User:Lbates2008

I am adding onto the existing article on PLCg1. I think I'm going to add my paragraphs under the function tab:

Common to all PLC isozymes, PLCg1 consists of an N-terminal PH domain, which translocates PLC to the plasma membrane and binds PIP3, four EF hands, an X and Y catalytic region comprising the TIM barrel, and a C-terminal C2 domain. Specific to the PLCg isozymes is a large separation between the X and Y domains consisting of a split PH domain, tandem SH2 domains, and an SH3 domain. The SH2 domains bind phosphorylated tyrosine residues on target proteins via their FLVR sequence motifs, activating the catalytic function of PLCg; and the SH3 domain binds to proline-rich sequences on the target protein.

PLCg1 can be activated by receptor tyrosine kinases (RTKs) and non-receptor tyrosine kinases. For example, when activated, fibroblast growth factor receptor 1 and epidermal growth factor receptor are RTKs that, upon ligand binding, have phosphorylated tyrosine residues, which provide docking sites for PLCg1 SH2 domains. The activated RTKs phosphorylate PLCg1 at tyrosines located at position 472, 771, 775, 783, and 1254. Non-receptor tyrosine kinases interact with PLCg1 in large complexes at the plasma membrane. For example, in T cells, Lck and Fyn (Src family kinases) phosphorylate immunoreceptor tyrosine-based activation motifs (ITAMs) on the T-cell antigen receptor (TCR). The phosphorylated ITAMs recruit ZAP-70, which phosphorylates tyrosines in LAT and SLP-76. PLCg1 binds to LAT through its n-terminal SH2 domain and to SLP-76 via its SH3 domain.