Multivariate-activity mining for molecular quasi-species in a glutathione transferase mutant library

doi:10.1093/protein/gzm017

PEDS Advance Access originally published online on April 27, 2007
Protein Engineering Design and Selection 2007 20(5):243-256; doi:10.1093/protein/gzm017

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Multivariate-activity mining for molecular quasi-species in a glutathione transferase mutant library

Sanela Kurtovic¹, Arna Runarsdottir¹, Lars O. Emrén², Anna-Karin Larsson and Bengt Mannervik³

Department of Biochemistry and Organic Chemistry, Uppsala University, BMC, Box 576, SE-75123 Uppsala, Sweden

³ To whom correspondence should be addressed. E-mail: Bengt.Mannervik{at}biorg.uu.se

A library of recombinant glutathione transferases (GSTs) generatedby shuffling of DNA encoding human GST M1-1 and GST M2-2 wasscreened with eight alternative substrates, and the activitieswere subjected to multivariate analysis. Assays were made inlysates of bacteria in which the GST variants had been expressed.The primary data showed clustering of the activities in eight-dimensionalsubstrate-activity space. For an incisive analysis, the rowsof the data matrix, corresponding to the different enzyme variants,were individually scaled to unit length, thus accounting fordifferent expression levels of the enzymes. The columns representingthe activities with alternative substrates were subsequentlyindividually normalized to unit variance and a zero mean. Bythis standardization, the data were adjusted to comparable ordersof magnitude. Three molecular quasi-species were recognizedby multivariate K-means and principal component analyses. Twoof them encompassed the parental GST M1-1 and GST M2-2. A thirdone diverged functionally by displaying enhanced activitieswith some substrates and suppressed activities with signaturesubstrates for GST M1-1 and GST M2-2. A fourth cluster containedmutants with impaired functions and was not regarded as a quasi-species.Sequence analysis of representatives of the mutant clustersdemonstrated that the majority of the variants in the divergingnovel quasi-species were structurally similar to the M1-likeGSTs, but distinguished themselves from GST M1-1 by a Ser toThr substitution in the active site. The data show that multivariateanalysis of functional profiles can identify small structuralchanges influencing the evolution of enzymes with novel substrate-activityprofiles.

Keywords: directed evolution/DNA shuffling/glutathione transferase/library/multivariate analysis

Received March 12, 2007; revised March 12, 2007; accepted March 14, 2007.

¹ Authors contributed equally to the work.

² Previously Lars O. Hansson.

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