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  • Assessing computational amino acid beta-turn propensities with a phage-displayed combinatorial library and directed evolution.

Assessing computational amino acid beta-turn propensities with a phage-displayed combinatorial library and directed evolution.

Structure (London, England : 1993) (2006-10-10)
Hung-Ju Hsu, Hong-Ju Chang, Hung-Pin Peng, Shan-Sheng Huang, Ming-Yen Lin, An-Suei Yang
ABSTRACT

Structure propensities of amino acids are important determinants in guiding proteins' local and global structure formation. We constructed a phage display library--a hexa-HIS tag upstream of a CXXC (X stands for any of the 20 natural amino acids) motif appending N-terminal to the minor capsid protein pIII of M13KE filamentous phage--and developed a novel directed-evolution procedure to select for amino acid sequences forming increasingly stable beta-turns in the disulfide-bridged CXXC motif. The sequences that emerged from the directed-evolution cycles were in good agreement with type II beta-turn propensities derived from surveys of known protein structures, in particular, Pro-Gly forming a type II beta-turn. The agreement strongly supported the notion that beta-turn formation plays an active role in initiating local structure folding in proteins.

MATERIALS
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Millipore
Montage Gel Extraction Kit, DNA Gel Extraction