4.3 Article

Lactoferrin, myeloperoxidase, and ceruloplasmin: complementary gearwheels cranking physiological and pathological processes

Journal

BIOMETALS
Volume 27, Issue 5, Pages 815-828

Publisher

SPRINGER
DOI: 10.1007/s10534-014-9755-2

Keywords

Ceruloplasmin; Lactoferrin; Myeloperoxidase; Protein-protein interactions; Synergism of antimicrobial proteins; Inflammation; Thiocyanate; Halogenative stress

Funding

  1. RFBR [12-04-00301, 13-04-01191, MK-6062.2014.4]
  2. Program Human Proteome

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Copper-containing plasma protein ceruloplasmin (Cp) forms a complex with lactoferrin (Lf), an iron-binding protein, and with the heme-containing myeloperoxidase (Mpo). In case of inflammation, Lf and Mpo are secreted from neutrophil granules. Among the plasma proteins, Cp seems to be the preferential partner of Lf and Mpo. After an intraperitoneal injection of Lf to rodents, the Cp-Lf complex has been shown to appear in their bloodstream. Cp prevents the interaction of Lf with protoplasts of Micrococcus luteus. Upon immunoprecipitation of Cp, the blood plasma becomes depleted of Lf and in a dose-dependent manner loses the capacity to inhibit the peroxidase activity of Mpo, but not the Mpo-catalyzed oxidation of thiocyanate in the (pseudo)halogenating cycle. Antimicrobial effect against E. coli displayed by a synergistic system that includes Lf and Mpo-H2O2-chloride, but not thiocyanate, as the substrate for Mpo is abrogated when Cp is added. Hence, Cp can be regarded as an anti-inflammatory factor that restrains the halogenating cycle and redirects the synergistic system Mpo-H2O2-chloride/thiocyanate to production of hypothiocyanate, which is relatively harmless for the human organism. Structure and functions of the 2Cp-2Lf-Mpo complex and binary complexes Cp-Lf and 2Cp-Mpo in inflammation are discussed.

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