Differential regulation of Pyk2 and focal adhesion kinase (FAK) - The C-terminal domain of FAK confers response to cell adhesion

Pyk2 is a recently described cytoplasmic tyrosine kinase that is related to focal adhesion kinase (FAK) and can be activated by a variety of stimuli that elevate intracellular calcium, in this report, we showed that Pyk2 and FAK tyrosine phosphorylation are regulated differentially by integrin-mediated cell adhesion and soluble factors both in rat aortic smooth muscle cells, which express endogenous Pyk2 and FAK, and in transfected Chinese hamster ovary cells, We also found that Pyk2 is diffusely present throughout the cytoplasm, while FAT( is localized in focal contacts as expected, suggesting that the different localization may account for their differential regulation, By analyzing a chimeric protein contain N-terminal and kinase domains of Pyk2 and C-terminal domain of FAK, we provided evidence that the distinctive C-terminal domains of Pyk2 and FAR were responsible for their differential regulation by integrins and soluble stimuli as well as their subcellular localization, Finally, we correlated FAR, Pyk2, and the chimeric protein binding to talin, but not paxillin, with their regulation by integrins and focal contact localization, These results demonstrate that the distinctive C-terminal domain of Pyk2 and FAK confer their differential regulation by different subcellular localization and association with the cytoskeletal protein talin.