Abstract

Serum mannan-binding protein (MBP), a lectin specific for mannose and N-acetylglucosamine, was revealed to activate the complement system as measured by passive hemolysis using sheep erythrocytes coated with yeast mannan. In contrast, rat liver MBP, which shares many properties in common with serum MBP, could not activate complement at all. The activation by serum MBP was inhibited effectively by the presence of haptenic sugars and dependent absolutely upon the presence of C4, indicating that the activation is initiated by the sugar binding activity of MBP and proceeds through the classical pathway. The 25 NH2-terminal amino acid sequence of rat serum MBP determined in this study was completely matched with that of MBP-A deduced from cDNA sequence by Drickamer et al. (Drickamer, K., Dordal, M. S., and Reynolds, L. (1986) J. Biol. Chem. 261, 6878-6887), revealing that MBP-A is in fact identical with serum MBP. On the basis of the knowledge of primary structures and physicochemical properties of rat serum and liver MBPs, a possible mechanism of the complement activation by serum MBP is discussed with reference to close similarity in the gross structures of serum MBP and C1q.

Highlights

  • Serum mannan-bindingprotein (MBP), alectin specific for mannoseand N-acetylglucosamine,wasrevealed to activate the complement system as measured by passive hemolysis using sheep erythrocytes coated with yeast mannan

  • We report that purified serum MBP from various sources activates complement via the classical pathway and discusspossible mechanisms of the complement activation with regards to the unusual structureof serum MBP

  • Complement-dependent Hemolysis of M E Sensitized with Serum MBP-Sensitization of washed ME with serum MBP

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Summary

Introduction

Serum mannan-bindingprotein (MBP), alectin specific for mannoseand N-acetylglucosamine,wasrevealed to activate the complement system as measured by passive hemolysis using sheep erythrocytes coated with yeast mannan. Investigate the capability of the serum MBP to activate the complement system.

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