Substrates and Cyclic Peptide Inhibitors of the Oligonucleotide‐Activated Sirtuin 7**

Abstract: The sirtuins are NAD+‐dependent lysine deacylases, comprising seven isoforms (SIRT1–7) in humans, which are involved in the regulation of a plethora of biological processes, including gene expression and metabolism. The sirtuins share a common hydrolytic mechanism but display preferences for different ε‐N‐acyllysine substrates. SIRT7 deacetylates targets in nuclei and nucleoli but remains one of the lesser studied of the seven isoforms; in part, due to a lack of chemical tools to specifically probe SIRT7 activ… Show more

“…HEK293T cells treated with Compound 41 demonstrated increased acetylation of the Sirt7 substrate histone H3K18, consistent with on-target cellular Sirt7 inhibition [ 241 ]. Compound 41 represents a substantial improvement in Sirt7 inhibitor potency and sirtuin isoform specificity [ 237 , 241 ]. Therefore, Compound 41 demonstrates that peptide lariats are an exciting new avenue for sirtuin inhibitors, especially since their precise mode of sirtuin inhibition is unknown [ 241 ].…”

“…This screen generated two cyclic peptide inhibitors with trifluoroacetyl-lysine warheads that inhibited Sirt2 with IC 50 values of 3.2–3.7 nM and demonstrated ~9–150-fold selectivity for Sirt2 over Sirt1/3 [ 239 ]. Recently, the same cell-free translation peptide screen used to identify the first cyclic peptide inhibitors [ 239 ] was employed to develop non-mechanism-based cyclic peptide and peptide lariat sirtuin inhibitors [ 241 ]. Peptide lariat Compound 41 ( Figure 6 ) was found to be a novel Sirt7 inhibitor (IC 50 = 2.7 μM) that exhibited ~55-fold selectivity for Sirt7 over Sirt6, with minimal impacts on Sirt1/2/3/5 at 10 μM [ 241 ].…”

“…Recently, the same cell-free translation peptide screen used to identify the first cyclic peptide inhibitors [ 239 ] was employed to develop non-mechanism-based cyclic peptide and peptide lariat sirtuin inhibitors [ 241 ]. Peptide lariat Compound 41 ( Figure 6 ) was found to be a novel Sirt7 inhibitor (IC 50 = 2.7 μM) that exhibited ~55-fold selectivity for Sirt7 over Sirt6, with minimal impacts on Sirt1/2/3/5 at 10 μM [ 241 ]. HEK293T cells treated with Compound 41 demonstrated increased acetylation of the Sirt7 substrate histone H3K18, consistent with on-target cellular Sirt7 inhibition [ 241 ].…”

“…Peptide lariat Compound 41 ( Figure 6 ) was found to be a novel Sirt7 inhibitor (IC 50 = 2.7 μM) that exhibited ~55-fold selectivity for Sirt7 over Sirt6, with minimal impacts on Sirt1/2/3/5 at 10 μM [ 241 ]. HEK293T cells treated with Compound 41 demonstrated increased acetylation of the Sirt7 substrate histone H3K18, consistent with on-target cellular Sirt7 inhibition [ 241 ]. Compound 41 represents a substantial improvement in Sirt7 inhibitor potency and sirtuin isoform specificity [ 237 , 241 ].…”

Current Trends in Sirtuin Activator and Inhibitor Development

“…HEK293T cells treated with Compound 41 demonstrated increased acetylation of the Sirt7 substrate histone H3K18, consistent with on-target cellular Sirt7 inhibition [ 241 ]. Compound 41 represents a substantial improvement in Sirt7 inhibitor potency and sirtuin isoform specificity [ 237 , 241 ]. Therefore, Compound 41 demonstrates that peptide lariats are an exciting new avenue for sirtuin inhibitors, especially since their precise mode of sirtuin inhibition is unknown [ 241 ].…”

“…This screen generated two cyclic peptide inhibitors with trifluoroacetyl-lysine warheads that inhibited Sirt2 with IC 50 values of 3.2–3.7 nM and demonstrated ~9–150-fold selectivity for Sirt2 over Sirt1/3 [ 239 ]. Recently, the same cell-free translation peptide screen used to identify the first cyclic peptide inhibitors [ 239 ] was employed to develop non-mechanism-based cyclic peptide and peptide lariat sirtuin inhibitors [ 241 ]. Peptide lariat Compound 41 ( Figure 6 ) was found to be a novel Sirt7 inhibitor (IC 50 = 2.7 μM) that exhibited ~55-fold selectivity for Sirt7 over Sirt6, with minimal impacts on Sirt1/2/3/5 at 10 μM [ 241 ].…”

“…Recently, the same cell-free translation peptide screen used to identify the first cyclic peptide inhibitors [ 239 ] was employed to develop non-mechanism-based cyclic peptide and peptide lariat sirtuin inhibitors [ 241 ]. Peptide lariat Compound 41 ( Figure 6 ) was found to be a novel Sirt7 inhibitor (IC 50 = 2.7 μM) that exhibited ~55-fold selectivity for Sirt7 over Sirt6, with minimal impacts on Sirt1/2/3/5 at 10 μM [ 241 ]. HEK293T cells treated with Compound 41 demonstrated increased acetylation of the Sirt7 substrate histone H3K18, consistent with on-target cellular Sirt7 inhibition [ 241 ].…”

“…Peptide lariat Compound 41 ( Figure 6 ) was found to be a novel Sirt7 inhibitor (IC 50 = 2.7 μM) that exhibited ~55-fold selectivity for Sirt7 over Sirt6, with minimal impacts on Sirt1/2/3/5 at 10 μM [ 241 ]. HEK293T cells treated with Compound 41 demonstrated increased acetylation of the Sirt7 substrate histone H3K18, consistent with on-target cellular Sirt7 inhibition [ 241 ]. Compound 41 represents a substantial improvement in Sirt7 inhibitor potency and sirtuin isoform specificity [ 237 , 241 ].…”

Current Trends in Sirtuin Activator and Inhibitor Development

“…We also performed Western blot-based cellular thermal shift assays (CETSA), , which we have previously used for investigating inhibitors targeting sirtuins (NAD + -dependent class III HDACs). − Because HDAC11 has very low expression levels in most cell lines, we were not able to produce a viable melting curve for this enzyme. Thus, we tested the most potent HDAC6 inhibitor of our collection ( E24 ).…”

Sulfur(VI) Fluoride Exchange Chemistry in Solid-Phase Synthesis of Compound Arrays: Discovery of Histone Deacetylase Inhibitors

Unraveling the multifaceted role of SIRT7 and its therapeutic potential in human diseases