α
            <sub>2A</sub>
            adrenergic receptor promotes amyloidogenesis through disrupting APP-SorLA interaction

Chen, Yunjia; Peng, Yin; Che, Pulin; Gannon, Mary; Liu, Yin; Li, Ling; Bu, Guojun; Groen, Thomas van; Jiao, Kai; Wang, Qin

doi:10.1073/pnas.1409513111

Cited by 62 publications

(58 citation statements)

References 34 publications

(22 reference statements)

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“…ATI also enhances motor recovery after two types of brain injury (TBI -present study; stroke - Puurunen et al, 2001). Moreover, the recently discovered favorable α2A-adrenergic receptor blockade-mediated effects on antiamyloidogenesis and insulin secretion could provide additional benefits for the use of noradrenergic α2A-antagonists in the treatment of TBI (Gribble, 2010;Chen et al, 2014). Therefore, we consider that further studies are warranted to investigate proconvulsant 2-adrenergic blockade and its downstream signaling as a therapeutic target for recovery enhancement and antiepileptogenesis in order to combat the development of co-morbidities after TBI.…”

Section: Discussionmentioning

confidence: 82%

Disease-modifying effect of atipamezole in a model of post-traumatic epilepsy

et al. 2017

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Treatment of TBI remains a major unmet medical need, with 2.5 million new cases of traumatic brain injury (TBI) each year in Europe and 1.5 million in the USA. This single-center proof-of-concept preclinical study tested the hypothesis that pharmacologic neurostimulation with proconvulsants, either atipamezole, a selective α-adrenoceptor antagonist, or the cannabinoid receptor 1 antagonist SR141716A, as monotherapy would improve functional recovery after TBI. A total of 404 adult Sprague-Dawley male rats were randomized into two groups: sham-injured or lateral fluid-percussion-induced TBI. The rats were treated with atipamezole (started at 30min or 7 d after TBI) or SR141716A (2min or 30min post-TBI) for up to 9 wk. Total follow-up time was 14 wk after treatment initiation. Outcome measures included motor (composite neuroscore, beam-walking) and cognitive performance (Morris water-maze), seizure susceptibility, spontaneous seizures, and cortical and hippocampal pathology. All injured rats exhibited similar impairment in the neuroscore and beam-walking tests at 2 d post-TBI. Atipamezole treatment initiated at either 30min or 7 d post-TBI and continued for 9 wk via subcutaneous osmotic minipumps improved performance in both the neuroscore and beam-walking tests, but not in the Morris water-maze spatial learning and memory test. Atipamezole treatment initiated at 7 d post-TBI also reduced seizure susceptibility in the pentylenetetrazol test 14 wk after treatment initiation, although it did not prevent the development of epilepsy. SR141716A administered as a single dose at 2min post-TBI or initiated at 30min post-TBI and continued for 9 wk had no recovery-enhancing or antiepileptogenic effects. Mechanistic studies to assess the α-adrenoceptor subtype specificity of the disease-modifying effects of atipametzole revealed that genetic ablation of α-noradrenergic receptor function in Adra2A mice carrying an N79P point mutation had antiepileptogenic effects after TBI. On the other hand, blockade of α-adrenoceptors using the receptor subtype-specific antagonist ORM-12741 had no favorable effects on the post-TBI outcome. Finally, to assess whether regulation of the post-injury inflammatory response by atipametzole in glial cells contributed to a favorable outcome, we investigated the effect of atipamezole on spontaneous and/or lipopolysaccharide-stimulated astroglial or microglial cytokine release in vitro. We observed no effect. Our data demonstrate that a 9-wk administration of α2A-noradrenergic antagonist, atipamezole, is recovery-enhancing after TBI.

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Section: Discussionmentioning

confidence: 82%

Disease-modifying effect of atipamezole in a model of post-traumatic epilepsy

et al. 2017

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“…Beneficial actions of an a2-antagonist have been described in the transgenic amyloid precursor protein (APP)/PS1 mouse model of AD (Chen et al 2014). In those studies, treatment with the a2-antagonist idazoxan for 10 weeks reduced Ab burden in the hippocampus and cortex, and improved short-term memory in a novel object recognition test and spatial memory in the Morris water maze test.…”

Section: Anti-inflammatory and Neuroprotective Actions Of Raising Na mentioning

confidence: 99%

Causes, consequences, and cures for neuroinflammation mediated via the locus coeruleus: noradrenergic signaling system

Feinstein

Kalinin

Braun

2016

Journal of Neurochemistry

131

128

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Aside from its roles in as a classical neurotransmitter involved in regulation of behavior, noradrenaline (NA) has other functions in the CNS. This includes restricting the development of neuroinflammatory activation, providing neurotrophic support to neurons, and providing neuroprotection against oxidative stress. In recent years, it has become evident that disruption of physiological NA levels or signaling is a contributing factor to a variety of neurological diseases and conditions including Alzheimer's disease (AD) and Multiple Sclerosis. The basis for dysregulation in these diseases is, in many cases, due to damage occurring to noradrenergic neurons present in the locus coeruleus (LC), the major source of NA in the CNS. LC damage is present in AD, multiple sclerosis, and a large number of other diseases and conditions. Studies using animal models have shown that experimentally induced lesion of LC neurons exacerbates neuropathology while treatments to compensate for NA depletion, or to reduce LC neuronal damage, provide benefit. In this review, we will summarize the anti-inflammatory and neuroprotective actions of NA, summarize examples of how LC damage worsens disease, and discuss several approaches taken to treat or prevent reductions in NA levels and LC neuronal damage. Further understanding of these events will be of value for the development of treatments for AD, multiple sclerosis, and other diseases and conditions having a neuroinflammatory component.

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“…We have demonstrated that stimulation of a 2A AR promotes amyloidogenic processing of APP through activation of G i/o proteins (23). The direct interaction between APP and a 2A AR would bring APP to the proximity of a 2A AR downstream signaling to modulate its processing route.…”

Section: Discussionmentioning

confidence: 88%

“…Using the BbsI restriction enzyme, the primers were introduced to the pSpCas9(BB)-2A-GFP plasmid. An N2a-HA-a 2A AR stable cell line (23) was transfected with the resulting plasmid using Lipofectamine 2000 and selected for GFP expression by fluorescence-activated cell sorting. Single clones were allowed to grow and screened for loss of expression of APP.…”

Section: Cell Culturementioning

confidence: 99%

The amyloid precursor protein modulates α _2A ‐adrenergic receptor endocytosis and signaling through disrupting arrestin 3 recruitment

et al. 2017

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The amyloid precursor protein (APP) has long been appreciated for its role in Alzheimer's disease (AD) pathology. However, less is known about the physiologic function of APP outside of AD. Particularly, whether and how APP may regulate functions of cell surface receptors, including GPCRs, remains largely unclear. In this study, we identified a novel direct interaction between APP and the α-adrenergic receptor (αAR) that occurs at the intracellular domains of both proteins. The APP interaction with αAR is promoted by agonist stimulation and competes with arrestin 3 binding to the receptor. Consequently, the presence of APP attenuates αAR internalization and desensitization, which are arrestin-dependent processes. Furthermore, in neuroblastoma neuro-2A cells and primary superior cervical ganglion neurons, where APP is highly expressed, the lack of APP leads to a dramatic increase in plasma membrane recruitment of endogenous arrestin 3 following αAR activation. Concomitantly, agonist-induced internalization of αAR is significantly enhanced in these neuronal cells. Our study provided the first evidence that APP fine tunes GPCR signaling and trafficking. Given the important role of αAR in controlling norepinephrine release and response, this novel regulation of αAR by APP may have an impact on modulation of noradrenergic activity and sympathetic tone.-Zhang, F., Gannon, M., Chen, Y., Zhou, L., Jiao, K., Wang, Q. The amyloid precursor protein modulates α-adrenergic receptor endocytosis and signaling through disrupting arrestin 3 recruitment.

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α _2A adrenergic receptor promotes amyloidogenesis through disrupting APP-SorLA interaction

Cited by 62 publications

References 34 publications

Disease-modifying effect of atipamezole in a model of post-traumatic epilepsy

Disease-modifying effect of atipamezole in a model of post-traumatic epilepsy

Causes, consequences, and cures for neuroinflammation mediated via the locus coeruleus: noradrenergic signaling system

The amyloid precursor protein modulates α _2A ‐adrenergic receptor endocytosis and signaling through disrupting arrestin 3 recruitment

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α 2A adrenergic receptor promotes amyloidogenesis through disrupting APP-SorLA interaction

Cited by 62 publications

References 34 publications

Disease-modifying effect of atipamezole in a model of post-traumatic epilepsy

Disease-modifying effect of atipamezole in a model of post-traumatic epilepsy

Causes, consequences, and cures for neuroinflammation mediated via the locus coeruleus: noradrenergic signaling system

The amyloid precursor protein modulates α 2A ‐adrenergic receptor endocytosis and signaling through disrupting arrestin 3 recruitment

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α _2A adrenergic receptor promotes amyloidogenesis through disrupting APP-SorLA interaction

The amyloid precursor protein modulates α _2A ‐adrenergic receptor endocytosis and signaling through disrupting arrestin 3 recruitment