Gene/Protein
Disease
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Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
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Drug
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Target Concepts:
Gene/Protein
Disease
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Drug
Enzyme
Compound
Query: EC:3.6.4.4 (
kinesin
)
5,033
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Targeting protein for Xklp2
(
TPX2
) activates the Ser/Thr kinase Aurora A in mitosis and targets it to the mitotic spindle [1, 2]. These effects on Aurora A are mediated by the N-terminal domain of
TPX2
, whereas a C-terminal fragment has been reported to affect microtubule nucleation [3]. Using the Xenopus system, we identified a novel role of
TPX2
during mitosis. Injection of
TPX2
or its C terminus (TPX2-CT) into blastomeres of two-cell embryos led to potent cleavage arrest. Despite cleavage arrest,
TPX2
-injected embryos biochemically undergo multiple rounds of DNA synthesis and mitosis, and arrested blastomeres have abnormal spindles, clustered centrosomes, and an apparent failure of cytokinesis. In Xenopus S3 cells, transfection of
TPX2
-FL causes spindle collapse, whereas
TPX2
-CT blocks pole segregation, resulting in apposing spindle poles with no evident displacement of Aurora A. Analysis of
TPX2
-CT deletion peptides revealed that only constructs able to interact with the class 5
kinesin
-like motor protein Eg5 induce the spindle phenotypes. Importantly, injection of Eg5 into
TPX2
-CT-arrested blastomeres causes resumption of cleavage. These results define a discrete domain within the C terminus of
TPX2
that exerts a novel Eg5-dependent function in spindle pole segregation.
...
PMID:Spindle pole regulation by a discrete Eg5-interacting domain in TPX2. 1837 77
The bipolar spindle is a highly dynamic structure that assembles transiently around the chromosomes and provides the mechanical support and the forces required for chromosome segregation. Spindle assembly and chromosome movements rely on the regulation of microtubule dynamics and a fine balance of forces exerted by various molecular motors. Chromosomes are themselves central players in spindle assembly. They generate a RanGTP gradient that triggers microtubule nucleation and stabilization locally and they interact dynamically with the microtubules through motors targeted to the chromatin. We have previously identified and characterized two of these so-called chromokinesins: Xkid (
kinesin
10) and Xklp1 (
kinesin
4). More recently, we found that Hklp2/kif15 (
kinesin
12) is targeted to the chromosomes through an interaction with Ki-67 in human cells and is therefore a novel chromokinesin. Hklp2 also associates with the microtubules specifically during mitosis, in a TPX2 (
targeting protein for Xklp2
)-dependent manner. We have shown that Hklp2 participates in spindle pole separation and in the maintenance of spindle bipolarity in metaphase. To better understand the function of Hklp2, we have performed a detailed domain analysis. Interestingly, from its positioning on the chromosome arms, Hklp2 seems to restrict spindle pole separation. In the present review, we summarize the current knowledge of the function and regulation of the different kinesins associated with chromosome arms during cell division, including Hklp2 as a novel member of this so-called chromokinesin family.
...
PMID:Chromokinesins: localization-dependent functions and regulation during cell division. 2193 81
TPX2 (
targeting protein for Xklp2
) is a multifunctional mitotic spindle assembly factor that in mammalian cells localizes and regulates mitotic motor protein
kinesin
-5 (also called Eg5 or kif11). We previously showed that upon depletion or inhibition of
kinesin
-5 in cultured neurons, microtubule movements increase, resulting in faster growing axons and thinner dendrites. Here, we show that depletion of TPX2 from cultured neurons speeds their rate of process outgrowth, similarly to
kinesin
-5 inhibition. The phenotype is rescued by TPX2 re-expression, but not if TPX2's
kinesin
-5-interacting domain is deleted. These results, together with studies showing a spike in TPX2 expression during dendritic differentiation, suggest that the levels and distribution of TPX2 are likely to be determinants of when and where
kinesin
-5 acts in neurons.
...
PMID:TPX2 regulates neuronal morphology through kinesin-5 interaction. 2625 90
