The displacement of calcium from osteocalcin at submicromolar concentrations of free lead

Abstract

Lead, an environmental toxin, is known to impair some of the functional properties of osteocalcin, a small protein (MW, 5700) active in bone mineralization and resorption. To investigate a possible mechanism of lead toxicity at the molecular level, we have studied the interaction of lead with osteocalcin using 43Ca and 1H NMR. The measured 43Ca NMR linewidth as well as longitudinal relaxation rate (1/T 1) of 43CaCl 2 progressively increased with increasing amounts of added osteocalcin. A titration measuring 43Ca linewidth as a function of [Ca 2+]/[Osteocalcin] ratio could be fitted to a single metal binding site with a dissociation constant of u μM. The 43Ca 1/T 1 of Ca-osteocalcin decreased in the presence of Pb 2+ due to competitive displacement of Ca 2+ by Pb 2+. The magnitude of decrease in the effect of osteocalcin on 43Ca 1/T 1 in the presence of Pb 2+ was consistent with the existence of only one tight divalent cation binding site. An analysis of the NMR T 1, data in osteocalcin solutions containing both Pb 2+ and Ca 2+ yielded a Pb-osteocalcin dissociation constant of about 2 nM. The 1H NMR spectra showed Pb-induced changes in the same aliphatic and aromatic resonances of osteocalcin that are also affected by Ca 2+-binding, supporting interaction of Pb 2+ at the Ca 2+ site. However, the existence of significant differences between the Pb-osteocalcin and Ca-osteocalcin NMR spectra indicates some differences in the structures of the two complexes. Since Pb 2+ inhibits the binding of osteocalcin to hydraxyapatite, the high affinity of Pb 2+ for osteocalcin would indicate significant inactivation of osteocalcin even at submicromolar free lead levels. Pb 2+-induced inactivation of osteocalcin could affect bone mineral dynamics and may be related to the observed inverse correlation between blood Pb 2+-levels and stature and chest circumference observed in growing children.