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GenNLC[V]


GenNLC[V] - [V] ZDD

The GenNLC[V] model is uses an asymmetric normal generalization of the GMG or Skew Normal density. The model reduces to the GenNLC[Z] as the GMG becomes a Gaussian. By combining the two primary statistical generalized normals, there are two third moment or skew adjustments. Because of the high likelihood of correlations between the a4 and a5 parameters, this model should be treated as experimental and used with caution.

By using the relationships of equivalence between the GenHVL and GenNLC models, we make the following simple substitution into the GenHVL[V] model equation to derive the GenNLC[V] model:

GENNLC[V]2.PNG

To convert the GenHVL[V] to the GenNLC[V], the a2 is transformed to a Giddings kinetic time constant, the a5 is transformed to a Gidding's indexed asymmetry.

a0 = Area

a1 = Center (as mean of generalized normal ZDD)

a2 = Kinetic Width (Giddings time constant of ZDD)

a3 = NLC/HVL Chromatographic distortion ( -1 > a3 > 1 )

a4 = The GMG half-Gaussian convolution width, adjusts skew (third moment)

a5 = NLC indexed asymmetry ( -10 > a5 > 10 ) a5=0.5 NLC (Giddings), adjusts skew (third moment)

 

Built in model: GenNLC[V]

User-defined peaks and view functions: GenNLC[V](x,a0,a1,a2,a3,a4,a5)

 

v5_GenNLC[V].png

The GenNLC[V] allows the skew in the ZDD to be additionally adjusted by a one-sided probabilisitic (Gaussian) convolution. For this model to be theoretically valid, you must assume the zero distortion peak shape, independent of instrumental effects, contains a one-sided Gaussian smearing, or delay, in the internal chromatographic broadening. The a4 value must be positive.

A convolution width, a right-sifted (positive) a4 in the same direction as the a3 chromatographic distortion, produces only small differences with tailed shapes. On the other hand, on fronted shapes where this convolution width is in the opposite direction of a3, the differences are more significant for the same magnitude of a4. This secondary skew adjustment should probably be very small to share the a4 parameter.

If such a one-sided Gaussian spreading is present in the ZDD, as furnished by this model, the F-statistic of the GenNLC[V] fit should be higher than the F-statistic of the GenNLC[Z] fit.

GenHVL[V] Considerations

When a4 approaches 0 and a5=0, the ZDD becomes a Gaussian and the model reduces to the HVL.

When a4 approaches 0 and a5=0.5, the ZDD becomes a Giddings and the model reduces to the NLC.

When a4 approaches 0, the ZDD becomes a [Z] generalized normal and the model reduces to the GenNLC[Z].

The [V] ZDD model represents a generalization of the Asymmetric Generalized Normal (the [Z] density) and the Skew Normal or GMG (the [G] density). If the logarithmic transform of the GenNLC or GenNLC[Z] is sufficient to statistically model the data, you will see the a4 GMG convolution width iterate to values that approach zero, and there will be no statistical significance for this parameter.

You will typically find the models which also adjust the kurtosis or fourth moment tailing, the GenNLC[Y] and GenNLC[T] densities, to be of greater utility than the GenNLC[V] density which combines two distinct third moment adjustments.

We have not found this model useful for fitting overload shapes.

The GenNLC[V] model should only be used if the simpler GenNLC or GenNLC[Z] models are unsuccessful in adjusting the skew of the fitted peaks. For most analytic peaks, GenNLC[V] fits will be statistically overspecified. Use cautiously.

The GenNLC[V]'s a5 asymmetry parameter is indexed to the NLC and thus the absolute peak asymmetry is not independent of the peak's a1 location. Use the GenHVL[V] if you wish to fit an absolute statistical asymmetry.

This a5 skew adjustment in the ZDD manages the deviations from the Giddings ideality assumed in the theoretical infinite dilution NLC. This is an asymmetry parameter indexed to the NLC at a5=0.5. For most IC and non-gradient HPLC peaks, you should expect an a5 between 1.1 and 2.0 (the deviation from non-ideality is right skewed or further tailed from the Giddings).

We have at times observed a small modeling power improvement when using the GenNLC[V] model with non-gradient analytic peaks. The a4 width is typically very small, perhaps 0.01-0.02 on a retention x-scale. You should use the GenNLC[V] model cautiously for fitting analytic peaks. Use the F-statistic of the fit of the GenNLC[V] model against the F-statistic for the GenNLC or GenNLC[Z] models to ensure there is an actual improvement in the modeling. The GenNLC[V] F-statistic will increase in contrast with the GenNLC or GenNLC[Z] model when this adjustment to the fourth moment is statistically beneficial. A high S/N will definitely be needed to even see this benefit. if the a4 GMG convolution width in the ZDD is managing anything real, this should appear consistently in the F-statistic of the GenNLC[V] model.

Only if a4 is very small, can it be assumed constant (shared) across all peaks in the chromatogram.

Both the a4 and a5 can be seen as indicators of the deviation from this Gaussian ideality, and thus indicative of column health.

Note that the a4 and a5 will be most effectively estimated and fitted when the peaks are skewed with some measure of fronting or tailing. Higher concentrations are very good for this model, assuming that one does not enter into a condition of overload that impacts the quality of the fit.

This model will be least effective in highly dilute samples with a poor S/N ratio since such peaks will generally have much less intrinsic skew.

Since peaks often increase in width with retention time, the a2 will likely be varied (independently fitted) for each peak.

Since peaks often evidence increased tailing with retention time, the a3 will probably be varied (independently fitted) for each peak.

If you are dealing with a small range of time, however, or of you are dealing with overlapping or hidden peaks in a narrow band, a2 and/or a3 can be held constant across the peaks in this band.

The GenHVL[V] model is part of the unique content in the product covered by its copyright.



PeakLab v1 Documentation GenHVL[V] GenHVL[T]