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Molecular Origin of Blood-Based Infrared Spectroscopic Fingerprints*.

Liudmila VoroninaCristina LeonardoJohannes B MüllerPhilipp E GeyerMarinus HuberMichael TrubetskovKosmas V KepesidisJürgen BehrMatthias MannFerenc KrauszMihaela Žigman
Published in: Angewandte Chemie (International ed. in English) (2021)
Infrared spectroscopy of liquid biopsies is a time- and cost-effective approach that may advance biomedical diagnostics. However, the molecular nature of disease-related changes of infrared molecular fingerprints (IMFs) remains poorly understood, impeding the method's applicability. Here we probe 148 human blood sera and reveal the origin of the variations in their IMFs. To that end, we supplemented infrared spectroscopy with biochemical fractionation and proteomic profiling, providing molecular information about serum composition. Using lung cancer as an example of a medical condition, we demonstrate that the disease-related differences in IMFs are dominated by contributions from twelve highly abundant proteins-that, if used as a pattern, may be instrumental for detecting malignancy. Tying proteomic to spectral information and machine learning advances our understanding of the infrared spectra of liquid biopsies, a framework that could be applied to probing of any disease.
Keyphrases
  • machine learning
  • single molecule
  • endothelial cells
  • healthcare
  • single cell
  • molecular docking
  • health information
  • ionic liquid
  • magnetic resonance
  • computed tomography
  • dna methylation
  • induced pluripotent stem cells