Epithelial restitution in 3D: Revealing biomechanical and physiochemical dynamics in intestinal organoids via fs laser nanosurgery

Publikation: Beitrag in FachzeitschriftArtikelForschungPeer-Review

Autoren

  • Sören Donath
  • Anna Elisabeth Seidler
  • Karlina Mundin
  • Johannes Wenzel
  • Jonas Scholz
  • Lara Gentemann
  • Julia Kalies
  • Jan Faix
  • Anaclet Ngezahayo
  • André Bleich
  • Alexander Heisterkamp
  • Manuela Buettner
  • Stefan Kalies

Organisationseinheiten

Externe Organisationen

  • NIFE- Niedersächsisches Zentrum für Biomedizintechnik, Implantatforschung und Entwicklung
  • Medizinische Hochschule Hannover (MHH)
  • REBIRTH Forschungszentrum für translationale regenerative Medizin
Forschungs-netzwerk anzeigen

Details

OriginalspracheEnglisch
Aufsatznummer108139
Seitenumfang17
FachzeitschriftiScience
Jahrgang26
Ausgabenummer11
Frühes Online-Datum5 Okt. 2023
PublikationsstatusVeröffentlicht - 17 Nov. 2023

Abstract

Intestinal organoids represent a three-dimensional cell culture system mimicking the mammalian intestine. The application of single-cell ablation for defined wounding via a femtosecond laser system within the crypt base allowed us to study cell dynamics during epithelial restitution. Neighboring cells formed a contractile actin ring encircling the damaged cell, changed the cellular aspect ratio, and immediately closed the barrier. Using traction force microscopy, we observed major forces at the ablation site and additional forces on the crypt sides. Inhibitors of the actomyosin-based mobility of the cells led to the failure of restoring the barrier. Close to the ablation site, high-frequency calcium flickering and propagation of calcium waves occured that synchronized with the contraction of the epithelial layer. We observed an increased signal and nuclear translocation of YAP-1. In conclusion, our approach enabled, for the first time, to unveil the intricacies of epithelial restitution beyond in vivo models by employing precise laser-induced damage in colonoids.

ASJC Scopus Sachgebiete

Zitieren

Epithelial restitution in 3D: Revealing biomechanical and physiochemical dynamics in intestinal organoids via fs laser nanosurgery. / Donath, Sören; Seidler, Anna Elisabeth; Mundin, Karlina et al.
in: iScience, Jahrgang 26, Nr. 11, 108139, 17.11.2023.

Publikation: Beitrag in FachzeitschriftArtikelForschungPeer-Review

Donath, S, Seidler, AE, Mundin, K, Wenzel, J, Scholz, J, Gentemann, L, Kalies, J, Faix, J, Ngezahayo, A, Bleich, A, Heisterkamp, A, Buettner, M & Kalies, S 2023, 'Epithelial restitution in 3D: Revealing biomechanical and physiochemical dynamics in intestinal organoids via fs laser nanosurgery', iScience, Jg. 26, Nr. 11, 108139. https://doi.org/10.1016/j.isci.2023.108139
Donath, S., Seidler, A. E., Mundin, K., Wenzel, J., Scholz, J., Gentemann, L., Kalies, J., Faix, J., Ngezahayo, A., Bleich, A., Heisterkamp, A., Buettner, M., & Kalies, S. (2023). Epithelial restitution in 3D: Revealing biomechanical and physiochemical dynamics in intestinal organoids via fs laser nanosurgery. iScience, 26(11), Artikel 108139. Vorabveröffentlichung online. https://doi.org/10.1016/j.isci.2023.108139
Donath S, Seidler AE, Mundin K, Wenzel J, Scholz J, Gentemann L et al. Epithelial restitution in 3D: Revealing biomechanical and physiochemical dynamics in intestinal organoids via fs laser nanosurgery. iScience. 2023 Nov 17;26(11):108139. Epub 2023 Okt 5. doi: 10.1016/j.isci.2023.108139
Donath, Sören ; Seidler, Anna Elisabeth ; Mundin, Karlina et al. / Epithelial restitution in 3D : Revealing biomechanical and physiochemical dynamics in intestinal organoids via fs laser nanosurgery. in: iScience. 2023 ; Jahrgang 26, Nr. 11.
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title = "Epithelial restitution in 3D: Revealing biomechanical and physiochemical dynamics in intestinal organoids via fs laser nanosurgery",
abstract = "Intestinal organoids represent a three-dimensional cell culture system mimicking the mammalian intestine. The application of single-cell ablation for defined wounding via a femtosecond laser system within the crypt base allowed us to study cell dynamics during epithelial restitution. Neighboring cells formed a contractile actin ring encircling the damaged cell, changed the cellular aspect ratio, and immediately closed the barrier. Using traction force microscopy, we observed major forces at the ablation site and additional forces on the crypt sides. Inhibitors of the actomyosin-based mobility of the cells led to the failure of restoring the barrier. Close to the ablation site, high-frequency calcium flickering and propagation of calcium waves occured that synchronized with the contraction of the epithelial layer. We observed an increased signal and nuclear translocation of YAP-1. In conclusion, our approach enabled, for the first time, to unveil the intricacies of epithelial restitution beyond in vivo models by employing precise laser-induced damage in colonoids.",
keywords = "Bioengineering, Cell biology, Molecular physiology, Optical imaging",
author = "S{\"o}ren Donath and Seidler, {Anna Elisabeth} and Karlina Mundin and Johannes Wenzel and Jonas Scholz and Lara Gentemann and Julia Kalies and Jan Faix and Anaclet Ngezahayo and Andr{\'e} Bleich and Alexander Heisterkamp and Manuela Buettner and Stefan Kalies",
note = "Funding Information: We acknowledge Puja Pandey, Maria Mellin, Anja Siebert (all Hannover Medical School) for providing colonoid culture medium. We thank Prof. Jan Faix (Hannover Medical School) for primary anti-VASP-antibody and help with antibody stainings. Furthermore, we thank Despina Kiriazi (Hannover Medical School) for actin and myosin 2 inhibitors. This study was funded by the REBIRTH Research Center for Translational Regenerative Medicine ( ZN3440 , State of Lower Saxony Ministry of Science and Culture (Nieders. Vorab)). J.K. and A.H. were supported by the biomedical research in endstage and obstructive lung disease Hannover (BREATH) from the german lung center (DZL). M.B. and A.B. were funded by R2N , Federal State of Lower Saxony . The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the article. Funding Information: We acknowledge Puja Pandey, Maria Mellin, Anja Siebert (all Hannover Medical School) for providing colonoid culture medium. We thank Prof. Jan Faix (Hannover Medical School) for primary anti-VASP-antibody and help with antibody stainings. Furthermore, we thank Despina Kiriazi (Hannover Medical School) for actin and myosin 2 inhibitors. This study was funded by the REBIRTH Research Center for Translational Regenerative Medicine (ZN3440, State of Lower Saxony Ministry of Science and Culture (Nieders. Vorab)). J.K. and A.H. were supported by the biomedical research in endstage and obstructive lung disease Hannover (BREATH) from the german lung center (DZL). M.B. and A.B. were funded by R2N, Federal State of Lower Saxony. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the article. Conceptualization, S.D. and S.K; methodology, S.K.; software, J.W. K.M. and S.K.; validation, S.D. A.E.S. L.G. J.W. and S.K.; formal analysis, S.D. and S.K.; investigation, S.D. A.E.S. J.W. K.M. J.S. J.K. J.F. and S.K.; resources, J.K. M.B. and S.K.; data curation, S.D. J.W. K.M. A.N. M.B. and S.K.; writing—original draft preparation, S.D. and S.K.; writing—review and editing, all authors; visualization, S.D. and S.K.; supervision, S.K.; project administration, A.B. A.N. A.H. M.B. and S.K.; funding acquisition, A.B. A.H. and S.K. All authors have read and agreed to the published version of the article. The authors declare no competing interest. ",
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Download

TY - JOUR

T1 - Epithelial restitution in 3D

T2 - Revealing biomechanical and physiochemical dynamics in intestinal organoids via fs laser nanosurgery

AU - Donath, Sören

AU - Seidler, Anna Elisabeth

AU - Mundin, Karlina

AU - Wenzel, Johannes

AU - Scholz, Jonas

AU - Gentemann, Lara

AU - Kalies, Julia

AU - Faix, Jan

AU - Ngezahayo, Anaclet

AU - Bleich, André

AU - Heisterkamp, Alexander

AU - Buettner, Manuela

AU - Kalies, Stefan

N1 - Funding Information: We acknowledge Puja Pandey, Maria Mellin, Anja Siebert (all Hannover Medical School) for providing colonoid culture medium. We thank Prof. Jan Faix (Hannover Medical School) for primary anti-VASP-antibody and help with antibody stainings. Furthermore, we thank Despina Kiriazi (Hannover Medical School) for actin and myosin 2 inhibitors. This study was funded by the REBIRTH Research Center for Translational Regenerative Medicine ( ZN3440 , State of Lower Saxony Ministry of Science and Culture (Nieders. Vorab)). J.K. and A.H. were supported by the biomedical research in endstage and obstructive lung disease Hannover (BREATH) from the german lung center (DZL). M.B. and A.B. were funded by R2N , Federal State of Lower Saxony . The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the article. Funding Information: We acknowledge Puja Pandey, Maria Mellin, Anja Siebert (all Hannover Medical School) for providing colonoid culture medium. We thank Prof. Jan Faix (Hannover Medical School) for primary anti-VASP-antibody and help with antibody stainings. Furthermore, we thank Despina Kiriazi (Hannover Medical School) for actin and myosin 2 inhibitors. This study was funded by the REBIRTH Research Center for Translational Regenerative Medicine (ZN3440, State of Lower Saxony Ministry of Science and Culture (Nieders. Vorab)). J.K. and A.H. were supported by the biomedical research in endstage and obstructive lung disease Hannover (BREATH) from the german lung center (DZL). M.B. and A.B. were funded by R2N, Federal State of Lower Saxony. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the article. Conceptualization, S.D. and S.K; methodology, S.K.; software, J.W. K.M. and S.K.; validation, S.D. A.E.S. L.G. J.W. and S.K.; formal analysis, S.D. and S.K.; investigation, S.D. A.E.S. J.W. K.M. J.S. J.K. J.F. and S.K.; resources, J.K. M.B. and S.K.; data curation, S.D. J.W. K.M. A.N. M.B. and S.K.; writing—original draft preparation, S.D. and S.K.; writing—review and editing, all authors; visualization, S.D. and S.K.; supervision, S.K.; project administration, A.B. A.N. A.H. M.B. and S.K.; funding acquisition, A.B. A.H. and S.K. All authors have read and agreed to the published version of the article. The authors declare no competing interest.

PY - 2023/11/17

Y1 - 2023/11/17

N2 - Intestinal organoids represent a three-dimensional cell culture system mimicking the mammalian intestine. The application of single-cell ablation for defined wounding via a femtosecond laser system within the crypt base allowed us to study cell dynamics during epithelial restitution. Neighboring cells formed a contractile actin ring encircling the damaged cell, changed the cellular aspect ratio, and immediately closed the barrier. Using traction force microscopy, we observed major forces at the ablation site and additional forces on the crypt sides. Inhibitors of the actomyosin-based mobility of the cells led to the failure of restoring the barrier. Close to the ablation site, high-frequency calcium flickering and propagation of calcium waves occured that synchronized with the contraction of the epithelial layer. We observed an increased signal and nuclear translocation of YAP-1. In conclusion, our approach enabled, for the first time, to unveil the intricacies of epithelial restitution beyond in vivo models by employing precise laser-induced damage in colonoids.

AB - Intestinal organoids represent a three-dimensional cell culture system mimicking the mammalian intestine. The application of single-cell ablation for defined wounding via a femtosecond laser system within the crypt base allowed us to study cell dynamics during epithelial restitution. Neighboring cells formed a contractile actin ring encircling the damaged cell, changed the cellular aspect ratio, and immediately closed the barrier. Using traction force microscopy, we observed major forces at the ablation site and additional forces on the crypt sides. Inhibitors of the actomyosin-based mobility of the cells led to the failure of restoring the barrier. Close to the ablation site, high-frequency calcium flickering and propagation of calcium waves occured that synchronized with the contraction of the epithelial layer. We observed an increased signal and nuclear translocation of YAP-1. In conclusion, our approach enabled, for the first time, to unveil the intricacies of epithelial restitution beyond in vivo models by employing precise laser-induced damage in colonoids.

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