4.6 Article

Drosophila myosin VIIA is a high duty ratio motor with a unique kinetic mechanism

Journal

JOURNAL OF BIOLOGICAL CHEMISTRY
Volume 281, Issue 11, Pages 7151-7160

Publisher

AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.M511592200

Keywords

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Funding

  1. NIAMS NIH HHS [AR 048526, AR 41653, AR 048898] Funding Source: Medline
  2. NIDCD NIH HHS [DC 006103] Funding Source: Medline

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Mutations of myosin VIIA cause deafness in various species from human and mice to Zebrafish and Drosophila. We analyzed the kinetic mechanism of the ATPase cycle of Drosophila myosin VIIA by using a single-headed construct with the entire neck domain. The steady-state ATPase activity (0.06 s(-1)) was markedly activated by actin to yield V-max and K-ATPase of 1.72 s(-1) and 3.2 mu M, respectively. The most intriguing finding is that the ATP hydrolysis predominantly takes place in the actin-bound form (actin-attached hydrolysis) for the actomyosin VIIA ATPase reaction. The ATP hydrolysis rate was much faster for the actin-attached form than the dissociated form, in contrast to other myosins reported so far. Both the ATP hydrolysis step and the phosphate release step were significantly faster than the entire ATPase cycle rate, thus not rate-determining. The rate of ADP dissociation from actomyosin VIIA was 1.86 s(-1), which was comparable with the overall ATPase cycle rate, thus assigned to be a rate-determining step. The results suggest that Drosophila myosin VIIA spends the majority of the ATPase cycle in an actomyosin . ADP form, a strong actin binding state. The duty ratio calculated from our kinetic model was similar to 0.9. Therefore, myosin VIIA is classified to be a high duty ratio motor. The present results suggested that myosin VIIA can be a processive motor to serve cargo trafficking in cells once it forms a dimer structure.

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