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Discovery of novel, highly potent and selective beta-hairpin mimetic CXCR4 inhibitors with excellent anti-HIV activity and pharmacokinetic profiles |
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| Authors: | DeMarco Steven J Henze Heiko Lederer Alexander Moehle Kerstin Mukherjee Reshmi Romagnoli Barbara Robinson John A Brianza Federico Gombert Frank O Lociuro Sergio Ludin Christian Vrijbloed Jan Willem Zumbrunn Jürg Obrecht Jean-Pierre Obrecht Daniel Brondani Vincent Hamy François Klimkait Thomas |
| Affiliation: | aChemistry Department, University of Zürich, Winterthurerstrasse 190, 8057 Zürich, Switzerland bPolyphor AG, CH-4123 Allschwil, Switzerland cInPheno AG, CH-4051 Basel, Switzerland |
| Abstract: | Novel highly potent CXCR4 inhibitors with good pharmacokinetic properties were designed and optimized starting from the naturally occurring β-hairpin peptide polyphemusin II. The design involved incorporating important residues from polyphemusin II into a macrocyclic template-bound β-hairpin mimetic. Using a parallel synthesis approach, the potency and ADME properties of the mimetics were optimized in iterative cycles, resulting in the CXCR4 inhibitors POL2438 and POL3026. The inhibitory potencies of these compounds were confirmed in a series of HIV-1 invasion assays in vitro. POL3026 showed excellent plasma stability, high selectivity for CXCR4, favorable pharmacokinetic properties in the dog, and thus has the potential to become a therapeutic compound for application in the treatment of HIV infections (as an entry inhibitor), cancer (for angiogenesis suppression and inhibition of metastasis), inflammation, and in stem cell transplant therapy. |
| Keywords: | CXCR4 inhibitor Peptide Protein epitope mimetics Drug design |
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