Journal
ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS
Volume 375, Issue 1, Pages 161-164Publisher
ACADEMIC PRESS INC
DOI: 10.1006/abbi.1999.1648
Keywords
myosin; Src homology; protozoa; amoeba; affinity
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The domain organization of Acanthamoeba myosin-I, an oligomodular motor protein, includes a potentially important protein interaction module that is mostly uncharacterized, The Src homology 3, SH3, domain of myosin-I binds Acan125, a protein containing at least two consensus ligand binding domains: C-terminal SH3 binding motifs (PXXP) and N-terminal leucine-rich repeats. We report the first affinities determined for an SH3 domain of any myosin, namely, K-d = 7 mu M for a 21-residue synthetic peptide based on the PXXP domain sequence and K-d = 0.15 mu M for the PXXP domain included in the C-terminus of Acan125. These values are consistent with affinities reported for peptides and proteins that associate with SH3, By deletional analysis me show that only the PXXP domain is required for Acan125 to interact with the SH3 domain of Acanthamoeba myosin-IC (AmyoC(SH3)). The synthetic peptide described above at a concentration near the K-d for SH3 binding blocked the interaction between native AmyoC and Acan125, mapping the interaction to the PXXP domain of Acan125 and the SH3 domain of myosin-I, These results are consistent with prototypical SH3 binding and suggest that a PXXP module is both necessary and sufficient to interact with an SH3 module of myosin-I. (C) 2000 Academic Press.
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