Asymmetric flow field flow fractionation
Asymmetrical flow field-flow fractionation (AF4) is a fractionation method that is used for the characterization of nanoparticles, polymers and proteins. The theory for AF4 was conceived in 1986 and was established in 1987. It is a separation technique based on the theory of field flow fractionation (FFF). AF4 is distinct from FFF because it contains only one permeable wall so the cross-flow is caused only by the carrier liquid. The cross-flow is induced by the carrier liquid constantly exiting by way of the semi-permeable wall on the bottom of the channel. It has been used to characterize condensed tannins oxidation.[1]
Operational procedures
The AF4 experiment can be separated into three stages:
1. Sample Injection
- Samples are injected into the system using a known amount of sample volume. This volume will depend on the AF4 instrument being utilized in the experiment. Starting fractionation immediately after sample injection is not ideal because the sample is going to spread out randomly from the injection site, so the beginning velocity and place of the particles are not all the same. This leads to line broadening and insufficiency. In order to correct such an error, sample focusing is proposed. Modern AF4 Systems allow both: manual and auto injection.
2. Sample focusing
- A current going opposite of the carrier solvent is used to focus all the particles in the sample to one specified area before fractionation begins. This corrects for any peak broadening that can occur due to particles being dispersed from the injection port to the channel outlet before fractionation begins. Sample preparation is an other option that can be achieved in the focus step. Once all the particles are in the same area of the channel, fractionation can occur.
3. Fractionation
- There are two components that make up the FFF system. Firstly, the laminar flow that carries the sample through the separation chamber and secondly the separation field applied perpendicular to the channel, against the sample flow.
- As particles flow along the channel the cross flow separation field pushes the molecules towards the bottom of the channel. As they pass by the bottom they undergo a counter acting diffusion back into the channel against the carrier flow. The extent to which the molecules can diffuse back into the channel is dictated by their natural Brownian motion, a characteristic based on size that is unique to each individual species. Smaller particles have a higher Brownian motion than larger ones and are able to diffuse higher into the channel against the carrier flow.
- The rate of laminar flow within the channel is not uniform. It travels in a parabolic pattern with the speed of the flow increasing towards the center of the channel and decreasing towards the sides. Therefore, the rate at which particles will be carried through will depend on their position within the channel. Those with a greater diffusion, located in the center of the channel, will be transported with a greater velocity. The larger particles in the shallow, slower moving stream are transported with lower flow velocity and elute later than smaller particles. This results in a gentle separation of particles based on mass with the elution order of smallest to largest.
Modern systems are using pumps instead of flow controllers to provide constant flow rates in a wide flow range with minimum of tubing and a metal free sample path.
Applications
Asymmetrical flow field flow fractionation (AF4) is nowadays a common and state-of-the art method for fractionation and separation of macromolecules and particles in a suspension. More commonly, HPLC would be used for liquid separations for molecules up to 10 kDa and nanoparticles up to 10 nm. AF4's application are flexible for many analytical conditions where a common method would be unable to properly separate the desired particles. For macromolecules and nanoparticles AF4 is an alternative method especially when the static phase in columns creating interaction with the sample. It has also been used to study aggregation of particles in a solution.
References
- ↑ Vernhet, A.; Dubascoux, S. P.; Cabane, B.; Fulcrand, H. L. N.; Dubreucq, E.; Poncet-Legrand, C. L. (2011). "Characterization of oxidized tannins: Comparison of depolymerization methods, asymmetric flow field-flow fractionation and small-angle X-ray scattering". Analytical and Bioanalytical Chemistry 401 (5): 1559–1569. doi:10.1007/s00216-011-5076-2. PMID 21573842.