Presentation is loading. Please wait.

Presentation is loading. Please wait.

Multi-Analyte LC-MS/MS Methods – Best Practice.

Published byAugusta Horn Modified over 6 years ago

Similar presentations

Presentation on theme: "Multi-Analyte LC-MS/MS Methods – Best Practice."— Presentation transcript:

1 Multi-Analyte LC-MS/MS Methods – Best Practice.
Martin Danaher

2 Contents LC-MS/MS Overview LC-MS/MS Optimisation Method Validation
Specificity and selectivity Stability studies WLr and WLR Data quality checks Conclusions

3 LC-MS/MS Overview Sample manager Column oven Injector Pumps MS/MS
(QqQ) 3 3

4 LC-MS/MS instrumentation (HT)
Column manager: 4 columns Sample organizer: 10 trays Injector : 48 positions

5 Electrospray Ionisation

6 MS Optimisation MS Optimisation Rafoxanide: EF = C19H11Cl2I2NO3
MW: g/mol (average value) Monoisotopic Which polarity? Optimum cone voltages ESI voltage Temperatures

7 Information sources

8 Isotopic Distribution of Rafoxanide

9 MS/MS Optimisation Collision induced dissociation with inert gas e.g. N2 or Argon. Identify most abundant?? daughter or product ions Product ions must be selective Avoid neutral losses -18 (H2O) and -17 (OH) Avoid non-specific fragments: 91 m/z, 105 m/z and 121 m/z. Consult literature, see what others are using.

10 Chromatographic development
Generic scouting gradient M. Phase A 100% Aqueous M. Phase B Acetonitrile or Methanol Column: 100 × 2.1 mm Inject each mix at high concentration and optimise separation Evaluate the impact of different additives acids and salts Optimise additive concentrations

11 Start method validation

12 2002/657/EC Criteria

13 Specificity – Similar compounds
Inject analyte standard and internal standard separately (highest concentration). Check for interference in each analyte or IS trace Isobaric interference Cross-talk Carry-over

14 Isobaric interference

15 Cross-talk phenomenon

16 Isotopic Distribution of Rafoxanide

17 Selectivity – Matrix components
HPLC-FLD separation of analyte from the matrix peak.

18 Selectivity – Matrix components
LC-MS/MS – Matrix peaks not visible Co-eluting peaks, late eluting peaks, etc. Ion suppression or enhancement Potential Solutions: Clean-up Chromatographic separation Matrix matched standards SILs

19 Matrix Effects Study – Approach I
Post-column infusion of standards with blank matrix samples

20 Matrix Effects Study Example

21 Matrix Effects Study – Approach II
Spike a range of representative samples post extraction and compare with solvent standards. Calculate enhancement or suppression effects Calculate the precision Evaluate the impact of the use of internal standards

22 Importance of Chromatography

23 Importance of Chromatography

24 Method Validation Stability studies Limit of detection
Standard stability (3, 6, 12, 24, 36 months). Different storage conditions. Sample extracts – intermediate or in final injection solvent. Over 7 days or continuous injection Stability in matrix – spike samples and store for different periods of time (1, 2, 3, 4, 6, 8, 12, 26, 52 weeks) Limit of detection Limit of quantitation/Limit of Reporting

25 Method Validation Within laboratory repeatability
18 samples spiked at three different levels Repeat by the same analyst Within laboratory reproducibility Minimum of 18 “different” samples spike at three different levels Repeat on different days by the different analysts. Use different equipment if possible. CCα Calculate using WLR data.

26 Data quality Checks (qualitative)
Identification RT (5%)/RRT (2.5%) S/N >3 Identification points (3 or 4) Ion ratio

27 Data quality Checks (quantitative)
CCα Compare CCα with MRL. Big gap  more precise method needed. Calibrations Use weighted linear regression not through (0,0) Inject at start and end of batch. Drift <30%. Inject LOQ as a response check throughout the run. Drift <30%. Residuals ±20%. Minimum of five points on curve.

28 Data quality Checks (quantitative)
Trueness Precision For analyses carried out under repeatability conditions, the intra-laboratory CV would typically be between ½ and 2/3 of the above values.

29 Conclusions SANCO validation document presents complementary validation guidelines. Provides more practical information on routine analysis Interpretation of data quality. Elements in 2002/657/EC validation that should be retained. Good ideas e.g. Ccα Ambiguity around the validation approach Considered as being inflexible.

Download ppt "Multi-Analyte LC-MS/MS Methods – Best Practice."

Similar presentations

Dr. Birgit Schmauser, BfArM, Bonn

Dr. Birgit Schmauser, BfArM, Bonn
Validation of screening methods (2002/657/EC)

Validation of screening methods (2002/657/EC)
Analytical Method Development and Validation

Analytical Method Development and Validation
Gas Chromatography There an be many parts to a gas chromatography system but the basic components include: An injection system. A column (controllable.

Gas Chromatography There an be many parts to a gas chromatography system but the basic components include: An injection system. A column (controllable.
Chromatographic Process Provides the analyte transport. Immobile phase. Mixture of components dispersed in the mobile phase.

Chromatographic Process Provides the analyte transport. Immobile phase. Mixture of components dispersed in the mobile phase.
HPLC 1. Introduction 1.Introduction CHROMATOGRAPHY Chromatography basically involves the separation of mixtures due to differences in the distribution.

HPLC 1. Introduction 1.Introduction CHROMATOGRAPHY Chromatography basically involves the separation of mixtures due to differences in the distribution.
HPLC Coupled with Quadrupole Mass Spectrometry and Forensic Analysis of Cocaine.

HPLC Coupled with Quadrupole Mass Spectrometry and Forensic Analysis of Cocaine.
World Health Organization

World Health Organization
Figure 1. Influence of sample solvent on peak shape. The sample is dissolved in buffer with (a) 0%, (b) 30%, (c) 50%, and (d) 70% acetonitrile. Sample.

Figure 1. Influence of sample solvent on peak shape. The sample is dissolved in buffer with (a) 0%, (b) 30%, (c) 50%, and (d) 70% acetonitrile. Sample.
Lecture 8. GC/MS.

Lecture 8. GC/MS.
Tandem Mass Spectrometry Newborn Screening Quality Assurance and Control Instrument and Method Validation Gary Hoffman Wisconsin Newborn Screening Laboratory.

Tandem Mass Spectrometry Newborn Screening Quality Assurance and Control Instrument and Method Validation Gary Hoffman Wisconsin Newborn Screening Laboratory.
Kyiv, 2005-10-061 TRAINING WORKSHOP ON PHARMACEUTICAL QUALITY, GOOD MANUFACTURING PRACTICE & BIOEQUIVALENCE Validation of Analytical Methods Used For Bioequivalence.

Kyiv, TRAINING WORKSHOP ON PHARMACEUTICAL QUALITY, GOOD MANUFACTURING PRACTICE & BIOEQUIVALENCE Validation of Analytical Methods Used For Bioequivalence.
The following minimum specified ranges should be considered: Drug substance or a finished (drug) product 80 to 120 % of the test concentration Content.

The following minimum specified ranges should be considered: Drug substance or a finished (drug) product 80 to 120 % of the test concentration Content.
Analytical considerations

Analytical considerations
LC-MS/MS Analysis of Naphthenic Acids in Environmental Waters Coreen Hamilton, Million B. Woudneh & Guanghui Wang Presented at Workshop on Analytical Strategies.

LC-MS/MS Analysis of Naphthenic Acids in Environmental Waters Coreen Hamilton, Million B. Woudneh & Guanghui Wang Presented at Workshop on Analytical Strategies.
Quality Assurance How do you know your results are correct? How confident are you?

Quality Assurance How do you know your results are correct? How confident are you?
Polybrominated diphenyl ethers by HRGC/HRMS Coreen Hamilton Brian Fowler Louis Haviland Axys Analytical Services, Ltd.

Polybrominated diphenyl ethers by HRGC/HRMS Coreen Hamilton Brian Fowler Louis Haviland Axys Analytical Services, Ltd.
7000A GC-QQQ Applications Pesticides in Foods (1).

7000A GC-QQQ Applications Pesticides in Foods (1).
Combining and Choosing Analytical Techniques Chapter 8.

Combining and Choosing Analytical Techniques Chapter 8.
* CORRESPONDING AUTHOR Glucagon Bioanalysis by LC-MS: “Unprecedented Level of Sensitivity (10pg/mL) for a Novel Formulation” Jean-Nicholas Mess 1, Louis-Philippe.

* CORRESPONDING AUTHOR Glucagon Bioanalysis by LC-MS: “Unprecedented Level of Sensitivity (10pg/mL) for a Novel Formulation” Jean-Nicholas Mess 1, Louis-Philippe.

Similar presentations

Ads by Google