Lithostathine is a calcium carbonate crystal habit modifier. It is found precipitated under the form of fibrils in chronic calcifying pancreatitis or Alzheimer’s disease. In order to gain better insight into the nature and the formation of fibrils, we have expressed and purified recombinant lithostathine. Analytical ultracentrifugation and quasi-elastic light scattering techniques were used to demonstrate that lithostathine remains essentially monomeric at acidic pH while it aggregates at physiological pH. Analysis of these aggregates by electron microscopy showed an apparently unorganized structure of numerous monomers which tend to precipitate forming regular unbranched fibrils. Aggregated forms seem to occur prior to the apparition of fibrils. In addition, we have demonstrated that these fibrils resulted from a proteolysis mechanism due to a specific cleavage of the Arg11-Ile12 peptide bond. It is deduced that the NH2-terminal undecapeptide of lithostathine normally impedes fiber formation but not aggregation. A theoretical model explaining the formation of amyloid plaques in neurodegenerative diseases or stones in lithiasis starting from lithostathine is described. Therefore we propose that lithostathine, whose major function is unknown, defines a new class of molecules which is activated by proteolysis and is not involved in cytoskeleton nor intermediate filament functions.
Biophysical Characterization of Lithostathine
C. Cérini,V. Peyrot,C. Garnier,L. Duplan,S. Veesler,J. L. Le Caer,J. Bernard,H. Bouteille,R. Michel,A. Vazi,Patricia Dupuy,B. Michel,Y. Berland,J. Verdier
Published 1999 in Journal of Biological Chemistry
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- Publication year
1999
- Venue
Journal of Biological Chemistry
- Publication date
1999-08-06
- Fields of study
Biology, Medicine, Chemistry
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Semantic Scholar, PubMed
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