Our PCR protocol requires nested PCR in order to be more sensitive. We would like to amplicon sequence such nested PCR fragments but we were wondering how much 'bias' it would be introduced by the second round PCR? Would this favor amplification of major variants and 'elimination' of the minors just because of the frequency of each variant, thus reducing the complexity (number of haplotypes) after deep sequencing?
Has anyone tryed amplicon sequence nested amplicons?
Is it recommended by Roche?
Has anyone tryed amplicon sequence nested amplicons?
Is it recommended by Roche?
Comment