You signed in with another tab or window. Reload to refresh your session.You signed out in another tab or window. Reload to refresh your session.You switched accounts on another tab or window. Reload to refresh your session.Dismiss alert
I’m planning to use the WisecondorX tool for analyzing 30,000 genomes. However, I don’t initially know whether there are samples with aneuploidy in this dataset.
Should I create the reference from all 30,000 samples and then make predictions based on that reference? Or would it be better to manually select 20-100 normal samples first and create the reference from them?
The text was updated successfully, but these errors were encountered:
I’m planning to use the WisecondorX tool for analyzing 30,000 genomes. However, I don’t initially know whether there are samples with aneuploidy in this dataset.
Should I create the reference from all 30,000 samples and then make predictions based on that reference? Or would it be better to manually select 20-100 normal samples first and create the reference from them?
The text was updated successfully, but these errors were encountered: