Fluorescence characteristics of human Barrett tissue specimens grafted on chick chorioallantoic membrane
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| Publication date | 01-2016 |
| Journal | Lasers in Medical Science |
| Volume | Issue number | 31 | 1 |
| Pages (from-to) | 137-144 |
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| Abstract |
To improve (pre)malignant lesion identification in Barrett’s esophagus
(BE), recent research focuses on new developments in fluorescence
imaging and spectroscopy to enhance tissue contrast. Our aim was to
validate the chorioallantoic membrane (CAM) model as a preclinical tool
to study the fluorescence characteristics such as autofluorescence and
exogenously induced fluorescence of human Barrett’s tissue. Therefore,
esophageal biopsy specimens from Barrett’s patients were freshly grafted
onto the CAM of fertilized hen’s eggs to simulate the in vivo
situation. The BE biopsy specimens stayed between 1 and 9 days on the
CAM to study the persistence of vitality. Fluorescence spectroscopy was
performed using six excitation wavelengths (369, 395, 400, 405, 410,
416 nm). Obtained autofluorescence spectra were compared with in vivo
spectra of an earlier study. Exogenous administration of
5-aminolevulinic-acid to the biopsy specimens was followed by
fluorescence spectroscopy at several time points. Afterwards, the biopsy
specimens were harvested and histologically evaluated. In total, 128
biopsy specimens obtained from 34 patients were grafted on the CAM.
Biopsy specimens which stayed on average 1.7 days on the CAM were still
vital. Autofluorescence spectra of the specimens correlated well with in
vivo spectra. Administered 5-aminolevulinic-acid to the biopsy
specimens showed conversion into protoporphyrin-IX. In conclusion, we
showed that grafting freshly collected human BE biopsy specimens on the
CAM is feasible. Our results suggest that the CAM model might be used to
study the fluorescence behavior of human tissue specimens. Therefore,
the CAM model might be a preclinical research tool for new
photosensitizers.
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| Document type | Article |
| Language | English |
| Published at | https://doi.org/10.1007/s10103-015-1839-x |
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