Did someone try the XGen blocking oligo from IDT instead of classical blocking oligos ? Is there a improvement of the off target ?
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Hi, thank you for your answer.
I understand that you use dual indexing.
My first question is : Did you try specific Xgen blocker or the universal one for Illumina HT libraries ?
My second one : what was the on-target before using the Xgen blocker ? Is there an improvement by using it ?
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Thanks superduper,
I'm doing to setup pre indexing hybridization method and test xGen IDT oligo blocks.
I'm happy to meet you here.
I am a little of bit surprised that on-target rate of perfect complementary blocking oligo was lower than xGen.
Conceptually some idea maybe was in synthesis of oligo for blocking.
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Originally posted by superduperI was using one barcode per library.
1. I used the universal 8nt blocking oligo (mix of TS-p5 and TS-p7(8nt))
2. my on-targets were:
single capture; barcoding happens after hyb step (basically XT protocol): 70%
XGen blocking: 58-73%
Inosines instead of barcode location: up to 33%
perfect complement: 45%
random nucleotides: up to 35%
This is for PE37 sequencing. To compare samples where I had run reads longer, I clipped them back to PE37 to have a fair comparison between different conditions.
Your % on-target will increase the longer your read lengths are; I saw PE101 of 82% translate to 69% when I clipped it to PE37.
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