FORMATION OF A NATIVE-LIKE SUBDOMAIN IN A PARTIALLY FOLDED INTERMEDIATE OF BOVINE PANCREATIC TRYPSIN-INHIBITOR

In the folding of bovine pancreatic trypsin inhibitor (BPTI), the single-disulfide intermediate [30-51] plays a key role. We have investigated a recombinant analog of [30-51] using 2-dimensional nuclear magnetic resonance (2D-NMR). This recombinant analog, named [30-51](Ala), contains a disulfide bond between Cys-30 and Cys-51, but contains alanine in place of the other cysteines in BPTI to prevent the formation of other intermediates. By 2D-NMR, [30-51](Ala) consists of 2 regions - one folded and one predominantly unfolded. The folded region resembles a previously characterized peptide model of [30-51], named P alpha P beta, that contains a native-like subdomain with tertiary packing. The unfolded region includes the first 14 N-terminal residues of [30-51] and is as unfolded as an isolated peptide containing these residues. Using protein dissection, we demonstrate that the folded and unfolded regions of [30-51](Ala) are structurally independent. The partially folded structure of [30-51](Ala) explains many of the properties of authentic [30-51] in the folding pathway of BPTI. Moreover, direct structural characterization of [30-51](Ala) has revealed that a crucial step in the folding pathway of BPTI coincides with the formation of a native-like subdomain, supporting models for protein folding that emphasize the formation of cooperatively folded subdomains.