Literature DB >> 9003183

Dictyostelium discoideum myosin II: characterization of functional myosin motor fragments.

S E Kurzawa1, D J Manstein, M A Geeves.   

Abstract

The transient kinetic properties of the recombinant myosin head fragments M761 and M781, which both lack the light chain binding domain (LCBD) and correspond to the first 761 and 781 residues of Dictyostelium discoideum myosin II, were compared with those of the subfragment 1-like fragment M864 and a shorter catalytic domain fragment M754. The properties of M761, M781, and M864 are almost identical in regard to nucleotide binding, nucleotide hydrolysis, actin binding, and the interactions between actin and nucleotide binding sites. Only the rate of the hydrolysis step was significantly faster for M761 and the affinity of M781 for actin significantly weaker than for M864. This indicates that the LCBD plays no major role in the biochemical behavior of the myosin head. In contrast, loss of the peptide between 754 and 761 produced several major changes in the property of M754 as documented previously [Woodward, S. K. A., Geeves, M. A., & Manstein, D. J. (1995) Biochemistry 34, 16056-16064]. We further show that C-terminal extension of M761 with one or two alpha-actinin repeats has very little effect on the behavior of the protein. The recombinant nature of M761 and the fact that it can be produced and purified in large amounts make it an ideal construct for systematic studies of the structure, kinetics, and function of the myosin motor.

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Year:  1997        PMID: 9003183     DOI: 10.1021/bi962166b

Source DB:  PubMed          Journal:  Biochemistry        ISSN: 0006-2960            Impact factor:   3.162


  31 in total

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2.  Structure of a genetically engineered molecular motor.

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3.  Mutations in the relay loop region result in dominant-negative inhibition of myosin II function in Dictyostelium.

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4.  Myosin subfragment 1 structures reveal a partially bound nucleotide and a complex salt bridge that helps couple nucleotide and actin binding.

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5.  Phenamacril is a reversible and noncompetitive inhibitor of Fusarium class I myosin.

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6.  Dynamics of myosin-driven skeletal muscle contraction: I. Steady-state force generation.

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Review 7.  Molecular engineering of myosin.

Authors:  Dietmar J Manstein
Journal:  Philos Trans R Soc Lond B Biol Sci       Date:  2004-12-29       Impact factor: 6.237

Review 8.  Dynamics of actomyosin interactions in relation to the cross-bridge cycle.

Authors:  Wei Zeng; Paul B Conibear; Jane L Dickens; Ruth A Cowie; Stuart Wakelin; András Málnási-Csizmadia; Clive R Bagshaw
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9.  Functional and biophysical analyses of the class XIV Toxoplasma gondii myosin D.

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10.  Solution properties of full length and truncated forms of myosin subfragment 1 from Dictyostelium discoideum.

Authors:  J R Reynoso; A Bobkov; A Muhlrad; E Reisler
Journal:  J Muscle Res Cell Motil       Date:  2001       Impact factor: 2.698

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