The debate of whether a glass substrate can be used in Fourier
transform infrared spectroscopy is strongly linked to its potential
clinical application. Histopathology glass slides of 1 mm thickness
absorb the mid-IR spectrum in the rich fingerprint spectral region.
Thus, it is important to assess whether emerging IR techniques can
be employed to study biological samples placed on glass substrates.
For this purpose, we used optical photothermal infrared (O-PTIR) spectroscopy
to study for the first time malignant and non-malignant lung cells
with the purpose of identifying IR spectral differences between these
cells placed on standard pathology glass slides. The data in this
feasibility study showed that O-PTIR can be used to obtain good-quality
IR spectra from cells from both the lipid region (3000–2700
cm–1) and the fingerprint region between 1770 and
950 cm–1 but with glass contributions from 1350
to 950 cm–1. A new single-unit dual-range (C–H/FP)
quantum cascade laser (QCL) IR pump source was applied for the first
time, delivering a clear synergistic benefit to the classification
results. Furthermore, O-PTIR is able to distinguish between lung cancer
cells and non-malignant lung cells both in the lipid and fingerprint
regions. However, when these two spectral ranges are combined, classification
accuracies are enhanced with Random Forest modeling classification
accuracy results ranging from 96 to 99% across all three studied cell
lines. The methodology described here for the first time with a single-unit
dual-range QCL for O-PTIR on glass is another step toward its clinical
application in pathology.
Cardiovascular diseases are still among the leading causes of mortality and morbidity worldwide. The build-up of fatty plaques in the arteries, leading to atherosclerosis, is the most common cause of...
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