Redirection of sialic acid metabolism in genetically engineered Escherichia coli

doi:10.1093/glycob/11.7.533

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Glycobiology, 2001, Vol. 11, No. 7 533-539
© 2001 Oxford University Press

Redirection of sialic acid metabolism in genetically engineered Escherichia coli

Michael Ringenberg, Carol Lichtensteiger and Eric Vimr¹

University of Illinois at Urbana-Champaign, Department of Pathobiology, College of Veterinary Medicine, University of Illinois at Urbana-Champaign, 2522 VMBSB, 2001 South Lincoln Avenue, Urbana, IL 61802, USA

Most microorganisms do not produce sialic acid (sialate), andthose that do appear to use a biosynthetic mechanism distinctfrom mammals. Genetic hybrids of nonpathogenic, sialate-negativelaboratory Escherichia coli K-12 strains designed for the denovo synthesis of the polysialic acid capsule from E. coli K1proved useful in elucidating the genetics and biochemistry ofcapsule biosynthesis. In this article we propose a dynamic modelof sialometabolism to investigate the effects of biosyntheticneu (N-acetylneuraminic acid) and catabolic nan (N-acylneuraminate)mutations on the flux of intermediates through the sialate syntheticpathway. Intracellular sialate concentrations were determinedby high pH anion exchange chromatography with pulsed amperometricdetection. The results indicated that a strain carrying a nulldefect in the gene encoding polysialyltransferase (neuS) accumulated> 50 times more CMP–sialic acid than the wild typewhen strains were grown in a minimal medium supplemented withglucose and casamino acids. Metabolic accumulation of CMP–sialicacid depended on a functional sialic acid synthase (neuB), asshown by the inability of a strain lacking this enzyme to accumulatea detectable endogenous sialate pool. The neuB mutant concentratedtrace sialate from the medium, indicating its potential valuefor quantitative analysis of free sialic acids in complex biologicalsamples. The function of the sialate aldolase (encoded by nanA)in limiting intermediate flux through the synthetic pathwaywas determined by analyzing free sialate accumulation in neuA(CMP–sialic acid synthetase) nanA double mutants. Thecombined results demonstrate how E. coli avoids a futile cyclein which biosynthetic sialate induces the system for its owndegradation and indicate the feasibility of generating sialooligosaccharideprecursors through targeted manipulation of sialate metabolism.

¹ To whom correspondence should be addressed

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