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The world leader in serving science LTQ Velos a jeho kombinace s FT-MS Orbitrap Je něco převratně nového v iontových pastech? Petr Verner ThermoFisher Scientific, Praha LTQ Velos Co je nového? • Hardware • HESI II probe standard • S-Lens ion optics • Dual Cell Linear Trap • Prakticky? • 2x Rychlejší skenování • Zvýšená citlivost • Lepší statistika • Vyšší rozlišení 2 Customer value Hardware features Benefit Customer Value Dual Cell Linear Trap 1.Higher Isolation efficiency 2.Higher CID efficiency 3.Faster scan speed 4.Higher resolution increased sample IDs S-Lens Increased ion flux Higher sensitivity Lower fill time Low-level analyte detection HESI II probe Better sample desolvation Higher sensitivity Less solvent noise Increased Robustness Low-level analyte detection The increased sensitivity and decreased cycle time of the LTQ Velos allow greater depth of sample analysis resulting in increased protein coverage and enhanced access to MSn structural elucidation on a chromatographic time scale. 3 LTQ Velos – What’s new? Source changes • HESI II standard • Nový design sweep cap • Stejné jako na TSQ Vantage 4 Dual Cell Linear Ion Trap Configuration No Tube Lens or Skimmer Front Lens Center Lens Detector 1 Octopole HPT HPC LPC Detector 2 5 Back Lens LTQ Velos S-Lens – podobné jako na TSQ Vantage 6 LTQ Velos – What’s new? Zahnutý Q0 7 LTQ Velos It has 2 linear traps 8 High Pressure Low Pressure High Trapping Efficiency High Dissociation Efficiency High Isolation Efficiency 5.0 x10-3 Torr He Square Quadrupoles Electrospray Source Ion Transfer Tube Higher Resolution/Scan Rate 3.5x10-4 Torr He Front Lens Center Lens Detector 1 Octopole HPT HPC SRIG Inter- multipole Lens 1 Split Gate Lens 9 LPC Detector 2 Back Lens n Ion Trap Scan Function - MS Ion Injection Ion Isolation Ion Dissociation n-1 Mass Analysis 1 10 Motivation 1: Trapping Efficiency He Pressure Effects - TIC 2000 Standard Pressure ~60% Trap Eff. TIC 1600 Higher Pressure >95% Trap Eff. 1200 800 400 0 0 1 2 3 4 He Pressure (mtorr) 11 5 6 Motivation 2: CID Efficiency He Pressure Effects – CID Efficiency for MRFA (m/z 524, 30 ms) 100 CID Efficiency 80 Higher Pressure >80% CID Eff. 60 Standard Pressure ~68% CID Eff. 40 20 0 2 4 6 He Pressure (mtorr) 12 8 10 Motivation 3: Resolution/Scan Rate He Pressure Effects - Peak Width at Scan Rate 16,667 amu/sec Peak Width (amu) 1.8 1.6 1.4 Standard Pressure 0.55 amu FWHM 1.2 1 0.8 0.6 0.4 Lower Pressure <0.4 amu FWHM 0.2 0 0 1 2 3 4 He Pressure (mtorr) 13 5 6 Motivation 3: Resolution/Scan Rate Effect of Scan Rate on Peak Width (Res. Ej. Optimized) 0.7 FWHM (amu) 0.6 0.5 2x Current Scan Rate 0.4 0.3 Current Scan Rate 0.2 Scan Rate Range 1 Scan Rate Range 2 0.1 Scan Rate Range 3 0 0 5000 10000 15000 20000 Scan Rate (amu/sec) 14 25000 30000 35000 LTQ Velos – dobrá, ale ještě něco nového? Nový RF system Nový Digital board Nový Source Board Nová geometrie lineárních pastí Nová Transfer ion optics Krátce: zvenku může připomínat staré dobré LTQ, ale uvnitř je mnoho novinek 15 LTQ Velos Co tedy přináší nového uživateli? • Dvojnásobnou rychlost skenování (vyjma TURBO a UltraZoom Skenu) • Lepší rozlišení (i v Ultra Zoom skenu) • Výrazně zkrácený tzv. Ion injection time • Zvýšená citlivost 4-5X 16 Scan Speed vs Resolution LCQ Fleet LTQ XL LTQ Velos TurboScan 80,000 amu/s @ 3 amu FWHM 125,000 amu/s @ 3 amu FWHM 125,000 amu/s @ 3 amu FWHM Normal 12,500 amu/s @ 0.7 amu FWHM 16,700 amu/s @ 0.7 amu FWHM 33,300 amu/s @ 0.6 amu FWHM Enhanced 5000 amu/s @ 0.35 amu FWHM 5000 amu/s @ 0.45 amu FWHM 10,000 amu/s @ 0.35 amu FWHM ZoomScan 1100 amu/s @ 0.25 amu FWHM 1100 amu/s @ 0.3 amu FWHM 2200 amu/s @ 0.25 amu FWHM Ultra ZoomScan N/A 27 amu/s @ 0.15 amu FWHM 27 amu/s @ 0.1 amu FWHM 17 Installation Specs LCQ Fleet LTQ XL LTQ Velos Reserpine Concentration 2 uL 1 pg/uL 2 uL 125 fg/uL 2 uL 50 fg/uL Signal to Noise 100:1 100:1 100:1 18 Co bude s LXQ? LXQ bude nadále vyráběno – jako součást ToxSpec analyzátoru (klinická biochemie) • Náhrada HPLC systému Remedy Jinak LCQ Fleet, LTQ XL, LTQ Velos 19 LCQ Fleet • Exceptional Analytical Value • Routine analysis of complex samples • Proven MSn performance for compound identification and structural elucidation • Familiar platform - provides ease of use Challenges • Sample/Process • • • • control Reliability Non MS operators Complex Matrices Multi-Component Samples Tools Customer Benefits LCQ Fleet Accela Hypersil Gold Columns Metworks Mass Frontier 20 Established reputation Structural elucidation with MSn Ease of use Greater sensitivity than UV/Single Quad Greater Specificity LTQ XL •Exceptional coverage at breakthrough speed •Fast cycle time, high sensitivity •Unmatched MSn spectral quality •Platform for hybridization Challenges • Post Translational • • • Modification Identification Rapid gradients Complex samples Biological matrices Tools Customer Benefits LTQ XL ETD MALDI Accela Hypersil Gold Columns Discoverer Metworks Mass Frontier 21 Identify the site of PTMs Multiple fragmentation techniques for maximum information Tissue Imaging Solution Excellent quality MSn spectra for library searching Upgradeable to Orbitrap Upgradeable to ETD LTQ Velos • Balanced 2D linear trap • Rapid reliable structural information • Ultra-Fast cycle time – up to 10Hz • The most sensitive full scan MS • Standard with HESI Challenges • Complex matrices • Co-Eluting • • compounds Post Translation Modification Early phase metabolite ID and Quan Tools Customer Benefits LTQ Velos ETD Dual Pump Metworks Mass Frontier Discoverer 22 Fast cycle time for identifying coeluters Simultaneous Quan and Qual Excellent quality MSn spectra on a u-HPLC time scale Data Dependant Decision Tree provides optimum fragmentation Upgradeable to Orbitrap Velos Upgradeable to ETD MALDI v kombinaci s LTQ MALDI bude dostupné pouze s LTQ XL • We will continue to work on the software, both control and data processing to improve this product further. MALDI will NOT be available on the LTQ Velos • Most of the LTQ Velos improvement are due to the source and optics which are removed for MALDI 23 Alprazolam in Plasma The world leader in serving science Alprazolam LTQ Velos – Plasma with IS 5 orders of Dynamic range – LOQ 40fg on column Alprazolam Y = 0.000554475+0.0347005*X R^2 = 0.9963 W: 1/X 140 120 Alprazolam Y = 0.000556373+0.0347005*X R^2 = 0.9963 W: 1/X 100 0.010 80 Area Ratio 0.008 60 0.006 0.004 40 0.002 20 0.000 0.00 0.05 0 0 1000 2000 3000 pg on column 25 4000 0.10 0.15 pg on column 0.20 0.25 Alprazolam LTQ Velos – Plasma with IS pg on column LTQ XL (%RSD) LTQ Velos (%RSD) 0.04 12.84 0.1 9.44 0.2 4.60 0.4 7.48 5.79 1 20.82 3.28 2 5.81 3.52 4 4.21 6.10 10 5.56 3.13 20 5.08 3.85 40 3.82 2.20 100 2.05 3.45 200 0.86 6.26 400 2.02 4.32 1000 4.21 3.05 2000 1.60 3.94 4000 1.42 26 LTQ XL vs. LTQ Velos – 400fg on column Relative Abundance RT: 0.70 - 1.30 SM: 7G 100 95 90 85 80 75 70 65 60 55 50 45 40 35 30 25 20 15 10 5 0 0.8 0.9 SM: 7G 1.0 Time (min) 1.1 1.2 30 scans across the peak Relative Abundance RT: 0.70 - 1.30 100 95 90 85 80 75 70 65 60 55 50 45 40 35 30 25 20 15 10 5 0 10 scans across the peak 0.8 0.9 1.0 Time (min) 27 1.1 1.2 1.3 The world leader in serving science Multi Component Quantification Amphetamine Y = -0.00047078+0.00210668*X R^2 = 0.9969 W: 1/X Codeine Y = 0.000139457+0.00158557*X R^2 = 0.9968 W: 1/X 4.5 4.0 3.0 3.5 2.5 3.0 Area Ratio 2.0 1.5 2.5 2.0 1.5 1.0 1.0 0.5 0.5 0.0 0 0.0 500 1000 1500 2000 pg on column Methamphetamine Y = 0.000175724+0.00417322*X R^2 = 0.9946 W: 1/X 0 500 1000 1500 pg on column 2000 1000 pg on Column 2000 Lidocaine Y = 0.000192073+0.00421984*X R^2 = 0.9966 W: 1/X 9 9 8 8 7 7 6 Area Ratio Area Ratio 4 Compound Quan LTQ Velos – IS (5 scan events) 5 4 6 5 4 3 3 2 2 1 1 0 0 0 500 1000 pg on Column 1500 2000 0 29 500 1500 4 Compound Quan LTQ Velos – IS (5 scan events) Level pg on Column Codeine %RSD Lidocaine %RSD Amphetamine %RSD Methamphetamine %RSD 0.1 24.6 3.0 34.2 0.2 4.1 8.1 13.1 0.4 12.9 10.5 3.5 9.0 1 11.7 3.6 2.9 4.2 2 6.0 6.0 5.8 4.8 4 4.1 2.8 4.8 3.0 10 5.4 3.8 8.6 4.9 20 2.9 2.9 4.8 5.5 40 3.3 4.7 2.3 2.8 30 4 Compound Quan LTQ XL – IS (5 scan events) Level pg on Column Codeine %RSD Lidocaine %RSD Amphetamine %RSD Methamphetamine %RSD 0.1 0.2 0.4 1 40.7 2 63.2 17.9 4 13.7 8.3 12.8 9.0 10 10.6 13.9 11.0 3.2 20 13.8 5.3 8.9 8.2 40 4.7 2.2 13.2 10.7 31 15.91 4 Compound Quan LTQ Velos – IS (5 scan events) 4pg on column - No Smoothing RT: 0.00 - 1.40 100 Amphetamine 80 60 40 20 100 0 80 Amphetamine-d6 60 40 20 100 0 80 Methamphetamine 60 40 20 100 0 80 60 Lidocaine 40 20 100 0 80 60 40 Codeine 20 0 0.0 0.2 0.4 0.6 0.8 Time (min) 32 1.0 1.2 1.4 4 Compound Quan LTQ XL – IS (5 scan events) 4 pg on column - No Smoothing RT: 0.00 - 1.41 100 Amphetamine 80 60 40 20 0 100 80 Amphetamine-d6 60 40 20 Relative Abundance 0 100 80 Methamphetamine 60 40 20 0 100 80 Lidocaine 60 40 20 0 100 80 Codeine 60 40 20 0 0.0 0.1 0.2 0.3 0.4 0.5 0.6 0.7 Time (min) 33 0.8 0.9 1.0 1.1 1.2 1.3 1.4 Source Ruggedness The world leader in serving science LTQ Velos Ruggedness – 600 injections singly crashed plasma 20 pg on Column of Alprazolam in Crashed Plasma 400000 350000 1.9% RSD with no internal standard 300000 Peak Area 250000 200000 150000 100000 50000 0 0 100 200 300 Number of injections 35 400 500 600 LTQ Velos Malathion The world leader in serving science LTQ Velos Full Scan MS2 – 10ppb Malathion The Full Scan Solution to Chemical Noise XIC m/z 99 Fragment XIC m/z 285 Fragment RT: 2.30 - 3.16 SM: 7G RT: 2.30 - 3.16 SM: 7G 85 NL: 4.78E1 100 m/z= 98.50-99.50 F: ITMS + c ESI Full ms2 [email protected] 95 [90.00-350.00] MS Genesis 90 MalathionQuan_039 85 80 80 75 75 70 70 65 65 60 60 100 95 Relative Abundance 90 55 50 45 50 45 40 35 35 30 30 25 25 20 20 15 15 10 10 5 5 2.4 2.5 2.6 2.7 2.8 Time (min) 2.9 3.0 NL: 4.1 m/z= 2 ITMS + 331.10 [90.00 Genes Malath 55 40 0 2.3 AH: 3977 SN: 44 0 2.3 3.1 37 2.4 2.5 2.6 2.7 2.8 Time (min) 2.9 3.0 3.1 Calibration Curve 0.1 to 20 ppb Malathion Malathion Y = 1030.8+27661.5*X R^2 = 0.9904 W: 1/X 600000 500000 Area 400000 300000 200000 100000 0 0 5 10 ppb 38 15 20 0.1 ppb Malathion in 50X Diluted QuEChERS Extract S/N 634 2.0E3 39 Proteomics The world leader in serving science Increase in Identification for the most complex mixtures Increase in Protein ID 500 ng Increase in Unique Peptide ID 500 ng Increase in Protein ID for LTQ Vs. Velos (500 ng) 1400 1200 64% Increase in Unique Peptide ID for LTQ Vs. Velos (500 ng) 55% 53% 3500 3000 77% 2500 1000 2000 800 LTQ LTQ Velos LTQ LTQ Velos 600 1500 400 1000 200 500 0 0 '60 min' '180 min' '60 min' 41 '180 min' Sensitivity for Low Level Injections (20 ng) Increase in ID LTQ Vs. LTQ Velos 20 ng (C. Elegans) 500 400 1200 1000 104% 124% 800 300 Series1 LTQ XL LTQ Velos 600 Series2 200 400 100 200 0 0 Unique Peptides Proteins 42 Metabolism The world leader in serving science Maropitant Dog Sample 60 min incubation on LTQ XL RT: 0.00 - 8.00 NL: 2.21E7 Base Peak F: ITMS + c ESI Full ms [300.00-700.00] MS Dog60min2_MS3Top5_LTQ 469.35 100 Base Peak Chromatogram 50 381.13 391.13 0 100 391.17 485.32 485.30 312.47 391.15 399.23 NL: 2.21E7 Base Peak m/z= 468.40-470.40 F: ITMS + c ESI Full ms [300.00-700.00] MS Dog60min2_MS3Top5_LTQ 469.35 Parent 50 +O 50 NL: 3.52E6 Base Peak m/z= 484.00-486.00 F: ITMS + c ESI Full ms [300.00-700.00] MS Dog60min2_MS3Top5_LTQ 485.31 485.27 484.30 485.95 485.29 484.93 0 100 469.30 469.33 469.31 469.33 469.20 469.32 485.32 485.30 468.61 469.23 0 100 485.36 485.27 NL: 1.63E6 Base Peak m/z= 454.00-456.00 F: ITMS + c ESI Full ms [300.00-700.00] MS Dog60min2_MS3Top5_LTQ 455.31 -CH2 50 454.77 0 100 +2O 50 455.29 501.29 501.22 454.02 454.33 501.19 501.29 501.09 500.25 500.21 0 0 1 2 454.39 454.38 455.30 455.60 3 4 Time (min) 501.60 500.26 5 6 44 501.39 7 NL: 2.00E5 Base Peak m/z= 500.00-502.00 F: ITMS + c ESI Full ms [300.00-700.00] MS Dog60min2_MS3Top5_LTQ 8 Maropitant Dog Sample 60 min incubation on LTQ Velos ~ 10X Higher signal RT: 0.00 - 8.00 NL: 2.09E8 Base Peak F: ITMS + c ESI Full ms [300.00-700.00] MS Dog60min2_Top5MS3_Velos 469.98 100 Base Peak Chromatogram 50 381.58 413.79 0 100 462.76 485.69 485.64 421.80 398.95 637.59 NL: 2.09E8 Base Peak m/z= 468.40-470.40 F: ITMS + c ESI Full ms [300.00-700.00] MS Dog60min2_Top5MS3_Velos 469.98 Parent 50 469.16 469.65 0 100 +O 50 NL: 2.10E7 Base Peak m/z= 484.00-486.00 F: ITMS + c ESI Full ms [300.00-700.00] MS Dog60min2_Top5MS3_Velos 485.67 485.69 484.65 485.67 485.18 0 100 469.79 469.87 469.67 469.65 469.74 469.86 485.69 485.64 485.90 485.85 NL: 1.15E7 Base Peak m/z= 454.00-456.00 F: ITMS + c ESI Full ms [300.00-700.00] MS Dog60min2_Top5MS3_Velos 455.68 -CH2 50 454.63 454.72 455.79 501.61 455.14 0 100 454.82 455.85 454.87 454.02 NL: 1.57E6 Base Peak m/z= 500.00-502.00 F: ITMS + c ESI Full ms [300.00-700.00] MS Dog60min2_Top5MS3_Velos +2O 50 501.35 0 0 501.69 500.56 501.55 1 2 500.58 3 4 Time (min) 5 501.75 501.85 6 45 7 Souhrn The LTQ Velos is 5X more sensitive than the LTQ XL The LTQ Velos is 2X faster than the LTQ XL The LTQ Velos can scan at 10Hz At low concentrations the LTQ Velos gets twice the number of unique peptides and protein identified as an LTQ XL LTQ Velos can be upgraded to ETD and Orbitrap Excellent Simultaneous Quan and Qual instrument High quality data (more samples identified in less time) Low level compound detection HESI II S-Lens Dual Cell Linear Trap Reliability 46
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