Location, location, location: PDE4D5 function is directed by its unique N-terminal region

Wills, Lauren P.; Ehsan, Munisah; Whiteley, Ellanor L.; Baillie, George S.

doi:10.1016/j.cellsig.2016.01.008

Cited by 10 publications

(15 citation statements)

References 47 publications

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“…Among others, this period is characterized by a distinct reduction of PKAc levels attributed to reduced ribosome translation or stability of the kinase subunit 17,18 . Activation of phosphodiesterases (PDE) counteracts cAMP levels and control the duration and amplitude of downstream signaling 19,20 . The binding of the endogenous protein kinase inhibitor (PKI) to PKAc also contributes to the attenuation of cAMP signaling in hormone-stimulated cells 21,22 .…”

Section: Introductionmentioning

confidence: 99%

Feedback inhibition of cAMP effector signaling by a chaperone-assisted ubiquitin system

Rinaldi¹,

Donne²,

Catalanotti

et al. 2019

Nat Commun

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Activation of G-protein coupled receptors elevates cAMP levels promoting dissociation of protein kinase A (PKA) holoenzymes and release of catalytic subunits (PKAc). This results in PKAc-mediated phosphorylation of compartmentalized substrates that control central aspects of cell physiology. The mechanism of PKAc activation and signaling have been largely characterized. However, the modes of PKAc inactivation by regulated proteolysis were unknown. Here, we identify a regulatory mechanism that precisely tunes PKAc stability and downstream signaling. Following agonist stimulation, the recruitment of the chaperone-bound E3 ligase CHIP promotes ubiquitylation and proteolysis of PKAc, thus attenuating cAMP signaling. Genetic inactivation of CHIP or pharmacological inhibition of HSP70 enhances PKAc signaling and sustains hippocampal long-term potentiation. Interestingly, primary fibroblasts from autosomal recessive spinocerebellar ataxia 16 (SCAR16) patients carrying germline inactivating mutations of CHIP show a dramatic dysregulation of PKA signaling. This suggests the existence of a negative feedback mechanism for restricting hormonally controlled PKA activities.

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Section: Introductionmentioning

confidence: 99%

Feedback inhibition of cAMP effector signaling by a chaperone-assisted ubiquitin system

Rinaldi¹,

Donne²,

Catalanotti

et al. 2019

Nat Commun

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“…For instance, PDE4D5 is involved in a number of processes common in almost all cells, such as cell growth, cell orientation, desensitization of Gs-coupled receptors, and inactivating the phosphorylation of ubiquitous chaperone HSP20 (263). The ability for PDE4D5 to have all these functions in a cell is a result of it being localized in different compartments by different anchors (e.g., RACK1 at leading edge of cells, beta-arrestin at transmembrane receptors, and HSP20 in the cytosol;…”

Section: Proofmentioning

confidence: 99%

Therapeutic targeting of 3′,5′-cyclic nucleotide phosphodiesterases: inhibition and beyond

Baillie

Tejeda

Kelly

2019

Nat Rev Drug Discov

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238

295

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“…4B). This situation has similarities to the association of PDE4D5 with beta-arrestin-2 where all PDE4s can interact with the scaffold but PDE4D5 is "preferred" due to an optimized binding motif within the PDE's Nterminal region (Wills et al, 2016).…”

Section: Popdc1 Interacts Directly With Pde4mentioning

confidence: 86%

“…A good example that illustrates the concept is the PDE type 4 isoform called PDE4D5 (Wills et al, 2016). It can be translocated to the vicinity of G s -coupled receptors by the signaling scaffold protein beta-arrestin in order to hydrolyze cAMP, while beta-arrestin concomitantly hinders G-protein signaling (Baillie et al, 2003).…”

Section: Introductionmentioning

confidence: 99%

Phosphodiesterase Type 4 anchoring regulates cAMP signaling to Popeye domain-containing proteins

Tibbo

Dobi

McFall

et al. 2020

Preprint

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Cyclic AMP is a ubiquitous second messenger used to transduce intracellular signals from a variety of Gs-coupled receptors. Compartmentalisation of protein intermediates within the cAMP signaling pathway underpins receptor-specific responses. The cAMP effector proteins protein-kinase A and EPAC are found in complexes that also contain phosphodiesterases whose presence ensures a coordinated cellular response to receptor activation events. Popeye proteins are the most recent class of cAMP effectors to be identified and have crucial roles in cardiac pacemaking and conduction. We report the first observation that Popeye proteins exist in complexes with members of the PDE4 family in cardiac myocytes thus restricting cAMP signaling. We show that POPDC1 preferentially binds the PDE4A sub-family via a specificity motif in the PDE4 UCR1 region and that PDE4s bind to the Popeye domain of POPDC1 in a region known to be susceptible to a mutation that causes human disease. Using a cell-permeable disruptor peptide that displaces the POPDC1-PDE4 complex we show that PDE4 activity localized to POPDC1 is essential to maintain action potential duration in beating cardiac myocytes.

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Location, location, location: PDE4D5 function is directed by its unique N-terminal region

Cited by 10 publications

References 47 publications

Feedback inhibition of cAMP effector signaling by a chaperone-assisted ubiquitin system

Feedback inhibition of cAMP effector signaling by a chaperone-assisted ubiquitin system

Therapeutic targeting of 3′,5′-cyclic nucleotide phosphodiesterases: inhibition and beyond

Phosphodiesterase Type 4 anchoring regulates cAMP signaling to Popeye domain-containing proteins

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