Design and synthesis of conformationally constrained amino acids as versatile scaffolds and peptide mimetics

Hanessian, Stephen; McNaughton‐Smith, Grant; Lombart, Henry‐Georges; Lubell, William D.

doi:10.1016/s0040-4020(97)00476-6

Cited by 602 publications

(327 citation statements)

References 116 publications

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“…Indolizidine-2-one and -9-one amino acids, representing 6,5 and 5,6 scaffolds, were used as β-turn scans to explore the conformational requirements for activity of analogues of Calcitonin-gene related peptide (CGRP) antagonist, together with aza-aminoacid scans [32]. The importance of a type II' β-turn centered at Gly 33 [27][28][29][30][31][32][33][34][35][36][37] has been illustrated by increased antagonistic potency of the azaGly 33 and indolizidine-2-one amino acid [33][34] analogues. In addition, the improved metabolic stability and longer duration of action qualifies those scans to be another peptidomimetic research tool.…”

Section: Conformationally Restricted β-Turn Dipeptide Mimeticsmentioning

confidence: 99%

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Peptidomimetics, a synthetic tool of drug discovery

Vagner

Hruby

2008

Current Opinion in Chemical Biology

479

302

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SummaryThe demand for modified peptides with improved stability profiles and pharmacokinetic properties is driving extensive research effort in this field. Many structural modifications of peptides guided by rational design and molecular modeling have been established to develop novel synthetic approaches. Recent advances in the synthesis of conformationally restricted building blocks and peptide bond isosteres are discussed.

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Section: Conformationally Restricted β-Turn Dipeptide Mimeticsmentioning

confidence: 99%

“…In addition, the improved metabolic stability and longer duration of action qualifies those scans to be another peptidomimetic research tool. The older reviews [33,34] related to azabicycloalkane scaffolds provide a general overview of synthetic and conformational possibilities.…”

Section: Conformationally Restricted β-Turn Dipeptide Mimeticsmentioning

confidence: 99%

Peptidomimetics, a synthetic tool of drug discovery

Vagner

Hruby

2008

Current Opinion in Chemical Biology

479

302

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“…The synthesis of conformationally constrained β-turn mimics with native-like side chains is hampered by the expense of designing an oligocyclic scaffold that is adequately protected for solid-phase peptide synthesis (13). Polyhydroxylated dipeptides with diversified stereochemistries can be obtained from uronolactones in a straightforward way (14,15).…”

Section: Resultsmentioning

confidence: 99%

Structural characterization of a β-turn mimic within a protein–protein interface

Eckhardt

Große

Essen

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

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β-turns are secondary structure elements not only exposed on protein surfaces, but also frequently found to be buried in protein–protein interfaces. Protein engineering so far considered mainly the backbone-constraining properties of synthetic β-turn mimics as parts of surface-exposed loops. A β-turn mimic, Hot═Tap, that is available in gram amounts, provides two hydroxyl groups that enhance its turn-inducing properties besides being able to form side-chain-like interactions. NMR studies on cyclic hexapeptides harboring the Hot═Tap dipeptide proved its strong β-turn-inducing capability. Crystallographic analyses of the trimeric fibritin-foldon/Hot═Tap hybrid reveal at atomic resolution how Hot═Tap replaces a βI’-turn by a βII’-type structure. Furthermore, Hot═Tap adapts to the complex protein environment by participating in several direct and water-bridged interactions across the foldon trimer interface. As building blocks, β-turn mimics capable of both backbone and side-chain mimicry may simplify the design of synthetic proteins.

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“…Bicyclic dipeptide mimetics have been designed and synthesized in this area for over ten years. 9,10 Previous studies have found that a [5,5]-bicyclic mimetic could approximate a type II ␤-turn, 11,12 a [6,5]-bicyclic could closely mimic a type IIЈ ␤-turn, 12,13 while a [7,5]-bicyclic structure can lead to different reverse turn structures depending on the chirality. 14 However, introduction of these bicyclic scaffolds into peptides has been quite limited because multistep syntheses were required, but were difficult to accomplish.…”

Section: Introductionmentioning

confidence: 99%

Parallel synthesis and biological evaluation of different sizes of bicyclo^[2,3]‐Leu‐enkephalin analogues

Gu¹,

Ying²,

Min³

et al. 2005

Biopolymers

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Design and synthesis of conformationally constrained amino acids as versatile scaffolds and peptide mimetics

Cited by 602 publications

References 116 publications

Peptidomimetics, a synthetic tool of drug discovery

Peptidomimetics, a synthetic tool of drug discovery

Structural characterization of a β-turn mimic within a protein–protein interface

Parallel synthesis and biological evaluation of different sizes of bicyclo^[2,3]‐Leu‐enkephalin analogues

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Design and synthesis of conformationally constrained amino acids as versatile scaffolds and peptide mimetics

Cited by 602 publications

References 116 publications

Peptidomimetics, a synthetic tool of drug discovery

Peptidomimetics, a synthetic tool of drug discovery

Structural characterization of a β-turn mimic within a protein–protein interface

Parallel synthesis and biological evaluation of different sizes of bicyclo[2,3]‐Leu‐enkephalin analogues

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Parallel synthesis and biological evaluation of different sizes of bicyclo^[2,3]‐Leu‐enkephalin analogues