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The world leader in serving science
Using Automated Software for Improved
Results in GC Triple Quadrupole MS
Pesticide Analysis
Jason Cole and Paul Silcock
Thermo Fisher Scientific
2
Triple Quadrupole GC-MS/MS
Fast becoming an essential tool
in high-throughput, routine
laboratories
• Especially true for laboratories
performing pesticides analysis
in food
• Becoming more so in
environmental analysis
• Mainly driven by the selectivity
advantages of MS/MS
3
http://books.google.com/ngrams 5.2 million books: ~4% of
all books ever published
4
5
GC-MS/MS – What’s So Special?
• Low detection limits
• Optimized sample
preparation
• Consolidated analytical
methods
• Faster, automated data
processing
...it’s a high
selectivity
technique...
6
Selectivity in a Method
McLafferty circa. 1980
7
Method Performance Requirement
• Target compounds
• Matrices
• Sensitivity
Method
performance
requirement
8
First - Sample Prep..
Step1–extraction
Step2-cleanup(1st)
Step3-cleanup(2nd)
Method
performance
requirement
9
...then Instrument Detection...
Step1–extraction
Step2-cleanup(1st)
Step3-cleanup(2nd)
Step4-GC-MSdetection(singlequadSIM)
Total method selectivity
Method
performance
requirement
10
...What about GC-MS/MS?...
Step1–extraction
Step2-cleanup(1st)
Step3-cleanup(2nd)
Total method selectivity
Step4-GC-MS/MSdetection(TriplequadSRM)
Method
performance
requirement
11
...Use GC-MS/MS to Reduce Clean-Up...
Step1–extraction
Total method selectivity
Step2-GC-MS/MSdetection(TriplequadSRM)
Method
performance
requirement
12
...Use GC-MS/MS to Consolidate Methods...
Step1–extraction
Total method selectivity
Step2-GC-MS/MSdetection(TriplequadSRM)
Method 1
performance
requirement
Method 2
performance
requirement
Method 3
performance
requirement
13
...Use GC-MS/MS to Consolidate Methods...
Step1–extraction
Total method selectivity
Step2-GC-MS/MSdetection(TriplequadSRM)
Consolidated
multi-residue
method
14
...so GC-MS/MS is Special as it Delivers...
High Selectivity
• Possibility to reduce
selectivity in sample
preparation
• Reduced sample prep steps
create a more generic
sample prep method – more
compounds & matrices
• Consolidated GC-MS
methods due to high
performance – buffer
against requirements
• Compressed
chromatography possible
• Easy peak evaluation –
auto-integrators
15
...and often in Pesticides Analysis Leads to...
High Selectivity
• Possibility to reduce
selectivity in sample
preparation
• Reduced sample prep steps
create a more generic
sample prep method – more
compounds & matrices
• Consolidated GC-MS
methods due to high
performance – buffer
against requirements
• Compressed
chromatography possible
• Easy peak evaluation –
auto-integrators
16
Why are we here today?
Discussion of the practical issues that
arise in the lab due to the extra
capability GC-MS/MS brings and nature
of the technique
• Most people working with this
instrumentation are looking for ways to
easily create, optimize and manage in
routine large multi-residue GC-MS/MS
methods
• Also, improve analytical performance in
pesticides analysis
17
Practical Issues?
The power of the technique
is great, but...
• We are consolidating more
and more compounds into a
single method
• We are having to develop
100s of Selected Reaction
Monitoring (SRM)
transitions
• We are having to maintain
and manage large, high
performance methods – in
routine!
• All this, in a variety of
complex matrices
18
What’s Really Needed...
To really benefit from the
productivity advantages
of these multi-residue
methodologies, we need
to:
• Create complex methods -
independent of where we
begin
• Manage all the complex
information associated with
large complex methods
• Maintain these methods in
routine
• Ensure we are not creating
a new bottleneck!
19
Demonstrate how we can
use automated software
• Integrated into the set-up
and operation of the GC-
MS/MS system
• Remove the pain (and avoid
the bottleneck)
• Method creation
• Method optimization
• Method management
• Method maintenance
• For improved results (and
productivity) in pesticide
analysis
20
Enabling Technology
“To make the productivity
advantages of high performance
GC-MS/MS easy to achieve and
available routinely; especially for
high-throughput laboratories.”
21
22
Anatomy of a Multi-Residue Pesticide Method
Peaks!
• Lots of them, too
• Multiple ions (SRM transitions)
• Multiple co-elutions
• Not much “clear baseline”
• Diverse chemistries
• Also chemistry similarities
• Large difference in response factors
• Different LOD requirements
• Different interference (matrix)
pressures
• COMPLEXITY!!
23
Complexity in Developing Multi-Residue MRM
Methods
15. Run sequence
16. Examine each data compounds product ion
spectrum in each run for each collision energy.
17. (Re-inject for any missed compounds)
18. Recording of best SRM transitions
19. Create MRM method to optimize collision
energies
20. Create a pilot method(s) – to test selectivity of
transitions in target matrices.
21. Choose final transitions
22. Segment method
23. Calculate appropriate dwell times (depending
of number of overlapping transitions)
24. Test final method in matrix.
25. Check for “chopped” or missed peaks
26. Re-adjust method as necessary
1. List compounds (350 pesticides)
2. Arrange standard solutions into vial (s)
3. Set-up GC method
4. Run a full-scan
5. Examine data files to find compounds
(extracting ions or using libraries)
6. Record retention times
7. Select and record appropriate pre-cursor ions
8. Create product ion scan methods
9. Segment these methods into windows based
on chromatogram
10. Calculate appropriate scan times for good
daughter ion experiments
11. Re-segment based on (10)
12. Set-up these methods for all collision energies
to see progressive fragmentation
13. Decide on number of injections
14. Set-up sequence list
24
Instrument & Data Processing Method Maintenance
• GC-MS/MS systems in routine
pesticide analysis face high
volumes of samples with high
matrix load
• Cumulative deterioration of the GC
column performance
• Backflushing set-up can help to
mitigate
• Inevitably compound retention
times drift and or GC columns need
to be cut or replaced
• Need to locate compounds, update
acquisition windows & update RT in
data processing method
• Very laborious & time consuming-
worse with a large method!
25
Demonstrate how we can
use automated software
• Integrated into the set-up
and operation of the GC-
MS/MS system
• Remove the pain (and avoid
the bottleneck)
• Method creation
• Method optimization
• Method management
• Method maintenance
• For improved results (and
productivity) in pesticide
analysis
26
Software Overview
Automated SRM Development
Timed-SRM Instrument Method
Batch Acquisition, Data Review, and
reporting software
27
Complexity in Developing Multi-Residue MRM
Methods
15. Run sequence
16. Examine each data compounds product ion
spectrum in each run for each collision energy.
17. (Re-inject for any missed compounds)
18. Initial selection of best SRM transitions
19. Create a pilot method(s) – to test selectivity of
transitions in target matrices.
20. Choose final transitions
21. Segment method
22. Calculate appropriate dwell times (depending
of number of overlapping transitions)
23. Test final method in matrix.
24. Check for “chopped” or missed peaks
25. Re-adjust method as necessary
1. List compounds (350 pesticides)
2. Arrange standard solutions into vial (s)
3. Set-up GC method
4. Run a full-scan
5. Examine data files to find compounds
(extracting ions or using libraries)
6. Record retention times
7. Select and record appropriate pre-cursor ions
8. Create product ion scan methods
9. Segment these methods into windows based
on chromatogram
10. Calculate appropriate scans times for good
daughter ion experiments
11. Re-segment based on (9)
12. Set-up these methods for all collision energies
to see progressive fragmentation
13. Decide on number of injections
14. Set-up sequence list
28
Surely, we have these pesticide transitions already!?
29
Surely, we have these pesticide transitions already!?
Of course!
30
Thermo Scientific TraceFinder Compound Data
Store
31
Compound-Based Method Creation
Selecting your compounds
from CDS…
and processing methods
populates synced acquisition…
32
Thoughts on Fishing and Triple Quadrupoles
"Give a man a fish; feed him for a day. Teach
a man to fish; feed him for a lifetime“
Lao Tzu circa. 5th Century BC
33
Thoughts on Fishing and Triple Quadrupoles
"Give a man a fish; feed him for a day. Teach
a man to fish; feed him for a lifetime“
Lao Tzu circa. 5th Century BC
34
AutoSRM Overview
1) Precursor ion selection
2) Product ion
selection
3) Collision
energy
optimization
SRMCreationWorkflow
35
Step 1 – Pick Your Precursor Ions
36
Step 1 – Pick Your Precursor Ions
37
Step 1 – Pick Your Precursor Ions
38
Step 2 – Pick Your Product Ions
39
Step 2 – Pick Your Product Ions
40
Step 3 – Optimize Your Transitions
41
Step 3 – Optimize Your Transitions
42
AutoSRM Use Case
• Created and optimized > 250 transitions for > 80 compounds
• Minimal user interaction over 24 hours
43
Export from AutoSRM to Instrument Method
44
Timed-SRM Method Overview
45
Timed-SRM Method Overview
Acquisition
windows centered
around retention
time
46
Timed-SRM Method Overview
Acquisition
windows allowed
to overlap
47
Timed-SRM Advantages
Segmented SRM
Timed SRM
48
Timed-SRM Advantages
Acquisition Windows
Segmented SRM
Timed SRM
49
Timed-SRM Advantages
• Removes wasted dwell time
• Allow higher overall dwell times
• Leads to higher sensitivity
Wasted Dwell Time
50
Timed-SRM Advantages
• Peaks centered in acquisition window
• No peak elutes near acquisition break
• Allows for retention time shift (e.g. due to heavy matrix)
51
Thermo Scientific TSQ 8000 GC-MS/MS Timed-SRM
Case Study
• Previous method: Segmented SIM
acquisition on single quad
• Required five injections for full
list of pesticides
• Needed to analyze more
pesticides (350 total), but current
methodology took too long
• Wanted to consolidate to a single
injection
52
• Segmented SRM
• Closest compound to segment
break:
5 seconds
• Average number of simultaneous
transitions:
55
• Timed SRM
• Closest compound to segment
break:
15 seconds
• Average number of simultaneous
transitions:
15 (4X higher dwell times)
TSQ™ 8000 GC-MS/MS Timed-SRM Case Study
53
TSQ 8000 GC-MS/MS Timed-SRM Case Study
Tea Analysis: 4 pg on-column
Terbacil
Alachlor
Tolylfluanid
Pyridaben
54
Export from Instrument Method to TraceFinder™
Software
55
TraceFinder Software Overview
Batch Creation
Data Review
Report Generation
Routine Workflow
56
Instrument & Data Processing Method Maintenance
• GC-MS/MS systems in routine
pesticide analysis face high
volumes of samples with high
matrix load
• Cumulative deterioration of the GC
column performance
• Backflushing set-up can help to
mitigate
• Inevitably compound retention
times drift and or GC columns need
to be cut or replaced
• Need to locate compounds, update
acquisition windows & update RT in
data processing method
• Very laborious & time consuming-
worse with a large method!
57
TraceFinder Software Method Sync
• Links TraceFinder Software Method with instrument
method
• Enables
• Compound based acquisition setup
• Automated update of acquisition windows
58
Method Sync – Automated RT Update
Updating retention times in data review…
59
Method Sync – Automated RT Update
…updates both TraceFinder Software Method and
Timed-SRM Method
60
Summary
We can use integrated and
automated software
• Easily adopt large multi-
residue methods
• Remove the pain (and avoid
bottlenecks)
• Method creation
• Method optimization
• Method management
• Method maintenance
• To create improved results
(and productivity) in routine
pesticide analysis
61
Thank You for Your Attention!
Questions?
Stay connected with us
Twitter
@ChromSolutions
Chromatography Solutions Blog
http://chromblog.thermoscientific.com/blog
YouTube
http://www.youtube.com/ChromSolutions
Facebook
http://www.facebook.com/Chromatography
Solutions
Pinterest
http://pinterest.com/chromsolutions/

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Automated Software for Improved Results in Triple Quadrupole Gas Chromatography-Mass Spectrometry Pesticide Analysis

  • 1. 1 The world leader in serving science Using Automated Software for Improved Results in GC Triple Quadrupole MS Pesticide Analysis Jason Cole and Paul Silcock Thermo Fisher Scientific
  • 2. 2 Triple Quadrupole GC-MS/MS Fast becoming an essential tool in high-throughput, routine laboratories • Especially true for laboratories performing pesticides analysis in food • Becoming more so in environmental analysis • Mainly driven by the selectivity advantages of MS/MS
  • 3. 3 http://books.google.com/ngrams 5.2 million books: ~4% of all books ever published
  • 4. 4
  • 5. 5 GC-MS/MS – What’s So Special? • Low detection limits • Optimized sample preparation • Consolidated analytical methods • Faster, automated data processing ...it’s a high selectivity technique...
  • 6. 6 Selectivity in a Method McLafferty circa. 1980
  • 7. 7 Method Performance Requirement • Target compounds • Matrices • Sensitivity Method performance requirement
  • 8. 8 First - Sample Prep.. Step1–extraction Step2-cleanup(1st) Step3-cleanup(2nd) Method performance requirement
  • 10. 10 ...What about GC-MS/MS?... Step1–extraction Step2-cleanup(1st) Step3-cleanup(2nd) Total method selectivity Step4-GC-MS/MSdetection(TriplequadSRM) Method performance requirement
  • 11. 11 ...Use GC-MS/MS to Reduce Clean-Up... Step1–extraction Total method selectivity Step2-GC-MS/MSdetection(TriplequadSRM) Method performance requirement
  • 12. 12 ...Use GC-MS/MS to Consolidate Methods... Step1–extraction Total method selectivity Step2-GC-MS/MSdetection(TriplequadSRM) Method 1 performance requirement Method 2 performance requirement Method 3 performance requirement
  • 13. 13 ...Use GC-MS/MS to Consolidate Methods... Step1–extraction Total method selectivity Step2-GC-MS/MSdetection(TriplequadSRM) Consolidated multi-residue method
  • 14. 14 ...so GC-MS/MS is Special as it Delivers... High Selectivity • Possibility to reduce selectivity in sample preparation • Reduced sample prep steps create a more generic sample prep method – more compounds & matrices • Consolidated GC-MS methods due to high performance – buffer against requirements • Compressed chromatography possible • Easy peak evaluation – auto-integrators
  • 15. 15 ...and often in Pesticides Analysis Leads to... High Selectivity • Possibility to reduce selectivity in sample preparation • Reduced sample prep steps create a more generic sample prep method – more compounds & matrices • Consolidated GC-MS methods due to high performance – buffer against requirements • Compressed chromatography possible • Easy peak evaluation – auto-integrators
  • 16. 16 Why are we here today? Discussion of the practical issues that arise in the lab due to the extra capability GC-MS/MS brings and nature of the technique • Most people working with this instrumentation are looking for ways to easily create, optimize and manage in routine large multi-residue GC-MS/MS methods • Also, improve analytical performance in pesticides analysis
  • 17. 17 Practical Issues? The power of the technique is great, but... • We are consolidating more and more compounds into a single method • We are having to develop 100s of Selected Reaction Monitoring (SRM) transitions • We are having to maintain and manage large, high performance methods – in routine! • All this, in a variety of complex matrices
  • 18. 18 What’s Really Needed... To really benefit from the productivity advantages of these multi-residue methodologies, we need to: • Create complex methods - independent of where we begin • Manage all the complex information associated with large complex methods • Maintain these methods in routine • Ensure we are not creating a new bottleneck!
  • 19. 19 Demonstrate how we can use automated software • Integrated into the set-up and operation of the GC- MS/MS system • Remove the pain (and avoid the bottleneck) • Method creation • Method optimization • Method management • Method maintenance • For improved results (and productivity) in pesticide analysis
  • 20. 20 Enabling Technology “To make the productivity advantages of high performance GC-MS/MS easy to achieve and available routinely; especially for high-throughput laboratories.”
  • 21. 21
  • 22. 22 Anatomy of a Multi-Residue Pesticide Method Peaks! • Lots of them, too • Multiple ions (SRM transitions) • Multiple co-elutions • Not much “clear baseline” • Diverse chemistries • Also chemistry similarities • Large difference in response factors • Different LOD requirements • Different interference (matrix) pressures • COMPLEXITY!!
  • 23. 23 Complexity in Developing Multi-Residue MRM Methods 15. Run sequence 16. Examine each data compounds product ion spectrum in each run for each collision energy. 17. (Re-inject for any missed compounds) 18. Recording of best SRM transitions 19. Create MRM method to optimize collision energies 20. Create a pilot method(s) – to test selectivity of transitions in target matrices. 21. Choose final transitions 22. Segment method 23. Calculate appropriate dwell times (depending of number of overlapping transitions) 24. Test final method in matrix. 25. Check for “chopped” or missed peaks 26. Re-adjust method as necessary 1. List compounds (350 pesticides) 2. Arrange standard solutions into vial (s) 3. Set-up GC method 4. Run a full-scan 5. Examine data files to find compounds (extracting ions or using libraries) 6. Record retention times 7. Select and record appropriate pre-cursor ions 8. Create product ion scan methods 9. Segment these methods into windows based on chromatogram 10. Calculate appropriate scan times for good daughter ion experiments 11. Re-segment based on (10) 12. Set-up these methods for all collision energies to see progressive fragmentation 13. Decide on number of injections 14. Set-up sequence list
  • 24. 24 Instrument & Data Processing Method Maintenance • GC-MS/MS systems in routine pesticide analysis face high volumes of samples with high matrix load • Cumulative deterioration of the GC column performance • Backflushing set-up can help to mitigate • Inevitably compound retention times drift and or GC columns need to be cut or replaced • Need to locate compounds, update acquisition windows & update RT in data processing method • Very laborious & time consuming- worse with a large method!
  • 25. 25 Demonstrate how we can use automated software • Integrated into the set-up and operation of the GC- MS/MS system • Remove the pain (and avoid the bottleneck) • Method creation • Method optimization • Method management • Method maintenance • For improved results (and productivity) in pesticide analysis
  • 26. 26 Software Overview Automated SRM Development Timed-SRM Instrument Method Batch Acquisition, Data Review, and reporting software
  • 27. 27 Complexity in Developing Multi-Residue MRM Methods 15. Run sequence 16. Examine each data compounds product ion spectrum in each run for each collision energy. 17. (Re-inject for any missed compounds) 18. Initial selection of best SRM transitions 19. Create a pilot method(s) – to test selectivity of transitions in target matrices. 20. Choose final transitions 21. Segment method 22. Calculate appropriate dwell times (depending of number of overlapping transitions) 23. Test final method in matrix. 24. Check for “chopped” or missed peaks 25. Re-adjust method as necessary 1. List compounds (350 pesticides) 2. Arrange standard solutions into vial (s) 3. Set-up GC method 4. Run a full-scan 5. Examine data files to find compounds (extracting ions or using libraries) 6. Record retention times 7. Select and record appropriate pre-cursor ions 8. Create product ion scan methods 9. Segment these methods into windows based on chromatogram 10. Calculate appropriate scans times for good daughter ion experiments 11. Re-segment based on (9) 12. Set-up these methods for all collision energies to see progressive fragmentation 13. Decide on number of injections 14. Set-up sequence list
  • 28. 28 Surely, we have these pesticide transitions already!?
  • 29. 29 Surely, we have these pesticide transitions already!? Of course!
  • 30. 30 Thermo Scientific TraceFinder Compound Data Store
  • 31. 31 Compound-Based Method Creation Selecting your compounds from CDS… and processing methods populates synced acquisition…
  • 32. 32 Thoughts on Fishing and Triple Quadrupoles "Give a man a fish; feed him for a day. Teach a man to fish; feed him for a lifetime“ Lao Tzu circa. 5th Century BC
  • 33. 33 Thoughts on Fishing and Triple Quadrupoles "Give a man a fish; feed him for a day. Teach a man to fish; feed him for a lifetime“ Lao Tzu circa. 5th Century BC
  • 34. 34 AutoSRM Overview 1) Precursor ion selection 2) Product ion selection 3) Collision energy optimization SRMCreationWorkflow
  • 35. 35 Step 1 – Pick Your Precursor Ions
  • 36. 36 Step 1 – Pick Your Precursor Ions
  • 37. 37 Step 1 – Pick Your Precursor Ions
  • 38. 38 Step 2 – Pick Your Product Ions
  • 39. 39 Step 2 – Pick Your Product Ions
  • 40. 40 Step 3 – Optimize Your Transitions
  • 41. 41 Step 3 – Optimize Your Transitions
  • 42. 42 AutoSRM Use Case • Created and optimized > 250 transitions for > 80 compounds • Minimal user interaction over 24 hours
  • 43. 43 Export from AutoSRM to Instrument Method
  • 45. 45 Timed-SRM Method Overview Acquisition windows centered around retention time
  • 49. 49 Timed-SRM Advantages • Removes wasted dwell time • Allow higher overall dwell times • Leads to higher sensitivity Wasted Dwell Time
  • 50. 50 Timed-SRM Advantages • Peaks centered in acquisition window • No peak elutes near acquisition break • Allows for retention time shift (e.g. due to heavy matrix)
  • 51. 51 Thermo Scientific TSQ 8000 GC-MS/MS Timed-SRM Case Study • Previous method: Segmented SIM acquisition on single quad • Required five injections for full list of pesticides • Needed to analyze more pesticides (350 total), but current methodology took too long • Wanted to consolidate to a single injection
  • 52. 52 • Segmented SRM • Closest compound to segment break: 5 seconds • Average number of simultaneous transitions: 55 • Timed SRM • Closest compound to segment break: 15 seconds • Average number of simultaneous transitions: 15 (4X higher dwell times) TSQ™ 8000 GC-MS/MS Timed-SRM Case Study
  • 53. 53 TSQ 8000 GC-MS/MS Timed-SRM Case Study Tea Analysis: 4 pg on-column Terbacil Alachlor Tolylfluanid Pyridaben
  • 54. 54 Export from Instrument Method to TraceFinder™ Software
  • 55. 55 TraceFinder Software Overview Batch Creation Data Review Report Generation Routine Workflow
  • 56. 56 Instrument & Data Processing Method Maintenance • GC-MS/MS systems in routine pesticide analysis face high volumes of samples with high matrix load • Cumulative deterioration of the GC column performance • Backflushing set-up can help to mitigate • Inevitably compound retention times drift and or GC columns need to be cut or replaced • Need to locate compounds, update acquisition windows & update RT in data processing method • Very laborious & time consuming- worse with a large method!
  • 57. 57 TraceFinder Software Method Sync • Links TraceFinder Software Method with instrument method • Enables • Compound based acquisition setup • Automated update of acquisition windows
  • 58. 58 Method Sync – Automated RT Update Updating retention times in data review…
  • 59. 59 Method Sync – Automated RT Update …updates both TraceFinder Software Method and Timed-SRM Method
  • 60. 60 Summary We can use integrated and automated software • Easily adopt large multi- residue methods • Remove the pain (and avoid bottlenecks) • Method creation • Method optimization • Method management • Method maintenance • To create improved results (and productivity) in routine pesticide analysis
  • 61. 61 Thank You for Your Attention! Questions? Stay connected with us Twitter @ChromSolutions Chromatography Solutions Blog http://chromblog.thermoscientific.com/blog YouTube http://www.youtube.com/ChromSolutions Facebook http://www.facebook.com/Chromatography Solutions Pinterest http://pinterest.com/chromsolutions/