Linearity in GC/MS/MS analysis for Mutagen X using ion trap
Posted: Fri Aug 30, 2013 8:04 pm
Hello,
I am working on an analysis for Mutagen X (MX) and Mucochloric acid (MCA) using Mucobromic acid (MBA) as an internal standard. The analysis is by GC/MS with EI using a Varian 400 GC/MS which employs a Paul-style ion trap.
I am having trouble with the linearity of response on the instrument while running in GC/MS/MS. I have played around with the charge on the filament, the bonus to the EMV, and the number of ions I try to allow to enter the trap, and although optimizing these can improve my signal, the relationship between concentration and signal is never linear.
I have been preparing a calibration curve (note, I also need to derivatize the compounds by heating them at 70 at concentrations of 50 ppb to 2 ppm of MX. I can run these samples in GC/MS without fragmentation and can get a linear calibration curve over this concentration range.
A previous student was initially able to get relatively linear calibration curves for both compounds in GC/MS (with less than optimized conditions), but this seemed to degrade over time.
Is it possible that something has gotten dirty, and that this would effect GC/MS/MS operation but not GC/MS operation?
Any advice you could provide would be greatly appreciated.
Thanks so much,
Jules Carlson
I am working on an analysis for Mutagen X (MX) and Mucochloric acid (MCA) using Mucobromic acid (MBA) as an internal standard. The analysis is by GC/MS with EI using a Varian 400 GC/MS which employs a Paul-style ion trap.
I am having trouble with the linearity of response on the instrument while running in GC/MS/MS. I have played around with the charge on the filament, the bonus to the EMV, and the number of ions I try to allow to enter the trap, and although optimizing these can improve my signal, the relationship between concentration and signal is never linear.
I have been preparing a calibration curve (note, I also need to derivatize the compounds by heating them at 70 at concentrations of 50 ppb to 2 ppm of MX. I can run these samples in GC/MS without fragmentation and can get a linear calibration curve over this concentration range.
A previous student was initially able to get relatively linear calibration curves for both compounds in GC/MS (with less than optimized conditions), but this seemed to degrade over time.
Is it possible that something has gotten dirty, and that this would effect GC/MS/MS operation but not GC/MS operation?
Any advice you could provide would be greatly appreciated.
Thanks so much,
Jules Carlson