2018
DOI: 10.1021/acsmedchemlett.8b00204
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Target-Directed Self-Assembly of Homodimeric Drugs Against β-Tryptase

Abstract: Tryptase, a serine protease released from mast cells, is implicated in many allergic and inflammatory disorders. Human tryptase is a donut-shaped tetramer with the active sites facing inward forming a central pore. Bivalent ligands spanning two active sites potently inhibit this configuration, but these large compounds have poor drug-like properties. To overcome some of these challenges, we developed self-assembling molecules, called coferons, which deliver a larger compound in two parts. Using a pharmacophori… Show more

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Cited by 6 publications
(29 citation statements)
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“…By reversibly joining two small molecules through bio-orthogonal linkers, coferons enable the delivery of larger, more specific, and higher-affinity dimeric molecules. 5,6 The coferon chemistry platform employs bio-orthogonal linker chemistries that allow the intracellular self-assembly of two distinct small molecule monomers, composed of a ligand, a connector, and a linker element, into a large dimeric inhibitor molecule designed to be capable of more potent and selective inhibition. This study confirms that polyvalent binding increases the affinity and specificity of interactions between molecules, 13 where a number of self-assembled heterodimeric tryptase inhibitors demonstrate marked improvements over the activity of their monomeric parts.…”
Section: ■ Discussion and Conclusionmentioning
confidence: 99%
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“…By reversibly joining two small molecules through bio-orthogonal linkers, coferons enable the delivery of larger, more specific, and higher-affinity dimeric molecules. 5,6 The coferon chemistry platform employs bio-orthogonal linker chemistries that allow the intracellular self-assembly of two distinct small molecule monomers, composed of a ligand, a connector, and a linker element, into a large dimeric inhibitor molecule designed to be capable of more potent and selective inhibition. This study confirms that polyvalent binding increases the affinity and specificity of interactions between molecules, 13 where a number of self-assembled heterodimeric tryptase inhibitors demonstrate marked improvements over the activity of their monomeric parts.…”
Section: ■ Discussion and Conclusionmentioning
confidence: 99%
“…A solution of 40 in MeCN (65 mL) was charged with TFA (10 mL) and stirred at RT for 12 h. The reaction mixture was concentrated in vacuo and purified by reverse-phase HPLC, resulting in a TFA salt that was subsequently converted into the HCl salt by stirring the pure product in 2 N HCl for 30 min under a N 2 atmosphere and lyophilized to dryness, which resulted in 81% yield of 9s. Synthesis of [3][4][5]phenyl]piperidine-1carbonyl]-2,3-dimethylphenyl]phenyl]boronic Acid (10a) and [3][4][5]…”
Section: Synthesis Of 5-[4-[3-(aminomethylmentioning
confidence: 99%
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