Putative Folding Pathway of Insulin-like Growth Factor-I

Putative Folding Pathway of Insulin-like Growth Factor-I

Insulin-like growth factor-1 (IGF-I) has three disulfide bonds and refolding of the fully reduced molecule generates varying ratios of correctly (PII) and incorrectly (PI) folded forms via several intermediates. All of the intermediates have the disulfide bond between Cys18 and 61 formed, indicating...

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Veröffentlicht in:Archives of biochemistry and biophysics 1997-06, Vol.342 (2), p.298-305
Hauptverfasser: Rosenfeld, Robert D., Miller, James A., Narhi, Linda O., Hawkins, Nessa, Katta, Viswanatham, Lauren, Scott, Weiss, Michael A., Arakawa, Tsutomu
Format: Artikel
Sprache:eng
Schlagworte:
Chromatography, High Pressure Liquid
Copper Sulfate - pharmacology
Disulfides - chemistry
Disulfides - metabolism
Glutathione - analogs & derivatives
Glutathione - pharmacology
Glutathione Disulfide
Insulin-Like Growth Factor I - chemistry
Insulin-Like Growth Factor I - metabolism
Oxidation-Reduction
Protein Folding
Sulfhydryl Compounds - chemistry
Sulfhydryl Compounds - metabolism
Trifluoroacetic Acid - pharmacology
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Zusammenfassung:Insulin-like growth factor-1 (IGF-I) has three disulfide bonds and refolding of the fully reduced molecule generates varying ratios of correctly (PII) and incorrectly (PI) folded forms via several intermediates. All of the intermediates have the disulfide bond between Cys18 and 61 formed, indicating that formation of this disulfide is the first step in refolding. In order to further understand the refolding pathway, two intermediate forms, PIII with the additional disulfide Cys(6/47) formed and PIIIawith Cys(6/48) formed, were isolated. The oxidation of the remaining Cys48 and 52 in PIII and Cys47 and 52 in PIIIawould lead to PI and PII, respectively; however, air oxidation of these resulted in a rapid reshuffling into other intermediates as well as folding into the fully oxidized forms, and this occurred whether refolding was started with PIII or PIIIa. When oxidation occurred in the presence of an excess of oxidized glutathione, the predominant species generated were various glutathione adducts regardless of the initial intermediate form, indicating that formation of the last disulfide bond is not a favorable process relative to disulfide exchange when excess disulfides from oxidized glutathione are present. Interestingly, if 80 μmcopper sulfate, an oxidant, is added to the refolding buffer, PIII resulted in formation of the PI form alone, whereas PIIIaresulted in the PII form alone. It was concluded from these results that the intermediate forms of IGF-1 can rapidly reshuffle between different disulfide structures, and that formation of the last disulfide bond is not as favorable a process as the conversion to other intermediates. The oxidation to form the last disulfide bond in PIII or PIIIais accelerated and hence the interconversion to other intermediates is kinetically minimized only in the presence of copper sulfate. It appears, therefore, that the two intermediate forms, PIII and PIIIa, are the precursors of the corresponding fully oxidized forms, but their conversions are not energetically a favorable process.
ISSN:0003-9861
1096-0384
DOI:10.1006/abbi.1997.9996