Vancomycin forms complexes with peptides terminating in d-alanyl-d-alanine that are analogous to the biosynthetic precursors of bacterial mucopeptides. The specificity of complex-formation has been studied by means of many synthetic peptides, prepared by both solid-phase and conventional methods. The following conclusions can be drawn: (a) three amide linkages are required to form a stable complex; (b) the terminal carboxyl group must be free; (c) the carboxyl terminal and subterminal residues must be either glycine or of the d-configuration; (d) the size of the side chain in these residues greatly influences the affinity for vancomycin, a methyl group being the optimum in each case; (e) the nature of the side chain in the third and fourth residues has a smaller effect on complex-formation, but an l-configuration was somewhat better than a d-configuration in the third position. In addition to acyl-d-alanyl-d-alanine, other peptides that occur in bacterial cell walls will combine with vancomycin, although less strongly, e.g. acyl-d-alanyl-d-α-amino acid (where the terminal d-residue may form the cross-link in mucopeptide structure) and acyl-l-alanyl-d-glutamylglycine (a sequence found in the mucopeptide of Micrococcus lysodeikticus and related organisms). These results throw some light on the specificity of the uptake of vancomycin by living bacteria.
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August 1971
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Research Article|
August 01 1971
Modifications of the acyl-d-alanyl-d-alanine terminus affecting complex-formation with vancomycin
M. Nieto;
M. Nieto
1National Institute for Medical Research, Mill Hill, London N.W.7, U.K.
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H. R. Perkins
H. R. Perkins
1National Institute for Medical Research, Mill Hill, London N.W.7, U.K.
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Publisher: Portland Press Ltd
© 1971 The Biochemical Society
1971
Biochem J (1971) 123 (5): 789–803.
Citation
M. Nieto, H. R. Perkins; Modifications of the acyl-d-alanyl-d-alanine terminus affecting complex-formation with vancomycin. Biochem J 1 August 1971; 123 (5): 789–803. doi: https://doi.org/10.1042/bj1230789
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