Modulation of macrophage phenotype through controlled release of interleukin-4 from gelatine coatings on titanium surfaces

Modulation of macrophage phenotype through controlled release of interleukin-4 from gelatine coatings on titanium surfaces

Pro-inflammatory phenotype (M1) macrophages initiate angiogenesis, while their prolonged activation can induce chronic inflammation. Anti-inflammatory phenotype (M2) macrophages promote vessel maturation and tissue regeneration. Biomaterials which can promote M2 polarisation after appropriate inflam...

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Bibliographic Details
Main Authors: CL Yang, YH Sun, WH Yu, XZ Yin, J Weng, B Feng
Format: Article
Language:English
Published: AO Research Institute Davos 2018-07-01
Series:European Cells & Materials
Subjects:
Genipin cross-linked gelatine
interleukin-4
controlled release
macrophage phenotype polarisation
inflammatory reaction.
Online Access:http://www.ecmjournal.org/papers/vol036/pdf/v036a02.pdf
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spelling doaj-82b2344518c348049e935cf089b888622020-11-24T20:45:57Zeng AO Research Institute DavosEuropean Cells & Materials1473-22622018-07-0136152910.22203/eCM.v036a02Modulation of macrophage phenotype through controlled release of interleukin-4 from gelatine coatings on titanium surfacesCL YangYH SunWH Yu XZ YinJ WengB Feng0Key Laboratory of Advanced Technology for Materials (Ministry of Education), School of Materials Science and Engineering, University of the Southwest Jiaotong University, Jinniu District, Chengdu, China.Pro-inflammatory phenotype (M1) macrophages initiate angiogenesis, while their prolonged activation can induce chronic inflammation. Anti-inflammatory phenotype (M2) macrophages promote vessel maturation and tissue regeneration. Biomaterials which can promote M2 polarisation after appropriate inflammation should enhance angiogenesis and wound healing. Herein, Interleukin-4 (IL-4), an anti-inflammatory cytokine, was adsorbed onto a titanium surface. Then, a genipin cross-linked gelatine hydrogel was coated onto the surface to delay IL-4 release. The cross-linking degree of the hydrogel was modulated by the different amount of genipin to control release of IL-4. When 0.7 wt% (weight %) genipin was used as a cross-linker, the sample (GG07-I) released less IL-4 within the first several days, followed by a sustained release time to 14 d. Meanwhile, the release rate of IL-4 in GG07-I reached a peak between 3 d and 7 d. In culture with macrophages in vitro, GG07-I and GG07 exhibited good cytocompatibility. The phenotypical switch of macrophages stimulated by the samples was determined by FACS, ELISA and PCR. Macrophages cultured with GG07-I, GG07 and PT were firstly activated to the M1 phenotype by interferon-gamma (IFN-γ). Then, due to the release of IL-4 in 5 to 7 d, GG07-I enhanced CD206, increased the secretion and gene expression of M2 marker, such as interleukin-10 (IL-10), arginase-1 (ARG-1) and platelet derived growth factor-BB (PDGF- BB). GG07-I prompted the switch from M1 to M2 phenotype. Those appropriate secretion of cytokines would benefit both vascularisation and osseointegration. Thus, the biomaterial directing inflammatory reaction has good prospects for clinical treatments.http://www.ecmjournal.org/papers/vol036/pdf/v036a02.pdfGenipin cross-linked gelatineinterleukin-4controlled releasemacrophage phenotype polarisationinflammatory reaction.
collection DOAJ
language English
format Article
sources DOAJ
author CL Yang
YH Sun
WH Yu
XZ Yin
J Weng
B Feng
spellingShingle CL Yang
YH Sun
WH Yu
XZ Yin
J Weng
B Feng
Modulation of macrophage phenotype through controlled release of interleukin-4 from gelatine coatings on titanium surfaces
European Cells & Materials
Genipin cross-linked gelatine
interleukin-4
controlled release
macrophage phenotype polarisation
inflammatory reaction.
author_facet CL Yang
YH Sun
WH Yu
XZ Yin
J Weng
B Feng
author_sort CL Yang
title Modulation of macrophage phenotype through controlled release of interleukin-4 from gelatine coatings on titanium surfaces
title_short Modulation of macrophage phenotype through controlled release of interleukin-4 from gelatine coatings on titanium surfaces
title_full Modulation of macrophage phenotype through controlled release of interleukin-4 from gelatine coatings on titanium surfaces
title_fullStr Modulation of macrophage phenotype through controlled release of interleukin-4 from gelatine coatings on titanium surfaces
title_full_unstemmed Modulation of macrophage phenotype through controlled release of interleukin-4 from gelatine coatings on titanium surfaces
title_sort modulation of macrophage phenotype through controlled release of interleukin-4 from gelatine coatings on titanium surfaces
publisher AO Research Institute Davos
series European Cells & Materials
issn 1473-2262
publishDate 2018-07-01
description Pro-inflammatory phenotype (M1) macrophages initiate angiogenesis, while their prolonged activation can induce chronic inflammation. Anti-inflammatory phenotype (M2) macrophages promote vessel maturation and tissue regeneration. Biomaterials which can promote M2 polarisation after appropriate inflammation should enhance angiogenesis and wound healing. Herein, Interleukin-4 (IL-4), an anti-inflammatory cytokine, was adsorbed onto a titanium surface. Then, a genipin cross-linked gelatine hydrogel was coated onto the surface to delay IL-4 release. The cross-linking degree of the hydrogel was modulated by the different amount of genipin to control release of IL-4. When 0.7 wt% (weight %) genipin was used as a cross-linker, the sample (GG07-I) released less IL-4 within the first several days, followed by a sustained release time to 14 d. Meanwhile, the release rate of IL-4 in GG07-I reached a peak between 3 d and 7 d. In culture with macrophages in vitro, GG07-I and GG07 exhibited good cytocompatibility. The phenotypical switch of macrophages stimulated by the samples was determined by FACS, ELISA and PCR. Macrophages cultured with GG07-I, GG07 and PT were firstly activated to the M1 phenotype by interferon-gamma (IFN-γ). Then, due to the release of IL-4 in 5 to 7 d, GG07-I enhanced CD206, increased the secretion and gene expression of M2 marker, such as interleukin-10 (IL-10), arginase-1 (ARG-1) and platelet derived growth factor-BB (PDGF- BB). GG07-I prompted the switch from M1 to M2 phenotype. Those appropriate secretion of cytokines would benefit both vascularisation and osseointegration. Thus, the biomaterial directing inflammatory reaction has good prospects for clinical treatments.
topic Genipin cross-linked gelatine
interleukin-4
controlled release
macrophage phenotype polarisation
inflammatory reaction.
url http://www.ecmjournal.org/papers/vol036/pdf/v036a02.pdf
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AT yhsun modulationofmacrophagephenotypethroughcontrolledreleaseofinterleukin4fromgelatinecoatingsontitaniumsurfaces
AT whyu modulationofmacrophagephenotypethroughcontrolledreleaseofinterleukin4fromgelatinecoatingsontitaniumsurfaces
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AT bfeng modulationofmacrophagephenotypethroughcontrolledreleaseofinterleukin4fromgelatinecoatingsontitaniumsurfaces
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