Construction of stabilized proteins by combinatorial consensus mutagenesis

doi:10.1093/protein/gzh091

PEDS Advance Access originally published online on December 1, 2004
Protein Engineering Design and Selection 2004 17(11):787-793; doi:10.1093/protein/gzh091

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Construction of stabilized proteins by combinatorial consensus mutagenesis

N. Amin¹, A.D. Liu¹, S. Ramer¹, W. Aehle², D. Meijer², M. Metin², S. Wong¹, P. Gualfetti¹ and V. Schellenberger¹^,3

¹Genencor International, 925 Page Mill Road, Palo Alto, CA 94304, USA and ²Genencor International BV, Leiden, The Netherlands

³ To whom correspondence should be addressed. E-mail: vschellenberger{at}genencor.com

We constructed stabilized variants of ß-lactamase(BLA) from Enterobacter cloacae by combinatorial recruitmentof consensus mutations. By aligning the sequences of 38 BLAhomologs, we identified 29 positions where the E.cloacae genediffers from the consensus sequence of lactamases and constructedcombinatorial libraries using mixtures of mutagenic oligonucleotidesencompassing all 29 positions. Screening of 90 random isolatesfrom these libraries identified 15 variants with significantlyincreased thermostability. The stability of these isolates suggestthat all tested mutations make additive contributions to proteinstability. A statistical analysis of sequence and stabilitydata identified 11 mutations that made stabilizing contributionsand eight mutations that destabilized the protein. A second-generationlibrary recombining these 11 stabilizing mutations led to theidentification of BLA variants that showed further stabilization.The most stable variant had a mid-point of thermal denaturation(T_m) that was 9.1°C higher than the starting molecule andcontained eight consensus mutations. Incubation of three stabilizedBLA variants with several proteases showed that all tested isolateshave significantly increased resistance to proteolysis. Ourdata demonstrate that combinatorial consensus mutagenesis (CCM)allows the rapid generation of protein variants with improvedthermal and proteolytic stability.

Received August 30, 2004; revised November 16, 2004; accepted November 19, 2004.

Edited by Jacques Fastrez

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