Implementing a meningioma organoid platform for testing new treatment approaches
Implementing a meningioma organoid platform for testing new treatment approaches
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Date of Embargo
01.12.2026Type of Scholarly Publication
DissertationDate of Exam
27.10.2025Date of Publication
17.11.2025Advisor
Toma, Marieta IoanaCo-Referee
Strizek, BrigitteMetadata
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Abstract
Meningioma represents the most common type of brain tumor, accounting for approximately 38.3% of all cases. Despite its prevalence, severe symptoms and potential lethality in high-grade forms, current therapeutic strategies remain limited to surgery and radiotherapy. The risk of recurrency is high. Up to date there are no established pharmacological treatments available.
This thesis explores the development of meningioma organoids. Various culturing techniques were evaluated. Suspension-based methods, such as low-attachment plate cultures and the CERO bioreactor were the most effective. Those methods led to the best meningioma organoid growth in size as well as in number. The resulting organoids resembled the fresh tumor samples derived from patients. Additionally, the feasibility of establishing a meningioma organoid biobank was demonstrated by successfully generating organoids from cryopreserved tumor tissue. Drug testing using the AKT-inhibitor capivasertib and the CDK 4/6-inhibitor abemaciclib showed decreased proliferation, determined by reduced Ki-67 mRNA expression. Interestingly, capivasertib treatment led to an unexpected increase in phosphorylated GSK protein levels, suggesting complex pathway dynamics.
Overall, this work establishes a platform for meningioma organoid culture and highlights its potential as a tool for drug screening and the future development of targeted pharmacological therapies.
This thesis explores the development of meningioma organoids. Various culturing techniques were evaluated. Suspension-based methods, such as low-attachment plate cultures and the CERO bioreactor were the most effective. Those methods led to the best meningioma organoid growth in size as well as in number. The resulting organoids resembled the fresh tumor samples derived from patients. Additionally, the feasibility of establishing a meningioma organoid biobank was demonstrated by successfully generating organoids from cryopreserved tumor tissue. Drug testing using the AKT-inhibitor capivasertib and the CDK 4/6-inhibitor abemaciclib showed decreased proliferation, determined by reduced Ki-67 mRNA expression. Interestingly, capivasertib treatment led to an unexpected increase in phosphorylated GSK protein levels, suggesting complex pathway dynamics.
Overall, this work establishes a platform for meningioma organoid culture and highlights its potential as a tool for drug screening and the future development of targeted pharmacological therapies.
Subjects
meningioma, organoid, abemaciclib, capivasertib, CDK4/6-inhibitor, AKT-inhibitor, biobank, culture, CERO-bioreactor, low-attachment plate
Classification (DDC)
610 Medizin, GesundheitRaffauf, Jasmin Andrea: Implementing a meningioma organoid platform for testing new treatment approaches. - Bonn, 2025. - Dissertation, Rheinische Friedrich-Wilhelms-Universität Bonn.
Online-Ausgabe in bonndoc: https://nbn-resolving.org/urn:nbn:de:hbz:5-86354
Online-Ausgabe in bonndoc: https://nbn-resolving.org/urn:nbn:de:hbz:5-86354
@phdthesis{handle:20.500.11811/13695,
urn: https://nbn-resolving.org/urn:nbn:de:hbz:5-86354,
doi: https://doi.org/10.48565/bonndoc-714,
author = {{Jasmin Andrea Raffauf}},
title = {Implementing a meningioma organoid platform for testing new treatment approaches},
school = {Rheinische Friedrich-Wilhelms-Universität Bonn},
year = 2025,
month = nov,
note = {Meningioma represents the most common type of brain tumor, accounting for approximately 38.3% of all cases. Despite its prevalence, severe symptoms and potential lethality in high-grade forms, current therapeutic strategies remain limited to surgery and radiotherapy. The risk of recurrency is high. Up to date there are no established pharmacological treatments available.
This thesis explores the development of meningioma organoids. Various culturing techniques were evaluated. Suspension-based methods, such as low-attachment plate cultures and the CERO bioreactor were the most effective. Those methods led to the best meningioma organoid growth in size as well as in number. The resulting organoids resembled the fresh tumor samples derived from patients. Additionally, the feasibility of establishing a meningioma organoid biobank was demonstrated by successfully generating organoids from cryopreserved tumor tissue. Drug testing using the AKT-inhibitor capivasertib and the CDK 4/6-inhibitor abemaciclib showed decreased proliferation, determined by reduced Ki-67 mRNA expression. Interestingly, capivasertib treatment led to an unexpected increase in phosphorylated GSK protein levels, suggesting complex pathway dynamics.
Overall, this work establishes a platform for meningioma organoid culture and highlights its potential as a tool for drug screening and the future development of targeted pharmacological therapies.},
url = {https://hdl.handle.net/20.500.11811/13695}
}
urn: https://nbn-resolving.org/urn:nbn:de:hbz:5-86354,
doi: https://doi.org/10.48565/bonndoc-714,
author = {{Jasmin Andrea Raffauf}},
title = {Implementing a meningioma organoid platform for testing new treatment approaches},
school = {Rheinische Friedrich-Wilhelms-Universität Bonn},
year = 2025,
month = nov,
note = {Meningioma represents the most common type of brain tumor, accounting for approximately 38.3% of all cases. Despite its prevalence, severe symptoms and potential lethality in high-grade forms, current therapeutic strategies remain limited to surgery and radiotherapy. The risk of recurrency is high. Up to date there are no established pharmacological treatments available.
This thesis explores the development of meningioma organoids. Various culturing techniques were evaluated. Suspension-based methods, such as low-attachment plate cultures and the CERO bioreactor were the most effective. Those methods led to the best meningioma organoid growth in size as well as in number. The resulting organoids resembled the fresh tumor samples derived from patients. Additionally, the feasibility of establishing a meningioma organoid biobank was demonstrated by successfully generating organoids from cryopreserved tumor tissue. Drug testing using the AKT-inhibitor capivasertib and the CDK 4/6-inhibitor abemaciclib showed decreased proliferation, determined by reduced Ki-67 mRNA expression. Interestingly, capivasertib treatment led to an unexpected increase in phosphorylated GSK protein levels, suggesting complex pathway dynamics.
Overall, this work establishes a platform for meningioma organoid culture and highlights its potential as a tool for drug screening and the future development of targeted pharmacological therapies.},
url = {https://hdl.handle.net/20.500.11811/13695}
}
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