Date published: 2025-9-8

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JRAB激活剂

JRAB Activators comprise a set of chemical compounds that enhance the functional activity of JRAB through various biochemical pathways. For instance, Forskolin, Isoproterenol, Epinephrine, Dibutyryl cAMP, and Rolipram all raise intracellular cAMP levels, which activate protein kinase A (PKA). PKA is known to phosphorylate numerous substrates within the cell, which can include interaction partners or regulatory proteins linked to JRAB's activity. This phosphorylation cascade can lead to an enhancement of JRAB's functional role, particularly in modulating cytoskeletal dynamics. Similarly, 8-Br-cAMP serves as a stable cAMP analog, ensuring sustained PKA activation and thus prolonged potential enhancement of JRAB function. Compounds like PMA activate protein kinase C (PKC), which also phosphorylates various substrates that might be involved in the pathways where JRAB operates, further promoting JRAB activity related to cytoskeletal architecture.

In addition to these cAMP- and PKA-mediated activations, JRAB's functional activity is influenced bycalcium signaling modulators such as Ionomycin and A23187, along with L-type calcium channel agonist Bay K8644, which increase intracellular calcium levels. Elevated calcium can trigger a multitude of signaling cascades that interact with JRAB's role in cytoskeletal organization and dynamics. Furthermore, the inhibition of protein phosphatases by Calyculin A and Okadaic acid results in a broader range of proteins remaining phosphorylated within JRAB-associated pathways. This hyperphosphorylation state can potentially lead to an enhanced activity of JRAB, as it might affect the proteins that interact with or regulate JRAB.

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