Sensor dimer disruption as a new mode of action to block the IRE1-mediated unfolded protein response

“…The lysine residue is not present in the same position in RNase L, making such Lysine-based covalent-targeting approach selective for IRE1. Furthermore, a docking study addressing the dimer interface of the RNase domain identified neomycin (IC 50 0.33 μM) as an IRE1 inhibitor …”

“…Furthermore, a docking study addressing the dimer interface of the RNase domain identified neomycin (IC 50 0.33 μM) as an IRE1 inhibitor. 112 ■ BIFUNCTIONAL MOLECULES TARGETING RNASES Bifunctional Dicer Inhibitors. An emerging approach to target ribonucleases is the design of bifunctional molecules to activate, bind, or inhibit an RNase in a specific context (Figure 7).…”

“…Thus, IRE1 activity is associated with cancer progression, aggressiveness, and poor prognosis. − In addition to being studied as an anticancer target, IRE1 has also been implicated in diabetes and angiogenesis regulation. , IRE1-targeting modulators were developed against the kinase and RNase domains (Figure ). Similar to RNase L, reported kinase inhibitors were repurposed for IRE1 inhibition. , Interestingly, some kinase inhibitors did not inhibit RNase function but activated IRE1 RNase activity instead. ,, In general, type I kinase inhibitors stabilized the active kinase conformation and activated IRE1 RNase activity promoting oligomerization, while type II kinase inhibitors stabilized the inactive kinase conformation and inhibited RNase enzymatic activities. ,, Assays for the identification of IRE1 modulators comprise splicing assays, fluorescence-based cleavage assays using fluorophore- and quencher-labeled XBP1 RNA substrate, and phosphorylation assays that focused on kinase activity instead of RNase activity. ,,, IRE1 inhibitor imidazo­[1,5-α]­pyrazine-8-amine compound 3 was identified based on screening of known type II kinase inhibitors, and further modification led to the development of compounds KIRA6 and KIRA7. ,, Both KIRA6 and KIRA7 were potent inhibitors in biochemical and cellular evaluations, but a photoaffinity labeling approach revealed low selectivity of the imidazo­[1,5-α]­pyrazine-8-amine scaffold toward IRE1. ,, The sulfonamide KIRA8 was an optimized hit with an IC 50 of 0.014 μM in biochemical assays, but it did not affect cancer cell viability when screened against more than 300 different cancer cell lines. , GSK2850163 is a screening-identified selective IRE1 inhibitor that bound to the kinase domain and displaced the kinase activation loop, thereby inhibiting RNase activity with an IC 50 of 200 nM . Compound 31 was further identified as an IRE1-selective inhibitor (IC 50 80 nM) that stabilized the inactive kinase conformation allosterically .…”

Targeting Ribonucleases with Small Molecules and Bifunctional Molecules

“…The lysine residue is not present in the same position in RNase L, making such Lysine-based covalent-targeting approach selective for IRE1. Furthermore, a docking study addressing the dimer interface of the RNase domain identified neomycin (IC 50 0.33 μM) as an IRE1 inhibitor …”

“…Furthermore, a docking study addressing the dimer interface of the RNase domain identified neomycin (IC 50 0.33 μM) as an IRE1 inhibitor. 112 ■ BIFUNCTIONAL MOLECULES TARGETING RNASES Bifunctional Dicer Inhibitors. An emerging approach to target ribonucleases is the design of bifunctional molecules to activate, bind, or inhibit an RNase in a specific context (Figure 7).…”

“…Thus, IRE1 activity is associated with cancer progression, aggressiveness, and poor prognosis. − In addition to being studied as an anticancer target, IRE1 has also been implicated in diabetes and angiogenesis regulation. , IRE1-targeting modulators were developed against the kinase and RNase domains (Figure ). Similar to RNase L, reported kinase inhibitors were repurposed for IRE1 inhibition. , Interestingly, some kinase inhibitors did not inhibit RNase function but activated IRE1 RNase activity instead. ,, In general, type I kinase inhibitors stabilized the active kinase conformation and activated IRE1 RNase activity promoting oligomerization, while type II kinase inhibitors stabilized the inactive kinase conformation and inhibited RNase enzymatic activities. ,, Assays for the identification of IRE1 modulators comprise splicing assays, fluorescence-based cleavage assays using fluorophore- and quencher-labeled XBP1 RNA substrate, and phosphorylation assays that focused on kinase activity instead of RNase activity. ,,, IRE1 inhibitor imidazo­[1,5-α]­pyrazine-8-amine compound 3 was identified based on screening of known type II kinase inhibitors, and further modification led to the development of compounds KIRA6 and KIRA7. ,, Both KIRA6 and KIRA7 were potent inhibitors in biochemical and cellular evaluations, but a photoaffinity labeling approach revealed low selectivity of the imidazo­[1,5-α]­pyrazine-8-amine scaffold toward IRE1. ,, The sulfonamide KIRA8 was an optimized hit with an IC 50 of 0.014 μM in biochemical assays, but it did not affect cancer cell viability when screened against more than 300 different cancer cell lines. , GSK2850163 is a screening-identified selective IRE1 inhibitor that bound to the kinase domain and displaced the kinase activation loop, thereby inhibiting RNase activity with an IC 50 of 200 nM . Compound 31 was further identified as an IRE1-selective inhibitor (IC 50 80 nM) that stabilized the inactive kinase conformation allosterically .…”

Targeting Ribonucleases with Small Molecules and Bifunctional Molecules

“…Small-molecule mediated modulation of IRE1 activity has been achieved by compounds targeting either the ATP-binding kinase pocket, the RNase domain 4 or allosteric sites 5 . Studies have demonstrated that Kinase inhibiting RNase attenuators (KIRAs) that binds the kinase pocket have a direct inhibitory effect on IRE1 RNase activity 6,7 .…”

A novel blood brain barrier-permeable IRE1 kinase inhibitor for adjuvant glioblastoma treatment in mice.

“…IRE1 RNase domain then channels the functional outputs of IRE1 by unconventionally splicing XBP1 mRNA to produce XBP1s, a potent transcription factor, or by cleaving a subset of mRNAs and miRNAs in a process called Regulated IRE1 Dependent Decay (of RNA). Inhibiting IRE1 activity can thus be achieved by compounds targeting the ATP-binding kinase pocket, the RNase domain (3) or targeting other domains (4). Studies have demonstrated that Kinase inhibiting RNase attenuators (KIRAs) may have an inhibitory effect on IRE1 RNase activity (5,6).…”

A novel blood brain barrier-permeable IRE1 kinase inhibitor for adjuvant glioblastoma treatment in mice.