Figure 7
Figure 7. Regulation of intracellular cAMP in platelets by thrombin. Thrombin restricts intracellular cAMP content by suppression of synthesis from ATP and acceleration of hydrolysis of cAMP to 5′AMP by PDE3A. After activation of PAR-1, thrombin inhibits adenylate cyclase either through PAR1-coupled Gi protein directly, through Gq protein directly, or through Gq protein-induced of ADP from dense granules via the PLCβ pathway. In the latter, secreted ADP binds to the outside surface P2Y12 receptor, which is coupled to Gi2 to inhibit adenylate cyclase. Furthermore, thrombin via PAR-1 links to Gq, stimulates PI3K and PDK1, which in turn phosphorylates Akt, which in turn phosphorylates PDE3A. Elevation of PDE3A lowers intracellular cAMP content.

Regulation of intracellular cAMP in platelets by thrombin. Thrombin restricts intracellular cAMP content by suppression of synthesis from ATP and acceleration of hydrolysis of cAMP to 5′AMP by PDE3A. After activation of PAR-1, thrombin inhibits adenylate cyclase either through PAR1-coupled Gi protein directly, through Gq protein directly, or through Gq protein-induced of ADP from dense granules via the PLCβ pathway. In the latter, secreted ADP binds to the outside surface P2Y12 receptor, which is coupled to Gi2 to inhibit adenylate cyclase. Furthermore, thrombin via PAR-1 links to Gq, stimulates PI3K and PDK1, which in turn phosphorylates Akt, which in turn phosphorylates PDE3A. Elevation of PDE3A lowers intracellular cAMP content.

Close Modal
This Feature Is Available To Subscribers Only

or Create an Account

Close Modal
Close Modal