Surface Immobilization Chemistry of a Laminin-Derived Peptide Affects Keratinocyte Activity

Surface Immobilization Chemistry of a Laminin-Derived Peptide Affects Keratinocyte Activity

Many chemical routes have been proposed to immobilize peptides on biomedical device surfaces, and in particular, on dental implants to prevent peri-implantitis. While a number of factors affect peptide immobilization quality, an easily controllable factor is the chemistry used to immobilize peptides...

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Main Authors: Nicholas G. Fischer, Jiahe He, Conrado Aparicio
Format: Article
Language:English
Published: MDPI AG 2020-06-01
Series:Coatings
Subjects:
surfaces
peptides
immobilization
keratinocytes
hemidesmosomes
dental implants
Online Access:https://www.mdpi.com/2079-6412/10/6/560
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spelling doaj-31e2479a5f674ba98c02845af429892f2020-11-25T03:24:10ZengMDPI AGCoatings2079-64122020-06-011056056010.3390/coatings10060560Surface Immobilization Chemistry of a Laminin-Derived Peptide Affects Keratinocyte ActivityNicholas G. Fischer0Jiahe He1Conrado Aparicio2Minnesota Dental Research Center for Biomaterials and Biomechanics, University of Minnesota, 515 Delaware Street S.E., Minneapolis, MN, 55455, USAMinnesota Dental Research Center for Biomaterials and Biomechanics, University of Minnesota, 515 Delaware Street S.E., Minneapolis, MN, 55455, USAMinnesota Dental Research Center for Biomaterials and Biomechanics, University of Minnesota, 515 Delaware Street S.E., Minneapolis, MN, 55455, USAMany chemical routes have been proposed to immobilize peptides on biomedical device surfaces, and in particular, on dental implants to prevent peri-implantitis. While a number of factors affect peptide immobilization quality, an easily controllable factor is the chemistry used to immobilize peptides. These factors affect peptide chemoselectivity, orientation, etc., and ultimately control biological activity. Using many different physical and chemical routes for peptide coatings, previous research has intensely focused on immobilizing antimicrobial elements on dental implants to reduce infection rates. Alternatively, our strategy here is different and focused on promoting formation of a long-lasting biological seal between the soft tissue and the implant surface through transmembrane, cell adhesion structures called hemidesmosomes. For that purpose, we used a laminin-derived call adhesion peptide. However, the effect of different immobilization chemistries on cell adhesion peptide activity is vastly unexplored but likely critical. Here, we compared the physiochemical properties and biological responses of a hemidesmosome promoting peptide immobilized using silanization and copper-free click chemistry as a model system for cell adhesion peptides. Successful immobilization was confirmed with water contact angle and X-ray photoelectron spectroscopy. Peptide coatings were retained through 73 days of incubation in artificial saliva. Interestingly, the non-chemoselective immobilization route, silanization, resulted in significantly higher proliferation and hemidesmosome formation in oral keratinocytes compared to chemoselective click chemistry. Our results highlight that the most effective immobilization chemistry for optimal peptide activity is dependent on the specific system (substrate/peptide/cell/biological activity) under study. Overall, a better understanding of the effects immobilization chemistries have on cell adhesion peptide activity may lead to more efficacious coatings for biomedical devices.https://www.mdpi.com/2079-6412/10/6/560surfacespeptidesimmobilizationkeratinocyteshemidesmosomesdental implants
collection DOAJ
language English
format Article
sources DOAJ
author Nicholas G. Fischer
Jiahe He
Conrado Aparicio
spellingShingle Nicholas G. Fischer
Jiahe He
Conrado Aparicio
Surface Immobilization Chemistry of a Laminin-Derived Peptide Affects Keratinocyte Activity
Coatings
surfaces
peptides
immobilization
keratinocytes
hemidesmosomes
dental implants
author_facet Nicholas G. Fischer
Jiahe He
Conrado Aparicio
author_sort Nicholas G. Fischer
title Surface Immobilization Chemistry of a Laminin-Derived Peptide Affects Keratinocyte Activity
title_short Surface Immobilization Chemistry of a Laminin-Derived Peptide Affects Keratinocyte Activity
title_full Surface Immobilization Chemistry of a Laminin-Derived Peptide Affects Keratinocyte Activity
title_fullStr Surface Immobilization Chemistry of a Laminin-Derived Peptide Affects Keratinocyte Activity
title_full_unstemmed Surface Immobilization Chemistry of a Laminin-Derived Peptide Affects Keratinocyte Activity
title_sort surface immobilization chemistry of a laminin-derived peptide affects keratinocyte activity
publisher MDPI AG
series Coatings
issn 2079-6412
publishDate 2020-06-01
description Many chemical routes have been proposed to immobilize peptides on biomedical device surfaces, and in particular, on dental implants to prevent peri-implantitis. While a number of factors affect peptide immobilization quality, an easily controllable factor is the chemistry used to immobilize peptides. These factors affect peptide chemoselectivity, orientation, etc., and ultimately control biological activity. Using many different physical and chemical routes for peptide coatings, previous research has intensely focused on immobilizing antimicrobial elements on dental implants to reduce infection rates. Alternatively, our strategy here is different and focused on promoting formation of a long-lasting biological seal between the soft tissue and the implant surface through transmembrane, cell adhesion structures called hemidesmosomes. For that purpose, we used a laminin-derived call adhesion peptide. However, the effect of different immobilization chemistries on cell adhesion peptide activity is vastly unexplored but likely critical. Here, we compared the physiochemical properties and biological responses of a hemidesmosome promoting peptide immobilized using silanization and copper-free click chemistry as a model system for cell adhesion peptides. Successful immobilization was confirmed with water contact angle and X-ray photoelectron spectroscopy. Peptide coatings were retained through 73 days of incubation in artificial saliva. Interestingly, the non-chemoselective immobilization route, silanization, resulted in significantly higher proliferation and hemidesmosome formation in oral keratinocytes compared to chemoselective click chemistry. Our results highlight that the most effective immobilization chemistry for optimal peptide activity is dependent on the specific system (substrate/peptide/cell/biological activity) under study. Overall, a better understanding of the effects immobilization chemistries have on cell adhesion peptide activity may lead to more efficacious coatings for biomedical devices.
topic surfaces
peptides
immobilization
keratinocytes
hemidesmosomes
dental implants
url https://www.mdpi.com/2079-6412/10/6/560
work_keys_str_mv AT nicholasgfischer surfaceimmobilizationchemistryofalamininderivedpeptideaffectskeratinocyteactivity
AT jiahehe surfaceimmobilizationchemistryofalamininderivedpeptideaffectskeratinocyteactivity
AT conradoaparicio surfaceimmobilizationchemistryofalamininderivedpeptideaffectskeratinocyteactivity
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