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Stopped Flow Analysis

Stopped flow is a technique used to rapidly mix reactants and observe reactions over short time periods. It involves rapidly mixing reactants in a mixing chamber and then stopping the flow before measurement in a detector, usually photometry. This allows better sensitivity and reduced dispersion compared to continuous flow. Stopped flow can observe half-times of 1-10 seconds and is used to study enzyme kinetics, protein folding, coordination chemistry, and catalysis. An example described used stopped flow NMR to determine rate constants and elucidate the catalytic pathway for a zirconium-catalyzed polymerization reaction.

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92 views16 pages

Stopped Flow Analysis

Stopped flow is a technique used to rapidly mix reactants and observe reactions over short time periods. It involves rapidly mixing reactants in a mixing chamber and then stopping the flow before measurement in a detector, usually photometry. This allows better sensitivity and reduced dispersion compared to continuous flow. Stopped flow can observe half-times of 1-10 seconds and is used to study enzyme kinetics, protein folding, coordination chemistry, and catalysis. An example described used stopped flow NMR to determine rate constants and elucidate the catalytic pathway for a zirconium-catalyzed polymerization reaction.

Uploaded by

varsha CR
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© © All Rights Reserved
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Andrew Yeung

CHEM636
2011-01-31
History
 First described by
Chance (1940) and
Gibson & Milnes (1964),
with a view to probing
enzyme kinetics
 Oscilloscopes were the
first detectors

Chance, B. J.Franklin Inst. 1940, 229, 613.


Gibson, Q. H.; Milnes, L. Biochem. J. 1964, 91, 161.
Overview
 Stopped flow is a type of flow-  Dead time – the time
injection analysis between the end of
mixing and the start of
 Reactants are rapidly mixed in a measurement Typically
mixing chamber, and the flow is ms range
stopped with the reactant stream in  Measured electronically
 Shorter is better
the flow cell (detector – usually some
form of photometry)
 Allows
 better measurement sensitivity due to
increased residence time
 reduced fluid dispersion by stopping
flow
Scope
Other developments
 Small sample volumes  Wide temperature ranges
(< 0.7 to 500 μL) (e.g. +100 to -100 °C)
 Fast analysis (3 to 60 s)  High pressure (2 kbar)
 t1/2 of 1-10 seconds possible  measurements of activation
volume
 Sensitivity depends on
detector  Stopped flow with fast scan
 Able to tolerate corrosive spectroscopy or with a
compounds (e.g. Br2, H2SO4) temperature jump
 determine transient reaction
 Many instruments
intermediates
commercially available

Gomez-Hens, A.; Perez-Bendito, D. Anal. Chim. Acta 1991, 242, 147.


Applications
 Enzymes
 Protein folding
 Redox reactions
 Coordination chemistry
 Catalysis (e.g. polymerization reactions)
Typical Instrument

An example of a mixer

Mottola, H. A. Kinetic aspects of analytical chemistry; Wiley: New York, 1988; pp 172-178.
Schematics
Drive ratio can be
conveniently varied
(Harvey).

Mottola, H. A. Kinetic aspects of analytical chemistry; Wiley: New York, 1988; pp 172-178.
Harvey, R. A.; Borcherdt, W. O. Anal. Chem. 1972, 44, 1926.
Detectors
 Usually photometric detectors
 UV/Vis & IR
 Fluorescence (more sensitive)
 Chemiluminescence
 Circular dichroism (good for protein work)
 Refractive index
 NMR* (e.g. 1H, 19F)
 EPR
 Voltammetry
 Electrical conductivity
Stopped Flow NMR
 NMR is the most information-rich type of
spectroscopy
 Hand-mixing of reagents – useful to get data points
within tens of seconds
 Stopped flow is useful to get data points within 2-
10 s
 Main delay in this technique is the spin-lattice
relaxation time, T1
 Reduced by addition of a relaxation agent, e.g.
Cr(acac)3, but causes line broadening
 Apparatus not commercially available yet

Christianson, M. D.; Tan, E. H. P.; Landis, C. R. J. Am. Chem. Soc. 2010, 132, 11461.
Green, D. B.; Lane, J.; Wing, R. Appl. Spectrosc. 1987, 41, 847.
Probing Ligand Substitutions
Cl k2 Cl k1
2- - Cl
+ Cl Pd Cl
r.d.s.
Pd Cl Pd
Cl Cl Cl

Cl
Pd 1,5-COD
Cl

Green, D. B.; Lane, J.; Wing, R. Appl. Spectrosc. 1987, 41, 847.
Further reading: Christianson, M. D.; Landis, C. R. Concepts Magn. Reson., Part A 2007,
30A, 165.
Studying the Mechanism of
Catalytic Polymerization
 Landis et al. studied the Zr-catalyzed
polymerization of 1-hexene CH3
Zr
 Commercial NMR flow probe modified
CH 3B(C 6F 5)3
to give mixing chamber & related
stopped flow apparatus
 Three reagent concentrations varied: 1-
hexene, and 2 catalyst precursors (rac-
(C2H4(1-indenyl)2)ZrMe2 & B(C6F5)3)
 Multiple “shots” used to sample the
course of each reaction for every set of
parameters

Christianson, M. D.; Tan, E. H. P.; Landis, C. R. J. Am. Chem. Soc. 2010, 132, 11461.
Data
Resting catalyst
Zr pre-catalyst

Active catalyst

Christianson, M. D.; Tan, E. H. P.; Landis, C. R. J. Am. Chem. Soc. 2010, 132, 11461.
Analysis
Chain Re-
Initiation Propagation Transfer initiation
entry ki/M−1 s−1 kp/M−1 s−1 kt/s−1 kr/M−1 s−1
1a 0.224(2) 13.2(1) 0.0317(4) 2.70(7)
2a 0.218(2) 18.6(2) 0.0345(4) 4.12(6)
3a 0.255(1) 18.3(1) 0.0303(3) 2.56(3)
4a 0.222(3) 17.8(2) 0.0264(5) 1.62(5)
5a 0.314(3) 21.8(2) 0.0369(6) 2.33(7)
6a 0.215(2) 15.2(1) 0.0339(4) 1.80(3)
global fit (COPASI) 0.2353(6) 16.83(6) 0.0323(2) 2.06(2)
Rapid Quenched Flow (25 °C) 0.25 8.1 0.0132 >10kp
Rapid Quenched Flow (0 °C) 0.033 2.2 0.00066 >10kp
Kinetic Modelling 0.031 3.7 0.0024 103kp

Christianson, M. D.; Tan, E. H. P.; Landis, C. R. J. Am. Chem. Soc. 2010, 132, 11461.
Catalytic Pathway

 Re-initiation of hydridoborate (6), originally thought


to be fast, found to be very slow
 43 % of catalyst (3) inactive

Christianson, M. D.; Tan, E. H. P.; Landis, C. R. J. Am. Chem. Soc. 2010, 132, 11461.
Data
Resting catalyst
Zr pre-catalyst

Active catalyst

Christianson, M. D.; Tan, E. H. P.; Landis, C. R. J. Am. Chem. Soc. 2010, 132, 11461.

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