Metal binding properties of single amino acid deletion mutants of zinc finger peptides: studies using cobalt(II) as a spectroscopic probe.

Y Shi, R D Beger and J M Berg

Department of Biophysics and Biophysical Chemistry, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205.

ABSTRACT

Peptides corresponding to Cys2His2 zinc finger domains fromwhich one amino acid has been deleted have been synthesizedand their metal-binding properties characterized. In contrastto earlier reports (Párraga, G., S. Horvath, L. Hood,E. T. Young, and R. E. Klevit. 1990. Proc. Natl. Acad. Sci.USA. 87:137-141.), such peptides do bind metal ions such ascobalt(II). A peptide with the sequence ProTyrLysCysProGluCysLysSerPheSerGlnLysSerAspLeuValLysHisGlnArgThrHisThrGly (which corresponds to a previously characterized consensuszinc finger sequence from which a Gly residue immediately followingthe second Cys residue has been deleted) was found to form a1:1 peptide to cobalt(II) complex with an absorption spectrumquite similar to those previously observed for zinc finger peptide-cobalt(II)complexes. The dissociation constant for this complex is 6 x10(-6)M, a factor of 100 times higher than that for the parentpeptide. A peptide with the sequence LysProTyrProCysGlyLeuCysArgCysPheThrArgArgAspLeuLeulleArgHisAlaGln- LyslleHisSerGlyAsnLeu corresponding to a similar mutationof the peptide ADR1 was also characterized. Spectroscopic studieswith cobalt(II) revealed that this peptide forms both 1:1 and2:1 peptide to cobalt(II) complexes. The absorption spectraof the two forms and the dissociation constants were determinedvia deconvolution methods. In contrast, the parent peptide ADR1awas found to form only a 1:1 complex under comparable conditionsand this 1:1 complex was found to be more stable than that forthe mutant. These results reveal that deletion mutations doadversely affect the stability of zinc finger peptide-metalcomplexes but that the effects are not as drastic as had beenpreviously described.

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