" Molecular and Cellular dynamics of the Healing
Response Associated
with Implanted Expanded Polytetrafluoroethylene"
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Abstract:Implantation of biomaterials leads to the formation
of an avascular, fibrotic capsule that isolates the implant from
the surrounding tissue. Previous studies have demonstrated
that ECM-modification of ePTFE promotes increased vascularity
and decreased fibrosity in peri-implant tissue, two desired characteristics
of engineered medical devices. However, little is known
as to what is happening at the molecular level in tissue surrounding
both ECM-modified and non-modified ePTFE during the healing process,
or for that matter, what cellular pathway is responsible for
the increased vascularity and improved healing response. Large-scale
gene expression analysis using DNA microarrays was used to assemble
gene expression patterns of peri-implant tissue. This data
revealed that tissue surrounding ECM-modified ePTFE is more transcriptionally
dynamic than tissue surrounding non-modified ePTFE. The
microarray data also exposed a set of macrophage-relevant genes
that directed investigation into how the ECM modification of
ePTFE affected macrophage activation. It was demonstrated
that ECM proteins secreted by the keratincocyte cell line HaCaT
promoted fusion of macrophages to form multinucleated foreign
body giant cells (FBGC’s), as more FBGC’s were seen
at the material-tissue interface of the ECM modified ePTFE. The
results of this work suggest a molecular mechanism through which
ECM proteins induce FBGC formation. Taken together, this
research advances the knowledge of material-associated healing
which will lead to the improved biocompatibility of implanted
medical devices.
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