Cdc42 and mDia3 regulate microtubule
attachment to kinetochores
Yasuda S, Oceguera-Yanez F, Kato T, Okamoto M, Yonemura S, Terada Y, Ishizaki
T and Narumiya S
Nature 428(6984):767-71 (2004)
SUMMARY
During mitosis, the mitotic spindle, a bipolar structure composed of microtubules
(MTs) and associated motor proteins, segregates sister chromatids to daughter
cells. Initially some MTs emanating from one centrosome attach to the
kinetochore at the centromere of one of the duplicated chromosomes. This
attachment allows rapid poleward movement of the bound chromosome. Subsequent
attachment of the sister kinetochore to MTs growing from the other centrosome
results in the bi-orientation of the chromosome, in which interactions
between kinetochores and the plus ends of MTs are formed and stabilized.
These processes ensure alignment of chromosomes during metaphase and their
correct segregation during anaphase. Although many proteins constituting
the kinetochore have been identified and extensively studied, the signalling
responsible for MT capture and stabilization is unclear. Small GTPases
of the Rho family regulate cell morphogenesis by organizing the actin
cytoskeleton and regulating MT alignment and stabilization. We now show
that one member of this family, Cdc42, and its effector, mDia3, regulate
MT attachment to kinetochores.
LINK
http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&dopt=Citation&list_uids=15085137
