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by chrisamiller
1261 days ago
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That's a pretty expansive statement. Are you doing error-corrected sequencing to look for rare mosaic variants? Do you care about transcripts expressed at very low levels? Are you trying to tease apart subclonal variation in cancer? All of these could be good reasons to sequence deeply. If anything, I see the opposite problem much more frequently: People who cheap out on the sequencing depth, neutering their statistical power! |
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