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User:Estelle Metzger/Sandbox
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Some study to find a treatment for the Parkinson's disease are focused on LRRK2. Indeed, mutations in LRRK2, which increases its kinase activity, are found in case of Parkinson’s disease. Thus, a kinase inhibitor for LRRK2 would be an interesting thetapeutic target. | Some study to find a treatment for the Parkinson's disease are focused on LRRK2. Indeed, mutations in LRRK2, which increases its kinase activity, are found in case of Parkinson’s disease. Thus, a kinase inhibitor for LRRK2 would be an interesting thetapeutic target. | ||
| - | Thanks to the similarity between LRRK2 and Roco4 from the ''Dictyostelium'', Roco4 is used in studies with a view to finding that inhibitor. One of the candidates to inhibit this activity is LRRK2-IN-1<ref>doi: 10.1021/jm5018779</ref>. | + | Thanks to the similarity between LRRK2 and Roco4 from the ''Dictyostelium'', Roco4 is used in studies with a view to finding that inhibitor. One of the candidates to inhibit this activity is LRRK2-IN-1<ref name="Bernd">doi: 10.1021/jm5018779</ref>. |
| - | Pour ajouter une référence : <ref> | + | Pour ajouter une référence : <ref>Rentrer doi:... de la publi</ref> et si on veut utiliser la réf plusieurs fois, il faut lui donner un nom |
== Humanized Roco4 == | == Humanized Roco4 == | ||
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This involves autophosphorylation of some residues in the activation loop. . Autophosphorylation not only results in the reorientation of the activation loop, but often also alters ATP binding and/or interaction with substrates. (Huse and Kuriyan 2002 kornev). In Roco4 kinase, there are four phosphorylation sites in the activation loop : Ser1181, Ser1184, Ser1187, and Ser1189. | This involves autophosphorylation of some residues in the activation loop. . Autophosphorylation not only results in the reorientation of the activation loop, but often also alters ATP binding and/or interaction with substrates. (Huse and Kuriyan 2002 kornev). In Roco4 kinase, there are four phosphorylation sites in the activation loop : Ser1181, Ser1184, Ser1187, and Ser1189. | ||
| - | The structure of ''Dictyostelium'' Roco4 kinase in complex with the LRRK2 inhibitor H1152 allows us to see that Roco4 and other Roco family proteins are essential for the optimization of the current, and identification of new LRRK2 kinase inhibitor. To have a Roco4 protein which have an active site resembling human LRRK2, researchers use a ''Dictyostelium'' Roco4 mutant (F1107L and F1161L) which is called humanized Roco4<ref | + | The structure of ''Dictyostelium'' Roco4 kinase in complex with the LRRK2 inhibitor H1152 allows us to see that Roco4 and other Roco family proteins are essential for the optimization of the current, and identification of new LRRK2 kinase inhibitor. To have a Roco4 protein which have an active site resembling human LRRK2, researchers use a ''Dictyostelium'' Roco4 mutant (F1107L and F1161L) which is called humanized Roco4<ref name="Bernd"/>. |
Revision as of 10:25, 26 January 2017
Humanized Roco4 bound to LRRK2-IN-1
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References
- ↑ 1.0 1.1 Gilsbach BK, Messias AC, Ito G, Sattler M, Alessi DR, Wittinghofer A, Kortholt A. Structural Characterization of LRRK2 Inhibitors. J Med Chem. 2015 May 1. PMID:25897865 doi:http://dx.doi.org/10.1021/jm5018779
- ↑ Rentrer doi:... de la publi

