Serum sensitivity of Neisseria gonorrhoeae: The role of lipopolysaccharide

W. M. Shafer; K. Joiner; L. F. Guymon; M. S. Cohen; P. F. Sparling

doi:10.1093/infdis/149.2.175

Serum sensitivity of Neisseria gonorrhoeae: The role of lipopolysaccharide

W. M. Shafer, K. Joiner, L. F. Guymon, M. S. Cohen, P. F. Sparling

Research output: Contribution to journal › Article › peer-review

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Abstract

A lipopolysaccharide (LPS) mutant (FA5100) of a serum-resistant strain of Neisseria gonorrhoeae (FA19) was found to be highly sensitive to the bactericidal activity of normal human serum (NHS). Both strain FA5100 and an unrelated serum-sensitive clinical isolate (F62) were killed by NHS via the classical complement pathway since killing required C2 and Ca⁺⁺. However, the fact that only strain FA5100 was sensitive to human hypogammaglobulinemic and cord serum suggested that this strain might activate the classical complement pathway in the absence of antibody. Anticomplementary concentrations of LPS from strain FA5100 inhibited the bactericidal activity of NHS against either strain FA5100 or strain F62. However, concentrations of LPS from strain FA5100 that exhibited marginal anticomplementary behavior also inhibited the killing of strain F62 by NHS. The ability of LPS from strain FA5100 to inhibit the bactericidal activity of NHS against strain FA5100 and to activate complement was reduced by treatment with mild alkali. However, alkali-treated LPS from strain FA5100 still inhibited the bactericidal activity of NHS against strain F62.

Original language	English (US)
Pages (from-to)	175-183
Number of pages	9
Journal	Journal of Infectious Diseases
Volume	149
Issue number	2
DOIs	https://doi.org/10.1093/infdis/149.2.175
State	Published - 1984
Externally published	Yes

ASJC Scopus subject areas

Immunology and Allergy
Infectious Diseases

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title = "Serum sensitivity of Neisseria gonorrhoeae: The role of lipopolysaccharide",

abstract = "A lipopolysaccharide (LPS) mutant (FA5100) of a serum-resistant strain of Neisseria gonorrhoeae (FA19) was found to be highly sensitive to the bactericidal activity of normal human serum (NHS). Both strain FA5100 and an unrelated serum-sensitive clinical isolate (F62) were killed by NHS via the classical complement pathway since killing required C2 and Ca++. However, the fact that only strain FA5100 was sensitive to human hypogammaglobulinemic and cord serum suggested that this strain might activate the classical complement pathway in the absence of antibody. Anticomplementary concentrations of LPS from strain FA5100 inhibited the bactericidal activity of NHS against either strain FA5100 or strain F62. However, concentrations of LPS from strain FA5100 that exhibited marginal anticomplementary behavior also inhibited the killing of strain F62 by NHS. The ability of LPS from strain FA5100 to inhibit the bactericidal activity of NHS against strain FA5100 and to activate complement was reduced by treatment with mild alkali. However, alkali-treated LPS from strain FA5100 still inhibited the bactericidal activity of NHS against strain F62.",

author = "Shafer, {W. M.} and K. Joiner and Guymon, {L. F.} and Cohen, {M. S.} and Sparling, {P. F.}",

note = "Funding Information: Received for publication May 25, 1983, and in revised form September 29, 1983. This work was supported by grant AI 15036 and by National R~search Service Award AI 06369 from the National Institute of Allergy and Infectious Diseases. We thank Mark Schmetz for technical assistance, D. C. Morrison and M. E. Wilson for editorial comments, J. Bowles for typing, and the individuals listed in the text for serum samples. Please address requests for reprints to Dr W. M. Shafer at his present address: Department of Microbiology and Immunology, Emory University School of Medicine, Atlanta, Georgia 30322.",

year = "1984",

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AU - Sparling, P. F.

N1 - Funding Information: Received for publication May 25, 1983, and in revised form September 29, 1983. This work was supported by grant AI 15036 and by National R~search Service Award AI 06369 from the National Institute of Allergy and Infectious Diseases. We thank Mark Schmetz for technical assistance, D. C. Morrison and M. E. Wilson for editorial comments, J. Bowles for typing, and the individuals listed in the text for serum samples. Please address requests for reprints to Dr W. M. Shafer at his present address: Department of Microbiology and Immunology, Emory University School of Medicine, Atlanta, Georgia 30322.

PY - 1984

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N2 - A lipopolysaccharide (LPS) mutant (FA5100) of a serum-resistant strain of Neisseria gonorrhoeae (FA19) was found to be highly sensitive to the bactericidal activity of normal human serum (NHS). Both strain FA5100 and an unrelated serum-sensitive clinical isolate (F62) were killed by NHS via the classical complement pathway since killing required C2 and Ca++. However, the fact that only strain FA5100 was sensitive to human hypogammaglobulinemic and cord serum suggested that this strain might activate the classical complement pathway in the absence of antibody. Anticomplementary concentrations of LPS from strain FA5100 inhibited the bactericidal activity of NHS against either strain FA5100 or strain F62. However, concentrations of LPS from strain FA5100 that exhibited marginal anticomplementary behavior also inhibited the killing of strain F62 by NHS. The ability of LPS from strain FA5100 to inhibit the bactericidal activity of NHS against strain FA5100 and to activate complement was reduced by treatment with mild alkali. However, alkali-treated LPS from strain FA5100 still inhibited the bactericidal activity of NHS against strain F62.

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Serum sensitivity of Neisseria gonorrhoeae: The role of lipopolysaccharide

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