Engineering Shape to Overcome Contraction: The Role of Polymer–Collagen Hybrids in Advanced Dermal Substitutes

Author:

Leon‐Valdivieso Christopher Y.12ORCID,Bethry Audrey1,Pinese Coline13,Dai Michèle4,Pompee Christian1,Pernot Jean‐Marc4,Garric Xavier13

Affiliation:

1. Polymers for Health and Biomaterials IBMM, University of Montpellier, CNRS, ENSCM Montpellier France

2. CARTIGEN University Hospital of Montpellier Montpellier France

3. Department of Pharmacy University Hospital of Nimes Nimes France

4. URGO Recherche Innovation et Développement Chenôve France

Abstract

ABSTRACTCollagen gels are the standard dermal equivalents par excellence, however the problem of rapid cell‐mediated contraction remains unresolved. Therefore, the development of hybrid constructs (HCs) based on collagen and polymeric scaffolds is proposed to address the mechanical instability that usually limits the formation of new, functional tissue. Equally important, these synthetic structures should be temporary (degradable) while ensuring that cells are well‐adapted to the new extracellular environment. In this study, we screened a library of scaffolds made of various polymers, including homopolymers of polycaprolactone (PCL) and poly D,L‐lactide (PLA50), their blends (PCL/PLA50), and copolymers (poly(D,L‐lactide‐co‐caprolactone), PCLLA50) to prepare HCs in a layer‐by‐layer fashion. The properties of polymers and copolymers along with their processability by electrospinning and 3D‐printing were evaluated. Then, we assessed the HCs resistance toward cell‐mediated contraction as well as the degradation of the polymeric scaffolds. Our results indicate that scaffolds with higher PLA50 content (e.g., PLA50 100%, PCL/PLA50 or PCLLA50, both at 50/50 caprolactone‐to‐D,L‐lactide molar ratio) presented more drawbacks in terms of handleability and processing, while those with greater PCL presence showed structural steadiness and ease to use. All the scaffolds integrated well with the collagen gel to form the corresponding HCs. With few exceptions, the HCs demonstrated good resistance to cell‐derived contraction over 3 weeks. Notably, HCs based on PCLLA50 90/10 (both versions, electrospun or 3D‐printed) performed best, showing only a 5%–17% area reduction compared to the 93% observed in collagen‐only gels. This copolymer displayed hydrolytic degradation depending on its shape, with up to 45% and 65% loss of molecular weight for the electrospun and 3D‐printed forms, respectively, correlating with their progressive change in mechanical features. HCs containing PCLLA50 90/10 also exhibited a better fibroblast distribution, enhanced myofibroblastic differentiation, and a three‐fold increase in cell proliferation (when the electrospun type was used) compared to collagen controls. These findings were instrumental in selecting a potential HC that might be used for future experiments in vivo.

Publisher

Wiley

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