Controlling the 3D architecture of Self-Lifting Auto-generated Tissue Equivalents (SLATEs) for optimized corneal graft composition and stability

Ideally, biomaterials designed to play specific physical and physiological roles in vivo should comprise components and microarchitectures analogous to those of the native tissues they intend to replace. For that, implantable biomaterials need to be carefully designed to have the correct structural...

Descripción completa

Detalles Bibliográficos
Autores principales: Gouveia, Ricardo M., González-Andrades, Elena, Cardona, Juan C., González-Gallardo, Carmen, Ionescu, Ana M., Garzon, Ingrid, Alaminos, Miguel, González-Andrades, Miguel, Connon, Che J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier Science 2017
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5267636/
https://www.ncbi.nlm.nih.gov/pubmed/28092777
http://dx.doi.org/10.1016/j.biomaterials.2016.12.023
_version_ 1782500668094808064
author Gouveia, Ricardo M.
González-Andrades, Elena
Cardona, Juan C.
González-Gallardo, Carmen
Ionescu, Ana M.
Garzon, Ingrid
Alaminos, Miguel
González-Andrades, Miguel
Connon, Che J.
author_facet Gouveia, Ricardo M.
González-Andrades, Elena
Cardona, Juan C.
González-Gallardo, Carmen
Ionescu, Ana M.
Garzon, Ingrid
Alaminos, Miguel
González-Andrades, Miguel
Connon, Che J.
author_sort Gouveia, Ricardo M.
collection PubMed
description Ideally, biomaterials designed to play specific physical and physiological roles in vivo should comprise components and microarchitectures analogous to those of the native tissues they intend to replace. For that, implantable biomaterials need to be carefully designed to have the correct structural and compositional properties, which consequently impart their bio-function. In this study, we showed that the control of such properties can be defined from the bottom-up, using smart surface templates to modulate the structure, composition, and bio-mechanics of human transplantable tissues. Using multi-functional peptide amphiphile-coated surfaces with different anisotropies, we were able to control the phenotype of corneal stromal cells and instruct them to fabricate self-lifting tissues that closely emulated the native stromal lamellae of the human cornea. The type and arrangement of the extracellular matrix comprising these corneal stromal Self-Lifting Analogous Tissue Equivalents (SLATEs) were then evaluated in detail, and was shown to correlate with tissue function. Specifically, SLATEs comprising aligned collagen fibrils were shown to be significantly thicker, denser, and more resistant to proteolytic degradation compared to SLATEs formed with randomly-oriented constituents. In addition, SLATEs were highly transparent while providing increased absorption to near-UV radiation. Importantly, corneal stromal SLATEs were capable of constituting tissues with a higher-order complexity, either by creating thicker tissues through stacking or by serving as substrate to support a fully-differentiated, stratified corneal epithelium. SLATEs were also deemed safe as implants in a rabbit corneal model, being capable of integrating with the surrounding host tissue without provoking inflammation, neo-vascularization, or any other signs of rejection after a 9-months follow-up. This work thus paves the way for the de novo bio-fabrication of easy-retrievable, scaffold-free human tissues with controlled structural, compositional, and functional properties to replace corneal, as well as other, tissues.
format Online
Article
Text
id pubmed-5267636
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Elsevier Science
record_format MEDLINE/PubMed
spelling pubmed-52676362017-03-01 Controlling the 3D architecture of Self-Lifting Auto-generated Tissue Equivalents (SLATEs) for optimized corneal graft composition and stability Gouveia, Ricardo M. González-Andrades, Elena Cardona, Juan C. González-Gallardo, Carmen Ionescu, Ana M. Garzon, Ingrid Alaminos, Miguel González-Andrades, Miguel Connon, Che J. Biomaterials Article Ideally, biomaterials designed to play specific physical and physiological roles in vivo should comprise components and microarchitectures analogous to those of the native tissues they intend to replace. For that, implantable biomaterials need to be carefully designed to have the correct structural and compositional properties, which consequently impart their bio-function. In this study, we showed that the control of such properties can be defined from the bottom-up, using smart surface templates to modulate the structure, composition, and bio-mechanics of human transplantable tissues. Using multi-functional peptide amphiphile-coated surfaces with different anisotropies, we were able to control the phenotype of corneal stromal cells and instruct them to fabricate self-lifting tissues that closely emulated the native stromal lamellae of the human cornea. The type and arrangement of the extracellular matrix comprising these corneal stromal Self-Lifting Analogous Tissue Equivalents (SLATEs) were then evaluated in detail, and was shown to correlate with tissue function. Specifically, SLATEs comprising aligned collagen fibrils were shown to be significantly thicker, denser, and more resistant to proteolytic degradation compared to SLATEs formed with randomly-oriented constituents. In addition, SLATEs were highly transparent while providing increased absorption to near-UV radiation. Importantly, corneal stromal SLATEs were capable of constituting tissues with a higher-order complexity, either by creating thicker tissues through stacking or by serving as substrate to support a fully-differentiated, stratified corneal epithelium. SLATEs were also deemed safe as implants in a rabbit corneal model, being capable of integrating with the surrounding host tissue without provoking inflammation, neo-vascularization, or any other signs of rejection after a 9-months follow-up. This work thus paves the way for the de novo bio-fabrication of easy-retrievable, scaffold-free human tissues with controlled structural, compositional, and functional properties to replace corneal, as well as other, tissues. Elsevier Science 2017-03 /pmc/articles/PMC5267636/ /pubmed/28092777 http://dx.doi.org/10.1016/j.biomaterials.2016.12.023 Text en © 2017 The Authors http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Gouveia, Ricardo M.
González-Andrades, Elena
Cardona, Juan C.
González-Gallardo, Carmen
Ionescu, Ana M.
Garzon, Ingrid
Alaminos, Miguel
González-Andrades, Miguel
Connon, Che J.
Controlling the 3D architecture of Self-Lifting Auto-generated Tissue Equivalents (SLATEs) for optimized corneal graft composition and stability
title Controlling the 3D architecture of Self-Lifting Auto-generated Tissue Equivalents (SLATEs) for optimized corneal graft composition and stability
title_full Controlling the 3D architecture of Self-Lifting Auto-generated Tissue Equivalents (SLATEs) for optimized corneal graft composition and stability
title_fullStr Controlling the 3D architecture of Self-Lifting Auto-generated Tissue Equivalents (SLATEs) for optimized corneal graft composition and stability
title_full_unstemmed Controlling the 3D architecture of Self-Lifting Auto-generated Tissue Equivalents (SLATEs) for optimized corneal graft composition and stability
title_short Controlling the 3D architecture of Self-Lifting Auto-generated Tissue Equivalents (SLATEs) for optimized corneal graft composition and stability
title_sort controlling the 3d architecture of self-lifting auto-generated tissue equivalents (slates) for optimized corneal graft composition and stability
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5267636/
https://www.ncbi.nlm.nih.gov/pubmed/28092777
http://dx.doi.org/10.1016/j.biomaterials.2016.12.023
work_keys_str_mv AT gouveiaricardom controllingthe3darchitectureofselfliftingautogeneratedtissueequivalentsslatesforoptimizedcornealgraftcompositionandstability
AT gonzalezandradeselena controllingthe3darchitectureofselfliftingautogeneratedtissueequivalentsslatesforoptimizedcornealgraftcompositionandstability
AT cardonajuanc controllingthe3darchitectureofselfliftingautogeneratedtissueequivalentsslatesforoptimizedcornealgraftcompositionandstability
AT gonzalezgallardocarmen controllingthe3darchitectureofselfliftingautogeneratedtissueequivalentsslatesforoptimizedcornealgraftcompositionandstability
AT ionescuanam controllingthe3darchitectureofselfliftingautogeneratedtissueequivalentsslatesforoptimizedcornealgraftcompositionandstability
AT garzoningrid controllingthe3darchitectureofselfliftingautogeneratedtissueequivalentsslatesforoptimizedcornealgraftcompositionandstability
AT alaminosmiguel controllingthe3darchitectureofselfliftingautogeneratedtissueequivalentsslatesforoptimizedcornealgraftcompositionandstability
AT gonzalezandradesmiguel controllingthe3darchitectureofselfliftingautogeneratedtissueequivalentsslatesforoptimizedcornealgraftcompositionandstability
AT connonchej controllingthe3darchitectureofselfliftingautogeneratedtissueequivalentsslatesforoptimizedcornealgraftcompositionandstability

Ejemplares similares