A comparison of folding techniques in the chemical synthesis of the epidermal growth factor-like domain in neu differentiation factor alpha/beta

Autor:	T J, Zamborelli, W S, Dodson, B J, Harding, J, Zhang, B D, Bennett, D M, Lenz, Y, Young, M, Haniu, C F, Liu, T, Jones, M A, Jarosinski
Rok vydání:	2000
Předmět:	Peptide Biosynthesis Protein Folding Time Factors Epidermal Growth Factor Sequence Homology Amino Acid Neuregulin-1 Molecular Sequence Data Mass Spectrometry Protein Structure Tertiary Amino Acid Sequence Cysteine Disulfides Amino Acids Peptides Chromatography High Pressure Liquid
Zdroj:	The journal of peptide research : official journal of the American Peptide Society. 55(5)
ISSN:	1397-002X
Popis:	The 52-residue alpha/beta chimera of the epidermal growth factor-like domain in neu differentiation factor (NDFealpha/beta) has been synthesized and folded to form a three disulfide bridge (Cys182-Cys196, Cys190-Cys210, Cys212-Cys221) containing peptide. We investigated two general strategies for the formation of the intramolecular disulfide bridges including, the single-step approach, which used fully deprotected and reduced peptide, and a sequential approach that relied on orthogonal cysteine protection in which specific pairs are excluded from the first oxidation step. Because there are 15 possible disulfide bridge arrangements in a peptide with six cysteines, the one-step approach may not always provide the desired disulfide pairing. Here, we compare the single-step approach with a systematic evaluation of the sequential approach. We employed the acetamidomethyl group to protect each pair of cysteines involved in disulfide bridges, i.e. Cys182 to Cys196, Cys190 to Cys210 and Cys212 to Cys221. This reduced the number of possible disulfide patterns from 15 to three in the first folding step. We compared the efficiencies of folding for each protected pair using RP-HPLC, mapped the disulfide connectivity of the predominant product and then formed the final disulfide from the partially folded intermediate via 12 oxidation. Only the peptide having the Cys182-Cys196 pair blocked with acetamidomethyl forms the desired disulfide isomer (Cys190-Cys210/Cys212-Cys221) as a single homogeneous product. By optimizing both approaches, as well as other steps in the synthesis, we can now rapidly provide large-scale syntheses of NDFealpha/beta and other novel EGF-like peptides.
Databáze:	OpenAIRE
Externí odkaz:	https://explore.openaire.eu/search/publication?articleId=pmid________::1ad7ae19b8bc92f8e3c738e21f565cbc https://pubmed.ncbi.nlm.nih.gov/10863933 Zobrazit plný text záznamu Plný text