The zinc-binding properties of an endogenous protein inhibitor of protein kinase C was studied. Equilibrium gel penetration revealed that 1 mol of this protein binds 0.97 mol of zinc with a dissociation constant of 4.3 μM. The site of zinc-binding. MVVNEGSDGGQSVYHVHLHVLGGR, was indentified by a multi-step process consisting of tryptic digestion, fragment isolation, transfer to nitrocellulose, and hybridization with ⁶⁵ZnCl₂. Binding of ⁶⁵ZnCl₂ to selected synthetic fragments further localized the site of interaction to the sequence QSVYHVHLHVL. This region contains 3 closely positioned histidine residues and represent a novel zinc-binding site.