Hypoxic induction of AKAP12 variant 2 shifts PKA-mediated protein phosphorylation to enhance migration and metastasis of melanoma cells

Finger, Elizabeth; Castellini, Laura; Rankin, Erinn B.; Vilalta, Marta; Krieg, Adam J.; Jiang, Dadi; Banh, Alice; Zundel, Wayne; Powell, Marianne Broome; Giaccia, Amato J.

doi:10.1073/pnas.1418164112

Cited by 44 publications

(37 citation statements)

References 23 publications

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“…Our findings that PKA activity was reduced in the cytosol may be an important consequence of gravin expression or upregulation in vivo . This possibility was recently highlighted in a study by Finger et al (2015), where hypoxia-induced gravin upregulation in human melanoma cells changed the phosphorylation profile of a wide variety of intracellular proteins [32]. Interestingly, the findings of Finger et al (2015) also support a second mechanistic observation from the current study, namely that gravin may direct the phosphorylation of a wider range of PKA substrates at or near the membrane than has been previously reported.…”

Section: Discussionsupporting

confidence: 84%

FRET biosensors reveal AKAP-mediated shaping of subcellular PKA activity and a novel mode of Ca2+/PKA crosstalk

Schott

Gonowolo

Maliske

et al. 2016

Cellular Signalling

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Scaffold proteins play a critical role in cellular homeostasis by anchoring signaling enzymes in close proximity to downstream effectors. In addition to anchoring static enzyme complexes, some scaffold proteins also form dynamic signalosomes that can traffic to different subcellular compartments upon stimulation. Gravin (AKAP12), a multivalent scaffold, anchors PKA and other enzymes to the plasma membrane under basal conditions, but upon [Ca2+]i elevation, is rapidly redistributed to the cytosol. Because gravin redistribution also impacts PKA localization, we postulate that gravin acts as a calcium “switch” that modulates PKA-substrate interactions at the plasma membrane, thus facilitating a novel crosstalk mechanism between Ca2+ and PKA-dependent pathways. To assess this, we measured the impact of gravin-V5/His expression on compartmentalized PKA activity using the FRET biosensor AKAR3 in cultured cells. Upon treatment with forskolin or isoproterenol, cells expressing gravin-V5/His showed elevated levels of plasma membrane PKA activity, but cytosolic PKA activity levels were reduced compared with control cells lacking gravin. This effect required both gravin interaction with PKA and localization at the plasma membrane. Pretreatment with calcium-elevating agents thapsigargin or ATP caused gravin redistribution away from the plasma membrane and prevented gravin from elevating PKA activity levels at the membrane. Importantly, this mode of Ca2+/PKA crosstalk was not observed in cells expressing a gravin mutant that resists calcium-mediated redistribution from the cell periphery. These results reveal that gravin impacts subcellular PKA activity levels through the spatial targeting of PKA, and that calcium elevation modulates downstream β-adrenergic/PKA signaling through gravin redistribution, thus supporting the hypothesis that gravin mediates crosstalk between Ca2+ and PKA-dependent signaling pathways. Based on these results, AKAP localization dynamics may represent an important paradigm for the regulation of cellular signaling networks.

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Section: Discussionsupporting

confidence: 84%

FRET biosensors reveal AKAP-mediated shaping of subcellular PKA activity and a novel mode of Ca2+/PKA crosstalk

Schott

Gonowolo

Maliske

et al. 2016

Cellular Signalling

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“…AKAP12 impacts tumor progression and metastasis through scaffolding of signaling molecules and downstream pathways that regulate tumorigenesis (30,31,63). AKAP12 expression is often downregulated in multiple cancer types, either associated with gene deletion, promoter hypermethylation or changes in chromatin modeling (64).…”

Section: Discussionmentioning

confidence: 99%

“…A-kinase anchoring proteins (AKAPs) are scaffolding proteins that regulate cellular cAMP responses by spatiotemporally coordinating PKA with target proteins specific to individual activation stimuli (27,28). AKAP12 (also called Gravin and SSeCKS) has been implicated in a wide range of cell functions, including tumor suppression (29–31), cytoskeletal architecture (32,33), β 2 -adrenergic receptor desensitization/resensitization (34,35) and cell cycle regulation (36–38). AKAP12 activities have been described at the plasma membrane, the cell periphery and at perinuclear regions of the cytoplasm (28).…”

Section: Introductionmentioning

confidence: 99%

Retracted: AKAP12 mediates PKA-induced phosphorylation of ATR to enhance nucleotide excision repair

Jarrett

Horrell

D’Orazio

2016

Nucleic Acids Research

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Loss-of-function in melanocortin 1 receptor (MC1R), a GS protein-coupled receptor that regulates signal transduction through cAMP and protein kinase A (PKA) in melanocytes, is a major inherited melanoma risk factor. Herein, we report a novel cAMP-mediated response for sensing and responding to UV-induced DNA damage regulated by A-kinase-anchoring protein 12 (AKAP12). AKAP12 is identified as a necessary participant in PKA-mediated phosphorylation of ataxia telangiectasia mutated and Rad3-related (ATR) at S435, a post-translational event required for cAMP-enhanced nucleotide excision repair (NER). Moreover, UV exposure promotes ATR-directed phosphorylation of AKAP12 at S732, which promotes nuclear translocation of AKAP12–ATR-pS435. This complex subsequently recruits XPA to UV DNA damage and enhances 5′ strand incision. Preventing AKAP12's interaction with PKA or with ATR abrogates ATR-pS435 accumulation, delays recruitment of XPA to UV-damaged DNA, impairs NER and increases UV-induced mutagenesis. Our results define a critical role for AKAP12 as an UV-inducible scaffold for PKA-mediated ATR phosphorylation, and identify a repair complex consisting of AKAP12–ATR-pS435-XPA at photodamage, which is essential for cAMP-enhanced NER.

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“…AKAP12v2 is a direct HIF target and regulates protein kinase A (PKA) activity under hypoxia (2% O 2 for 16 h), favoring tumor cell invasion and migration in vitro , but most importantly, metastasis in an in vivo orthotopic model of melanoma [101]. Additionally, metastatic samples have higher levels of AKAP12v2 than the primary tumor has [101–105]. It is possible that hypoxia-induced splicing of AKAP12v2 at the primary site provides an advantage for dissemination and/or colonization at the metastatic sites.…”

Section: Routes By Which Hypoxia Affects Dtc Fatementioning

confidence: 99%

The Different Routes to Metastasis via Hypoxia-Regulated Programs

Nobre

Entenberg

Wang

et al. 2018

Trends in Cell Biology

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Hypoxia is linked to metastasis; however, how it affects metastatic progression is not clear due to limited consensus in the literature. We posit that this lack of consensus is due to hypoxia being studied using different approaches, such as in vitro, primary tumor, or metastasis assays in an isolated manner. Here, we review the pros and cons of in vitro hypoxia assays, highlight in vivo studies that inform on physiological hypoxia, and review the evidence that primary tumor hypoxia might influence the fate of disseminated tumor cells (DTCs) in secondary organs. Our analysis suggests that consensus can be reached by using in vivo methods of study, which also allow better modeling of how hypoxia affects DTC fate and metastasis.

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Hypoxic induction of AKAP12 variant 2 shifts PKA-mediated protein phosphorylation to enhance migration and metastasis of melanoma cells

Cited by 44 publications

References 23 publications

FRET biosensors reveal AKAP-mediated shaping of subcellular PKA activity and a novel mode of Ca2+/PKA crosstalk

FRET biosensors reveal AKAP-mediated shaping of subcellular PKA activity and a novel mode of Ca2+/PKA crosstalk

Retracted: AKAP12 mediates PKA-induced phosphorylation of ATR to enhance nucleotide excision repair

The Different Routes to Metastasis via Hypoxia-Regulated Programs

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