Identification of a genetic locus essential for capsule sialylation in type III group B streptococci.

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Infect Immun. 1992 February; 60(2): 392-400

Identification of a genetic locus essential for capsule sialylation in type III group B streptococci.

M R Wessels, R F Haft, L M Heggen and C E Rubens

Channing Laboratory, Department of Medicine, Brigham and Women's Hospital, Boston, Massachusetts.

ABSTRACT

The type III capsular polysaccharide of group B streptococci(GBS) consists of a linear backbone with short side chains endingin residues of N-acetylneuraminic acid, or sialic acid. Thepresence of sialic acid on the surface of the organism inhibitsactivation of the alternative pathway of complement and is thoughtto be an important element in the virulence function of thecapsule. We showed previously that a mutant strain of GBS thatexpressed a sialic acid-deficient, or asialo, form of the typeIII polysaccharide was avirulent, supporting a virulence functionfor capsular sialic acid. We now report the derivation of anasialo capsule mutant from a highly encapsulated wild-type strainof type III GBS, strain COH1, by insertional mutagenesis withtransposon Tn916 delta E. In contrast to the wild-type strain,the asialo mutant strain COH1-11 was sensitive to phagocytickilling by human leukocytes in vitro and was relatively avirulentin a neonatal rat model of GBS infection. The asialo mutantaccumulated free intracellular sialic acid, suggesting a defectsubsequent to sialic acid synthesis in the biosynthetic pathwayleading to capsule sialylation. The specific biosynthetic defectin mutant strain COH1-11 was found to be in the activation offree sialic acid to CMP-sialic acid: CMP-sialic acid synthetaseactivity was present in the wild-type strain COH1 but was notdetected in the asialo mutant strain COH1-11. One of the twotransposon insertions in the asialo mutant COH1-11 mapped tothe same chromosomal location as one of the two Tn916 insertionsin the previously reported asialo mutant COH31-21, identifyingthis site as a genetic locus necessary for expression of CMP-sialicacid synthetase activity. These studies demonstrate that theenzymatic synthesis of CMP-sialic acid by GBS is an essentialstep in sialylation of the type III capsular polysaccharide.

Infect Immun. 1992 February; 60(2): 392-400

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