Strain-promoted azide–alkyne cycloadditions (SPAAC) are widely used for labeling azide-functionalized
biomolecules in living cells but create mixtures of isomeric triazoles. We recently
expanded the scope of SPAAC to the isomer-free generation of large functional molecules
in living cells by designing the symmetrical pyrrolocyclooctynes PYRROC and SYPCO,
which do not form isomers in SPAAC. Here, we present the synthesis and kinetic characterization
of the cyclooctyne TRIPCO as a new reagent for isomer-free SPAAC (iSPAAC). TRIPCO
was found to react faster than PYRROC and SYPCO in the [3+2] cycloaddition with benzyl
azide.
Key words
bioorthogonal chemistry - cycloalkynes - isomer-free SPAAC - cycloaddition - azides