Geometry-Driven Cell Organization Determines Tissue Growths in Scaffold Pores: Consequences for Fibronectin Organization

dc.bibliographicCitation.firstPagee73545eng
dc.bibliographicCitation.issue9eng
dc.bibliographicCitation.journalTitlePLoS ONEeng
dc.bibliographicCitation.volume8eng
dc.contributor.authorJoly, P.
dc.contributor.authorDuda, G.N.
dc.contributor.authorSchöne, M.
dc.contributor.authorWelzel, P.B.
dc.contributor.authorFreudenberg, U.
dc.contributor.authorWerner, C.
dc.contributor.authorPetersen, A.
dc.date.accessioned2020-11-20T17:21:06Z
dc.date.available2020-11-20T17:21:06Z
dc.date.issued2013
dc.description.abstractTo heal tissue defects, cells have to bridge gaps and generate new extracellular matrix (ECM). Macroporous scaffolds are frequently used to support the process of defect filling and thus foster tissue regeneration. Such biomaterials contain micro-voids (pores) that the cells fill with their own ECM over time. There is only limited knowledge on how pore geometry influences cell organization and matrix production, even though it is highly relevant for scaffold design. This study hypothesized that 1) a simple geometric description predicts cellular organization during pore filling at the cell level and that 2) pore closure results in a reorganization of ECM. Scaffolds with a broad distribution of pore sizes (macroporous starPEG-heparin cryogel) were used as a model system and seeded with primary fibroblasts. The strategies of cells to fill pores could be explained by a simple geometrical model considering cells as tensioned chords. The model matched qualitatively as well as quantitatively by means of cell number vs. open cross-sectional area for all pore sizes. The correlation between ECM location and cell position was higher when the pores were not filled with tissue (Pearson's coefficient ρ = 0.45±0.01) and reduced once the pores were closed (ρ = 0.26±0.04) indicating a reorganization of the cell/ECM network. Scaffold pore size directed the time required for pore closure and furthermore impacted the organization of the fibronectin matrix. Understanding how cells fill micro-voids will help to design biomaterial scaffolds that support the endogenous healing process and thus allow a fast filling of tissue defects.eng
dc.description.versionpublishedVersioneng
dc.identifier.urihttps://doi.org/10.34657/4568
dc.identifier.urihttps://oa.tib.eu/renate/handle/123456789/5939
dc.language.isoengeng
dc.publisherSan Francisco, CA : Public Library of Scienceeng
dc.relation.doihttps://doi.org/10.1371/journal.pone.0073545
dc.relation.issn1932-6203
dc.rights.licenseCC BY 3.0 Unportedeng
dc.rights.urihttps://creativecommons.org/licenses/by/3.0/eng
dc.subject.ddc570eng
dc.subject.otherbiomaterialeng
dc.subject.otherfibronectineng
dc.subject.otherheparineng
dc.subject.othertissue scaffoldeng
dc.subject.otherarticleeng
dc.subject.othercell counteng
dc.subject.othercell organizationeng
dc.subject.othercellular, subcellular and molecular biological phenomena and functionseng
dc.subject.othercontrolled studyeng
dc.subject.otherextracellular matrixeng
dc.subject.otherfibroblasteng
dc.subject.othergeometrical modeleng
dc.subject.otherhealingeng
dc.subject.otherhumaneng
dc.subject.otherhuman celleng
dc.subject.othermathematical modeleng
dc.subject.otherporosityeng
dc.subject.othertissue growtheng
dc.subject.othertissue injuryeng
dc.subject.othertissue regenerationeng
dc.subject.otherBiocompatible Materialseng
dc.subject.otherCell Proliferationeng
dc.subject.otherCells, Culturedeng
dc.subject.otherCryogelseng
dc.subject.otherExtracellular Matrixeng
dc.subject.otherFibroblastseng
dc.subject.otherFibronectinseng
dc.subject.otherHumanseng
dc.subject.otherPorosityeng
dc.subject.otherTissue Engineeringeng
dc.subject.otherTissue Scaffoldseng
dc.titleGeometry-Driven Cell Organization Determines Tissue Growths in Scaffold Pores: Consequences for Fibronectin Organizationeng
dc.typeArticleeng
dc.typeTexteng
tib.accessRightsopenAccesseng
wgl.contributorIPFeng
wgl.subjectBiowissenschaften/Biologieeng
wgl.typeZeitschriftenartikeleng
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