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Direct Construction of Peaks from Free Induction Decay Curves for Gas Chromatography–Molecular Rotational Resonance Spectroscopy without Fourier Transforms

Authors :
Wahab, M. Farooq
Neill, Justin L.
Armstrong, Daniel W.
Source :
Analytical Chemistry; October 2022, Vol. 94 Issue: 42 p14611-14617, 7p
Publication Year :
2022

Abstract

The concept of coupling gas chromatography with molecular rotational resonance spectroscopy (GC-MRR) was introduced in 2020, combining the separation capabilities of GC with the unparalleled specificity of MRR. In this study, we address the challenge of the high data throughput of MRR spectrometers, as GC-MRR spectrometers can generate thousands to millions of data points per second. In the previous GC-MRR studies, a free induction decay (FID) measurement was Fourier transformed to generate each point on the chromatogram. Such extensive calculations limit the performance, sensitivity, and speed of GC-MRR. A direct approach is proposed here to extract peak intensity from FID using the Gram–Schmidt vector orthogonalization method. First, analyte-free FIDs are used to construct a basis set representing the instrument’s background noise, and then the remaining FIDs are orthogonalized to this fixed basis set. Each FID yields a single intensity value after Gram–Schmidt orthogonalization. The magnitude of the orthogonalized analyte FID is the signal intensity plotted in the chromatogram. This approach is computationally much faster (up to 10 times) than the conventional Fourier transform algorithm, is at least as sensitive as the FT algorithm, and maintains or improves the chromatographic peak shape. We compare the sensitivity, linearity, and chromatographic peak shapes for the Fourier transform and Gram–Schmidt approaches using both synthetically generated FIDs and instrumental data. This approach would allow the summed peak intensity to be displayed essentially in real-time, following which identified peaks can be further investigated to identify and quantify the species associated with each.

Details

Language :
English
ISSN :
00032700 and 15206882
Volume :
94
Issue :
42
Database :
Supplemental Index
Journal :
Analytical Chemistry
Publication Type :
Periodical
Accession number :
ejs60983283
Full Text :
https://doi.org/10.1021/acs.analchem.2c02535