Hello markbailey,

Thank you for your response! This is very interesting study because we saw improvement for the % monomer when we added various sodium chloride concentrations to the sample (from 20% without sodium chloride to about 50% monomer with 500mM). So, we were very interested to see if we can improve % monomer intensity by adding not just sodium chloride itself, but other types of chemicals (either one factor at a time or mix of factors).

During the DoE run, % monomer intensity fluctuates about 5-10%. This is because the instrument is very sensitive for even dimer or large particulates. Additionally, the sample that we picked for the study is already unstable (17-20% monomer). The instrument measures total of 10 times and take average of that to make it as 1 measurement. I took two measurements and take the average from the two. If the % monomer gave me 30% on the first one and 55%, I redo the measurement and compare the measurement with the previous data (including those 10 separate measurements). Then, if repeat measurement showed about 28%, and then 32%, I simply remove 55% off the equation.

You mentioned that Summary of Fit table estimates the standard deviation of the response to be 12%. I think this makes sense to me given that the sample is already not too stable. Perhaps I should've focused more on much higher salt concentrations (there is a paper suggest that high salt concentration may be necessary to optimize % monomer).

This is very helpful! Perhaps I should do a quick test with each salt as high as 500mM instead of 100mM.

Hi markbailey,

I've added two measurements per sample to the JMP file and attached the file to this message (this experiment was performed in the row order).

I used Fit Model to test for % monomer 1 and % monomer 2. I saw some improvement in Pvalue under Effect Summary, but I think I need to test out for higher level than 200mM sodium chloride, 100mM sodium citrate, or 100mM glycine.

Please take a look at this file and let me know if you can provide me some feedback on the data result or recommendation for the future experiment. 

Thank you!

There seems to be a large range of results for same conditions:

Are the two results for each condition / treatment two independent runs or two measures for one run? I wonder if it is measurement error, not experiment error. I mean error in the statistical sense (random variation). I do not mean that a mistake was made.

I also tried the full factorial model hoping that it might suggest some strong effects. The weaker effects might then be removed and a clearer picture would emerge. But instead I got a significant lack of fit.

This test compares the estimate of the random variation in the response using the sum of squares error from the model with the estimate from the replicates. Again, I do not know if the two response for each treatment represent replication (new run) or repeated measurement of the same run. The total error sum of squares is from the model. The pure error is from the 'replicates.' You can see that the difference is large and it suggests that there remain unaccounted effects in the data. The effect of a lurking variable?

Hi @Mark_Bailey , it is a repeated measurement of the same run. Each run measures other useful information not just % monomer, and I am hoping to get some answers/trends once I include all response data to JMP. But I think this may be the effect of a lurking variable. The sample itself is unstable (as you can see from sample#111 with ~30%. Ideal sample would be 100%).

It could be due to the measurement error or these factors are just not the right choice for this sample.

Perhaps these factors and levels are not the most optimal conditions.

I need to do more analysis on this data but thank you for providing me with your feedback!

if the sample is unstable, is the time between the end of the run and the measurement constant?

The choice of factors, in terms of finding effects, is obviously critical. Perhaps a 'wider net' following brainstorming or review of a process map or the chemical reaction could identify other factors. it is too easy (i.e., it happens all the time) to think you know more than you really know because your understanding is based on OFAT data or anecdotal experience. One purpose of the experiment is to realistically explore as many variables in 'the system' as you can to learn how it actually works. I have been teaching and helping users with DOE for decades and it is the exception in just my experience that the results fail to surprise, to challenge what is know.

I am not sure what you mean when you say, "", but your DOE space should provoke a change in the response for better and for worse. You want to model the range of the response. The experiment is NOT about finding the optimal conditions or 'pick the winner' among the treatments. It is about providing the best data you can afford to support the estimation of the model parameters. The model is about finding the optimal conditions. Again, I might have misinterpreted your meaning.

Hello P_Bartell,

Thank you for your response!

Yes you are correct. In this study, zero values meaning total absence from the trial. 

The team wanted to see if we can improve the sample % monomer by introducing either all three combinations (with various concentrations), two combinations or just one factor to the sample. We had one experiment last time where the sodium chloride actually improved the % monomer of the sample, but the outcome was 50% monomer at 500mM NaCl, about 47% at 150mM NaCl from 20% monomer without salt addition. 100mM NaCl to the sample last time gave us about 38% monomer (slight improvement from 20%). The team was also interested to see if there is any relationship between two factors (or all three).

I wonder f the team selected the incorrect concentration for each factor for this experiment.

Thank you for your feedback!

I'm not sure I follow the sequence of factor levels in the "...one experiment last time..." but it sure sounds like 'the team?' may have been trying a little OFAT experimentation and making conclusions after each run...kind of chasing something that would be much more fruitful (efficiency chief among 'em) using a rational DOE approach? This OFAT approach can be very misleading especially with systems where interactions abound.

I was never a big fan of having chemical based experiments/systems where a factor was set to 'zero' in the way in which you describe. Too often this absence of 'something' created large non linearities in the response space we were really interested in, making linear modeling methods problematic.