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Hi @ploy-np, Could you give us some more insight on how to interpret the results from Without providing a KO or unmodified sample: for one NNANN, if there is a methylation on A in all treatments, is it correct that we would not be able to identify the modified site using From our understanding, we can see that in certain DRACH motifs we have differential methylation across treatments, but with the lack of a demethylated sample we were wondering if we can identify whether treatment X has a modified site and treatments Y and Z do not have a modified site, or if it were the other way around. When it comes to Thank you in advance! |
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Replies: 2 comments
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Hi Alex, Sorry for the late reply! Yes, Still, it is possible to identify that a site is differentially modified in treatment X but not treatments Y and Z, for xpore does every pairwise comparison between the treatments (X vs Y, X vs. Z, and Y vs. Z). You will have to see whether the differential methylation magnitude A “lower” Best wishes, |
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Hello @yuukiiwa! We are familiar with When it comes to differentially modified between treatments, yes, that is what we initially understood. However, when you refer to whether the differential methylation magnitude between conditions being large enough, is this in reference to what you state in your publication "we first selected those differentially modified sites with effect size >0.5 and P value <0.001"? When you refer to effect size, is it Kind regards, |
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Hi Alex,
Sorry for the late reply!
Yes,
xpore
will not be able to identify the modification site if the same site is methylated across all treatments. To identify the non-differentially expressed m6A sites, we suggest runningm6anet
(https://github.com/GoekeLab/m6anet), which can detect m6A directly from a single sample, on all your samples and compare the m6anet results from there.Still, it is possible to identify that a site is differentially modified in treatment X but not treatments Y and Z, for xpore does every pairwise comparison between the treatments (X vs Y, X vs. Z, and Y vs. Z). You will have to see whether the differential methylation magnitude
diff_mod_rate_<condition1>_vs_<…