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-[[Image:2cxt.gif|left|200px]]<br /><applet load="2cxt" size="450" color="white" frame="true" align="right" spinBox="true"
+[[Image:2cxt.gif|left|200px]]<br /><applet load="2cxt" size="350" color="white" frame="true" align="right" spinBox="true"
 caption="2cxt, resolution 1.50&Aring;" />
 '''Crystal structure of mouse AMF / F6P complex'''<br />
 ==Overview==
-Autocrine motility factor (AMF), a tumor-secreted cytokine, stimulates, cell migration in vitro and metastasis in vivo. AMF is identical to the, extracellular cytokines neuroleukin and maturation factor and, interestingly, to the intracellular enzyme phosphoglucose isomerase. The, cytokine activity of AMF is inhibited by carbohydrate phosphate compounds, as they compete for AMF binding with the carbohydrate moiety of the AMF, receptor (AMFR), which is a glycosylated seven transmembrane helix, protein. Here, we report the first comprehensive high-resolution crystal, structure analyses of the inhibitor-free form and the eight types of, inhibitor (phosphate, erythrose 4-phosphate (E4P), arabinose 5-phosphate, (A5P), sorbitol 6-phosphate (S6P), 6-phosphogluconic acid (6PGA), fructose, 6-phosphate (F6P), glucose 6-phosphate (G6P), or mannose 6-phosphate, (M6P)) complexes of mouse AMF (mAMF). We assayed the inhibitory activities, of these inhibitors against the cytokine activity of mAMF. The inhibitory, activities of the six-carbon sugars (G6P, F6P, M6P, and 6PGA) were found, to be significantly higher than those of the four or five-carbon sugars, (E4P or A5P). The inhibitory activities clearly depend on the length of, the inhibitor molecules. A structural comparison revealed that a, water-mediated hydrogen bond between one end of the inhibitor and a rigid, portion of the protein surface in the shorter-chain inhibitor (E4P), complex is replaced by a direct hydrogen bond in the longer-chain, inhibitor (6PGA) complex. Thus, to obtain a new compound with higher, inhibitory activities against AMF, water molecules at the inhibitor, binding site of AMF should be replaced by a functional group of inhibitors, in order to introduce direct interactions with the protein surface. The, present structure-activity relationship studies will be valuable not only, for designing more effective AMF inhibitors but also for studying general, protein-inhibitor interactions.
+Autocrine motility factor (AMF), a tumor-secreted cytokine, stimulates cell migration in vitro and metastasis in vivo. AMF is identical to the extracellular cytokines neuroleukin and maturation factor and, interestingly, to the intracellular enzyme phosphoglucose isomerase. The cytokine activity of AMF is inhibited by carbohydrate phosphate compounds as they compete for AMF binding with the carbohydrate moiety of the AMF receptor (AMFR), which is a glycosylated seven transmembrane helix protein. Here, we report the first comprehensive high-resolution crystal structure analyses of the inhibitor-free form and the eight types of inhibitor (phosphate, erythrose 4-phosphate (E4P), arabinose 5-phosphate (A5P), sorbitol 6-phosphate (S6P), 6-phosphogluconic acid (6PGA), fructose 6-phosphate (F6P), glucose 6-phosphate (G6P), or mannose 6-phosphate (M6P)) complexes of mouse AMF (mAMF). We assayed the inhibitory activities of these inhibitors against the cytokine activity of mAMF. The inhibitory activities of the six-carbon sugars (G6P, F6P, M6P, and 6PGA) were found to be significantly higher than those of the four or five-carbon sugars (E4P or A5P). The inhibitory activities clearly depend on the length of the inhibitor molecules. A structural comparison revealed that a water-mediated hydrogen bond between one end of the inhibitor and a rigid portion of the protein surface in the shorter-chain inhibitor (E4P) complex is replaced by a direct hydrogen bond in the longer-chain inhibitor (6PGA) complex. Thus, to obtain a new compound with higher inhibitory activities against AMF, water molecules at the inhibitor binding site of AMF should be replaced by a functional group of inhibitors in order to introduce direct interactions with the protein surface. The present structure-activity relationship studies will be valuable not only for designing more effective AMF inhibitors but also for studying general protein-inhibitor interactions.
 ==About this Structure==
-CXT is a [http://en.wikipedia.org/wiki/Single_protein Single protein] structure of sequence from [http://en.wikipedia.org/wiki/Mus_musculus Mus musculus] with F6P and GOL as [http://en.wikipedia.org/wiki/ligands ligands]. Active as [http://en.wikipedia.org/wiki/Glucose-6-phosphate_isomerase Glucose-6-phosphate isomerase], with EC number [http://www.brenda-enzymes.info/php/result_flat.php4?ecno=5.3.1.9 5.3.1.9] Full crystallographic information is available from [http://ispc.weizmann.ac.il/oca-bin/ocashort?id=2CXT OCA].
+CXT is a [http://en.wikipedia.org/wiki/Single_protein Single protein] structure of sequence from [http://en.wikipedia.org/wiki/Mus_musculus Mus musculus] with <scene name='pdbligand=F6P:'>F6P</scene> and <scene name='pdbligand=GOL:'>GOL</scene> as [http://en.wikipedia.org/wiki/ligands ligands]. Active as [http://en.wikipedia.org/wiki/Glucose-6-phosphate_isomerase Glucose-6-phosphate isomerase], with EC number [http://www.brenda-enzymes.info/php/result_flat.php4?ecno=5.3.1.9 5.3.1.9] Full crystallographic information is available from [http://oca.weizmann.ac.il/oca-bin/ocashort?id=2CXT OCA].
 ==Reference==
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 [[Category: Naba, N.]]
 [[Category: Nagase, H.]]
-[[Category: Nakamura, K.T.]]
+[[Category: Nakamura, K T.]]
 [[Category: Raz, A.]]
 [[Category: Shiraiwa, K.]]
@@ Line 28: / Line 28: @@
 [[Category: isomerase]]
-''Page seeded by [http://ispc.weizmann.ac.il/oca OCA ] on Wed Nov 21 09:19:55 2007''
+''Page seeded by [http://oca.weizmann.ac.il/oca OCA ] on Thu Feb 21 16:53:28 2008''