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- Posts: 52
- Joined: Sat Feb 12, 2011 2:43 am
Hi all,
While developing a method for impurities on a drug product with a reporting threshold of 0.05%, the LOQ of the impurities was established first and based on the least sensitive of the impurities the sample preparation concentration was determined so the LOQ of the impurity would be below 0.05%. let's assume the chromatographic method is set in place with no room to change. A new impurity came in and the LOQ of this impurity is above the reporting threshold. We have looked at other wavelengths but we are working at the maxima in this case, increasing sample concentration is not possible due to solubility problems and injecting more sample is not possible as we are at 100uL. This impurity is not observed during stability and it barely shows up during forced degradation experiments. It is a potential degradation product, should this be included in the validation protocol? I need suggestions please. Thank you
While developing a method for impurities on a drug product with a reporting threshold of 0.05%, the LOQ of the impurities was established first and based on the least sensitive of the impurities the sample preparation concentration was determined so the LOQ of the impurity would be below 0.05%. let's assume the chromatographic method is set in place with no room to change. A new impurity came in and the LOQ of this impurity is above the reporting threshold. We have looked at other wavelengths but we are working at the maxima in this case, increasing sample concentration is not possible due to solubility problems and injecting more sample is not possible as we are at 100uL. This impurity is not observed during stability and it barely shows up during forced degradation experiments. It is a potential degradation product, should this be included in the validation protocol? I need suggestions please. Thank you
