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In vivo fluorescence imaging of apoptosis during foreign body response. | LitMetric

In vivo fluorescence imaging of apoptosis during foreign body response.

Biomaterials

CrossBIT, Center for Biocompatibility and Implant-Immunology, Department of Orthopaedic Surgery, Hannover Medical School, Hannover, Germany.

Published: October 2012

AI Article Synopsis

  • A non-invasive fluorescence imaging method was developed to quantify apoptotic tissues during inflammation caused by implanted biomaterials in mice.
  • The study assessed the levels of apoptosis around titanium and copper-coated titanium discs at various time points (4, 8, and 23 days) to evaluate the biocompatibility of these materials.
  • Results from fluorescence imaging were validated against traditional histological methods, indicating that this technique could help minimize animal use in future biocompatibility research.

Article Abstract

Quantification of apoptotic tissues during inflammatory processes induced by biomaterials is challenging in vivo. Here we present a non-invasive method using a fluorescence imaging system which facilitates intermittent snap shots of the current state of local apoptotic tissue. For this purpose, apoptotic cells around two different subcutaneously implanted materials (titanium discs and copper-coated titanium discs) in hairless but immunocompetent mice were quantified after 4, 8 and 23 days of implantation. For validation, the results of fluorescence signals were compared to the histology of the inflammatory tissue using apoptotic-specific TUNEL-, macrophage-specific F4/80-, neutrophile-specific NIMP-R14- and chloroacetate esterase-staining. We could demonstrate that the fluorescence signals were well suited to quantify the extent of apoptosis in vivo and this is a good indication for the biocompatibility of biomaterials. This study shows that non-invasive monitoring of tissue processes following the implantation of biomaterials is possible in vivo and may help to reduce the number of animals in studies addressing biocompatibility.

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Source
http://dx.doi.org/10.1016/j.biomaterials.2012.06.039DOI Listing

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