cyclic amp control measured in two compartments in hek293 cells phosphodiesterase km is more important than phosphodiesterase localization环腺苷酸控制测量两个隔间在hek293细胞中磷酸二酯酶公里比磷酸二酯酶定位更重要.pdfVIP
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cyclic amp control measured in two compartments in hek293 cells phosphodiesterase km is more important than phosphodiesterase localization环腺苷酸控制测量两个隔间在hek293细胞中磷酸二酯酶公里比磷酸二酯酶定位更重要
Cyclic AMP Control Measured in Two Compartments in
HEK293 Cells: Phosphodiesterase KM Is More Important
than Phosphodiesterase Localization
Karina Matthiesen, Jacob Nielsen*
Synaptic Transmission 2, H. Lundbeck A/S, Copenhagen, Denmark
Abstract
The intracellular second messenger cyclic AMP (cAMP) is degraded by phosphodiesterases (PDE). The knowledge of
individual families and subtypes of PDEs is considerable, but how the different PDEs collaborate in the cell to control a cAMP
signal is still not fully understood. In order to investigate compartmentalized cAMP signaling, we have generated a
membrane-targeted variant of the cAMP Bioluminiscence Resonance Energy Transfer (BRET) sensor CAMYEL and have
compared intracellular cAMP measurements with it to measurements with the cytosolic BRET sensor CAMYEL in HEK293
cells. With these sensors we observed a slightly higher cAMP response to adenylyl cyclase activation at the plasma
membrane compared to the cytosol, which is in accordance with earlier results from Fluorescence Resonance Energy
Transfer (FRET) sensors. We have analyzed PDE activity in fractionated lysates from HEK293 cells using selective PDE
inhibitors and have identified PDE3 and PDE10A as the major membrane-bound PDEs and PDE4 as the major cytosolic PDE.
Inhibition of membrane-bound or cytosolic PDEs can potentiate the cAMP response to adenylyl cyclase activation, but we
see no significant difference between the potentiation of the cAMP response at the plasma membrane and in cytosol when
membrane-bound and cytosolic PDEs are inhibited. When different levels of stimulation were tested, we found that PDEs 3
and 10 are mainly responsible for cAMP degradation at low intracellular cAMP concentrations, whereas PDE4 is more
important for con
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