Descemet's Membrane Biomimetic Microtopography Differentiates Human Mesenchymal Stem Cells Into Corneal Endothelial-Like Cells.


Journal

Cornea
ISSN: 1536-4798
Titre abrégé: Cornea
Pays: United States
ID NLM: 8216186

Informations de publication

Date de publication:
Jan 2019
Historique:
pubmed: 12 10 2018
medline: 12 1 2019
entrez: 12 10 2018
Statut: ppublish

Résumé

Loss of corneal endothelial cells (CECs) bears disastrous consequences for the patient, including corneal clouding and blindness. Corneal transplantation is currently the only therapy for severe corneal disorders. However, the worldwide shortages of corneal donor material generate a strong demand for personalized stem cell-based alternative therapies. Because human mesenchymal stem cells are known to be sensitive to their mechanical environments, we investigated the mechanotransductive potential of Descemet membrane-like microtopography (DLT) to differentiate human mesenchymal stem cells into CEC-like cells. Master molds with inverted DLT were produced by 2-photon lithography (2-PL). To measure the mechanotransductive potential of DLT, mesenchymal stem cells were cultivated on silicone or collagen imprints with DLT. Changes in morphology were imaged, and changes in gene expression of CEC typical genes such as zonula occludens (ZO-1), sodium/potassium (Na/K)-ATPase, paired-like homeodomain 2 (PITX2), and collagen 8 (COL-8) were measured with real-time polymerase chain reaction. At least immunofluorescence analysis has been conducted to confirm gene data on the protein level. Adhesion of MSCs to DLT molded in silicone and particularly in collagen initiates polygonal morphology and monolayer formation and enhances not only transcription of CEC typical genes such as ZO-1, Na/K-ATPase, PITX2, and COL-8 but also expression of the corresponding proteins. Artificial reproduction of Descemet membrane with respect to topography and similar stiffness offers a potential innovative way to bioengineer a functional CEC monolayer from autologous stem cells.

Identifiants

pubmed: 30308581
doi: 10.1097/ICO.0000000000001765
pmc: PMC6282677
doi:

Types de publication

Journal Article

Langues

eng

Sous-ensembles de citation

IM

Pagination

110-119

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Auteurs

Angela Gutermuth (A)

Department for Applied Cell Biology, Fraunhofer Institute for Production Technology, Aachen, Germany.

Jessika Maassen (J)

Department for Applied Cell Biology, Fraunhofer Institute for Production Technology, Aachen, Germany.

Emely Harnisch (E)

Department for Applied Cell Biology, Fraunhofer Institute for Production Technology, Aachen, Germany.

Daniel Kuhlen (D)

Department for Applied Cell Biology, Fraunhofer Institute for Production Technology, Aachen, Germany.

Alexis Sauer-Budge (A)

Exponent, Department for Polymer Science & Materials Chemistry, Natick, MA.

Claudia Skazik-Voogt (C)

Department for Applied Cell Biology, Fraunhofer Institute for Production Technology, Aachen, Germany.

Katrin Engelmann (K)

Medical Center for Ophthalmology, Chemnitz, Germany.
Experimental Ophthalmology, Institute of Anatomy Dresden, Technical University of Dresden, Dresden, Germany.

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