,
,Vol. 96, Issue 10, 5482-5485, May 11, 1999
,,* Baker Laboratory of Chemistry and Chemical Biology, Cornell
University, Ithaca, NY 14853-1301; Faculty
of Chemistry, University of Gdan
k,
Sobieskiego 18, 80-952 Gdank,
Poland; and Cornell
Theory Center, Ithaca, NY 14853-3801
Contributed by H. A. Scheraga, March 9, 1999
An approach based exclusively on finding the global minimum of an
appropriate potential energy function has been used to predict the
unknown structures of five globular proteins with sizes ranging from
89 to 140 amino acid residues. Comparison of the computed lowest-energy
structures of two of them (HDEA and MarA) with the crystal
structures, released by the Protein Data Bank after the predictions
were made, shows that large fragments (61 residues) of both
proteins were predicted with rms deviations of 4.2 and 6.0 Å for
the C
atoms, for
HDEA and MarA, respectively. This represents 80% and 53% of the
observed structures of HDEA and MarA, respectively. Similar rms
deviations were obtained for ~60-residue fragments of the other three
proteins. These results constitute an important step toward the
prediction of protein structure based solely on global
optimization of a potential energy function for a given amino
acid sequence.