Increased PKA signaling disrupts recognition memory and spatial memory: role in Huntington's disease

Giralt, Albert; Saavedra, Ana; Carretón, Olga; Xifró, Xavier; Alberch, Jordi; Pérez‐Navarro, Esther

doi:10.1093/hmg/ddr351

Cited by 103 publications

(110 citation statements)

References 81 publications

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“…Colony maintenance resulted in a decrease of the CAG repeat length, in agreement with CAG repeat instability as previously described by other groups (41)(42)(43). Mouse genotype was determined as previously described (44). CAG repeat length was determined by PCR amplification of the repeat using HD1 and HD2 fluorescently labeled primers (45) and subsequent size determination in an ABI 3100 analyzer (Applied Biosystems).…”

Section: Hd Mouse Modelmentioning

confidence: 60%

Targeting CAG repeat RNAs reduces Huntington’s disease phenotype independently of huntingtin levels

Rué¹,

Báñez-Coronel²,

Creus-Muncunill³

et al. 2016

Journal of Clinical Investigation

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Section: Hd Mouse Modelmentioning

confidence: 60%

Targeting CAG repeat RNAs reduces Huntington’s disease phenotype independently of huntingtin levels

Rué¹,

Báñez-Coronel²,

Creus-Muncunill³

et al. 2016

Journal of Clinical Investigation

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“…This cross talk between PKA and the proteasome might be brain area specific or disease stage dependent. In the hippocampus of an HD mouse model (R6/1), PKA was upregulated before the onset of motor impairment because of the downregulation of phosphodiesterase 4, which might have contributed to defects in recognition memory and spatial memory (35). Cell-type-specific regulation of Rpt subunits and UPS activity, probably due to differential structural changes in the proteasome in different tissues (5), might also account for this brain-area-specific regulation of PKA in HD.…”

Section: Discussionmentioning

confidence: 99%

Regulation of Feedback between Protein Kinase A and the Proteasome System Worsens Huntington's Disease

Lin

Chang

Chen

et al. 2013

Molecular and Cellular Biology

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Huntington's disease (HD) is a neurodegenerative disease caused by the expansion of a CAG repeat in the Huntingtin (HTT) gene. Abnormal regulation of the cyclic AMP (cAMP)/protein kinase A (PKA) pathway occurs during HD progression. Here we found that lower PKA activity was associated with proteasome impairment in the striatum for two HD mouse models (R6/2 and N171-82Q) and in mutant HTT (mHTT)-expressing striatal cells. Because PKA regulatory subunits (PKA-Rs) are proteasome substrates, the mHTT-evoked proteasome impairment caused accumulation of PKA-Rs and subsequently inhibited PKA activity. Conversely, activation of PKA enhanced the phosphorylation of Rpt6 (a component of the proteasome), rescued the impaired proteasome activity, and reduced mHTT aggregates. The dominant-negative Rpt6 mutant (Rpt6 S120A ) blocked the ability of a cAMP-elevating reagent to enhance proteasome activity, whereas the phosphomimetic Rpt6 mutant (Rpt6 S120D ) increased proteasome activity, reduced HTT aggregates, and ameliorated motor impairment. Collectively, our data demonstrated that positive feedback regulation between PKA and the proteasome is critical for HD pathogenesis. Huntington's disease (HD) is an autosomal dominant neurodegenerative disease caused by expansion of a CAG repeat in the Huntingtin (HTT) gene. The normal HTT gene has 35 or fewer CAG repeats in its N-terminal region, whereas expansion of the repeat beyond 35 units confers toxicity to the Huntingtin protein (HTT) and evokes HD pathogenesis (1). The major clinical presentations of HD include chorea, cognitive decline, psychiatric symptoms, and a systemic metabolic defect (2). Selective neuronal loss occurs in multiple brain regions, particularly in the striatum and cortex. Since a great number of cellular machineries (including transcription, vesicle transport, molecular chaperones, and the ubiquitin-proteasome system [UPS]) are compromised by the expression of mutant HTT (mHTT) (3), effective removal of mHTT has become one of the most challenging aspects of drug development for HD.The UPS, which degrades misfolded and/or damaged proteins in eukaryotes, is the major regulatory proteolytic pathway. It regulates many essential cellular processes, including transcription, translation, DNA repair, chromatin remodeling, cell survival, signal transduction, protein trafficking, and synaptic plasticity (4). A recent study demonstrated that AAA-ATPase subunits are critical for cell-type-specific regulation of UPS activity (5). Interestingly, UPS activity is under metabolic control. Posttranslational modifications, such as O-GlcNacylation and phosphorylation of 19S subunits, affect the proteolytic activity of the UPS (6). In addition, impaired functioning of the UPS is believed to contribute to the pathogenic processes of many neurodegenerative diseases, including Alzheimer's disease, Parkinson's disease (PD), and HD. Recent studies revealed that the UPS might be impaired in HD mouse models and patients (7,8). Intriguingly, although the degradation of polyubiquitin-tagg...

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“…First, several of the PDE families have notably restricted distributions, including PDE10A, which is very highly expressed in striatal medium spiny neurons, PDE11, which shows particularly high expression levels in dorsal root ganglia, and PDE6, which is only expressed in retina. For PDE10A, localization has been an important clue and guide in directing the evaluation of PDE10A inhibitors for the treatment of schizophrenia [18] and Huntington's disease [19]. However, PDE10A is an exception, and the majority of PDEs are more broadly distributed.…”

Section: Pde Localizationmentioning

confidence: 99%

PDE Inhibition and cognition enhancement

Blokland¹,

Menniti

Prickaerts

2012

Expert Opinion on Therapeutic Patents

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Increased PKA signaling disrupts recognition memory and spatial memory: role in Huntington's disease

Cited by 103 publications

References 81 publications

Targeting CAG repeat RNAs reduces Huntington’s disease phenotype independently of huntingtin levels

Targeting CAG repeat RNAs reduces Huntington’s disease phenotype independently of huntingtin levels

Regulation of Feedback between Protein Kinase A and the Proteasome System Worsens Huntington's Disease

PDE Inhibition and cognition enhancement

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