Molecular structure of an aspartic proteinase zymogen, porcine pepsinogen, at 1.8 Å resolution

1 January 1986

journal article
research article
Published by Springer Nature in Nature

Vol. 319 (6048), 33-38
https://doi.org/10.1038/319033a0

Abstract

The only well-understood mechanism of zymogen activation is that of the serine proteinases, in which proteolytic cleavage leads to conformational changes resulting in a functional active site. A different mechanism is now unveiled by the crystal structure of pepsinogen. Salt bridges that stabilize the positioning of the N-terminal proenzyme segment across the active site of pepsin are disrupted at low pH, releasing the amino-terminal segment and thereby exposing the catalytic apparatus and the substrate-binding sites.

Keywords

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