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Enzyme
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Target Concepts:
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Query: EC:3.6.4.4 (
kinesin
)
5,033
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Smg GDS is a regulator having two activities on a group of small G proteins including the Rho and Rap1 family members and Ki-Ras; one is to stimulate their GDP/GTP exchange reactions, and the other is to inhibit their interactions with membranes. Structurally, it has 11 Arm repeats, a protein interaction motif, found in the Drosophila Armadillo protein, a homolog of mammalian beta-catenin. We have isolated here an Smg GDS-interacting protein from a human brain cDNA library by use of the yeast two-hybrid method and named it
SMAP
(Smg GDS-associated protein).
SMAP
was a protein with a Mr of 91,189 and 792 amino acids.
SMAP
had 9 Arm repeats. Recombinant
SMAP
interacted with recombinant Smg GDS but did not affect the two activities of Smg GDS on RhoA.
SMAP
was tyrosine phosphorylated by v-Src, and this phosphorylation reduced the affinity of
SMAP
for Smg GDS. Tissue and subcellular distribution analyses indicated that
SMAP
was ubiquitously expressed and highly concentrated at the endoplasmic reticulum area. Searches for sequence homology to
SMAP
revealed that
SMAP
was significantly homologous to sea urchin SpKAP115, suggesting that
SMAP
is a mammalian counterpart of SpKAP115 or its related protein. SpKAP115 is an accessory subunit of sea urchin
kinesin
II, an ATPase motor that transports vesicles along microtubules. These results suggest that
SMAP
serves as an adaptor for both Smg GDS and
kinesin
II or its related protein and links them with both the Smg GDS-regulated small G protein and Src tyrosine kinase signalings.
...
PMID:SMAP, an Smg GDS-associating protein having arm repeats and phosphorylated by Src tyrosine kinase. 890 Jan 89
We have recently isolated
SMAP
(Smg GDS-associated protein; Smg GDS: small G protein GDP dissociation stimulator) as a novel Smg GDS-associated protein, which has Armadillo repeats and is phosphorylated by Src tyrosine kinase.
SMAP
is a human counterpart of mouse KAP3 (
kinesin
superfamily-associated protein) that is associated with mouse KIF3A/B (a kinesin superfamily protein), which functions as a microtubule-based ATPase motor for organelle transport. We isolated here a
SMAP
-interacting protein from a human brain cDNA library, identified it to be a human homolog of Xenopus XCAP-E (Xenopus chromosome-associated polypeptide), a subunit of condensins that regulate the assembly and structural maintenance of mitotic chromosomes, and named it HCAP (Human chromosome-associated polypeptide). Tissue and subcellular distribution analyses indicated that HCAP was ubiquitously expressed and highly concentrated in the nuclear fraction, where
SMAP
and KIF3B were also present.
SMAP
was extracted as a ternary complex with HCAP and KIF3B from the nuclear fraction in the presence of Mg-ATP. The results suggest that
SMAP
/KAP3 serves as a linker between HCAP and KIF3A/B in the nucleus, and that
SMAP
/KAP3 plays a role in the interaction of chromosomes with an ATPase motor protein.
...
PMID:Complex formation of SMAP/KAP3, a KIF3A/B ATPase motor-associated protein, with a human chromosome-associated polypeptide. 950 51
We have identified the Drosophila homologue of the non-motor accessory subunit of
kinesin
-II motor complex. It is homologous to the SpKAP115 of the sea urchin, KAP3A and KAP3B of the mouse, and
SMAP
protein in humans. In situ hybridization using a DmKAP specific cRNA probe has revealed a dynamic pattern of expression in the developing nervous system. The staining first appears in a subset of cells in the embryonic central nervous system at stage 13 and continues till the first instar larva stage. At the third instar larva stage the staining gets restricted to a few cells in the optic lobe and in the ventral ganglion region. It has also stained a subset of sensory neurons from late stage 13 and till the first instar larva stage. The DmKAP expression pattern in the nervous system corresponds well with that of Klp64D and Klp68D as reported earlier. In addition, we have found that the DmKAP gene is constitutively expressed in the germline cells and in follicle cells during oogenesis. These cells are also stained using an antibody to KLP68D protein, but mRNA in situ hybridization using KLP64D specific probe has not stained these cells. Together these results proved a basis for further analysis of tissue specific function of DmKAP in future.
...
PMID:Dynamic expression pattern of kinesin accessory protein in Drosophila. 1238 71
