Mechanism of Regulation of Group IVA Phospholipase A2 Activity by Ser727 Phosphorylation

Tian, Wen; Wijewickrama, Gihani T.; Kim, Junghwan; Das, Sudipto; Tun, Moe P.; Gokhale, Nikhil A.; Jung, Jin Woo; Kim, Kwang Pyo; Cho, Wonhwa

doi:10.1074/jbc.m707345200

Cited by 45 publications

(33 citation statements)

References 51 publications

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“…Phosphorylation at this site might promote the dissociation of a heterotetramer of cPLA2, Annexin A2, and p11 and increases cPLA2 enzymatic activity. 42 As direct regulators of intracellular calcium, we found the calcium release-activated calcium channel Orai1 being dephosphorylated (Thr295: ↓60 2nM ) and the inositol phosphate receptor regulator MRVI1 (IRAG) increasingly phosphorylated at Ser657 and Ser670 (↑10 2/5nM ). Both sites are known to be PKG targets preventing the release of Ca 21 from inositol phosphate sensitive stores and subsequent platelet aggregation.…”

Section: Kinases and Phosphatases Involved In Platelet Inhibitionmentioning

confidence: 97%

Time-resolved characterization of cAMP/PKA-dependent signaling reveals that platelet inhibition is a concerted process involving multiple signaling pathways

Beck

Geiger

Gambaryan

et al. 2014

Blood

114

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Key Points• First comprehensive and timeresolved characterization of platelet cAMP/PKA signaling upon iloprost treatment.• More than 2700 phosphorylation sites quantified between 4 time points and from 3 individual healthy donors.One of the most important physiological platelet inhibitors is endothelium-derived prostacyclin which stimulates the platelet cyclic adenosine monophosphate/protein kinase A (cAMP/PKA)-signaling cascade and inhibits virtually all platelet-activating key mechanisms. Using quantitative mass spectrometry, we analyzed time-resolved phosphorylation patterns in human platelets after treatment with iloprost, a stable prostacyclin analog, for 0, 10, 30, and 60 seconds to characterize key mediators of platelet inhibition and activation in 3 independent biological replicates. We quantified over 2700 different phosphorylated peptides of which 360 were significantly regulated upon stimulation. This comprehensive and time-resolved analysis indicates that platelet inhibition is a multipronged process involving different kinases and phosphatases as well as many previously unanticipated proteins and pathways. (Blood. 2014;123(5):e1-e10)

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Section: Kinases and Phosphatases Involved In Platelet Inhibitionmentioning

confidence: 97%

Time-resolved characterization of cAMP/PKA-dependent signaling reveals that platelet inhibition is a concerted process involving multiple signaling pathways

Beck

Geiger

Gambaryan

et al. 2014

Blood

114

View full text Add to dashboard Cite

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“…Activation of cPLA 2 ␣ in vascular smooth muscle cells by calcium/calmodulin-dependent kinase II that phosphorylates S515 has been described ( 101 ). Phosphorylation of cPLA 2 ␣ on S727 by MAPK-interacting kinase does not enhance catalytic activity per se, but blocks its binding to an inhibitory complex in the cytosol composed of p11(S100A10)/annexin A2 ( 74,(102)(103)(104)(105) ( Fig. 1 ).…”

Section: Downloaded Frommentioning

confidence: 99%

Cytosolic phospholipase A2: physiological function and role in disease

Leslie

2015

Journal of Lipid Research

337

257

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“…The role that serine phosphorylation plays in regulating both cPLA 2 ␣ activity and its release from the Golgi apparatus requires defining and could represent an important target for modulating phospholipid turnover. This is highlighted by the recent finding that phosphorylation of cPLA 2 ␣ on serine 727 disrupted binding to p11 and annexin A2 allowing the enzyme to access its phospholipid substrate (41). Another unique function of endothelial cells is their ability to proliferate, migrate, and differentiate to form new capillaries during angiogenesis.…”

Section: Discussionmentioning

confidence: 94%

Activation of Cytosolic Phospholipase A2-α as a Novel Mechanism Regulating Endothelial Cell Cycle Progression and Angiogenesis

Herbert¹,

Odell²,

Ponnambalam

et al. 2009

Journal of Biological Chemistry

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Release of endothelial cells from contact-inhibition and cell cycle re-entry is required for the induction of new blood vessel formation by angiogenesis. Using a combination of chemical inhibition, loss of function, and gain of function approaches, we demonstrate that endothelial cell cycle re-entry, S phase progression, and subsequent angiogenic tubule formation are dependent upon the activity of cytosolic phospholipase A 2 -␣ (cPLA 2 ␣). Inhibition of cPLA 2 ␣ activity and small interfering RNA (siRNA)-mediated knockdown of endogenous cPLA 2 ␣ reduced endothelial cell proliferation. In the absence of cPLA 2 ␣ activity, endothelial cells exhibited retarded progression from G 1 through S phase, displayed reduced cyclin A/cdk2 expression, and generated less arachidonic acid. In quiescent endothelial cells, cPLA 2 ␣ is inactivated upon its sequestration at the Golgi apparatus. Upon the stimulation of endothelial cell proliferation, activation of cPLA 2 ␣ by release from the Golgi apparatus was critical to the induction of cyclin A expression and efficient cell cycle progression. Consequently, inhibition of cPLA 2 ␣ was sufficient to block angiogenic tubule formation in vitro. Furthermore, the siRNA-mediated retardation of endothelial cell cycle re-entry and proliferation was reversed upon overexpression of an siRNA-resistant form of cPLA 2 ␣. Thus, activation of cPLA 2 ␣ acts as a novel mechanism for the regulation of endothelial cell cycle re-entry, cell cycle progression, and angiogenesis.

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Mechanism of Regulation of Group IVA Phospholipase A2 Activity by Ser727 Phosphorylation

Cited by 45 publications

References 51 publications

Time-resolved characterization of cAMP/PKA-dependent signaling reveals that platelet inhibition is a concerted process involving multiple signaling pathways

Time-resolved characterization of cAMP/PKA-dependent signaling reveals that platelet inhibition is a concerted process involving multiple signaling pathways

Cytosolic phospholipase A2: physiological function and role in disease

Activation of Cytosolic Phospholipase A2-α as a Novel Mechanism Regulating Endothelial Cell Cycle Progression and Angiogenesis

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