Overview
Method scouting
Method optimization
Robustness & validation
Resources
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The steps for developing your HPLC-CAD method should follow the usual process: method scouting, optimization, robustness testing and validation.

A Charged Aerosol Detector (CAD) works by measuring particle charge and can detect all non-volatile and many semi-volatile analytes, independent of chemical structure. This detection mechanism makes the CAD response sensitive to mobile phase quality, so the presence of semi-volatile and non-volatile impurities is often the limiting factor for method sensitivity.

An important pre-requisite for any mobile phase used with the CAD is the solvent must be volatile and not contain any non-volatile components. In addition to mobile phase quality and composition, things like your lab environment, nitrogen gas supply, LC instrument usage history and column stability can also impact the detector response.

To ensure optimal performance and consistent results, you’ll want to identify sources of mobile phase impurities and other interferences and develop strategies to minimize the introduction and interference with your chromatographic analysis.

 
 
 
Factors to consider for your HPLC-CAD method development

FactorsMain considerations
Nitrogen gas flow, mobile phase and additive purity impact baseline signalStable gas flow and additive-free mobile phases with no column in line should give you a background current of around 1 pA at EvapT of 35 °C
Column bleed impacts baseline signalColumn stability can slowly deteriorate with use, especially near the pH limit and at elevated temperatures
Analyte volatility impacts responseUse flow injection analysis to see if your analytes behave as volatiles, semi-volatiles or non-volatiles
Evaporation temperature (EvapT) impacts response and baseline signalSome analytes might behave as non-volatiles at lower temperatures but as semi-volatiles at higher temperatures
Gradient elution impacts signal, noise and driftApply inverse gradient methods to restore the uniform response for non-volatiles
Power function value (PFV) impacts the linear response rangeAn optimal PFV gives you a more accurate calculation of peak resolution and limit of detection
Multi-detection setups can increase your detection rangeKeep your fluidic connections simple and short

 
 
 
Method setup

Once you’ve properly set up your HPLC-CAD system in the lab, you’re ready to begin method development. Here’s some essential best practices you should follow, recommended by our experts:

  1. Have a dedicated HPLC-CAD system, free of use with non-volatile additives, like phosphate buffers or non-volatile ion pairing reagents.

  2. Only use LCMS grade solvents and additives that contain the lowest “residue after evaporation” specification.

  3. Use volatile mobile phase additives only, as non-volatiles are extremely incompatible with the CAD and can adversely affect performance.

  4. Start with a regular gradient and then add an inverse gradient for optimization later, if needed.

  5. For all new methods, use the respective default settings on your CAD as a starting point:

    • Evaporation temperature at 35 °C

    • Data collection rate at 10 Hz

    • Power function value at 1.0

    • Filter time constant at 5.0 s

Besides screening various column and eluent mixtures to select the best combinations for successful separation, you’ll need to assess if your chemicals and method conditions are compatible with the CAD.

Using a step-by-step systematic approach, you’ll see how each component affects the baseline signal or background current.

Your main goal is to get an idea of what background signal is normal for the method conditions and application.

Here are the general steps to follow for method scouting:

1. Verify your target analytes meet the   CAD volatility requirements

If you do not have the numbers at hand, you can test for analyte volatility as described in our white paper:   A reliable UHPLC/UV/CAD/MS multidetector method for routine quantification and library matching of extractable and leachables in pharmaceutical-grade plastics.

2.  Assess the purity and stability of your nitrogen gas

This step involves running nitrogen gas through your HPLC-CAD system in the absence of a column and mobile phase flow to see if the gas flow and background signal are stable.

3. Verify your HPLC system lines and pump are free of residual salts.*

For this step, you’ll run ultra-pure lab water only, with no additives or column connected, at a flow rate of 1 mL/min and EvapT at 35 °C.

  • Your background signal should be no higher than 1 pA.

*We highly suggest having a dedicated HPLC system to use only with your CAD. If this situation is not possible, then you’ll need to flush the instrument to remove residual salts from the lines and pumps, and online degasser (if present) before connecting the CAD.

4. Check the quality of your mobile phase, without and with additives, in the absence of a column with the EvapT at 35 °C

Here, you want to track how the CAD background signal changes as the mobile phase flows, and how you can expect the signal to change with and without mobile phase additives, as well as the influence of the stationary phase.

  • Clean solvents with no additives and no column in line should give you a maximum signal of 1 pA.
How to check mobile phase quality

To adequately evaluate the quality of a new batch of mobile phase, especially when using a new type or lot of solvent or additive you should establish a frame of reference and continuously monitor the performance of each application.

One approach to evaluating mobile phase quality is to first verify the detector performance using the qualification conditions described in our white paper:   Getting the most out of your charged aerosol detector - factors influencing charged aerosol detector performance

  • You can measure the noise with a methanol/water (20/80, v/v) mobile phase, a flow rate of 1 mL/min, and the following detector settings: EvapT 35 °C, data collection rate 10 Hz, and a filter constant of 5. Replace the column with a restriction capillary (or only a small cartridge).

  • Once the baseline noise is known, you can quickly screen other mobile phases, solvent lots and additives. You can even simplify the screening process by installing a large loop in a suitable valve in the system. This setup is rapid and does not require extensive purging and flushing of your HPLC-CAD system.

5. Connect the column to ensure there is no bleed from stationary phase decomposition

Run the mobile phase with any additives through your HPLC-CAD system at your desired method conditions including gradients and column heating to verify the background signal is stable with low current.

  • Some columns show significant bleed throughout the operating pH range (e.g. silica-based amino and cyano columns) while others only show significant bleed when operated near the specified operating limits such as pH and temperature (e.g. silica-based C18 columns).

  • Although   column bleed can increase noise and background currents, column performance is often acceptable, and columns may still show fairly stable retention times and peak shapes.

6. Run your analysis

Again, the same rules apply here as for your general method development: stable baseline, resolved peaks and enough equilibration time.

  • Check the resolution and, depending on qualification or quantitation focus area, you might proceed with method optimization – like gradient fine-tuning, complementary detectors (in case of overlaying peaks) or complementary gradient (inverse gradient).

Optimizing your HPLC-CAD method involves iterative testing of various method conditions to achieve the best resolution, speed, and reproducibility.

  • You can convert non-volatiles to semi-volatiles by   changing the EvapT. Best practice is to increase the EvapT by 5 °C if your model allows, not to exceed the maximum temperature setting on your CAD. Higher temperatures may reduce background noise but will also reduce the signal for semi-volatiles.

  • Apply an   inverse gradient. The inverse gradient composition is the exact opposite of your analytical gradient. Under these conditions, the CAD response among non-volatile analytes is more uniform, which gives you more accurate quantitation with a single calibrant.
    • Our inverse gradient wizard allows you to easily generate a complementary gradient by maximizing the organic content to increase the response. Our   white paper highlights a quick overview of the three options available with inverse gradient.
       
  • Other possible adjustments include altering the   power function to help you optimize the range over which the CAD response is sufficiently linear for a given method's range of quantitation.

  • In some cases, you can   convert semi-volatile analytes to non-volatile ones with additives. Please contact our technical support team to learn more.

Robustness testing is done to determine the impact of changing parameters of the separation method and is important for both your   method validation and transfer processes.

  • Assess calibration curves and standards at different EvapT settings to look at drift and ranges, and by changing the injection volume.

  • Run your method on different raw materials, columns, bulk and finished good lots to see if small variations cause a large change in data.

  • Test replicates across independent batches to establish your method's reproducibility.
On-demand webinars

No chromophore – no HPLC analysis?

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Absolute quantification of lipids in complex mixtures by HPLC without authentic standards

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How HPLC-CAD analysis can allow you to see hidden extractable oligomers

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White papers

Characterization of lipid nanoparticle (LNP) composition using UHPLC-CAD

  Download paper

Polysorbate 80 profiling by HPLC with mass and charged aerosol detection

  Download paper

A reliable UHPLC/UV/CAD/MS multidetector method for routine quantification and library matching of extractables and leachables in pharmaceutical-grade plastics

  Download paper

See our full collection of HPLC-CAD method development and transfer resources.


 

Resources

 
 
 
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