Evolutionary Framework for Protein Sequence Evolution and Gene Pleiotropy

Xun Gu¹

Department of Genetics, Development and Cell Biology, Center for Bioinformatics and Biological Statistics, Iowa State University, Ames, IA 50011

^¹ Address for correspondence: Department of Genetics, Developmental and Cell Biology, 536 Science II Hall, Iowa State University, Ames, IA 50011.
E-mail: xgu{at}iastate.edu

In this article, we develop an evolutionary model for proteinsequence evolution. Gene pleiotropy is characterized by K distinctbut correlated components (molecular phenotypes) that affectthe organismal fitness. These K molecular phenotypes are understabilizing selection with microadaptation (SM) due to randomoptima shifts, the SM model. Random coding mutations generatea correlated distribution of K molecular phenotypes. Under thisSM model, we further develop a statistical method to estimatethe "effective" number of molecular phenotypes (K_e) of the gene.Therefore, for the first time we can empirically evaluate genepleiotropy from the protein sequence analysis. Case studiesof vertebrate proteins indicate that K_e is typically $~$ 6–9.We demonstrate that the newly developed SM model of proteinevolution may provide a basis for exploring genomic evolutionand correlations.