Cumulant

Cumulant-based expressions for the multibody terms for the correlation between local and electrostatic interactions in the united-residue force field

Adam Liwo and Cezary Czaplewski

Baker Laboratory of Chemistry and Chemical Biology, Cornell University, Ithaca, New York 14853-1301
Faculty of Chemistry, University of Gdask, ul. Sobieskiego 18, 80-952 Gdask, Poland

Jaros

aw Pillardy and Harold A. Scheraga

Baker Laboratory of Chemistry and Chemical Biology, Cornell University, Ithaca, New York 14853-1301

(Received 21 March 2001; accepted 15 May 2001)

Ageneral method to derive site-site or united-residue potentials is presented.The basic principle of the method is the separation ofthe degrees of freedom of a system into the primaryand secondary ones. The primary degrees of freedom describe thebasic features of the system, while the secondary ones areaveraged over when calculating the potential of mean force, whichis hereafter referred to as the restricted free energy (RFE)function. The RFE can be factored into one-, two-, andmultibody terms, using the cluster-cumulant expansion of Kubo. These factorscan be assigned the functional forms of the corresponding lowest-ordernonzero generalized cumulants, which can, in most cases, be evaluatedanalytically, after making some simplifying assumptions. This procedure to derivecoarse-grain force fields is very valuable when applied to multibodyterms, whose functional forms are hard to deduce in anotherway (e.g., from structural databases). After the functional forms havebeen derived, they can be parametrized based on the RFEsurfaces of model systems obtained from all-atom models or onthe statistics derived from structural databases. The approach has beenapplied to our united-residue force field for proteins. Analytical expressionswere derived for the multibody terms pertaining to the correlationbetween local and electrostatic interactions within the polypeptide backbone; theseexpressions correspond to up to sixth-order terms in the cumulantexpansion of the RFE. These expressions were subsequently parametrized byfitting to the RFEs of selected peptide fragments, calculated withthe empirical conformational energy program for peptides force field. Thenew multibody terms enable not only the heretofore predictable -helicalsegments, but also regular -sheets, to form as the lowest-energystructures, as assessed by test calculations on a model helicalprotein A, as well as a model 20-residue polypeptide (betanova);the latter was not possible without introducing these new terms.©2001 American Institute of Physics.