Literature DB >> 11375757

Macrocycles mimic the extended peptide conformation recognized by aspartic, serine, cysteine and metallo proteases.

J D Tyndall1, D P Fairlie.   

Abstract

It has been previously demonstrated that aspartic, serine, metallo and cysteine proteases bind to their inhibitors and substrate analogues in a single conformation, the saw-tooth or extended beta-strand. Consequently a generic approach to the development of protease inhibitors is the use of constraints that conformationally restrict putative inhibitor molecules to an extended form. In this way the inhibitor is pre-organized for binding to a protease and does not need to rearrange its structure. One constraining device that has proven to be effective for such pre-organization is macrocyclization. This article illustrates the general principle that macrocycles, especially those composed of 3-4 amino acids and usually 13-17 ring atoms, can effectively mimic the extended conformation of short peptide sequences. Such structure-stabilising macrocycles are stable to degradation by proteases, valuable components of potent protease inhibitors, and in many cases they are also bioavailable.

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Year:  2001        PMID: 11375757     DOI: 10.2174/0929867013372715

Source DB:  PubMed          Journal:  Curr Med Chem        ISSN: 0929-8673            Impact factor:   4.530


  19 in total

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2.  Policresulen, a novel NS2B/NS3 protease inhibitor, effectively inhibits the replication of DENV2 virus in BHK-21 cells.

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3.  β-Strand mimics based on tetrahydropyridazinedione (tpd) peptide stitching.

Authors:  Chang Won Kang; Matthew P Sarnowski; Sujeewa Ranatunga; Lukasz Wojtas; Rainer S Metcalf; Wayne C Guida; Juan R Del Valle
Journal:  Chem Commun (Camb)       Date:  2015-11-21       Impact factor: 6.222

4.  Multicomponent macrocyclization reactions (MCMRs) employing highly reactive acyl ketene and nitrile oxide intermediates.

Authors:  John M Knapp; James C Fettinger; Mark J Kurth
Journal:  Org Lett       Date:  2011-08-09       Impact factor: 6.005

5.  Putative structural rearrangements associated with the interaction of macrocyclic inhibitors with norovirus 3CL protease.

Authors:  Anushka C Galasiti Kankanamalage; Pathum M Weerawarna; Athri D Rathnayake; Yunjeong Kim; Nurjahan Mehzabeen; Kevin P Battaile; Scott Lovell; Kyeong-Ok Chang; William C Groutas
Journal:  Proteins       Date:  2019-04-01

6.  Computer modeling and nanosecond simulation of the enzyme-substrate complex of the common lymphoblastic leukemia antigen (neprilysin) indicates shared residues at the primary specificity pocket (S1') with matrix metalloproteases.

Authors:  Sergio Manzetti
Journal:  J Mol Model       Date:  2003-08-29       Impact factor: 1.810

7.  Translation of DNA into a library of 13,000 synthetic small-molecule macrocycles suitable for in vitro selection.

Authors:  Brian N Tse; Thomas M Snyder; Yinghua Shen; David R Liu
Journal:  J Am Chem Soc       Date:  2008-10-29       Impact factor: 15.419

8.  Amide Rotation Hindrance Predicts Proteolytic Resistance of Cystine-Knot Peptides.

Authors:  Yanzi Zhou; Daiqian Xie; Yingkai Zhang
Journal:  J Phys Chem Lett       Date:  2016-03-11       Impact factor: 6.475

Review 9.  Recent Advances in the Discovery of Norovirus Therapeutics.

Authors:  Yunjeong Kim; Anushka C Galasiti Kankanamalage; Kyeong-Ok Chang; William C Groutas
Journal:  J Med Chem       Date:  2015-08-17       Impact factor: 7.446

10.  Modeling of enzyme-substrate complexes for the metalloproteases MMP-3, ADAM-9 and ADAM-10.

Authors:  Sergio Manzetti; Daniel R McCulloch; Adrian C Herington; David van der Spoel
Journal:  J Comput Aided Mol Des       Date:  2003-09       Impact factor: 3.686

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