(BO/764/20) Funder: Bolyai János Kutatási Ösztöndíj
(K134968)
Streptococcus pyogenes Cas9 (SpCas9) nuclease exhibits considerable position-dependent
sequence preferences. The reason behind these preferences is not well understood and
is difficult to rationalise, since the protein establishes interactions with the target-spacer
duplex in a sequence-independent manner. We revealed here that intramolecular interactions
within the single guide RNA (sgRNA), between the spacer and the scaffold, cause most
of these preferences. By using in cellulo and in vitro SpCas9 activity assays with
systematically designed spacer and scaffold sequences and by analysing activity data
from a large SpCas9 sequence library, we show that some long (>8 nucleotides) spacer
motifs, that are complementary to the RAR unit of the scaffold, interfere with sgRNA
loading, and that some motifs of more than 4 nucleotides, that are complementary to
the SL1 unit, inhibit DNA binding and cleavage. Furthermore, we show that intramolecular
interactions are present in the majority of the inactive sgRNA sequences of the library,
suggesting that they are the most important intrinsic determinants of the activity
of the SpCas9 ribonucleoprotein complex. We also found that in pegRNAs, sequences
at the 3′ extension of the sgRNA that are complementary to the SL2 unit are also inhibitory
to prime editing, but not to the nuclease activity of SpCas9.
