Computer readable storage mediums, methods and systems for normalizing chemical profiles in biological or medical samples detected by mass spectrometry

We claim: 1. A method of analyzing a test sample of a material type via a mass spectrometry instrument, the method comprising the steps of: providing normalization data for a material type, the normalization data including one or more mass to charge (m/z) intensity ratios for one or more m/z features, the normalization data being based on at least one reference set of mass spectrometry data obtained from a first external standard sample including a first reference sample of the material type and one or more isotopic standards; receiving a first set of mass spectrometry data obtained from a test sample of a material type and the one or more isotopic standards analyzed by a mass spectrometry instrument, wherein the first set of mass spectrometry data comprises one or more m/z intensity ratios for each m/z feature; receiving at least a second set of mass spectrometry data obtained from a second external standard sample including a second reference sample of the material type and the one or more isotopic standards analyzed by the mass spectrometry instrument, wherein the second set of mass spectrometry data comprises one or more m/z intensity ratios; generating one or more m/z intensity ratio normalization factors using the second set of mass spectrometry data and the normalization data, each m/z intensity ratio normalization factor representing a response for the mass spectrometry instrument for each m/z feature; and generating normalized mass spectrometry data for the test sample using the one or more m/z intensity ratio normalization factors and the first set of mass spectrometry data, the normalized mass spectrometry data including a normalized intensity ratio for each m/z feature included in the test sample. 2. The method of claim 1 , wherein the first reference sample and the second reference sample are same, substantially the same or from a same biologically derived material. 3. The method of claim 1 , wherein each m/z feature refers to a portion of the at least one reference set of mass spectrometry data. 4. The method of claim 1 , further comprising: generating a normalization data table including the normalization data for the material type. 5. The method of claim 1 , further comprising: generating the normalization data, wherein the generating the normalization data includes: processing the at least one reference set of mass spectrometry data obtained from the first external standard sample to determine the m/z intensity ratios of each m/z feature for each isotropic standard; comparing the m/z intensity ratios for each m/z features with the m/z intensity ratios for the one or more isotopic standards to determine an intensity ratio coefficient of variation for the one or more m/z features; selecting a reference isotopic standard or a combination of reference isotopic standards for each m/z feature from the at least one reference set of mass spectrometry data based on the intensity ratio coefficient of variation; and generating the normalization data, wherein the normalization data includes the one or more m/z features from the at least one reference set of mass spectrometry data associated with at least each selected corresponding intensity ratio. 6. The method of claim 5 , wherein the step of receiving includes receiving a plurality of reference sets of mass spectrometry data. 7. The method of claim 5 , wherein the criteria for selecting the reference isotopic standard or the combination of reference isotopic standards for each m/z feature from the at least one reference set of mass spectrometry data includes a lowest intensity ratio coefficient of variation for that m/z feature. 8. The method of claim 1 , wherein the first, second and reference sets of mass spectrometry data comprise liquid chromatography-mass spectrometry data, gas chromatography-mass spectrometry data or Fourier transform mass spectrometry data, direct infusion mass spectrometry data, capillary electrophoresis mass spectrometry data, ion mobility shift mass spectrometry data, desorption electrospray ionization mass spectrometry data, nanostructure initiator mass spectrometry or matrix assisted mass spectrometry data. 9. The method of claim 1 , wherein concentrations of the one or more isotopic standards in the test sample, the first external standard sample and the second standard sample are the same. 10. The method of claim 1 , wherein the first reference sample, the test sample and the second reference sample is a biological fluid. 11. The method of claim 10 , wherein the first set of mass spectrometry data, the second set of mass spectrometry data and the normalization data comprise metabolomic data or metabonomic data. 12. The method of claim 1 , wherein the normalization data is received before or after the second set of mass spectrometry data, and wherein the second set of mass spectrometry data is received before or after the first set of mass spectrometry data. 13. The method of claim 1 , wherein the providing the normalization data includes providing a generated normalization data table and the providing the normalization data includes: receiving a mass spectrometry data set on a standard sample including one or more isotopic standards and a sample of the material type, the mass spectrometry data set comprising intensities for one or more m/z features and corresponding one or more isotopic standards; comparing intensities for the one or more m/z features with intensities for the one or more isotopic standards to determine a coefficient of variation for the one or more m/z features; determining a reference isotopic standard or a combination of reference isotopic standards for each of the one or more m/z features based on the coefficient of variation; and generating the normalization data table for the material type, the data table including one or more m/z entries corresponding to the one or more m/z features, wherein each m/z entry of the data table comprises an intensity ratio of the one or more m/z features divided by an intensity of the reference isotopic standard or the combination of reference isotopic standards for the one or more m/z features. 14. The method of claim 13 , wherein the step of receiving the mass spectrometry data is repeated one or more times. 15. The method of claim 14 , wherein the determining the reference isotopic standard or the combination of reference isotopic standards for each of the one or more m/z features is based on criteria for the coefficient of variation, and the criteria includes a lowest intensity ratio coefficient of variation for that m/z feature. 16. The method of claim 1 , wherein the mass spectrometry instrument is a liquid chromatography-mass spectrometry instrument. 17. A non-transitory computer readable storage medium for storing instructions for analyzing a test sample of a material type via mass spectrometry instrument, the instructions comprising: providing normalization data for a material type, the normalization data including one or more mass to charge (m/z) intensity ratios for one or more m/z features, the normalization data being based on at least one reference set of mass spectrometry data obtained from a first external standard sample including a first reference sample and one or more isotopic standards; receiving a first set of mass spectrometry data obtained from a test sample of the material type and the one or more isotopic standards analyzed by a mass spectrometry instrument, wherein the first set of mass spectrometry data comprises one or more m/z intensity ratios; receiving at least a second set of mass spectr