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1.  The Path of DNA in the kinetochore 
Current biology : CB  2006;16(8):R276-R278.
doi:10.1016/j.cub.2006.03.054
PMCID: PMC2112771  PMID: 16631569
3.  Emergence of Protein Fold Families through Rational Design 
PLoS Computational Biology  2006;2(7):e85.
Diverse proteins with similar structures are grouped into families of homologs and analogs, if their sequence similarity is higher or lower, respectively, than 20%–30%. It was suggested that protein homologs and analogs originate from a common ancestor and diverge in their distinct evolutionary time scales, emerging as a consequence of the physical properties of the protein sequence space. Although a number of studies have determined key signatures of protein family organization, the sequence-structure factors that differentiate the two evolution-related protein families remain unknown. Here, we stipulate that subtle structural changes, which appear due to accumulating mutations in the homologous families, lead to distinct packing of the protein core and, thus, novel compositions of core residues. The latter process leads to the formation of distinct families of homologs. We propose that such differentiation results in the formation of analogous families. To test our postulate, we developed a molecular modeling and design toolkit, Medusa, to computationally design protein sequences that correspond to the same fold family. We find that analogous proteins emerge when a backbone structure deviates only 1–2 Å root-mean-square deviation from the original structure. For close homologs, core residues are highly conserved. However, when the overall sequence similarity drops to ~25%–30%, the composition of core residues starts to diverge, thereby forming novel families of protein homologs. This direct observation of the formation of protein homologs within a specific fold family supports our hypothesis. The conservation of amino acids in designed sequences recapitulates that of the naturally occurring sequences, thereby validating our computational design methodology.
Synopsis
Studies of known proteins have revealed intriguing co-organization of their sequences and structures. Proteins with sequence similarity higher than 25%–30% usually adopt a similar structure and are called homologs, whereas those with low sequence similarity (<20%) can share the same structure and are referred as analogs. The origin of such co-organization has been a topic of extensive discussions among protein folding, design, and evolution research communities, because understanding of the emergence of homologs and analogs in the protein universe has broad implications for our ability to rationally manipulate proteins. In this study, the authors developed a molecular modeling and design method, Medusa, to computationally design diversified protein sequences that correspond to similar backbone structures, which determine a protein fold family. Using Medusa, the authors directly demonstrated the formation of distinct protein homologs within a specific fold family when the structure deviates only 1–2 Å away from the original structure. The study suggests that subtle structural changes, which appear due to accumulating mutations in the families of homologs, lead to a distinct packing of the protein core and, thus, novel compositions of core residues. The latter process leads to the formation of distinct families of homologs.
doi:10.1371/journal.pcbi.0020085
PMCID: PMC1487181  PMID: 16839198

Results 1-3 (3)