MKLP1 Motor Domain

2.153,00 €

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ArtNr	MP01-XL
Hersteller	Cytoskeleton
Menge	1 x 1 mg
Kategorie	Metabolism Glucose Homeostasis Peptides & Proteins Recombinant Proteins Cell Biology Cell Stainings Nuclear
Typ	Proteins
Citations	Funk, C. J., Davis, A. S., Hopkins, J. A. and Middleton, K. M. (2004). Development of high-throughput screens for discovery of kinesin adenosine triphosphatase modulators. Anal. Biochem. 329, 68-76. Wada, Y., Hamasaki, T. and Satir, P. (2000). Evidence for a novel affinity mechanism of motor-assisted transport along microtubules. Mol. Biol. Cell 11, 161-169. Endow, S. A. and Waligora, K. W. (1998). Determinants of kinesin motor polarity. Science 281, 1200-1202.
ECLASS 10.1	32160409
ECLASS 11.0	32160409
UNSPSC	12352202
Alias	Kinesin Motor Domains, Kinesin, microtubule-activated ATPase, kinesin motility, MKLP kinesin motor domain protein, MKLP, MKLP kinesin
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Additional info	Product uses Measurement of microtubule-activated ATPase activity Identification/characterization of proteins or small molecules that affect motor ATPase activity Identification/characterization of proteins or small molecules that affect kinesin motility Identification/characterization of proteins or small molecules that affect motor/microtubule interactions Material There are approximately 50 human kinesins that are currently divided into at least 14 classes. Kinesins are involved in almost all aspects of intracellular transport and their well documented role in cell division suggests that they may be excellent targets for anti-mitotic drug discovery. All kinesin proteins contain a conserved motor domain that contains a microtubule binding site and the ATP binding / hydrolysis site. The motor domain of various kinesins have been shown to have widely differing sensitivities to ATP analogs and inhibitory compounds such as monastrol, such results lead the way to the identification of therapeutically useful kinesin specific inhibitors. Cytoskeleton, Inc. has made available a selection of recombinant human kinesin motor domain proteins from 8 of the 14 reported kinesin classes. The proteins are extensively quality controlled for purity (> 85%) and biological activity (microtubule activated ATPase activity must be at least comparable to published data). The protein domains are useful as targets for anti-mitotic drug discovery and as reagents for comparative studies of kinesin class specific motor activities. Purity Protein purity is determined by scanning densitometry of Coomassie Blue stained protein on a 12% polyacrylamide gel. All kinesin motor domains are > 85% pure. See figure 1 for example purities. Figure 1. Purity of kinesin motor domain proteins. BimC (BM01), CENP-E (CP01) and Eg5 (EG01) were run on SDS-PAGE gels and stained with coomassie blue. Biological Activity Kinesn motor activity is driven by ATP hydrolysis. All motor domain proteins therefore are tested with regards to their microtubule activated ATPase activity. Stringent quality controls that all Cytoskeleton, Inc's purified kinesin motor domains have ATPase activities comparable to published data. Figure 2. Microtubule activated kinesin ATPase assay (Cat. # BK060) using kinesin heavy chain motor domain protein (Cat. # KR01) and pre-formed microtubules (Cat. # MT001). Each condition (microtubules (MT) alone, kinesin alone and microtubules + kinesin) was performed in triplicates.
Delivery Time	1-2 Weeks
Shipping Temp.	AT
Storage on Arrival	4C
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