Squash inhibitors: from structural motifs to macrocyclic knottins

In this article, we will first introduce the squash inhibitor, a well established family of highly potent canonical serine proteinase inhibitors isolated from Cucurbitaceae. The squash inhibitors were among the first discovered proteins with the typical knottin fold shared by numerous peptides extra...

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Published inCurrent protein & peptide science Vol. 5; no. 5; p. 341
Main Authors Chiche, Laurent, Heitz, Annie, Gelly, Jean-Christophe, Gracy, Jérôme, Chau, Pham T T, Ha, Phan T, Hernandez, Jean-François, Le-Nguyen, Dung
Format Journal Article
LanguageEnglish
Published United Arab Emirates 01.10.2004
Subjects
Amino Acid Sequence
Cucurbita - chemistry
Cyclization
Drug Design
Humans
Molecular Sequence Data
Protein Folding
Proteins - chemistry
Proteins - genetics
Proteins - isolation & purification
Proteins - pharmacology
Serine Proteinase Inhibitors - chemical synthesis
Serine Proteinase Inhibitors - chemistry
Serine Proteinase Inhibitors - isolation & purification
Serine Proteinase Inhibitors - pharmacology
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Summary:In this article, we will first introduce the squash inhibitor, a well established family of highly potent canonical serine proteinase inhibitors isolated from Cucurbitaceae. The squash inhibitors were among the first discovered proteins with the typical knottin fold shared by numerous peptides extracted from plants, animals and fungi. Knottins contain three knotted disulfide bridges, two of them arranged as a Cystine-Stabilized Beta-sheet motif. In contrast to cyclotides for which no natural linear homolog is known, most squash inhibitors are linear. However, Momordica cochinchinensis Trypsin Inhibitor-I and (MCoTI-I and -II), 34-residue squash inhibitors isolated from seeds of a common Cucurbitaceae from Vietnam, were recently shown to be macrocyclic. In these circular squash inhibitors, a short peptide linker connects residues that correspond to the N- and C-termini in homologous linear squash inhibitors. In this review we present the isolation, characterization, chemical synthesis, and activity of these macrocyclic knottins. The solution structure of MCoTI-II will be compared with topologically similar cyclotides, homologous linear squash inhibitors and other knottins, and potential applications of such scaffolds will be discussed.
ISSN:1389-2037
1875-5550
DOI:10.2174/1389203043379477