Abstract
Objective
C4βderived activation fragments are the only complement ligands present on the surfaces of normal erythrocytes. The significance of this observation is unknown, and the role of erythrocyteβbound C4 (EβC4) in human disease has not been explored. More than any other human disease, the pathogenesis of systemic lupus erythematosus (SLE) has been characterized by defects in clearance of complementβbearing immune complexes via erythrocytes expressing complement receptor 1 (CR1). This study was undertaken to determine whether these functional defects might be reflected by abnormal patterns of EβC4 and EβCR1 expression on erythrocytes of patients with SLE.
Methods
We conducted a crossβsectional study of 100 patients with SLE, 133 patients with other diseases, and 84 healthy controls. Erythrocytes were characterized by indirect immunofluorescence and by flow cytometry for determination of levels of C4d and CR1.
Results
Patients with SLE had higher levels of EβC4d and lower levels of EβCR1 than did patients with other diseases (P β€ 0.001) or healthy controls (P β€ 0.001). The test was 81% sensitive and 91% specific for SLE versus healthy controls and 72% sensitive and 79% specific for SLE versus other diseases, and it had an overall negative predictive value of 92%.
Conclusion
This is the first report of abnormal levels of EβC4d in human disease. We found that abnormally high levels of EβC4d and low levels of EβCR1 are characteristic of SLE, and combined measurement of the 2 molecules has high diagnostic sensitivity and specificity for lupus. Determination of EβC4d/EβCR1 levels may be a useful addition to current tests and criteria for SLE diagnosis.