Nanotopographical Coatings Induce an Early Phenotype-Specific Response of Primary Material-Resident M1 and M2 Macrophages

Implants elicit an immunological response after implantation that results in the worst case in a complete implant rejection. This biomaterial-induced inflammation is modulated by macrophages and can be influenced by nanotopographical surface structures such as titania nanotubes or fractal titanium n...

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Main Authors: Tobias Schmitz, Maren Jannasch, Tobias Weigel, Claus Moseke, Uwe Gbureck, Jürgen Groll, Heike Walles, Jan Hansmann
Format: Article
Language:English
Published: MDPI AG 2020-03-01
Series:Materials
Subjects:
Online Access:https://www.mdpi.com/1996-1944/13/5/1142
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spelling doaj-4b3fb81da1a7401ba193da9cab2db99c2020-11-25T02:09:30ZengMDPI AGMaterials1996-19442020-03-01135114210.3390/ma13051142ma13051142Nanotopographical Coatings Induce an Early Phenotype-Specific Response of Primary Material-Resident M1 and M2 MacrophagesTobias Schmitz0Maren Jannasch1Tobias Weigel2Claus Moseke3Uwe Gbureck4Jürgen Groll5Heike Walles6Jan Hansmann7Department Tissue Engineering and Regenerative Medicine (TERM), University Hospital, 97070 Würzburg, GermanyDepartment Tissue Engineering and Regenerative Medicine (TERM), University Hospital, 97070 Würzburg, GermanyDepartment Tissue Engineering and Regenerative Medicine (TERM), University Hospital, 97070 Würzburg, GermanyInstitute for Biomedical Engineering (IBMT), University of Applied Sciences Mittelhessen (THM), 35390 Gießen, GermanyDepartment of Functional Materials in Medicine and Dentistry (FMZ), University Hospital, 97070 Würzburg, GermanyDepartment of Functional Materials in Medicine and Dentistry (FMZ), University Hospital, 97070 Würzburg, GermanyCore Facility Tissue Engineering, Otto von Guericke University, 39106 Magdeburg, GermanyDepartment Tissue Engineering and Regenerative Medicine (TERM), University Hospital, 97070 Würzburg, GermanyImplants elicit an immunological response after implantation that results in the worst case in a complete implant rejection. This biomaterial-induced inflammation is modulated by macrophages and can be influenced by nanotopographical surface structures such as titania nanotubes or fractal titanium nitride (TiN) surfaces. However, their specific impact on a distinct macrophage phenotype has not been identified. By using two different levels of nanostructures and smooth samples as controls, the influence of tubular TiO<sub>2</sub> and fractal TiN nanostructures on primary human macrophages with M1 or M2-phenotype was investigated. Therefore, nanotopographical coatings were either, directly generated by physical vapor deposition (PVD) or by electrochemical anodization of titanium PVD coatings. The cellular response of macrophages was quantitatively assessed to demonstrate a difference in biocompatibility of nanotubes in respect to human M1 and M2-macrophages. Depending on the tube diameter of the nanotubular surfaces, low cell numbers and impaired cellular activity, was detected for M2-macrophages, whereas the impact of nanotubes on M1-polarized macrophages was negligible. Importantly, we could confirm this phenotypic response on the fractal TiN surfaces. The results indicate that the investigated topographies specifically impact the macrophage M2-subtype that modulates the formation of the fibrotic capsule and the long-term response to an implant.https://www.mdpi.com/1996-1944/13/5/1142nanotopographical surfacescombination of physical vapor deposition and electrochemical etchingdefined humanized test systeminflammatory response
collection DOAJ
language English
format Article
sources DOAJ
author Tobias Schmitz
Maren Jannasch
Tobias Weigel
Claus Moseke
Uwe Gbureck
Jürgen Groll
Heike Walles
Jan Hansmann
spellingShingle Tobias Schmitz
Maren Jannasch
Tobias Weigel
Claus Moseke
Uwe Gbureck
Jürgen Groll
Heike Walles
Jan Hansmann
Nanotopographical Coatings Induce an Early Phenotype-Specific Response of Primary Material-Resident M1 and M2 Macrophages
Materials
nanotopographical surfaces
combination of physical vapor deposition and electrochemical etching
defined humanized test system
inflammatory response
author_facet Tobias Schmitz
Maren Jannasch
Tobias Weigel
Claus Moseke
Uwe Gbureck
Jürgen Groll
Heike Walles
Jan Hansmann
author_sort Tobias Schmitz
title Nanotopographical Coatings Induce an Early Phenotype-Specific Response of Primary Material-Resident M1 and M2 Macrophages
title_short Nanotopographical Coatings Induce an Early Phenotype-Specific Response of Primary Material-Resident M1 and M2 Macrophages
title_full Nanotopographical Coatings Induce an Early Phenotype-Specific Response of Primary Material-Resident M1 and M2 Macrophages
title_fullStr Nanotopographical Coatings Induce an Early Phenotype-Specific Response of Primary Material-Resident M1 and M2 Macrophages
title_full_unstemmed Nanotopographical Coatings Induce an Early Phenotype-Specific Response of Primary Material-Resident M1 and M2 Macrophages
title_sort nanotopographical coatings induce an early phenotype-specific response of primary material-resident m1 and m2 macrophages
publisher MDPI AG
series Materials
issn 1996-1944
publishDate 2020-03-01
description Implants elicit an immunological response after implantation that results in the worst case in a complete implant rejection. This biomaterial-induced inflammation is modulated by macrophages and can be influenced by nanotopographical surface structures such as titania nanotubes or fractal titanium nitride (TiN) surfaces. However, their specific impact on a distinct macrophage phenotype has not been identified. By using two different levels of nanostructures and smooth samples as controls, the influence of tubular TiO<sub>2</sub> and fractal TiN nanostructures on primary human macrophages with M1 or M2-phenotype was investigated. Therefore, nanotopographical coatings were either, directly generated by physical vapor deposition (PVD) or by electrochemical anodization of titanium PVD coatings. The cellular response of macrophages was quantitatively assessed to demonstrate a difference in biocompatibility of nanotubes in respect to human M1 and M2-macrophages. Depending on the tube diameter of the nanotubular surfaces, low cell numbers and impaired cellular activity, was detected for M2-macrophages, whereas the impact of nanotubes on M1-polarized macrophages was negligible. Importantly, we could confirm this phenotypic response on the fractal TiN surfaces. The results indicate that the investigated topographies specifically impact the macrophage M2-subtype that modulates the formation of the fibrotic capsule and the long-term response to an implant.
topic nanotopographical surfaces
combination of physical vapor deposition and electrochemical etching
defined humanized test system
inflammatory response
url https://www.mdpi.com/1996-1944/13/5/1142
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