An in vitro model system based on calcium- and phosphate ion-induced hMSC spheroid mineralization

Steven Vermeulen; Kèvin Knoops; Hans Duimel; Maryam Parvizifard; Denis van Beurden; Carmen López-Iglesias; Stefan Giselbrecht; Roman Truckenmüller; Pamela Habibovic; Zeinab Tahmasebi Birgani

doi:10.1016/j.mtbio.2023.100844

An in vitro model system based on calcium- and phosphate ion-induced hMSC spheroid mineralization

Steven Vermeulen, Kèvin Knoops, Hans Duimel, Maryam Parvizifard, Denis van Beurden, Carmen López-Iglesias, Stefan Giselbrecht, Roman Truckenmüller, Pamela Habibovic, Zeinab Tahmasebi Birgani^*

^*Corresponding author for this work

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

Abstract

A challenge in regenerative medicine is creating the three-dimensional organic and inorganic in vitro microenvironment of bone, which would allow the study of musculoskeletal disorders and the generation of building blocks for bone regeneration. This study presents a microwell-based platform for creating spheroids of human mesenchymal stromal cells, which are then mineralized using ionic calcium and phosphate supplementation. The resulting mineralized spheroids promote an osteogenic gene expression profile through the influence of the spheroids’ biophysical environment and inorganic signaling and require less calcium or phosphate to achieve mineralization compared to a monolayer culture. We found that mineralized spheroids represent an in vitro model for studying small molecule perturbations and extracellular mediated calcification. Furthermore, we demonstrate that understanding pathway signaling elicited by the spheroid environment allows mimicking these pathways in traditional monolayer culture, enabling similar rapid mineralization events. In sum, this study demonstrates the rapid generation and employment of a mineralized cell model system for regenerative medicine applications.

Original language	English
Article number	100844
Number of pages	15
Journal	Materials today. Bio
Volume	23
Issue number	1
DOIs	https://doi.org/10.1016/j.mtbio.2023.100844
Publication status	Published - 1 Dec 2023

Keywords

Bone
Calcium
Mesenchymal stromal cells
Mineralization
Phosphate
Regenerative medicine
Spheroids

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10.1016/j.mtbio.2023.100844Licence: CC BY

Cite this

@article{5346e03b876c4b8c8ef84c52c5ab235f,

title = "An in vitro model system based on calcium- and phosphate ion-induced hMSC spheroid mineralization",

abstract = "A challenge in regenerative medicine is creating the three-dimensional organic and inorganic in vitro microenvironment of bone, which would allow the study of musculoskeletal disorders and the generation of building blocks for bone regeneration. This study presents a microwell-based platform for creating spheroids of human mesenchymal stromal cells, which are then mineralized using ionic calcium and phosphate supplementation. The resulting mineralized spheroids promote an osteogenic gene expression profile through the influence of the spheroids{\textquoteright} biophysical environment and inorganic signaling and require less calcium or phosphate to achieve mineralization compared to a monolayer culture. We found that mineralized spheroids represent an in vitro model for studying small molecule perturbations and extracellular mediated calcification. Furthermore, we demonstrate that understanding pathway signaling elicited by the spheroid environment allows mimicking these pathways in traditional monolayer culture, enabling similar rapid mineralization events. In sum, this study demonstrates the rapid generation and employment of a mineralized cell model system for regenerative medicine applications.",

keywords = "Bone, Calcium, Mesenchymal stromal cells, Mineralization, Phosphate, Regenerative medicine, Spheroids",

author = "Steven Vermeulen and K{\`e}vin Knoops and Hans Duimel and Maryam Parvizifard and {van Beurden}, Denis and Carmen L{\'o}pez-Iglesias and Stefan Giselbrecht and Roman Truckenm{\"u}ller and Pamela Habibovic and {Tahmasebi Birgani}, Zeinab",

note = "Funding Information: The authors thank Dr. Pinak Samal and Dr. Philipp Maurer from the MERLN institute for the design, fabrication, and provision of the brass molds. SV, SG, RT, PH and ZTB acknowledge the financial support of the European Union Interreg Vlaanderen-Nederland project (“BIOMAT on microfluidic chip”; grant no. 0433 ), the Dutch Province of Limburg (program “Limburg INvesteert in haar Kenniseconomie/LINK”; grant nos. SAS-2014-00837 and SAS-2018-02477 ) and the Gravitation Program of the Netherlands Organization for Scientific Research (NWO) (project {\textquoteleft}Materials-Driven Regeneration{\textquoteright}; grant no. 024.003.013 ). ZTB gratefully acknowledges the NWO Incentive Grant for Women in STEM (Project “Biotetris”, grant no. 18748 ). Fig. 1 was created with BioRender.com. Publisher Copyright: {\textcopyright} 2023 The Authors",

year = "2023",

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doi = "10.1016/j.mtbio.2023.100844",

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T1 - An in vitro model system based on calcium- and phosphate ion-induced hMSC spheroid mineralization

AU - Vermeulen, Steven

AU - Knoops, Kèvin

AU - Duimel, Hans

AU - Parvizifard, Maryam

AU - van Beurden, Denis

AU - López-Iglesias, Carmen

AU - Giselbrecht, Stefan

AU - Truckenmüller, Roman

AU - Habibovic, Pamela

AU - Tahmasebi Birgani, Zeinab

N1 - Funding Information: The authors thank Dr. Pinak Samal and Dr. Philipp Maurer from the MERLN institute for the design, fabrication, and provision of the brass molds. SV, SG, RT, PH and ZTB acknowledge the financial support of the European Union Interreg Vlaanderen-Nederland project (“BIOMAT on microfluidic chip”; grant no. 0433 ), the Dutch Province of Limburg (program “Limburg INvesteert in haar Kenniseconomie/LINK”; grant nos. SAS-2014-00837 and SAS-2018-02477 ) and the Gravitation Program of the Netherlands Organization for Scientific Research (NWO) (project ‘Materials-Driven Regeneration’; grant no. 024.003.013 ). ZTB gratefully acknowledges the NWO Incentive Grant for Women in STEM (Project “Biotetris”, grant no. 18748 ). Fig. 1 was created with BioRender.com. Publisher Copyright: © 2023 The Authors

PY - 2023/12/1

Y1 - 2023/12/1

N2 - A challenge in regenerative medicine is creating the three-dimensional organic and inorganic in vitro microenvironment of bone, which would allow the study of musculoskeletal disorders and the generation of building blocks for bone regeneration. This study presents a microwell-based platform for creating spheroids of human mesenchymal stromal cells, which are then mineralized using ionic calcium and phosphate supplementation. The resulting mineralized spheroids promote an osteogenic gene expression profile through the influence of the spheroids’ biophysical environment and inorganic signaling and require less calcium or phosphate to achieve mineralization compared to a monolayer culture. We found that mineralized spheroids represent an in vitro model for studying small molecule perturbations and extracellular mediated calcification. Furthermore, we demonstrate that understanding pathway signaling elicited by the spheroid environment allows mimicking these pathways in traditional monolayer culture, enabling similar rapid mineralization events. In sum, this study demonstrates the rapid generation and employment of a mineralized cell model system for regenerative medicine applications.

AB - A challenge in regenerative medicine is creating the three-dimensional organic and inorganic in vitro microenvironment of bone, which would allow the study of musculoskeletal disorders and the generation of building blocks for bone regeneration. This study presents a microwell-based platform for creating spheroids of human mesenchymal stromal cells, which are then mineralized using ionic calcium and phosphate supplementation. The resulting mineralized spheroids promote an osteogenic gene expression profile through the influence of the spheroids’ biophysical environment and inorganic signaling and require less calcium or phosphate to achieve mineralization compared to a monolayer culture. We found that mineralized spheroids represent an in vitro model for studying small molecule perturbations and extracellular mediated calcification. Furthermore, we demonstrate that understanding pathway signaling elicited by the spheroid environment allows mimicking these pathways in traditional monolayer culture, enabling similar rapid mineralization events. In sum, this study demonstrates the rapid generation and employment of a mineralized cell model system for regenerative medicine applications.

KW - Bone

KW - Calcium

KW - Mesenchymal stromal cells

KW - Mineralization

KW - Phosphate

KW - Regenerative medicine

KW - Spheroids

U2 - 10.1016/j.mtbio.2023.100844

DO - 10.1016/j.mtbio.2023.100844

M3 - Article

SN - 2590-0064

VL - 23

JO - Materials today. Bio

JF - Materials today. Bio

IS - 1

M1 - 100844

ER -