TCR- and CD28-Mediated Recruitment of Phosphodiesterase 4 to Lipid Rafts Potentiates TCR Signaling

Abrahamsen, Hilde; Baillie, George S.; Ngai, Jacob; Vang, Torkel; Nika, Konstantina; Ruppelt, Anja; Mustelin, Tomas; Zaccolo, Manuela; Houslay, Miles D.; Taskén, Kjetil

doi:10.4049/jimmunol.173.8.4847

Cited by 122 publications

(145 citation statements)

References 65 publications

Supporting

Mentioning

138

Contrasting

Unclassified

Order By: Relevance

“…In addition, as mentioned previously, cAMP levels are increased in T cells upon activation (Ledbetter et al, 1986) which if unopposed leads to PKA activation and inhibition of TCR signaling (Abrahamsen et al, 2004). Elevated cAMP, and thus PKA activity, may be part of the normal homeostatic mechanism to dampen signaling and therefore restrict T-cell activation, especially in the absence of costimula-tion (see below).…”

Section: Control Of Csk Activitymentioning

confidence: 93%

“…Elevated cAMP, and thus PKA activity, may be part of the normal homeostatic mechanism to dampen signaling and therefore restrict T-cell activation, especially in the absence of costimula-tion (see below). A counter-regulatory mechanism exists which functions to limit cAMP-induced PKA-mediated inactivation of p56 lck and is envisioned to be operative under conditions of robust T-cell activation, i.e., TCR plus CD28 costimulation (Abrahamsen, 2004). As mentioned above, lipid raftassociated PDE4 activity is enhanced upon concomitant ligation of the TCR and CD28.…”

Section: Control Of Csk Activitymentioning

confidence: 99%

“…In this regard, Tasken and colleagues have hypothesized that signals generated by TCR ligation appear to result in a constitutively active "default pathway" of increased cAMP levels leading to inhibition of signaling (Abrahamsen, 2004). Only when TCR ligation is accompanied by CD28 costimulation are cAMP levels reduced therein relieving PKA/Csk activity and permitting sustained T-cell activation.…”

Section: Control Of Csk Activitymentioning

confidence: 99%

“…Conversely, activation of T cells by crosslinking both the TCR and the costimu-latory receptor CD28 results in a reduction of cAMP levels and concomitant diminished activation of PKA, therein avoiding inactivation of p56 lck since Csk is not robustly activated (or is sequestered away from its substrate, see below) (Abrahamsen, 2004). Inhibition of cAMP is mediated by phosphodiesterases (PDE), which in T cells is largely accounted for by the PDE type 4 family ("PDE4", containing four genes and multiple isoforms) (Oh and Schnitzer, 2001).…”

Section: Control Of Csk Activitymentioning

confidence: 99%

See 3 more Smart Citations

Cancer-Induced Signaling Defects in Antitumor T Cells

Frey¹

Tumor-Induced Immune Suppression

View full text Add to dashboard Cite

Section: Control Of Csk Activitymentioning

confidence: 93%

Section: Control Of Csk Activitymentioning

confidence: 99%

Section: Control Of Csk Activitymentioning

confidence: 99%

Section: Control Of Csk Activitymentioning

confidence: 99%

See 2 more Smart Citations

Cancer-Induced Signaling Defects in Antitumor T Cells

Frey¹

Tumor-Induced Immune Suppression

View full text Add to dashboard Cite

“…For example, PDE3B is localized predominately at membrane surfaces and is thought to regulate cAMP in regions proximal to these surfaces (11). Similarly, in activated T cells, PDE4 is recruited to the T-cell receptor in a β-arrestin-dependent manner, thus lowering cAMP in the vicinity of this part of the T-cell activation pathway (12).…”

mentioning

confidence: 99%

Analyses of PDE-regulated phosphoproteomes reveal unique and specific cAMP-signaling modules in T cells

Beltejar

Lau

Golkowski

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Specific functions for different cyclic nucleotide phosphodiesterases (PDEs) have not yet been identified in most cell types. Conventional approaches to study PDE function typically rely on measurements of global cAMP, general increases in cAMP-dependent protein kinase (PKA), or the activity of exchange protein activated by cAMP (EPAC). Although newer approaches using subcellularly targeted FRET reporter sensors have helped define more compartmentalized regulation of cAMP, PKA, and EPAC, they have limited ability to link this regulation to downstream effector molecules and biological functions. To address this problem, we have begun to use an unbiased mass spectrometry-based approach coupled with treatment using PDE isozyme-selective inhibitors to characterize the phosphoproteomes of the functional pools of cAMP/PKA/EPAC that are regulated by specific cAMP-PDEs (the PDE-regulated phosphoproteomes). In Jurkat cells we find multiple, distinct PDE-regulated phosphoproteomes that can be defined by their responses to different PDE inhibitors. We also find that little phosphorylation occurs unless at least two different PDEs are concurrently inhibited in these cells. Moreover, bioinformatics analyses of these phosphoproteomes provide insight into the unique functional roles, mechanisms of action, and synergistic relationships among the different PDEs that coordinate cAMP-signaling cascades in these cells. The data strongly suggest that the phosphorylation of many different substrates contributes to cAMP-dependent regulation of these cells. The findings further suggest that the approach of using selective, inhibitor-dependent phosphoproteome analysis can provide a generalized methodology for understanding the roles of different PDEs in the regulation of cyclic nucleotide signaling.

show abstract

The heterotrimeric G‐protein α‐subunit Gαq regulates TCR‐mediated immune responses through an Lck‐dependent pathway

et al. 2008

Self Cite

View full text Add to dashboard Cite

Here, we examined the functional involvement of heterotrimeric G-proteins in TCR-induced immune responses. TCR/CD3 crosslinking resulted in activation of both Gaq and Gas, but not Gai-2. Targeting of Gas, Gai-2 and Gaq using siRNA demonstrated a specific role of Gaq in TCR signaling. Jurkat TAg T cells with Gaq knockdown displayed reduced activation of Lck and LAT phosphorylation, but paradoxically showed sustained ERK1/2 phosphorylation and increased NFAT-AP-1-reporter activity implicating Gaq in the negative control of downstream signaling and IL-2-promoter activity. Primary T cells isolated from Gaq-deficient mice had a similar TCR signaling response with reduced proximal LAT phosphorylation, sustained ERK1/2 phosphorylation and augmented immune responses including increased secretion of IL-2, IL-5, IL-12 and TNF-a. The effects on NFAT-AP-1-reporter activity were sensitive to the Src family kinase inhibitor PP2 and were reversed by transient expression of constitutively active Lck. Furthermore, expression of constitutively active Gaq Q209L elevated Lck activity and Zap-70 phosphorylation. Together these data argue for a role of Gaq in the fine-tuning of proximal TCR signals at the level of Lck and a negative regulatory role of Gaq in transcriptional activation of cytokine responses. Key words: Signal transduction . T cells . TCR . Transgenic/knockout mice IntroductionThe TCR/CD3 complex is composed of a ligand-binding TCR-ab heterodimer and signal transducing dimers of CD3eg, CD3ed and zz that upon interaction with its MHC-peptide ligand initiate an activation process that, although not fully understood, probably involves both receptor clustering and conformational changes of the cytoplasmic part of the CD3 complex [1,2]. Considering the physiological significance of correct T-cell activation, this signal interpretation probably involves complex molecular integration proximal to the TCR. A key early event is the mobilization and activation of the protein tyrosine kinase Lck, which in turn phosphorylates ITAM within the CD3 component that can recruit ZAP-70 through its two SH2-domains [3]. ZAP-70 is then phosphorylated by Lck on Y493 leading to full catalytic activation [4]. One important substrate of activated ZAP-70 is the transmembrane adaptor LAT, which acts as a scaffold to assemble signaling complexes essential for T-cell activation [5].The 3208TCR necessary for the development and activation of T cells. In addition, several lines of evidence suggest that initiation of modulating pathways is controlled by Lck. Both TCR desensitization by internalization and induction of apoptosis through the mitochondrial death pathway are regulated by Lck [7,8]. Furthermore, the activation of Lck by partial antagonist and the ability of Lck to negatively regulate superantigen-induced T-cell activation support a dual role of Lck [9,10]. Interestingly, acute elimination of Lck in either Jurkat or primary T cells using RNA interference results in sustained and elevated ERK1/2 phosphorylation and augmented NFAT-reporter ac...

show abstract

TCR- and CD28-Mediated Recruitment of Phosphodiesterase 4 to Lipid Rafts Potentiates TCR Signaling

Cited by 122 publications

References 65 publications

Cancer-Induced Signaling Defects in Antitumor T Cells

Cancer-Induced Signaling Defects in Antitumor T Cells

Analyses of PDE-regulated phosphoproteomes reveal unique and specific cAMP-signaling modules in T cells

The heterotrimeric G‐protein α‐subunit Gαq regulates TCR‐mediated immune responses through an Lck‐dependent pathway

Contact Info

Product

Resources

About