Cellular mechanisms of abscess formation: macrophage procoagulant activity and major histocompatibility complex recognition.

BACKGROUND

Macrophage procoagulant activity (PCA) has been proposed as a key mediator of abscess formation. Experimentally, transient systemic bacterial infection lead to increased numbers of intraabdominal abscesses after a subsequent episode of peritonitis. We tested the hypothesis that these events were regulated by classic major histocompatibility complex (MHC)-restricted antigen processing and presentation to lymphocytes followed by lymphocyte-mediated up-regulation of macrophage PCA.

METHODS

In vitro, macrophages and lymphocytes from BALB/c or C57BL/6 mice either untreated or preexposed to Escherichia coli were coincubated with bacteria or lipopolysaccharide. Cell lysates were tested for PCA in a one-step dotting assay. In vivo, mice were either preexposed to E. coli or received passive transfer of lymphocytes from MHC-compatible or MHC-incompatible and naive or preexposed donors; peritonitis and intraabdominal abscesses were afterwards induced with E. coli, Bacteroides fragilis, and a sterile fecal adjuvant. Mice were killed after 10 days and were studied for abscess number and bacterial composition.

RESULTS

The presence of lymphocytes consistently increased macrophage PCA; lymphocytes from preexposed donors induced twice as much PCA as lymphocytes from naive donors regardless of MHC background. Both bacterial preexposure and passive transfer of lymphocytes from preexposed donors increased later intraabdominal abscess number in an MHC-restricted fashion.

CONCLUSIONS

Transient infections enhance subsequent lymphocyte-mediated macrophage PCA, correlating with increases in abscess formation after peritonitis. The need for MHC identity to reproduce these results via passive transfer in vivo is consistent with classic T-cell receptor-mediated antigen presentation and lymphocyte activation before enhancement of PCA during peritonitis.