Skip to main content

Lund University Publications

LUND UNIVERSITY LIBRARIES

Dissecting Dopaminergic Neuron Specification at Single Cell Resolution - Insights from 3D brain organoids and xenograft models

Sozzi, Edoardo LU orcid (2025) In Lund University, Faculty of Medicine Doctoral Dissertation Series
Abstract
Midbrain dopaminergic neurons exhibit a wide diversity in their projection patterns, disease vulnerability, and functions, playing key roles in voluntary motor control, cognition, and reward processing. Parkinson’s Disease, one of the most common neurodegenerative disorders, is characterized by the selective degeneration of the A9 dopaminergic neuron subtype, leading to severe motor dysfunction. Despite advancements in symptomatic treatments, current approaches fail to halt disease progression, highlighting the need for novel therapeutic strategies such as cell replacement therapy. Generating authentic human dopaminergic neurons for transplantation and therapeutic purposes relies on a comprehensive understanding of the factors driving... (More)
Midbrain dopaminergic neurons exhibit a wide diversity in their projection patterns, disease vulnerability, and functions, playing key roles in voluntary motor control, cognition, and reward processing. Parkinson’s Disease, one of the most common neurodegenerative disorders, is characterized by the selective degeneration of the A9 dopaminergic neuron subtype, leading to severe motor dysfunction. Despite advancements in symptomatic treatments, current approaches fail to halt disease progression, highlighting the need for novel therapeutic strategies such as cell replacement therapy. Generating authentic human dopaminergic neurons for transplantation and therapeutic purposes relies on a comprehensive understanding of the factors driving their development. However, the molecular mechanisms underlying the specification of midbrain dopaminergic neurons into distinct subtypes remain poorly understood. Due to the inaccessibility of developing and adult human brain tissue, novel methodologies are needed for investigating these processes in a human-relevant context. This thesis investigates the development, diversity, and specification of human dopaminergic neurons using advanced human stem cell models, with a particular focus on their application in cell replacement therapies for Parkinson’s Disease. In the first part, I established ventral midbrain-patterned organoids that recapitulate developmental trajectories and the molecular identities of distinct dopaminergic neuron subtypes. To overcome limitations in conventional organoid technology, silk scaffolding was also introduced, enhancing cell viability and neuronal maturation. In the second part, I linked the molecular identities of human dopaminergic neurons to their projection patterns using homotopic transplantation models. Finally, co-grafting experiments examined the influence of support cell types on dopaminergic neuron maturation and lineage commitment, identifying critical factors shaping subtype identity. These findings advance our understanding of human dopaminergic neuron development and subtype specification, offering valuable insights for refining cell replacement therapies for Parkinson’s Disease. (Less)
Please use this url to cite or link to this publication:
author
supervisor
opponent
  • Professor of Glial Cell Biology Castelo-Branco, Gonçalo, Department of Medical Biochemistry and Biophysics, Karolinska Institutet, Stockholm
organization
publishing date
type
Thesis
publication status
published
subject
keywords
brain organoids, Parkinson Disease, Dopaminergic neurons, Development, Cell replacement therapy, Single cell RNA sequencing
in
Lund University, Faculty of Medicine Doctoral Dissertation Series
issue
2025:12
pages
114 pages
publisher
Lund University, Faculty of Medicine
defense location
Segerfalksalen, BMC A10, Sölvegatan 17 i Lund. Join by Zoom: https://lu-se.zoom.us/j/61104232511
defense date
2025-02-07 09:00:00
ISSN
1652-8220
ISBN
978-91-8021-665-4
language
English
LU publication?
yes
id
b0d711f1-8a44-4648-9076-386ccc4947d4
date added to LUP
2025-01-16 15:59:13
date last changed
2025-04-04 14:35:43
@phdthesis{b0d711f1-8a44-4648-9076-386ccc4947d4,
  abstract     = {{Midbrain dopaminergic neurons exhibit a wide diversity in their projection patterns, disease vulnerability, and functions, playing key roles in voluntary motor control, cognition, and reward processing. Parkinson’s Disease, one of the most common neurodegenerative disorders, is characterized by the selective degeneration of the A9 dopaminergic neuron subtype, leading to severe motor dysfunction. Despite advancements in symptomatic treatments, current approaches fail to halt disease progression, highlighting the need for novel therapeutic strategies such as cell replacement therapy. Generating authentic human dopaminergic neurons for transplantation and therapeutic purposes relies on a comprehensive understanding of the factors driving their development. However, the molecular mechanisms underlying the specification of midbrain dopaminergic neurons into distinct subtypes remain poorly understood. Due to the inaccessibility of developing and adult human brain tissue, novel methodologies are needed for investigating these processes in a human-relevant context. This thesis investigates the development, diversity, and specification of human dopaminergic neurons using advanced human stem cell models, with a particular focus on their application in cell replacement therapies for Parkinson’s Disease. In the first part, I established ventral midbrain-patterned organoids that recapitulate developmental trajectories and the molecular identities of distinct dopaminergic neuron subtypes. To overcome limitations in conventional organoid technology, silk scaffolding was also introduced, enhancing cell viability and neuronal maturation. In the second part, I linked the molecular identities of human dopaminergic neurons to their projection patterns using homotopic transplantation models. Finally, co-grafting experiments examined the influence of support cell types on dopaminergic neuron maturation and lineage commitment, identifying critical factors shaping subtype identity. These findings advance our understanding of human dopaminergic neuron development and subtype specification, offering valuable insights for refining cell replacement therapies for Parkinson’s Disease.}},
  author       = {{Sozzi, Edoardo}},
  isbn         = {{978-91-8021-665-4}},
  issn         = {{1652-8220}},
  keywords     = {{brain organoids; Parkinson Disease; Dopaminergic neurons; Development; Cell replacement therapy; Single cell RNA sequencing}},
  language     = {{eng}},
  number       = {{2025:12}},
  publisher    = {{Lund University, Faculty of Medicine}},
  school       = {{Lund University}},
  series       = {{Lund University, Faculty of Medicine Doctoral Dissertation Series}},
  title        = {{Dissecting Dopaminergic Neuron Specification at Single Cell Resolution - Insights from 3D brain organoids and xenograft models}},
  url          = {{https://lup.lub.lu.se/search/files/206075434/Edoardo_Sozzi_PhD_Thesis_-_kappa.pdf}},
  year         = {{2025}},
}