System and method for determining three-dimensional structure of protein sequences

Assignee

• The Regents of the University of California · US

Inventors

• Fred E. Cohen · Los Angeles, US
• Thomas Defay · San Bruno, US

Key dates

Classification

• Technology area (CPC G)Physics
• CPC primaryG16B40/00
• WIPO fieldComputer technology
• WIPO sectorElectrical engineering

Abstract

The present invention pertains to a system and method for predicting the protein fold of a target amino acid residue sequence of unknown protein structure. A target sequence is represented by a sequence of residue variability types that utilizes positional variability information present in an associated family of homologous sequences to the target sequence. The use of the positional variability information increases the likelihood of matching the target sequence with a known protein structure. In a first preferred embodiment, a target sequence is mapped into a sequence of residue variability types that are based on the solubility variability present between amino acid residues in homologous sequences. In a second preferred embodiment, each residue variability type represents a cluster of residue types at each position of aligned sets of homologous protein sequences. Each distinct cluster represents a pattern of residue variability at various positions in sets of homologous protein sequences. The sequence of residue variability types is aligned with one or more environment strings, each of which represents a known protein structure in accordance with the degree of surface exposure …