Nonimmune Complexes of Pregnancy-Specific β1-Glycoprotein Explain Its Heterogeneity

Abstract

Nonimmune complexes of pregnancy-specific β₁-glycoprotein (SP₁) explain its heterogeneity. Two proteins reacting with antisera specific to pregnancy-specific β₁-glycoprotein (SP₁) have previously been detected in serum from pregnant women by use of crossed immunoelectrophoresis (CIE). The major SP₁-reactive protein, SP₁β, has a molecular weight of about 90,000 and the minor, antigenically deficient protein, SP₁α, about 200,000. In this study, gel filtration of serum on Ultrogel AcA 34 and Sephacryl S-300 has revealed that classical radioimmunoassay (RIA) techniques of two types only measure SP₁. With RIAs specially designed to detect complexed SP₁ two higher molecular weight, SP₁-containing complexes could be identified. CIE of serum or fractions from gel nitrations revealed a loss of the anodal part of the SP₁ precipitate. However, when 4% polyethylene glycol (PEG) was incorporated in the anti-SP₁-containing gel an antigenically deficient precipitate developed in the α-region. Incorporation of antialbumin in an intermediate gel in CIE reduced the anodal loss of the SP₁, precipitate in anti-SP₁ containing gels without PEG which resulted in a homogenous peak. In addition, in anti-SP₁-containing gels with PEG the anodal precipitate was reduced. This SP₁-albumin complex fulfills all criteria for the previously described SP₁α. For measuring low levels of SP₁ RIAs can be used. For higher values nephelometry is preferable. Although the amount of complexed SP₁ is small in comparison with the amount of native SP₁ methods employing electrophoresis are not recommended. In such tests SP₁ complexed to fast-moving proteins like albumin might influence the results.