AI Article Synopsis

  • Kinesins are essential motor proteins that play vital roles in processes like intracellular transport and cell division, with specific kinesins, such as Eg5 and Kif15, being key during mitosis.
  • Drugs targeting kinesins like Eg5 show potential in cancer treatment, and Kif15 may serve as a promising drug target due to its ability to compensate for Eg5’s functions.
  • The study discusses the detailed biochemical and structural characteristics of Kif15, highlighting its differences and similarities with Eg5, which illuminates their unique mechanisms of action in relation to microtubule interactions.

Article Abstract

Kinesins constitute a superfamily of microtubule-based motor proteins with important cellular functions ranging from intracellular transport to cell division. Some kinesin family members function during the mitotic phase of the eukaryotic cell cycle and are crucial for the successful progression of cell division. In the early stages of mitosis, during prometaphase, certain kinesins are required for the formation of the bipolar spindle, such as Eg5 and Kif15, which seem to possess partially overlapping functions. Because kinesins transform the chemical energy from ATP hydrolysis into mechanical work, inhibition of their function is a tractable approach for drug development. Drugs targeting Eg5 have shown promise as anticancer agents. Kif15 has recently come to the fore because it can substitute the functions of Eg5, and may itself have potential as a prospective drug target. Here, the initial biochemical, kinetic and structural characterization of Kif15 is reported and it is compared with the functionally related motor Eg5. Although Kif15 contains ADP in the catalytic site, its motor-domain structure was captured in the `ATP-like' configuration, with the neck linker docked to the catalytic core. The interaction of Kif15 with microtubules was also investigated and structural differences between these two motors were elucidated which indicate profound differences in their mode of action, in agreement with current models of microtubule cross-linking and sliding.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3919264PMC
http://dx.doi.org/10.1107/S1399004713028721DOI Listing

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