Geraldine Scott scite author profile

Monoclonal antibodies were raised against surface determinants of Streptococcus pneumoniae by hyperimmunizing X-linked immunodeficient (xid) CBA/N mice with the heat-killed rough strain R36A. 17 hybridomas produced antibody that bound intact R36A and did not cross-react with phosphocholine, an antigen common in the cell wall of all S. pneumoniae. The antibody produced by at least two of these hybridomas, Xi64 (IgM) and Xi126 (IgG2b), could protect mice from a lethal intravenous challenge of type 3 S. pneumoniae strains WU2 and A66 and of the type 2 strain D39. The minimum amount of antibody required to protect xid mice from 100 WU2 was 4.5 micrograms/mouse for Xi64 and 2.6 micrograms/mouse for Xi126,. Free phosphocholine, C-polysaccharide, and type 3 capsular polysaccharide all failed to inhibit the binding of Xi64 or Xi126 to R36A. These antibodies appeared to bind surface polypeptides, since treatment of R36A with either pepsin or trypsin, or of R36A lysate with trypsin, effectively eliminated the ability of Xi64 and Xi126 to bind antigens in these preparations. Binding studies indicated that these two antibodies recognized different epitopes that were expressed on several but not all serotypes of pneumococci.

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Analysis of a surface protein of Streptococcus pneumoniae recognised by protective monoclonal antibodies

McDaniel

Scott

Widenhofer

et al. 1986

Microbial Pathogenesis

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Genetic Control of the Susceptibility to Pneumococcal Infection

Briles

Horowitz

McDaniel

et al. 1986

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Naturally Occurring Antibodies to Phosphocholine as a Potential Index of Antibody Responsiveness to Polysaccharides

Briles¹,

Scott²,

Gray³

et al. 1987

Journal of Infectious Diseases

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Naturally occurring antibodies reactive with the phosphocholine (PC) determinant of pneumococcal teichoic acids may be useful for evaluating the potential of patients to make antibodies to polysaccharides. Antibodies to PC are present in most adults under the age of 60 years, are absent in very young children, and are present at low levels in Wiscott-Aldrich patients and in IgG2-deficient adults. These last three groups respond very poorly to polysaccharide antigens. Antibodies to PC are also found at low levels in the elderly, a group that has previously been shown to have low levels of antibody to blood groups A and B carbohydrates. The levels of antibody to PC over time were constant in most individuals and, in adults, seemed to show slightly less variation than did titers of antibody to blood group B. Our findings suggest that titers of antibody to PC may be superior to titers of antibody to blood group A or B for monitoring responsiveness to carbohydrate antigens.

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A Comparison of the Behavior of Insulin and Insulin Labeled with I131 in Serum

Scott

Prout

Weaver

et al. 1958

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Geraldine Scott

Monoclonal antibodies against protease-sensitive pneumococcal antigens can protect mice from fatal infection with Streptococcus pneumoniae.

Analysis of a surface protein of Streptococcus pneumoniae recognised by protective monoclonal antibodies

Genetic Control of the Susceptibility to Pneumococcal Infection

Naturally Occurring Antibodies to Phosphocholine as a Potential Index of Antibody Responsiveness to Polysaccharides

A Comparison of the Behavior of Insulin and Insulin Labeled with I131 in Serum

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