Table 1.
Summary of the most broadly applied secondary structure probing methods. Different techniques may fit best for different applications.
| Technique | Type | Pro | Contra | Reagent |
|---|---|---|---|---|
| PARS [10] | enzymatic | digests paired/unpaired bases; suited for riboswitches; transcriptome | poly(A) selected; over-digestion of RNA; in vitro | ssRNase S1 dsRNase V1 |
| Fraq-Seq [13] | enzymatic | P1 is thermal stable; transcriptome | control needed; for smaller RNA molecules; poly(A) selection; in vitro | ssRNAase P1 |
| DMS-Seq [14,16] | chemical | in vitro/in vivo; DMS cell permeable; transcriptome in vivo | poly(A) selection; needs control sample; RBPs influence; in vivo | DMS |
| SHAPE [18] | chemical | single nucleotide resolution; multiple RNA profiling | in vitro; needs control sample | IM7, NMIA, NAI-N3, FAI |
| IcSHAPE [22] | chemical | in vivo; single nucleotide resolution; transcriptome | influenced by RBP binding | IM7, NMIA, NAI-N3, FAI |