Publication | Open Access
Required Immunoproteasome Subunit Inhibition Profile for Anti-Inflammatory Efficacy and Clinical Candidate KZR-616 ((2<i>S</i>,3<i>R</i>)-<i>N</i>-((<i>S</i>)-3-(Cyclopent-1-en-1-yl)-1-((<i>R</i>)-2-methyloxiran-2-yl)-1-oxopropan-2-yl)-3-hydroxy-3-(4-methoxyphenyl)-2-((<i>S</i>)-2-(2-morpholinoacetamido)propanamido)propenamide)
97
Citations
20
References
2018
Year
ImmunologyDual Lmp7/lmp2PharmacotherapyImmunotherapySelective Immunoproteasome InhibitionInflammationMolecular PharmacologyClinical Candidate Kzr-616Inflammatory Rheumatic DiseaseAnti-inflammatory EfficacyNovel TherapyAutoimmune DiseaseAllergyPharmacological AgentAutoimmunitySubunit InhibitorsNon-peptide LigandPharmacologyInflammatory DiseaseAnti-inflammatoryPeptide TherapeuticMedicineDrug Discovery
Selective immunoproteasome inhibition is a promising approach for treating autoimmune disorders, but optimal proteolytic active site subunit inhibition profiles remain unknown. We reveal here our design of peptide epoxyketone-based selective low molecular mass polypeptide-7 (LMP7) and multicatalytic endopeptidase complex subunit-1 (MECL-1) subunit inhibitors. Utilizing these and our previously disclosed low molecular mass polypeptide-2 (LMP2) inhibitor, we demonstrate a requirement of dual LMP7/LMP2 or LMP7/MECL-1 subunit inhibition profiles for potent cytokine expression inhibition and in vivo efficacy in an inflammatory disease model. These and additional findings toward optimized solubility led the design and selection of KZR-616 disclosed here and presently in clinical trials for treatment of rheumatic disease.
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