Author
Listed:
- Homa Majd
(University of California, San Francisco
University of California, San Francisco)
- Ryan M. Samuel
(University of California, San Francisco
University of California, San Francisco)
- Andrius Cesiulis
(University of California, San Francisco
University of California, San Francisco)
- Jonathan T. Ramirez
(University of California, San Francisco
University of California, San Francisco)
- Ali Kalantari
(University of California, San Francisco)
- Kevin Barber
(University of California, San Francisco)
- Sina Farahvashi
(University of California, San Francisco
University of California, San Francisco)
- Zaniar Ghazizadeh
(School of Medicine, Stanford University)
- Alireza Majd
(University of California, San Francisco
University of California, San Francisco)
- Angeline K. Chemel
(University of California, San Francisco
University of California, San Francisco)
- Mikayla N. Richter
(University of California, San Francisco
University of California, San Francisco)
- Subhamoy Das
(School of Medicine, Stanford University)
- Jacqueline L. Bendrick
(Stanford University
Stanford University)
- Matthew G. Keefe
(University of California, San Francisco
University of California, San Francisco)
- Jeffrey Wang
(University of California, San Francisco)
- Rahul K. Shiv
(Stanford University)
- Samyukta Bhat
(University of California, San Francisco)
- Matvei Khoroshkin
(University of California, San Francisco)
- Johnny Yu
(University of California, San Francisco)
- Tomasz J. Nowakowski
(University of California, San Francisco
University of California, San Francisco
University of California, San Francisco)
- Kwun Wah Wen
(University of California, San Francisco)
- Hani Goodarzi
(University of California, San Francisco
Arc Institute)
- Nikhil Thapar
(UCL Great Ormond Street Institute of Child Health
Queensland Children’s Hospital
University of Queensland
Queensland University of Technology)
- Julia A. Kaltschmidt
(School of Medicine, Stanford University
Stanford University)
- Conor J. McCann
(UCL Great Ormond Street Institute of Child Health
NIHR Great Ormond Street Hospital BRC)
- Faranak Fattahi
(University of California, San Francisco
University of California, San Francisco)
Abstract
Gastrointestinal (GI) motility disorders represent a major medical challenge, with few effective therapies available. These disorders often result from dysfunction of inhibitory nitric oxide (NO)-producing motor neurons in the enteric nervous system, which are essential for regulating gut motility. Loss or dysfunction of NO neurons is linked to severe conditions, including achalasia, gastroparesis, intestinal pseudo-obstruction and chronic constipation1,2. Here we introduce a platform based on human pluripotent stem cells (hPSCs) for therapeutic development targeting GI motility disorders. Using an unbiased screen, we identified drug candidates that modulate NO neuron activity and enhance motility in mouse colonic tissue ex vivo. We established a high-throughput strategy to define developmental programs driving the specification of NO neurons and found that inhibition of platelet-derived growth factor receptors (PDGFRs) promotes their differentiation from precursors of the enteric nervous system. Transplantation of these neurons into NO-neuron-deficient mice led to robust engraftment and improved GI motility, offering a promising cell-based therapy for neurodegenerative GI disorders. These studies provide a new framework for understanding and treating enteric neuropathies.
Suggested Citation
Homa Majd & Ryan M. Samuel & Andrius Cesiulis & Jonathan T. Ramirez & Ali Kalantari & Kevin Barber & Sina Farahvashi & Zaniar Ghazizadeh & Alireza Majd & Angeline K. Chemel & Mikayla N. Richter & Subh, 2025.
"Engrafted nitrergic neurons derived from hPSCs improve gut dysmotility in mice,"
Nature, Nature, vol. 645(8079), pages 158-167, September.
Handle:
RePEc:nat:nature:v:645:y:2025:i:8079:d:10.1038_s41586-025-09208-3
DOI: 10.1038/s41586-025-09208-3
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