swati Singh
, Yair Shiber
, Tal Rafaeli Yehudai
, Hadas Volkov
, Dani Folkman Genet
, Achia Urbach
, Sylvie Polak-Charcon
, Igor Grinberg
, Naomi Pode-Shakked
, Boaz Weisz
, Zvi Vaknin
, Benjamin S. Freedman
, Benjamin Dekel

Research output: Contribution to journal › Article › peer-review

4 Scopus citations

Abstract

Pluripotent stem cell (PSC)–derived kidney organoids are used to model human renal development and disease; however, accessible models of human fetal development to benchmark PSC-derived organoids remain underdeveloped. Here, we establish a chemically defined, serum-free protocol for prolonged culture of human fetal kidney-derived organoids (hFKOs) in vitro. hFKOs self-organize into polarized renal epithelium, reinitiate from NCAM1⁺ progenitors, and recapitulate nephrogenic and ureteric bud lineages. Bulk transcriptomics, single-cell RNA sequencing, pseudotime analysis, and immunostaining revealed diverse renal tissue cell populations, with a preserved epithelial progenitor pool and tubular differentiation axis. hFKOs were enriched for Notch signaling genes, enabling single-cell analysis of pharmacological Notch inhibition. This revealed a maturation block with increased nephron progenitors and a shift toward distal over early proximal tubule fates. We also identified a novel prominin-1-expressing cell state that evades Notch inhibition to generate both proximal and distal tubules. Overall, hFKOs provide a faithful model to gain insights into human kidney development, advancing the fields of stem cell biology and regenerative medicine.

Original language	English
Pages (from-to)	4681-4719
Number of pages	39
Journal	EMBO Journal
Volume	44
Issue number	17
DOIs	https://doi.org/10.1038/s44318-025-00504-2
State	Published - 1 Sep 2025
Externally published	Yes

Keywords

Human Fetal Kidney
Kidney Organoids
Nephrogenesis
Notch Pathway
Single-cell Transcriptomics

ASJC Scopus subject areas

General Neuroscience
Molecular Biology
General Biochemistry, Genetics and Molecular Biology
General Immunology and Microbiology

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10.1038/s44318-025-00504-2

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Namestnikov, M., Cohen-Zontag, O., Omer, D., Gnatek, Y., Goldberg, S., Vincent, T., Singh, S., Shiber, Y., Rafaeli Yehudai, T., Volkov, H., Folkman Genet, D., Urbach, A., Polak-Charcon, S., Grinberg, I., Pode-Shakked, N., Weisz, B., Vaknin, Z., Freedman, B. S., & Dekel, B. (2025). Human fetal kidney organoids model early human nephrogenesis and Notch-driven cell fate. EMBO Journal, 44(17), 4681-4719. https://doi.org/10.1038/s44318-025-00504-2

@article{7e39115bb4454240ba86705da1912a13,

title = "Human fetal kidney organoids model early human nephrogenesis and Notch-driven cell fate",

abstract = "Pluripotent stem cell (PSC)–derived kidney organoids are used to model human renal development and disease; however, accessible models of human fetal development to benchmark PSC-derived organoids remain underdeveloped. Here, we establish a chemically defined, serum-free protocol for prolonged culture of human fetal kidney-derived organoids (hFKOs) in vitro. hFKOs self-organize into polarized renal epithelium, reinitiate from NCAM1+ progenitors, and recapitulate nephrogenic and ureteric bud lineages. Bulk transcriptomics, single-cell RNA sequencing, pseudotime analysis, and immunostaining revealed diverse renal tissue cell populations, with a preserved epithelial progenitor pool and tubular differentiation axis. hFKOs were enriched for Notch signaling genes, enabling single-cell analysis of pharmacological Notch inhibition. This revealed a maturation block with increased nephron progenitors and a shift toward distal over early proximal tubule fates. We also identified a novel prominin-1-expressing cell state that evades Notch inhibition to generate both proximal and distal tubules. Overall, hFKOs provide a faithful model to gain insights into human kidney development, advancing the fields of stem cell biology and regenerative medicine.",

keywords = "Human Fetal Kidney, Kidney Organoids, Nephrogenesis, Notch Pathway, Single-cell Transcriptomics",

author = "Michael Namestnikov and Osnat Cohen-Zontag and Dorit Omer and Yehudit Gnatek and Sanja Goldberg and Thomas Vincent and Swati Singh and Yair Shiber and \{Rafaeli Yehudai\}, Tal and Hadas Volkov and \{Folkman Genet\}, Dani and Achia Urbach and Sylvie Polak-Charcon and Igor Grinberg and Naomi Pode-Shakked and Boaz Weisz and Zvi Vaknin and Freedman, \{Benjamin S.\} and Benjamin Dekel",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2025.",

year = "2025",

month = sep,

day = "1",

doi = "10.1038/s44318-025-00504-2",

language = "English",

volume = "44",

pages = "4681--4719",

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Namestnikov, M, Cohen-Zontag, O, Omer, D, Gnatek, Y, Goldberg, S, Vincent, T, Singh, S, Shiber, Y, Rafaeli Yehudai, T, Volkov, H, Folkman Genet, D, Urbach, A, Polak-Charcon, S, Grinberg, I, Pode-Shakked, N, Weisz, B, Vaknin, Z, Freedman, BS & Dekel, B 2025, 'Human fetal kidney organoids model early human nephrogenesis and Notch-driven cell fate', EMBO Journal, vol. 44, no. 17, pp. 4681-4719. https://doi.org/10.1038/s44318-025-00504-2

TY - JOUR

T1 - Human fetal kidney organoids model early human nephrogenesis and Notch-driven cell fate

AU - Namestnikov, Michael

AU - Cohen-Zontag, Osnat

AU - Omer, Dorit

AU - Gnatek, Yehudit

AU - Goldberg, Sanja

AU - Vincent, Thomas

AU - Singh, Swati

AU - Shiber, Yair

AU - Rafaeli Yehudai, Tal

AU - Volkov, Hadas

AU - Folkman Genet, Dani

AU - Urbach, Achia

AU - Polak-Charcon, Sylvie

AU - Grinberg, Igor

AU - Pode-Shakked, Naomi

AU - Weisz, Boaz

AU - Vaknin, Zvi

AU - Freedman, Benjamin S.

AU - Dekel, Benjamin

PY - 2025/9/1

Y1 - 2025/9/1

N2 - Pluripotent stem cell (PSC)–derived kidney organoids are used to model human renal development and disease; however, accessible models of human fetal development to benchmark PSC-derived organoids remain underdeveloped. Here, we establish a chemically defined, serum-free protocol for prolonged culture of human fetal kidney-derived organoids (hFKOs) in vitro. hFKOs self-organize into polarized renal epithelium, reinitiate from NCAM1+ progenitors, and recapitulate nephrogenic and ureteric bud lineages. Bulk transcriptomics, single-cell RNA sequencing, pseudotime analysis, and immunostaining revealed diverse renal tissue cell populations, with a preserved epithelial progenitor pool and tubular differentiation axis. hFKOs were enriched for Notch signaling genes, enabling single-cell analysis of pharmacological Notch inhibition. This revealed a maturation block with increased nephron progenitors and a shift toward distal over early proximal tubule fates. We also identified a novel prominin-1-expressing cell state that evades Notch inhibition to generate both proximal and distal tubules. Overall, hFKOs provide a faithful model to gain insights into human kidney development, advancing the fields of stem cell biology and regenerative medicine.

AB - Pluripotent stem cell (PSC)–derived kidney organoids are used to model human renal development and disease; however, accessible models of human fetal development to benchmark PSC-derived organoids remain underdeveloped. Here, we establish a chemically defined, serum-free protocol for prolonged culture of human fetal kidney-derived organoids (hFKOs) in vitro. hFKOs self-organize into polarized renal epithelium, reinitiate from NCAM1+ progenitors, and recapitulate nephrogenic and ureteric bud lineages. Bulk transcriptomics, single-cell RNA sequencing, pseudotime analysis, and immunostaining revealed diverse renal tissue cell populations, with a preserved epithelial progenitor pool and tubular differentiation axis. hFKOs were enriched for Notch signaling genes, enabling single-cell analysis of pharmacological Notch inhibition. This revealed a maturation block with increased nephron progenitors and a shift toward distal over early proximal tubule fates. We also identified a novel prominin-1-expressing cell state that evades Notch inhibition to generate both proximal and distal tubules. Overall, hFKOs provide a faithful model to gain insights into human kidney development, advancing the fields of stem cell biology and regenerative medicine.

KW - Human Fetal Kidney

KW - Kidney Organoids

KW - Nephrogenesis

KW - Notch Pathway

KW - Single-cell Transcriptomics

UR - https://www.scopus.com/pages/publications/105011277272

U2 - 10.1038/s44318-025-00504-2

DO - 10.1038/s44318-025-00504-2

M3 - Article

C2 - 40691416

AN - SCOPUS:105011277272

SN - 0261-4189

VL - 44

SP - 4681

EP - 4719

JO - EMBO Journal

JF - EMBO Journal

IS - 17

ER -

Human fetal kidney organoids model early human nephrogenesis and Notch-driven cell fate

Abstract

Keywords

ASJC Scopus subject areas

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