Transcriptomic and proteomic profiling of bi-partite and tri-partite murine iPSC-derived neurospheroids under steady-state and inflammatory condition

Julia Di Stefano; Laura Garcia-Pupo; Federica Di Marco; Helena Motaln; Jonas Govaerts; Elise Van Breedam; Ligia Monica Mateiu; Siebe Van Calster; Leonardo Ricciardi; Alessandra Quarta; Peter Verstraelen; Winnok H. De Vos; Boris Rogelj; Ilaria Cicalini; Vincenzo De Laurenzi; Piero Del Boccio; Una FitzGerald; Wim Vanden Berghe; Marleen Verhoye; Damiana Pieragostino; Peter Ponsaerts

doi:10.1016/j.bbi.2024.07.008

Transcriptomic and proteomic profiling of bi-partite and tri-partite murine iPSC-derived neurospheroids under steady-state and inflammatory condition

Julia Di Stefano, Laura Garcia-Pupo, Federica Di Marco, Helena Motaln, Jonas Govaerts, Elise Van Breedam, Ligia Monica Mateiu, Siebe Van Calster, Leonardo Ricciardi, Alessandra Quarta, Peter Verstraelen, Winnok H. De Vos, Boris Rogelj, Ilaria Cicalini, Vincenzo De Laurenzi, Piero Del Boccio, Una FitzGerald, Wim Vanden Berghe, Marleen Verhoye, Damiana PieragostinoPeter Ponsaerts

Biomedical Engineering

Research output: Contribution to a Journal (Peer & Non Peer) › Article › peer-review

3 Citations (Scopus)

Abstract

induced-pluripotent stem cell (iPSC)-derived neurospheroid (NSPH) models are an emerging in vitro toolkit to study the influence of inflammatory triggers on neurodegeneration and repair in a 3D neural environment. In contrast to their human counterpart, the absence of murine iPSC-derived NSPHs for profound characterisation and validation studies is a major experimental research gap, even though they offer the only possibility to truly compare or validate in vitro NSPH responses with in vivo brain responses. To contribute to these developments, we here describe the generation and characterisation of 5-week-old CX₃CR1^eGFP+/- CCR2^RFP+/- murine (m)iPSC-derived bi-partite (neurons + astrocytes) and tri-partite (neurons + astrocytes + microglia) NSPH models that can be subjected to cellular activation following pro-inflammatory stimulation. First, cytokine analysis demonstrates that both bi-partite and tri-partite NSPHs can be triggered to release IL6 and CXCL10 following three days of stimulation with, respectively, TNFα + IL1β + IFNγ and LPS + IFNγ. Additionally, immunocytochemical analysis for G3BP1 and PABPC1 revealed the development of stress granules in both bi-partite and tri-partite NSPHs after 3 days of stimulation. To further investigate the observed signs of inflammatory response and cellular stress, we performed an untargeted transcriptomic and proteomic analysis of bi- and tri-partite NSPHs under steady-state and inflammatory conditions. Here, using the combined differential gene and protein expression profiles between unstimulated and stimulated NSPHs, Ingenuity Pathway Analysis (IPA) confirms the activation of canonical pathways associated with inflammation and cellular stress in both bi-partite and tri-partite NSPHs. Moreover, our multi-omics analysis suggests a higher level of downstream inflammatory responses, impairment of homeostatic and developmental processes, as well as activation of cell death processes in stimulated tri-partite NSPHs compared to bi-partite NSPHs. Concluding, these results emphasise the advantages of including microglia in NSPH research to study inflammation-induced neurodegeneration in a 3D neural environment.

Original language	English
Pages (from-to)	1-12
Number of pages	12
Journal	Brain, Behavior, and Immunity
Volume	121
DOIs	https://doi.org/10.1016/j.bbi.2024.07.008
Publication status	Published - Oct 2024

Keywords

Inflammatory response
Microglia
Murine iPSC
Neurospheroids
Proteomics
Stress granules
Transcriptomics

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10.1016/j.bbi.2024.07.008

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Di Stefano, J., Garcia-Pupo, L., Di Marco, F., Motaln, H., Govaerts, J., Van Breedam, E., Mateiu, L. M., Van Calster, S., Ricciardi, L., Quarta, A., Verstraelen, P., De Vos, W. H., Rogelj, B., Cicalini, I., De Laurenzi, V., Del Boccio, P., FitzGerald, U., Vanden Berghe, W., Verhoye, M., ... Ponsaerts, P. (2024). Transcriptomic and proteomic profiling of bi-partite and tri-partite murine iPSC-derived neurospheroids under steady-state and inflammatory condition. Brain, Behavior, and Immunity, 121, 1-12. https://doi.org/10.1016/j.bbi.2024.07.008

@article{84d3621239a94e7793143dcf9527af57,

title = "Transcriptomic and proteomic profiling of bi-partite and tri-partite murine iPSC-derived neurospheroids under steady-state and inflammatory condition",

abstract = "induced-pluripotent stem cell (iPSC)-derived neurospheroid (NSPH) models are an emerging in vitro toolkit to study the influence of inflammatory triggers on neurodegeneration and repair in a 3D neural environment. In contrast to their human counterpart, the absence of murine iPSC-derived NSPHs for profound characterisation and validation studies is a major experimental research gap, even though they offer the only possibility to truly compare or validate in vitro NSPH responses with in vivo brain responses. To contribute to these developments, we here describe the generation and characterisation of 5-week-old CX3CR1eGFP+/- CCR2RFP+/- murine (m)iPSC-derived bi-partite (neurons + astrocytes) and tri-partite (neurons + astrocytes + microglia) NSPH models that can be subjected to cellular activation following pro-inflammatory stimulation. First, cytokine analysis demonstrates that both bi-partite and tri-partite NSPHs can be triggered to release IL6 and CXCL10 following three days of stimulation with, respectively, TNFα + IL1β + IFNγ and LPS + IFNγ. Additionally, immunocytochemical analysis for G3BP1 and PABPC1 revealed the development of stress granules in both bi-partite and tri-partite NSPHs after 3 days of stimulation. To further investigate the observed signs of inflammatory response and cellular stress, we performed an untargeted transcriptomic and proteomic analysis of bi- and tri-partite NSPHs under steady-state and inflammatory conditions. Here, using the combined differential gene and protein expression profiles between unstimulated and stimulated NSPHs, Ingenuity Pathway Analysis (IPA) confirms the activation of canonical pathways associated with inflammation and cellular stress in both bi-partite and tri-partite NSPHs. Moreover, our multi-omics analysis suggests a higher level of downstream inflammatory responses, impairment of homeostatic and developmental processes, as well as activation of cell death processes in stimulated tri-partite NSPHs compared to bi-partite NSPHs. Concluding, these results emphasise the advantages of including microglia in NSPH research to study inflammation-induced neurodegeneration in a 3D neural environment.",

keywords = "Inflammatory response, Microglia, Murine iPSC, Neurospheroids, Proteomics, Stress granules, Transcriptomics",

author = "\{Di Stefano\}, Julia and Laura Garcia-Pupo and \{Di Marco\}, Federica and Helena Motaln and Jonas Govaerts and \{Van Breedam\}, Elise and Mateiu, \{Ligia Monica\} and \{Van Calster\}, Siebe and Leonardo Ricciardi and Alessandra Quarta and Peter Verstraelen and \{De Vos\}, \{Winnok H.\} and Boris Rogelj and Ilaria Cicalini and \{De Laurenzi\}, Vincenzo and \{Del Boccio\}, Piero and Una FitzGerald and \{Vanden Berghe\}, Wim and Marleen Verhoye and Damiana Pieragostino and Peter Ponsaerts",

note = "Publisher Copyright: {\textcopyright} 2024 Elsevier Inc.",

year = "2024",

month = oct,

doi = "10.1016/j.bbi.2024.07.008",

language = "English",

volume = "121",

pages = "1--12",

journal = "Brain, Behavior, and Immunity",

issn = "0889-1591",

publisher = "Academic Press Inc.",

}

Di Stefano, J, Garcia-Pupo, L, Di Marco, F, Motaln, H, Govaerts, J, Van Breedam, E, Mateiu, LM, Van Calster, S, Ricciardi, L, Quarta, A, Verstraelen, P, De Vos, WH, Rogelj, B, Cicalini, I, De Laurenzi, V, Del Boccio, P, FitzGerald, U, Vanden Berghe, W, Verhoye, M, Pieragostino, D & Ponsaerts, P 2024, 'Transcriptomic and proteomic profiling of bi-partite and tri-partite murine iPSC-derived neurospheroids under steady-state and inflammatory condition', Brain, Behavior, and Immunity, vol. 121, pp. 1-12. https://doi.org/10.1016/j.bbi.2024.07.008

TY - JOUR

T1 - Transcriptomic and proteomic profiling of bi-partite and tri-partite murine iPSC-derived neurospheroids under steady-state and inflammatory condition

AU - Di Stefano, Julia

AU - Garcia-Pupo, Laura

AU - Di Marco, Federica

AU - Motaln, Helena

AU - Govaerts, Jonas

AU - Van Breedam, Elise

AU - Mateiu, Ligia Monica

AU - Van Calster, Siebe

AU - Ricciardi, Leonardo

AU - Quarta, Alessandra

AU - Verstraelen, Peter

AU - De Vos, Winnok H.

AU - Rogelj, Boris

AU - Cicalini, Ilaria

AU - De Laurenzi, Vincenzo

AU - Del Boccio, Piero

AU - FitzGerald, Una

AU - Vanden Berghe, Wim

AU - Verhoye, Marleen

AU - Pieragostino, Damiana

AU - Ponsaerts, Peter

PY - 2024/10

Y1 - 2024/10

N2 - induced-pluripotent stem cell (iPSC)-derived neurospheroid (NSPH) models are an emerging in vitro toolkit to study the influence of inflammatory triggers on neurodegeneration and repair in a 3D neural environment. In contrast to their human counterpart, the absence of murine iPSC-derived NSPHs for profound characterisation and validation studies is a major experimental research gap, even though they offer the only possibility to truly compare or validate in vitro NSPH responses with in vivo brain responses. To contribute to these developments, we here describe the generation and characterisation of 5-week-old CX3CR1eGFP+/- CCR2RFP+/- murine (m)iPSC-derived bi-partite (neurons + astrocytes) and tri-partite (neurons + astrocytes + microglia) NSPH models that can be subjected to cellular activation following pro-inflammatory stimulation. First, cytokine analysis demonstrates that both bi-partite and tri-partite NSPHs can be triggered to release IL6 and CXCL10 following three days of stimulation with, respectively, TNFα + IL1β + IFNγ and LPS + IFNγ. Additionally, immunocytochemical analysis for G3BP1 and PABPC1 revealed the development of stress granules in both bi-partite and tri-partite NSPHs after 3 days of stimulation. To further investigate the observed signs of inflammatory response and cellular stress, we performed an untargeted transcriptomic and proteomic analysis of bi- and tri-partite NSPHs under steady-state and inflammatory conditions. Here, using the combined differential gene and protein expression profiles between unstimulated and stimulated NSPHs, Ingenuity Pathway Analysis (IPA) confirms the activation of canonical pathways associated with inflammation and cellular stress in both bi-partite and tri-partite NSPHs. Moreover, our multi-omics analysis suggests a higher level of downstream inflammatory responses, impairment of homeostatic and developmental processes, as well as activation of cell death processes in stimulated tri-partite NSPHs compared to bi-partite NSPHs. Concluding, these results emphasise the advantages of including microglia in NSPH research to study inflammation-induced neurodegeneration in a 3D neural environment.

AB - induced-pluripotent stem cell (iPSC)-derived neurospheroid (NSPH) models are an emerging in vitro toolkit to study the influence of inflammatory triggers on neurodegeneration and repair in a 3D neural environment. In contrast to their human counterpart, the absence of murine iPSC-derived NSPHs for profound characterisation and validation studies is a major experimental research gap, even though they offer the only possibility to truly compare or validate in vitro NSPH responses with in vivo brain responses. To contribute to these developments, we here describe the generation and characterisation of 5-week-old CX3CR1eGFP+/- CCR2RFP+/- murine (m)iPSC-derived bi-partite (neurons + astrocytes) and tri-partite (neurons + astrocytes + microglia) NSPH models that can be subjected to cellular activation following pro-inflammatory stimulation. First, cytokine analysis demonstrates that both bi-partite and tri-partite NSPHs can be triggered to release IL6 and CXCL10 following three days of stimulation with, respectively, TNFα + IL1β + IFNγ and LPS + IFNγ. Additionally, immunocytochemical analysis for G3BP1 and PABPC1 revealed the development of stress granules in both bi-partite and tri-partite NSPHs after 3 days of stimulation. To further investigate the observed signs of inflammatory response and cellular stress, we performed an untargeted transcriptomic and proteomic analysis of bi- and tri-partite NSPHs under steady-state and inflammatory conditions. Here, using the combined differential gene and protein expression profiles between unstimulated and stimulated NSPHs, Ingenuity Pathway Analysis (IPA) confirms the activation of canonical pathways associated with inflammation and cellular stress in both bi-partite and tri-partite NSPHs. Moreover, our multi-omics analysis suggests a higher level of downstream inflammatory responses, impairment of homeostatic and developmental processes, as well as activation of cell death processes in stimulated tri-partite NSPHs compared to bi-partite NSPHs. Concluding, these results emphasise the advantages of including microglia in NSPH research to study inflammation-induced neurodegeneration in a 3D neural environment.

KW - Inflammatory response

KW - Microglia

KW - Murine iPSC

KW - Neurospheroids

KW - Proteomics

KW - Stress granules

KW - Transcriptomics

UR - https://www.scopus.com/pages/publications/85198700946

U2 - 10.1016/j.bbi.2024.07.008

DO - 10.1016/j.bbi.2024.07.008

M3 - Article

SN - 0889-1591

VL - 121

SP - 1

EP - 12

JO - Brain, Behavior, and Immunity

JF - Brain, Behavior, and Immunity

ER -

Transcriptomic and proteomic profiling of bi-partite and tri-partite murine iPSC-derived neurospheroids under steady-state and inflammatory condition

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Keywords

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