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Analysis of Biomarkers in Crude Oil Using the Agilent 7200 GC/Q-TOF

Applications | 2011 | Agilent TechnologiesInstrumentation
GC/MSD, GC/MS/MS, GC/HRMS, GC/Q-TOF
Industries
Energy & Chemicals
Manufacturer
Agilent Technologies

Summary

Significance of Biomarker Analysis in Crude Oil


Biomarkers such as dibenzothiophenes, hopanes, and steranes provide unique molecular fingerprints that support source identification, maturity assessment, and weathering studies of crude oil in both petrochemical and environmental applications. High-resolution analysis of these trace components enhances confidence in forensic investigations of oil spills and reservoir characterization.

Objectives and Study Overview


This study evaluates the performance of the Agilent 7200 GC/Q-TOF system for direct analysis of crude oil biomarkers without prior fractionation. Key aims include demonstrating accurate mass extraction for selective detection of sulfur-containing polycyclic aromatic hydrocarbons and triterpanes, and exploiting MS/MS mode to improve sensitivity for low-abundance steranes.

Methodology and Instrumentation


Crude oil samples were diluted in hexane (1 mg/mL) and injected on an Agilent 7890A GC coupled to a 7200 Q-TOF. Key instrumental settings:
  • Inlet: splitless at 300 °C, 1 µL injection
  • Column: DB-5MS (30 m × 0.25 mm, 0.25 µm)
  • Oven program: 50 °C (1 min) to 320 °C at 10 °C/min, hold 8 min
  • Carrier: He constant flow, 1.5 mL/min
  • Ionization: EI, full scan 40–500 Da at 5 Hz
  • MS/MS: precursor scan 40–500 Da, collision energy 10 eV

Main Results and Discussion


High–resolution extracted ion chromatograms (EICs) at exact masses (±5 ppm) enabled clear separation of dibenzothiophene (m/z 184.0341), methyl-DBTs (m/z 198.0498), and C2-DBTs (m/z 212.0645) from matrix interferences.

Accurate mass EICs of hopanes at m/z 191.1794 (±10 ppm) eliminated co-eluting background ions, revealing nor-hopane homologues between 26–30 min. For steranes, full-scan detection at m/z 400.4064 was limited by overlaps, but MS/MS monitoring of the 400 > 217.1951 transition delivered high selectivity and improved signal-to-noise ratios for ethylcholestane isomers.

Benefits and Practical Applications


  • Eliminates time-consuming fractionation steps by direct injection of diluted crude oil.
  • High mass accuracy (<2 ppm) enhances selectivity and reduces false positives.
  • MS/MS functionality permits confident detection of low-level biomarkers in complex matrices.
  • Supports both targeted and untargeted screening workflows in environmental forensics and reservoir studies.

Future Trends and Potential Applications


Continued advances in high-resolution MS will enable deeper profiling of novel biomarker classes, including heteroatom-rich compounds. Integration with data-mining algorithms and suspect screening libraries will broaden untargeted discovery. Portable or miniaturized TOF instruments may eventually facilitate on-site crude oil fingerprinting for rapid spill response.

Conclusion


The Agilent 7200 GC/Q-TOF platform streamlines crude oil biomarker analysis by combining accurate mass full-scan with MS/MS selectivity. This approach delivers robust, high-throughput detection of DBTs, hopanes, and steranes directly from a diluted matrix, eliminating pre-fractionation and improving analytical confidence for petrochemical and environmental investigations.

References


  1. Wang Z., Fingas M., Developments in the analysis of petroleum hydrocarbons in oils, petroleum products and oil-spill-related environmental samples by gas chromatography, J. Chromatogr. A, 774 (1997) 51–78.
  2. Wang Z., Fingas M., Yang C., Hollebone B., Biomarker Fingerprinting: Application and Limitation for Correlation and Source Identification of Oils and Petroleum Products, Prep. Pap.-Am. Chem. Soc., Div. Fuel Chem. 49(1) (2004) 331–334.

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