Abstract
Intramolecular carbon isotope ratios reflect the source of a compound and the reaction conditions prevailing during synthesis and degradation. We report here a method for determination of relative (Deltadelta13C) and absolute (delta13C) intramolecular isotope ratios using the volatile lactic acid analogue propylene glycol as a model compound, measured by on-line gas chromatography-pyrolysis coupled to GC-combustion-isotope ratio mass spectrometry. Pyrolytic fragmentation of about one-third of the analyte mass produces optimal fragments for isotopic analysis, from which relative isotope ratios (Deltadelta13C) are calculated according to guidelines presented previously. Calibration to obtain absolute isotope ratios is achieved by quantifying isotope fractionation during pyrolysis with an average fractionation factor, alpha, and evaluated by considering extremes in isotopic fractionation behavior. The method is demonstrated by calculating ranges of absolute intramolecular isotope ratios in four samples of propylene glycol. Relative and absolute isotope ratios were calculated with average precisions of SD(Deltadelta13C) <0.84 per thousand and SD(delta13C) <3.0 per thousand, respectively. The various fractionation scenarios produce an average delta(13)C range of 2 per thousand for each position in each sample. Relative isotope ratios revealed all four samples originated from unique sources, with samples A, B, and D only distinguishable at the position-specific level. Regardless of pyrolysis fractionation distribution, absolute isotope ratios showed a consistent pattern for all samples, with delta13C(3) > delta13C(2) > delta13C(1). The validity of the method was determined by examining the difference in relative isotope ratios calculated through two independent methods: Deltadelta13C calculated directly using previous methods and Deltadelta13C extracted from absolute isotope ratios. Deviation between the two Deltadelta13C values for all positions averaged 0.1-0.2 per thousand, with the smallest deviation obtained assuming equal fractionation across all fragment positions. This approach applies generally to all compounds analyzed by pyrolytic PSIA.
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