Spleen Tyrosine Kinase
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Tyrosine-protein kinase SYK | ||
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nach PDB 1A81 | ||
Andere Namen |
Spleen tyrosine kinase, p72-Syk | |
Eigenschaften des menschlichen Proteins | ||
Masse/Länge Primärstruktur | 635 Aminosäuren, 72.066 Da | |
Bezeichner | ||
Externe IDs | ||
Enzymklassifikation | ||
EC, Kategorie | 2.7.10.2 | |
Orthologe (Mensch) | ||
Entrez | 6850 | |
Ensembl | ENSG00000165025 | |
UniProt | P43405 | |
Refseq (mRNA) | NM_001135052.3 | |
Refseq (Protein) | NP_001128524.1 | |
PubMed-Suche | 6850
|
SYK ist ein Enzym aus der Gruppe der Tyrosinkinasen.
Eigenschaften
Als Tyrosinkinase phosphoryliert Syk Tyrosine in Proteinen. Syk besitzt eine SH2-Proteindomäne und bindet damit an aktivierte Rezeptor-Tyrosinkinasen in der Zellmembran. In Folge einer Aktivierung von Syk werden VAV1, PLCG1, PI-3-Kinase, LCP2 und BLNK phosphoryliert. Syk ist phosphoryliert.
Syk katalysiert die Reaktion: ATP + [Protein]-L-Tyrosin = ADP + [Protein]-L-Tyrosinphosphat
Syk bindet an Cbl,[1][2][3] CRKL,[4] FCGR2A,[5][6] FYN,[7][8] Grb2,[9][10] Lck,[11] LYN,[12] PTK2,[13] PTPN6,[9][14] und VAV1.[1][15][16]
Weblinks
Einzelnachweise
- ↑ a b Bertagnolo V, Marchisio M, Brugnoli F, Bavelloni A, Boccafogli L, Colamussi ML, Capitani S: Requirement of tyrosine-phosphorylated Vav for morphological differentiation of all-trans-retinoic acid-treated HL-60 cells. In: Cell Growth & Differentiation. 12, Nr. 4, April 2001, S. 193–200. PMID 11331248.
- ↑ Lupher ML, Rao N, Lill NL, Andoniou CE, Miyake S, Clark EA, Druker B, Band H: Cbl-mediated negative regulation of the Syk tyrosine kinase. A critical role for Cbl phosphotyrosine-binding domain binding to Syk phosphotyrosine 323. In: The Journal of Biological Chemistry. 273, Nr. 52, Dezember 1998, S. 35273–81. doi:10.1074/jbc.273.52.35273. PMID 9857068.
- ↑ Melander F, Andersson T, Dib K: Fgr but not Syk tyrosine kinase is a target for beta 2 integrin-induced c-Cbl-mediated ubiquitination in adherent human neutrophils. In: The Biochemical Journal. 370, Nr. Pt 2, März 2003, S. 687–94. doi:10.1042/BJ20021201. PMID 12435267. PMC 1223185 (freier Volltext).
- ↑ Oda A, Ochs HD, Lasky LA, Spencer S, Ozaki K, Fujihara M, Handa M, Ikebuchi K, Ikeda H: CrkL is an adapter for Wiskott-Aldrich syndrome protein and Syk. In: Blood. 97, Nr. 9, Mai 2001, S. 2633–9. doi:10.1182/blood.V97.9.2633. PMID 11313252.
- ↑ Ibarrola I, Vossebeld PJ, Homburg CH, Thelen M, Roos D, Verhoeven AJ: Influence of tyrosine phosphorylation on protein interaction with FcgammaRIIa. In: Biochimica et Biophysica Acta. 1357, Nr. 3, Juli 1997, S. 348–58. doi:10.1016/S0167-4889(97)00034-7. PMID 9268059.
- ↑ Kim MK, Pan XQ, Huang ZY, Hunter S, Hwang PH, Indik ZK, Schreiber AD: Fc gamma receptors differ in their structural requirements for interaction with the tyrosine kinase Syk in the initial steps of signaling for phagocytosis. In: Clinical Immunology. 98, Nr. 1, Januar 2001, S. 125–32. doi:10.1006/clim.2000.4955. PMID 11141335.
- ↑ Deckert M, Elly C, Altman A, Liu YC: Coordinated regulation of the tyrosine phosphorylation of Cbl by Fyn and Syk tyrosine kinases. In: The Journal of Biological Chemistry. 273, Nr. 15, April 1998, S. 8867–74. doi:10.1074/jbc.273.15.8867. PMID 9535867.
- ↑ Chung J, Gao AG, Frazier WA: Thrombspondin acts via integrin-associated protein to activate the platelet integrin alphaIIbbeta3. In: The Journal of Biological Chemistry. 272, Nr. 23, Juni 1997, S. 14740–6. doi:10.1074/jbc.272.23.14740. PMID 9169439.
- ↑ a b Ganju RK, Brubaker SA, Chernock RD, Avraham S, Groopman JE: Beta-chemokine receptor CCR5 signals through SHP1, SHP2, and Syk. In: The Journal of Biological Chemistry. 275, Nr. 23, Juni 2000, S. 17263–8. doi:10.1074/jbc.M000689200. PMID 10747947.
- ↑ Saci A, Liu WQ, Vidal M, Garbay C, Rendu F, Bachelot-Loza C: Differential effect of the inhibition of Grb2-SH3 interactions in platelet activation induced by thrombin and by Fc receptor engagement. In: The Biochemical Journal. 363, Nr. Pt 3, Mai 2002, S. 717–25. doi:10.1042/0264-6021:3630717. PMID 11964172. PMC 1222524 (freier Volltext).
- ↑ Thome M, Duplay P, Guttinger M, Acuto O: Syk and ZAP-70 mediate recruitment of p56lck/CD4 to the activated T cell receptor/CD3/zeta complex. In: The Journal of Experimental Medicine. 181, Nr. 6, Juni 1995, S. 1997–2006. doi:10.1084/jem.181.6.1997. PMID 7539035. PMC 2192070 (freier Volltext).
- ↑ Sidorenko SP, Law CL, Chandran KA, Clark EA: Human spleen tyrosine kinase p72Syk associates with the Src-family kinase p53/56Lyn and a 120-kDa phosphoprotein. In: Proceedings of the National Academy of Sciences. 92, Nr. 2, Januar 1995, S. 359–63. doi:10.1073/pnas.92.2.359. PMID 7831290. PMC 42739 (freier Volltext).
- ↑ Sada K, Minami Y, Yamamura H: Relocation of Syk protein-tyrosine kinase to the actin filament network and subsequent association with Fak. In: European Journal of Biochemistry. 248, Nr. 3, September 1997, S. 827–33. doi:10.1111/j.1432-1033.1997.00827.x. PMID 9342235.
- ↑ Dustin LB, Plas DR, Wong J, Hu YT, Soto C, Chan AC, Thomas ML: Expression of dominant-negative src-homology domain 2-containing protein tyrosine phosphatase-1 results in increased Syk tyrosine kinase activity and B cell activation. In: Journal of Immunology. 162, Nr. 5, März 1999, S. 2717–24. PMID 10072516.
- ↑ Deckert M, Tartare-Deckert S, Couture C, Mustelin T, Altman A: Functional and physical interactions of Syk family kinases with the Vav proto-oncogene product. In: Immunity. 5, Nr. 6, Dezember 1996, S. 591–604. doi:10.1016/S1074-7613(00)80273-3. PMID 8986718.
- ↑ Song JS, Gomez J, Stancato LF, Rivera J: Association of a p95 Vav-containing signaling complex with the FcepsilonRI gamma chain in the RBL-2H3 mast cell line. Evidence for a constitutive in vivo association of Vav with Grb2, Raf-1, and ERK2 in an active complex. In: The Journal of Biological Chemistry. 271, Nr. 43, Oktober 1996, S. 26962–70. doi:10.1074/jbc.271.43.26962. PMID 8900182.