Pneumococcal type-associated variability in alternate complement pathway activation

Opsonization of Streptococcus pneumoniae may be mediated by the alternate complement pathway. To study the importance of this interaction to human disease, complement consumption by pneumococci of various serotypes was measured in humwn serum chelated with ethyleneglycoltraacetic acid, a substance that blocks the classic but not the alternate complement pathwway. Serotype I, in contrast to all other types studied, lacked ability to consume complement in this system. The ability for serotypes III, IV, and VIII to activate the alternate pathway could be eliminated by prior serum absorption at O C with they type in question, a condition that would remove antibody but not complement. Types VII, XII, XIV, and XXV readily activated the alternate pathway in unabsorbed and absorbed sera. Differences could not be related to properties of the capsules. It was concluded that types I, III, IV, and VIII lack intrinsic ability to activate and thus be opsonized by the alternate complement pathway, although types III, IV, and VIII can do so in concert with specific antibody. The fact that these same types are especially prominent in human disease suggests that the ability to evade opsonization by the alternate complement pathway in pre-antibody phases of infection may be a virulence factor in pneumococci.

[1]  E. Lund Types of pneumococci found in blood, spinal fluid and pleural exudate during a period of 15 years (1954-1969). , 2009, Acta pathologica et microbiologica Scandinavica. Section B: Microbiology and immunology.

[2]  M. Mufson,et al.  Capsular types and outcome of bacteremic pneumococcal disease in the antibiotic era. , 1974, Archives of internal medicine.

[3]  A. Forsgren,et al.  Influence of the Alternate Complement Pathway on Opsonization of Several Bacterial Species , 1974, Infection and immunity.

[4]  A. Forsgren,et al.  Opsonic activity in human serum chelated with ethylene glycoltetra-acetic acid. , 1974, Immunology.

[5]  J. Winkelstein,et al.  The role of immunoglobulin in the interaction of pneumococci and the properdin pathway: evidence for its specificity and lack of requirement for the Fc portion of the molecule. , 1974, Journal of immunology.

[6]  A K Bahn,et al.  Basic medical statistics. , 1973, Journal of the American Medical Women's Association.

[7]  J. Winkelstein,et al.  Opsonins: their function, identity, and clinical significance. , 1973, The Journal of pediatrics.

[8]  S. Marney,et al.  C3 shunt activation in human serum chelated with EGTA. , 1972, Journal of immunology.

[9]  H. Jasin,et al.  Human heat labile opsonins: evidence for their mediation via the alternate pathway of complement activation. , 1972, Journal of immunology.

[10]  W. Wood,et al.  Heat Labile Opsonins to Pneumococcus , 1972, The Journal of Immunology.

[11]  O. Götze,et al.  THE C3-ACTIVATOR SYSTEM: AN ALTERNATE PATHWAY OF COMPLEMENT ACTIVATION , 1971, The Journal of experimental medicine.

[12]  M. Frank,et al.  IN VITRO STUDIES OF COMPLEMENT FUNCTION IN SERA OF C4-DEFICIENT GUINEA PIGS , 1971, The Journal of experimental medicine.

[13]  P. Quie,et al.  Opsonic activity of agammaglobulinemic human sera. , 1971, Journal of immunology.

[14]  H. Gewurz,et al.  COMPLEMENT AND COMPLEMENT-LIKE ACTIVITY IN LOWER VERTEBRATES AND INVERTEBRATES , 1970, The Journal of experimental medicine.

[15]  I. Gigli,et al.  Methods for the separation, purification and measurement of nine components of hemolytic complement in guinea-pig serum. , 1966, Immunochemistry.

[16]  R. Austrian,et al.  PNEUMOCOCCAL BACTEREMIA WITH ESPECIAL REFERENCE TO BACTEREMIC PNEUMOCOCCAL PNEUMONIA. , 1964, Annals of internal medicine.

[17]  W. R. Mccabe,et al.  Intracellular Bacteria in the Peripheral Blood in Staphylococcal Bacteremia , 1962 .

[18]  I. Gigli,et al.  Phylogeny and function of the complement system. , 1971, Annual review of microbiology.

[19]  H. Rapp,et al.  Molecular Basis of Complement Action , 1970 .

[20]  W. McDermott Microbial persistence. , 1969, Harvey lectures.