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Literature DB >> 2377603

Folding and activity of hybrid sequence, disulfide-stabilized peptides.

Abstract

Peptides have been synthesized that have hybrid sequences, partially derived from the bee venom peptide apamin and partially from the S peptide of ribonuclease A. The hybrid peptides were demonstrated by NMR spectroscopy to fold, forming the same disulfides and basic three-dimensional structure as native apamin, containing a beta-turn and an alpha-helix. These hybrids were active in complementing S protein, reactivating nuclease activity. In addition, the hybrid peptide was effective in inducing antibodies that cross-react with the RNase, without conjugation to a carrier protein. The stability of the folded structure of this peptide suggests that it should be possible to elicit antibodies that will react not only with a specific sequence, but also with a specific secondary structure. Hybrid sequence peptides also provide opportunities to study separately nucleation and propagation steps in formation of secondary structure. We show that in S peptide the alpha-helix does not end abruptly but rather terminates gradually over four or five residues. In general, these hybrid sequence peptides, which fold predictably because of disulfide bond formation, can provide opportunities for examining structure-function relationships for many biologically active sequences.

Entities: Chemical

Mesh：

Substances：

Year: 1990 PMID： 2377603 PMCID： PMC54383 DOI： 10.1073/pnas.87.15.5643

Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN： 0027-8424 Impact factor: 11.205

22 in total

1. Protein structures in solution by nuclear magnetic resonance and distance geometry. The polypeptide fold of the basic pancreatic trypsin inhibitor determined using two different algorithms, DISGEO and DISMAN.

Authors: G Wagner; W Braun; T F Havel; T Schaumann; N Go; K Wüthrich
Journal: J Mol Biol Date: 1987-08-05 Impact factor: 5.469

2. Helix-coil transition of the isolated amino terminus of ribonuclease.

Authors: J E Brown; W A Klee
Journal: Biochemistry Date: 1971-02-02 Impact factor: 3.162

3. Enzymatically active angiogenin/ribonuclease A hybrids formed by peptide interchange.

Authors: J W Harper; D S Auld; J F Riordan; B L Vallee
Journal: Biochemistry Date: 1988-01-12 Impact factor: 3.162

4. Low-temperature 1H-NMR evidence of the folding of isolated ribonuclease S-peptide.

Authors: M Rico; J L Nieto; J Santoro; F J Bermejo; J Herranz; E Gallego
Journal: FEBS Lett Date: 1983-10-17 Impact factor: 4.124

5. A competing salt-bridge suppresses helix formation by the isolated C-peptide carboxylate of ribonuclease A.

Authors: P S Kim; A Bierzynski; R L Baldwin
Journal: J Mol Biol Date: 1982-11-25 Impact factor: 5.469

6. A comparative structural study of apamin and related bee venom peptides.

Authors: R C Hider; U Ragnarsson
Journal: Biochim Biophys Acta Date: 1981-01-30

7. Persistence of the alpha-helix stop signal in the S-peptide in trifluoroethanol solutions.

Authors: J W Nelson; N R Kallenbach
Journal: Biochemistry Date: 1989-06-13 Impact factor: 3.162

8. Synthesis of apamin, a neurotoxic peptide from bee venom.

Authors: J van Rietschoten; C Granier; H Rochat; S Lissitzky; F Miranda
Journal: Eur J Biochem Date: 1975-08-01

9. Use of synthetic analogs for a study on the structure-activity relationship of apamin.

Authors: C Granier; E Pedroso Muller; J Van Rietschoten
Journal: Eur J Biochem Date: 1978-01-02

10. Concept of internal structural controls for evaluation of inactive synthetic peptide analogs: synthesis of [Orn13,14]apamin and its guanidination to an apamin derivative with full neurotoxic activity.

Authors: W L Cosand; R B Merrifield
Journal: Proc Natl Acad Sci U S A Date: 1977-07 Impact factor: 11.205

5 in total

Folding and activity of hybrid sequence, disulfide-stabilized peptides.

1. Protein structures in solution by nuclear magnetic resonance and distance geometry. The polypeptide fold of the basic pancreatic trypsin inhibitor determined using two different algorithms, DISGEO and DISMAN.

2. Helix-coil transition of the isolated amino terminus of ribonuclease.

3. Enzymatically active angiogenin/ribonuclease A hybrids formed by peptide interchange.

4. Low-temperature 1H-NMR evidence of the folding of isolated ribonuclease S-peptide.

5. A competing salt-bridge suppresses helix formation by the isolated C-peptide carboxylate of ribonuclease A.

6. A comparative structural study of apamin and related bee venom peptides.

7. Persistence of the alpha-helix stop signal in the S-peptide in trifluoroethanol solutions.

8. Synthesis of apamin, a neurotoxic peptide from bee venom.

9. Use of synthetic analogs for a study on the structure-activity relationship of apamin.

10. Concept of internal structural controls for evaluation of inactive synthetic peptide analogs: synthesis of [Orn13,14]apamin and its guanidination to an apamin derivative with full neurotoxic activity.

1. The CXXC motif at the N terminus of an alpha-helical peptide.

2. The disulfide-coupled folding pathway of apamin as derived from diselenide-quenched analogs and intermediates.

3. A genetic algorithm that seeks native states of peptides and proteins.

4. Apamin as a template for structure-based rational design of potent peptide activators of p53.

5. Lybatides from Lycium barbarum Contain An Unusual Cystine-stapled Helical Peptide Scaffold.