https://community.jmp.com/t5/Discussions/Variance-components-analysis-for-lyophilization-process/m-p/667471#M85553 <P>I am not an SME for your situation, but I have some thoughts:</P> <P>1. The situation you describe appears to be a nested/systematic component of variation study.&nbsp; The hierarchical layers are:</P> <P><STRONG>Batch</STRONG> (although this appears to be manipulated)</P> <P><STRONG>Shelf</STRONG> (Systematic locations, though you do not specify how many)</P> <P><STRONG>Samples</STRONG> (Confounded with the Sample component is the measurement system variation)</P> <P>2. How confident are you in the measurement system? Why do you need 10 samples? You are somewhat biasing this layer.</P> <P>3. Robustness is the measure of how consistent the&nbsp;<SPAN>lyophilization process is over changing noise.&nbsp; I would be suspicious that in 3 batches you have exposed all of the possible noise effects.&nbsp; You will not be able to assess the consistency of the batch-to-batch variation.</SPAN></P> <P><SPAN>4. For analysis you may be able to use the control chart method or ANOVA method.&nbsp; I would start with variability plots (make sure the data types are nominal) and let JMP calculate the quantitative components.</SPAN></P> <P>&nbsp;</P> Fri, 11 Aug 2023 13:21:01 GMT statman 2023-08-11T13:21:01Z https://community.jmp.com/t5/Discussions/Variance-components-analysis-for-lyophilization-process/m-p/667242#M85534 <P>Hello all,</P><P>&nbsp;</P><P>I would like to perform a variance components analysis to characterize the robustness of a lyophilization process.</P><P>&nbsp;</P><P>Here is the background:</P><UL><LI>I have performed three lyophilization batches with three different cycle parameters.</LI><LI>I have intentionally placed product vials in defined locations across the shelf for each batch.</LI><LI>At the end of each batch, I have taken 10 samples from each of those defined locations and analyzed them. Each sample of the 10 samples is a replicate sample.</LI><LI>I want to understand the potential variation of analytical results due to the lyophilization batch and shelf location</LI></UL><P>Considering this information, is it appropriate to carry out a variance components analysis or are there other statistical methods that would be more appropriate e.g. one-way ANOVA? How can this be done in JMP?</P><P>&nbsp;</P><P>Thanks in advance.</P> Thu, 10 Aug 2023 13:10:49 GMT https://community.jmp.com/t5/Discussions/Variance-components-analysis-for-lyophilization-process/m-p/667242#M85534 MichaelM92 2023-08-10T13:10:49Z https://community.jmp.com/t5/Discussions/Variance-components-analysis-for-lyophilization-process/m-p/667471#M85553 <P>I am not an SME for your situation, but I have some thoughts:</P> <P>1. The situation you describe appears to be a nested/systematic component of variation study.&nbsp; The hierarchical layers are:</P> <P><STRONG>Batch</STRONG> (although this appears to be manipulated)</P> <P><STRONG>Shelf</STRONG> (Systematic locations, though you do not specify how many)</P> <P><STRONG>Samples</STRONG> (Confounded with the Sample component is the measurement system variation)</P> <P>2. How confident are you in the measurement system? Why do you need 10 samples? You are somewhat biasing this layer.</P> <P>3. Robustness is the measure of how consistent the&nbsp;<SPAN>lyophilization process is over changing noise.&nbsp; I would be suspicious that in 3 batches you have exposed all of the possible noise effects.&nbsp; You will not be able to assess the consistency of the batch-to-batch variation.</SPAN></P> <P><SPAN>4. For analysis you may be able to use the control chart method or ANOVA method.&nbsp; I would start with variability plots (make sure the data types are nominal) and let JMP calculate the quantitative components.</SPAN></P> <P>&nbsp;</P> Fri, 11 Aug 2023 13:21:01 GMT https://community.jmp.com/t5/Discussions/Variance-components-analysis-for-lyophilization-process/m-p/667471#M85553 statman 2023-08-11T13:21:01Z https://community.jmp.com/t5/Discussions/Variance-components-analysis-for-lyophilization-process/m-p/667499#M85555 <P>To add a bit to&nbsp;<a href="https://community.jmp.com/t5/user/viewprofilepage/user-id/4358">@statman</a>&nbsp;'s advise you may want to take a look at this On Demand webinar hosted by my former (I'm now retired) JMP colleague <a href="https://community.jmp.com/t5/user/viewprofilepage/user-id/8239">@JerryFish</a>&nbsp;.&nbsp;<A href="https://community.jmp.com/t5/Mastering-JMP/Using-the-EMP-Method-for-Measurement-System-Analysis/ta-p/407690?_ga=2.23440184.326626311.1691679338-518099710.1652727774" target="_self">Measurement Systems Analysis</A>&nbsp;Jerry shows the Wheeler EMP method which is essentially the control chart method referred to by&nbsp;<a href="https://community.jmp.com/t5/user/viewprofilepage/user-id/4358">@statman</a>&nbsp;</P> Fri, 11 Aug 2023 14:20:17 GMT https://community.jmp.com/t5/Discussions/Variance-components-analysis-for-lyophilization-process/m-p/667499#M85555 P_Bartell 2023-08-11T14:20:17Z