Allosteric inhibition of kinesin-5 modulates its processive directional motility

被引:86
|
作者
Kwok, Benjamin H.
Kapitein, Lukas C.
Kim, Jeffrey H.
Peterman, Erwin J. G.
Schmidt, Christoph F.
Kapoor, Tarun M.
机构
[1] Vrije Univ Amsterdam, Dept Phys & Astron, NL-1081 HV Amsterdam, Netherlands
[2] Vrije Univ Amsterdam, Ctr Laser, NL-1081 HV Amsterdam, Netherlands
[3] Rockefeller Univ, Lab Chem & Cell Biol, New York, NY 10021 USA
[4] Univ Gottingen, Inst Phys 3, Fak Phys, D-37077 Gottingen, Germany
关键词
D O I
10.1038/nchembio812
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Small-molecule inhibitors of kinesin-5 (refs. 1-3), a protein essential for eukaryotic cell division(4), represent alternatives to antimitotic agents that target tubulin(5,6). While tubulin is needed for multiple intracellular processes, the known functions of kinesin-5 are limited to dividing cells, making it likely that kinesin-5 inhibitors would have fewer side effects than do tubulin-targeting drugs. Kinesin-5 inhibitors, such as monastrol(1), act through poorly understood allosteric mechanisms, not competing with ATP binding(7,8). Moreover, the microscopic mechanism of full-length kinesin-5 motility is not known. Here we characterize the motile properties and allosteric inhibition of Eg5, a vertebrate kinesin-5, using a GFP fusion protein in single-molecule fluorescence assays(9). We find that Eg5 is a processive kinesin whose motility includes, in addition to ATP-dependent directional motion, a diffusive component not requiring ATP hydrolysis. Monastrol suppresses the directional processive motility of microtubule-bound Eg5. These data on Eg5' s allosteric inhibition will impact these inhibitors' use as probes and development as chemotherapeutic agents.
引用
收藏
页码:480 / 485
页数:6
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