RNAi– induced silencing of the plasma membrane Ca2+– ATPase 2 in neuronal cells: effects on Ca2+ homeostasis and cell viability

Fernandes, Denzyl; Zaidi, Almas; Bean, Jennifer L.; Hui, Dongwei; Michaelis, Mary L.

doi:10.1111/j.1471-4159.2007.04592.x

Cited by 27 publications

(19 citation statements)

References 56 publications

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“…Cells with elevated Ca 2+ levels would likely exhibit an increased vulnerability to various metabolic and oxidative insults. Consistent with this idea, PMCA 2 deficient cells are more susceptible to cellular stresses particularly those involving Ca 2+ overload [82] . Although experimental lowering of the PMCAs in cultured cells cannot be extrapolated to the in vivo situation that exists in brain, they greatly emphasize the importance of maintaining normal levels of PMCA protein in neuronal survival and growth.…”

Section: Pmca Expressionmentioning

confidence: 53%

“…PMCA activity is significantly reduced in response to cellular cholesterol depletion suggesting the possibility of local regulation of the pump activity in lipid rafts [78] . Antisense-(AS) plasmid-mediated reduction of specific isoforms has yielded valuable information on the role of individual PMCA subtypes in regulating the dynamics of cellular Ca 2+ handling and also their contribution to a diverse array of neuronal functions [80][81][82][83][84] . For example, blockade of PMCA 1 causes no change in the levels of resting free [Ca 2+ ]i or its release from intracellular stores but results in a significantly slower rate of Ca 2+ clearance following release from intracellular stores [80] .…”

Section: Pmca Expressionmentioning

confidence: 99%

“…We utilized an RNA interference strategy to experimentally lower PMCA 2 expression [82] . Short interference RNA treatment led to 80% reduction of PMCA 2 expression, which remained suppressed throughout a 6 d period.…”

Section: Pmca Expressionmentioning

confidence: 99%

“…Short interference RNA treatment led to 80% reduction of PMCA 2 expression, which remained suppressed throughout a 6 d period. siRNA-treated cells exhibit marked changes in total PMCA activity, with a shift from Michaelis-Menten kinetic properties, a three-fold increase in Kact for Ca 2+ and 22% suppression of Vmax [82] . Ca 2+ imaging studies using Fura 2 show that neurons with lowered PMCA 2 have (1) elevated resting [Ca 2+ ]i; (2) a significantly slower recovery following depolarization; and (3) inability to return to their own resting levels present prior to depolarization, signifying the importance of PMCA 2 in maintaining resting [Ca 2+ ]i.…”

Section: Pmca Expressionmentioning

confidence: 99%

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Plasma membrane Ca²⁺-ATPases: Targets of oxidative stress in brain aging and neurodegeneration

Zaidi¹

2010

WJBC

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The plasma membrane Ca 2+ -ATPase (PMCA) pumps play an important role in the maintenance of precise levels of intracellular Ca 2+ [Ca 2+ ]i, essential to the functioning of neurons. In this article, we review evidence showing age-related changes of the PMCAs in synaptic plasma membranes (SPMs). PMCA activity and protein levels in SPMs diminish progressively with increasing age. The PMCAs are very sensitive to oxidative stress and undergo functional and structural changes when exposed to oxidants of physiological relevance. The major signatures of oxidative modification in the PMCAs are rapid inactivation, conformational changes, aggregation, internalization from the plasma membrane and proteolytic degradation. PMCA proteolysis appears to be mediated by both calpains and caspases. The predominance of one proteolytic pathway vs the other, the ensuing pattern of PMCA degradation and its consequence on pump activity depends largely on the type of insult, its intensity and duration. Experimental reduction of PMCA expression not only alters the dynamics of cellular Ca 2+ handling but also has a myriad of downstream consequences on various aspects of cell function, indicating a broad role of these pumps. Age-and oxidation-related down-regulation of the PMCAs may play an important role in compromised neuronal function in the aging brain and its several-fold increased susceptibility to neurodegenerative disorders such as Alzheimer's disease, Parkinson's disease, and stroke. Therapeutic approaches that protect the PMCAs and stabilize [Ca 2+ ]i homeostasis may be capable of slowing and/or preventing neuronal degeneration. The PMCAs are therefore emerging as a new class of drug targets for therapeutic interventions in various chronic degenerative disorders.

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Section: Pmca Expressionmentioning

confidence: 53%

Section: Pmca Expressionmentioning

confidence: 99%

Section: Pmca Expressionmentioning

confidence: 99%

Section: Pmca Expressionmentioning

confidence: 99%

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Plasma membrane Ca²⁺-ATPases: Targets of oxidative stress in brain aging and neurodegeneration

Zaidi¹

2010

WJBC

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“…This makes the search for new approaches to study the physiological contribution of PMCA2 and its isoforms both timely and necessary. In vivo viral-based delivery of timed siRNA PMCA2 knockdown might offer a more useful approach [43,44] together with the development of transgenic mice approaches for knock-in or knock-out, especially if expression could be limited to specific cell types within the cerebellum, such as the PNs [45] . In addition, improvement of PMCA-specific pharmacological tools beyond the advances made by the development of the caloxins [46] would further aid physiological studies.…”

Section: Cerebellar Cortexmentioning

confidence: 99%

Contribution of plasma membrane Ca²⁺ATPase to cerebellar synapse function

Huang

Nagaraja²,

Garside³

et al. 2010

WJBC

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The cerebellum expresses one of the highest levels of the plasma membrane Ca 2+ ATPase, isoform 2 in the mammalian brain. This highly efficient plasma membrane calcium transporter protein is enriched within the main output neurons of the cerebellar cortex; i.e. the Purkinje neurons (PNs). Here we review recent evidence, including electrophysiological and calcium imaging approaches using the plasma membrane calcium ATPase 2 (PMCA2) knockout mouse, to show that PMCA2 is critical for the physiological control of calcium at cerebellar synapses and cerebellar dependent behaviour. These studies have also revealed that deletion of PMCA2 throughout cerebellar development in the PMCA2 knockout mouse leads to permanent signalling and morphological alterations in the PN dendrites. Whilst these findings highlight the importance of PMCA2 during cerebellar synapse function and development, they also reveal some limitations in the use of the PMCA2 knockout mouse and the need for additional experimental approaches including cell-specific and reversible manipulation of PMCAs. THE CEREBELLUM, THE PURKINJE NEURON AND THE IMPORTANCE OF CALCIUM DYNAMICS AT CEREBELLAR SYNAPSESThe cerebellum is a major centre for the integration of sensory and motor information in the brain and plays a central role in our ability to learn and refine motor tasks; the specialised function of the cerebellum allows us to execute motor tasks in a finely controlled but, at the same time, "unaware" manner that can still be improved by learning. For a detailed review of cerebellar function TOPIC HIGHLIGHTWorld J Biol Chem 2010 May 26; 1(5): 95-102 ISSN 1949-8454 (online)

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Inhibition of transglutaminase 2 mitigates transcriptional dysregulation in models of Huntington disease

et al. 2010

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Caused by a polyglutamine expansion in the huntingtin protein, Huntington's disease leads to striatal degeneration via the transcriptional dysregulation of a number of genes, including those involved in mitochondrial biogenesis. Here we show that transglutaminase 2, which is upregulated in HD, exacerbates transcriptional dysregulation by acting as a selective corepressor of nuclear genes; transglutaminase 2 interacts directly with histone H3 in the nucleus. In a cellular model of HD, transglutaminase inhibition de-repressed two established regulators of mitochondrial function, PGC-1α and cytochrome c and reversed susceptibility of human HD cells to the mitochondrial toxin, 3-nitroproprionic acid; however, protection mediated by transglutaminase inhibition was not associated with improved mitochondrial bioenergetics. A gene microarray analysis indicated that transglutaminase inhibition normalized expression of not only mitochondrial genes but also 40% of genes that are dysregulated in HD striatal neurons, including chaperone and histone genes. Moreover, transglutaminase inhibition attenuated degeneration in a Drosophila model of HD and protected mouse HD striatal neurons from excitotoxicity. Altogether these findings demonstrate that selective TG inhibition broadly corrects transcriptional dysregulation in HD and defines a novel HDAC-independent epigenetic strategy for treating neurodegeneration.

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RNA_i– induced silencing of the plasma membrane Ca²⁺– ATPase 2 in neuronal cells: effects on Ca²⁺ homeostasis and cell viability

Cited by 27 publications

References 56 publications

Plasma membrane Ca²⁺-ATPases: Targets of oxidative stress in brain aging and neurodegeneration

Plasma membrane Ca²⁺-ATPases: Targets of oxidative stress in brain aging and neurodegeneration

Contribution of plasma membrane Ca²⁺ATPase to cerebellar synapse function

Inhibition of transglutaminase 2 mitigates transcriptional dysregulation in models of Huntington disease

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RNAi– induced silencing of the plasma membrane Ca2+– ATPase 2 in neuronal cells: effects on Ca2+ homeostasis and cell viability

Cited by 27 publications

References 56 publications

Plasma membrane Ca2+-ATPases: Targets of oxidative stress in brain aging and neurodegeneration

Plasma membrane Ca2+-ATPases: Targets of oxidative stress in brain aging and neurodegeneration

Contribution of plasma membrane Ca2+ATPase to cerebellar synapse function

Inhibition of transglutaminase 2 mitigates transcriptional dysregulation in models of Huntington disease

Contact Info

Product

Resources

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RNA_i– induced silencing of the plasma membrane Ca²⁺– ATPase 2 in neuronal cells: effects on Ca²⁺ homeostasis and cell viability

Plasma membrane Ca²⁺-ATPases: Targets of oxidative stress in brain aging and neurodegeneration

Plasma membrane Ca²⁺-ATPases: Targets of oxidative stress in brain aging and neurodegeneration

Contribution of plasma membrane Ca²⁺ATPase to cerebellar synapse function