Your search keyword '"Rosa M. Solano"' showing total 26 results

1. Trehalose ameliorates dopaminergic and tau pathology in parkin deleted/tau overexpressing mice through autophagy activation

Author

Jose A. Rodríguez-Navarro, Laura Rodríguez, María J. Casarejos, Rosa M. Solano, Ana Gómez, Juan Perucho, Ana María Cuervo, Justo García de Yébenes, and María A. Mena

Subjects

Autophagy, Parkinson's disease, Tauopathies, Dopamine, Parkin, Tau, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Tauopathies are neurodegenerative diseases, sporadic or familial, mainly characterized by dementia and parkinsonism associated to atrophy of the frontotemporal cortex and the basal ganglia, with deposition of abnormal tau in brain. Hereditary tauopathies are related with mutations of the tau gene. Up to the present, these diseases have not been helped by any disease-modifying treatment, and patients die a few years after the onset of symptoms.We have developed and characterized a mouse model of tauopathy with parkinsonism, overexpressing human mutated tau protein with deletion of parkin (PK−/−/TauVLW). At 3 months of age, these mice present abnormal dopamine-related behavior, severe dropout of dopamine neurons in the ventral midbrain, reduced dopamine levels in the striatum and abundant phosphorylated tau-positive neuritic plaques, neurofibrillary tangles, astrogliosis, and, at 12 months old, plaques of murine β-amyloid in the hippocampus.Trehalose is a natural disaccharide that increases the removal of abnormal proteins through enhancement of autophagy. In this work, we tested if 1% trehalose in the drinking water reverts the PK−/−/TauVLW phenotype. The treatment with trehalose of 3-month-old PK−/−/TauVLW mice for 2.5 months reverted the dropout of dopamine neurons, which takes place in the ventral midbrain of vehicle treated PK−/−/TauVLW and the reduced dopamine-related proteins levels in the midbrain and striatum. The number of phosphorylated tau-positive neuritic plaques and the levels of phosphorylated tau decreased, as well as astrogliosis in brain regions. The autophagy markers in the brain, the autophagic vacuoles isolated from the liver, and the electron microscopy data indicate that these effects of trehalose are mediated by autophagy. The treatment with trehalose for 4 months of 3-month-old PK−/−/TauVLW mice maintained the amelioration of the tau pathology and astrogliosis but failed to revert DA-related pathology in the striatum. Furthermore, the 3-week treatment with trehalose of 14-month-old PK−/−/TauVLW mice, at the limit of their life expectancy, improved the motor behavior and anxiety of these animals, and reduced their levels of phosphorylated tau and the number of murine β-amyloid plaques.Trehalose is neuroprotective in this model of tauopathy. Since trehalose is free of toxic effects at high concentrations, this study opens the way for clinical studies of the effects of trehalose in human tauopathies.

Published

2010

2. Parkin Null Cortical Neuronal/Glial Cultures are Resistant to Amyloid-β1-42 Toxicity: A Role for Autophagy?

Author

Justo García de Yébenes, Ana M. Gómez, Juan Perucho, Maria Angeles Mena, Rosa M. Solano, and María José Casarejos

Subjects

Proteasome Endopeptidase Complex, Programmed cell death, Cell Survival, Ubiquitin-Protein Ligases, Blotting, Western, tau Proteins, Parkin, Mice, Autophagy, medicine, Animals, Protein kinase B, Cells, Cultured, Cerebral Cortex, Mice, Knockout, Neurons, Glutathione Peroxidase, Amyloid beta-Peptides, Chemistry, General Neuroscience, Ubiquitination, Wild type, General Medicine, medicine.disease, Glutathione, Immunohistochemistry, Peptide Fragments, Culture Media, Astrogliosis, Cell biology, Psychiatry and Mental health, Clinical Psychology, Proteasome, Geriatrics and Gerontology, Signal transduction, Neuroglia, Molecular Chaperones

Abstract

Dementia occurs often in late stages of Parkinson's disease (PD) but its cause is unknown. Likewise there is little information about the interaction between proteins that produce PD and those implicated in Alzheimer's disease (AD). Here we have investigated the interactions between parkin protein and the amyloid-β (Aβ)1-42 peptide. We examined the effects of oligomeric Aβ1-42 peptide on the survival, differentiation, and signaling pathways in cortical cultures from wild type (WT) and parkin null (PK-KO) mice. We discovered that PK-KO cells were more resistant than WT to Aβ1-42. This peptide induced neuronal cell death, astrogliosis, microglial proliferation, and increased total and hyperphosphorylated tau and levels of chaperones HSP-70 and CHIP in WT, but not in Aβ-treated PK-KO cultures. Aβ1-42 decreased proteasome activities in WT and PK-KO cultures, but the ubiquitination of proteins only increased in WT cultures. Aβ1-42 induced a short activation of ERK1/2 and AKT signaling pathways, implicated in cell survival, in PK-KO-treated cells, and a shift in the autophagy marker LC3-II/LC3-I ratio. In addition, the percentage of cells immunoreactive to both HSC70 and LAMP-2A increased in PK-KO cultures versus WT and furthermore in PK-KO cultures treated with Aβ1-42. Pre-treatment with inhibitors of glutathione synthesis or autophagy reverted the resistance to Aβ1-42 of the PK-KO cultures. In conclusion, the loss of parkin protein triggers the compensatory mechanisms of cell protection against Aβ1-42. Parkin suppression, therefore, is not a risk factor for dementia of AD type.

Published

2012

3. Trehalose Protects from Aggravation of Amyloid Pathology Induced by Isoflurane Anesthesia in APPswe Mutant Mice

Author

Maria Angeles Mena, Rosa M. Solano, Justo García de Yébenes, María José Casarejos, Ana M. Gómez, and Juan Perucho

Subjects

Hippocampus, Mice, Transgenic, Plaque, Amyloid, Pathogenesis, Mice, chemistry.chemical_compound, Alzheimer Disease, In vivo, medicine, Animals, Humans, Isoflurane, business.industry, Trehalose, medicine.disease, In vitro, Astrogliosis, Mice, Inbred C57BL, Disease Models, Animal, Neuroprotective Agents, Treatment Outcome, medicine.anatomical_structure, Neurology, chemistry, Cerebral cortex, Anesthesia, Anesthetics, Inhalation, Female, Neurology (clinical), business, medicine.drug

Abstract

There is an open controversy about the role of surgery and anesthesia in the pathogenesis of Alzheimer's disease (AD). Clinical studies have shown a high prevalence of these procedures in subjects with AD but the interpretation of these studies is difficult because of the co-existence of multiple variables. Experimental studies in vitro and in vivo have shown that small molecular weight volatile anesthetics enhance amyloidogenesis in vitro and produce behavioral deficits and brain lesions similar to those found in patients with AD. We examined the effect of co-treatment with trehalose on isoflurane-induced amyloidogenesis in mice. WT and APP(swe) mice, of 11 months of age, were exposed to 1% isoflurane, 3 times, for 1.5 hours each time and sacrificed 24 hours after their last exposure to isoflurane. The right hemi-brain was used for histological analysis and the contra-lateral hemi-brain used for biochemical studies. In this study, we have shown that repetitive exposure to isoflurane in pre-symptomatic mature APP(swe) mice increases apoptosis in hippocampus and cerebral cortex, enhances astrogliosis and the expression of GFAP and that these effects are prevented by co-treatment with trehalose, a disaccharide with known effects as enhancer of autophagy. We have also confirmed that in our model the co-treatment with trehalose increases the expression of autophagic markers as well as the expression of chaperones. Cotreatment with trehalose reduces the levels of β amyloid peptide aggregates, tau plaques and levels of phospho-tau. Our study, therefore, provides new therapeutic avenues that could help to prevent the putative pro-amyloidogenic properties of small volatile anesthetics.

Published

2012

4. Anesthesia with Isoflurane Increases Amyloid Pathology in Mice Models of Alzheimer'S Disease

Author

Isabel Rubio, María José Casarejos, Juan Perucho, Ana M. Gómez, Justo García de Yébenes, Jose A. Rodriguez-Navarro, Maria Angeles Mena, and Rosa M. Solano

Subjects

Programmed cell death, Apoptosis, Anesthesia, General, Hippocampal formation, Hippocampus, Mice, Alzheimer Disease, medicine, Animals, Amyloid beta-Peptides, TUNEL assay, Behavior, Animal, Isoflurane, business.industry, General Neuroscience, Autophagy, Neurodegeneration, General Medicine, medicine.disease, In vitro, Mice, Inbred C57BL, Disease Models, Animal, Psychiatry and Mental health, Clinical Psychology, Astrocytes, Anesthesia, Anesthetics, Inhalation, Nerve Degeneration, Geriatrics and Gerontology, business, medicine.drug

Abstract

There is a great interest in the environmental and genetic factors which modify the risk of Alzheimer's disease since the manipulation of these factors could help to change the prevalence and natural course of this disease. Among the first group, anesthesia and surgery have been considered as risk enhancers, based mostly on "in vitro" experiments and epidemiological studies. We have investigated the effects of repetitive anesthesia, twice a week, for 3 months, from 7 to 10 months of age, with isoflurane on survival, behavior, apoptosis in hippocampal cells, amyloid-beta (Abeta) peptide and tau patterns, chaperones and autophagy in WT and AbetaPP{swe} mice. We have found that AbetaPP{swe} mice treated with isoflurane have increased mortality, less responsiveness after anesthesia, long lasting reduced exploratory behavior, increased number of TUNEL{+} apoptotic cells, and increased ratio of pro-apoptotic proteins in hippocampus, reduced astroglial and increased microglial responses, increased Abeta aggregates and high molecular weight peptides, abnormal chaperone responses and reduced autophagy. These effects were not present in WT mice, suggesting that the deleterious impact of isoflurane on behavior, survival, neuronal cell death, and processing of proteins involved in neurodegeneration is restricted to subjects with increased susceptibility but does not affect normal subjects.

Published

2010

5. The effects of parkin suppression on the behaviour, amyloid processing, and cell survival in APP mutant transgenic mice

Author

Israel Ampuero, Maria Angeles Mena, Isabel Rubio, Jose A. Rodriguez-Navarro, Justo García de Yébenes, Rosa M. Solano, María José Casarejos, Izaskun Rodal, Juan Perucho, Eva Carro, and Ana Gómez

Subjects

Genetically modified mouse, Ratón, Ubiquitin-Protein Ligases, Transgene, Mutant, Apoptosis, Mice, Transgenic, tau Proteins, Motor Activity, Parkin, Amyloid beta-Protein Precursor, Mice, Developmental Neuroscience, Glial Fibrillary Acidic Protein, mental disorders, In Situ Nick-End Labeling, Animals, Interpersonal Relations, Gliosis, Senile plaques, Maze Learning, Analysis of Variance, Amyloid beta-Peptides, Behavior, Animal, Chemistry, Age Factors, Brain, Molecular biology, Peptide Fragments, Hsp70, Mice, Inbred C57BL, Neurology, Rotarod Performance Test, Mutation, Exploratory Behavior, Cognition Disorders, Neuroscience, Molecular Chaperones

Abstract

Parkin suppression induces accumulation of beta-amyloid in mutant tau mice. We studied the effect of parkin suppression on behaviour and brain pathology in APP(swe) mutant mice. We produced double mutant mice with human mutated APP(swe)+partial (hemizygote) or total (homozygote) deletion of Park-2 gene. We studied the development, behaviour, brain histology, and biochemistry of 12- and 16-month-old animals in 6 groups of mice, with identical genetic background: wild-type (WT), APP(swe) overexpressing (APP), hemizygote and homozygote deletion of Park-2 (PK(+/-) and PK(-/-), respectively), and double mutants (APP/PK(+/-) and APP/PK(-/-)). APP mice have reduced weight gain, decreased motor activity, and reduced number of entrances and of arm alternation in the Y-maze, abnormalities which were partially or completely normalized in APP/PK(+/-) and APP/PK(-/-) mice. The double mutants had similar number of mutant human APP transgene copies than the APP and levels of 40 and 80 kDa proteins; but both of them, APP/PK(+/-) and APP/PK(-/-) mice, had less plaques in cortex and hippocampus than the APP mice. APP mutant mice had increased apoptosis, proapoptotic Bax/Bcl2 ratios, and gliosis, but these death-promoting factors were normalized in APP/PK(+/-) and APP/PK(-/-) mice. APP mutant mice had an increased number of tau immunoreactive neuritic plaques in the cerebral cortex as well as increased levels of total and phosphorylated tau protein, and these changes were partially normalized in APP/PK(+/-) heterozygotic and homozygotic APP/PK(-/-) mice. Compensatory protein-degrading systems such as HSP70, CHIP, and macroautophagy were increased in APP/PK(+/-) and APP/PK(-/-). Furthermore, the chymotrypsin- and trypsin-like proteasome activities, decreased in APP mice in comparison with WT, were normalized in the APP/PK(-/-) mice. We proposed that partial and total suppression of parkin triggers compensatory mechanisms, such as chaperone overexpression and increased autophagy, which improved the behavioural and cellular phenotype of APP(swe) mice.

Published

2010

6. NP7 protects from cell death induced by oxidative stress in neuronal and glial midbrain cultures from parkin null mice

Author

Maria Angeles Mena, Izaskun Rodal, Ana M. Gómez, J.G. de Yebenes, Jose A. Rodriguez-Navarro, Rosa M. Solano, María José Casarejos, and Miguel Medina

Subjects

Programmed cell death, Ubiquitin-Protein Ligases, Biophysics, Apoptosis, Biology, medicine.disease_cause, Biochemistry, Antioxidants, Parkin, Dopamine neurons, Antiparkinson Agents, Mice, Mesencephalon, Structural Biology, Dopamine, Glia, Genetics, medicine, Animals, p-ERK and p-AKT signaling pathways, Molecular Biology, Protein kinase B, Cells, Cultured, Mice, Knockout, Neurons, Free Radical Scavengers, Hydrogen Peroxide, Cell Biology, Parkin knockout mice, Free radical scavenger, Molecular biology, Neuroprotective Agents, medicine.anatomical_structure, nervous system, Cytoprotection, Oxidative stress, Aged glia, Parkinson’s disease, Neuroglia, medicine.drug

Abstract

Parkin mutations produce Parkinson's disease (PD) in humans and nigrostriatal dopamine lesions related to increased free radicals in mice. We examined the effects of NP7, a synthetic, marine derived, free radical scavenger which enters the brain, on H(2)O(2) toxicity in cultured neurons and glia from wild-type (WT) and parkin null mice (PK-KO). NP7, 5-10 microM, prevented the H(2)O(2) induced apoptosis and necrosis of midbrain neuronal and glial cultures from WT and PK-KO mice. NP7 suppressed microglial activation and the H(2)O(2) induced drop-out of dopamine neurons(.) Furthermore, NP7 prevented the increased phosphorylation of ERK and AKT induced by H(2)O(2). NP7 may be a promising neuroprotector against oxidative stress in PD.

Published

2008

7. Gender differences and estrogen effects in parkin null mice

Author

Maria Angeles Mena, Justo García de Yébenes, María José Casarejos, Rosa M. Solano, Jose A. Rodriguez-Navarro, Ana M. Gómez, and Juan Perucho

Subjects

Male, medicine.medical_specialty, Tyrosine 3-Monooxygenase, medicine.drug_class, Dopamine, Ubiquitin-Protein Ligases, Estrogen receptor, Apoptosis, Biochemistry, Neuroprotection, Parkin, Mice, Cellular and Molecular Neuroscience, Internal medicine, Glial Fibrillary Acidic Protein, medicine, Animals, Gliosis, Protein kinase B, Cells, Cultured, Mice, Knockout, Neurons, Sex Characteristics, Estradiol, Tyrosine hydroxylase, Glial fibrillary acidic protein, biology, Estrogen Receptor alpha, Estrogens, Parkinson Disease, Substantia Nigra, Endocrinology, Cytoprotection, Estrogen, Nerve Degeneration, biology.protein, Female, Microglia, medicine.drug

Abstract

Estrogens are considered neurotrophic for dopamine neurons. Parkinson's disease is more frequent in males than in females, and more prevalent in females with short reproductive life. Estrogens are neuroprotective against neurotoxic agents for dopamine neurons in vivo and in vitro. Here, we have investigated the role of estrogens in wild-type (WT) and parkin null mice (PK-/-). WT mice present sexual dimorphisms in neuroprotective mechanisms (Bcl-2/Bax, chaperones, and GSH), but some of these inter-sex differences disappear in PK-/-. Tyrosine hydroxylase (TH) protein and TH+ cells decreased earlier and more severely in female than in male PK-/- mice. Neuronal cultures from midbrain of WT and PK-/- mice were treated with estradiol from 10 min to 48 h. Short-term treatments activated the mitogen-activated protein kinase pathway of WT and PK-/- neurons and the phosphatidylinositol 3'-kinase/AKT/glycogen synthase kinase-3 pathway of WT but not of PK-/- cultures. Long-term treatments with estradiol increased the number of TH+ neurons, the TH expression, and the extension of neurites, and decreased the level of apoptosis, the expression of glial fibrillary acidic protein, and the number of microglial cells in WT but not in PK-/- cultures. The levels of estrogen receptor-alpha were elevated in midbrain cultures and in the striatum of adult PK-/- male mice, suggesting that suppression of parkin changes the estrogen receptor-alpha turnover. From our data, it appears that parkin participates in the cellular estrogen response which could be of interest in the management of parkin-related Parkinson's disease patients.

Published

2008

8. Glial Dysfunction in Parkin Null Mice: Effects of Aging

Author

Jamie Menéndez-Cuervo, Maria Angeles Mena, Justo García de Yébenes, María José Casarejos, Rosa M. Solano, and Jose A. Rodriguez-Navarro

Subjects

Aging, Proliferation index, Ubiquitin-Protein Ligases, bcl-X Protein, Protein degradation, Neuroprotection, Parkin, Mice, chemistry.chemical_compound, Mesencephalon, Glial Fibrillary Acidic Protein, medicine, Animals, Cells, Cultured, Mice, Knockout, Neurons, chemistry.chemical_classification, Analysis of Variance, Dose-Response Relationship, Drug, L-Lactate Dehydrogenase, Glial fibrillary acidic protein, biology, CD11 Antigens, General Neuroscience, Glutathione peroxidase, Articles, Glutathione, Embryo, Mammalian, Cell biology, Oxidative Stress, medicine.anatomical_structure, nervous system, chemistry, Biochemistry, Culture Media, Conditioned, biology.protein, Neuroglia, Signal Transduction

Abstract

Parkin mutations in humans produce parkinsonism whose pathogenesis is related to impaired protein degradation, increased free radicals, and abnormal neurotransmitter release. The role of glia in parkin deficiency is little known. We cultured midbrain glia from wild-type (WT) and parkin knock-out (PK-KO) mice. After 18–20 din vitro, PK-KO glial cultures had less astrocytes, more microglia, reduced proliferation, and increased proapoptotic protein expression.PK-KO glia had greater levels of intracellular glutathione (GSH), increased mRNA expression of the GSH-synthesizing enzyme γ-glutamylcysteine synthetase, and greater glutathioneS-transferase and lower glutathione peroxidase activities than WT. The reverse happened in glia cultured in serum-free defined medium (EF12) or in old cultures. PK-KO glia was more susceptible than WT to transference to EF12 or neurotoxins (1-methyl-4-phenylpyridinium, blockers of GSH synthesis or catalase, inhibitors of extracellular signal-regulated kinase 1/2 and phosphatidylinositol 3 kinases), aging of the culture, or combination of these insults. PK-KO glia was less susceptible than WT to Fe2+plus H2O2and less responsive to protection by deferoxamine.Old WT glia increased the expression of heat shock protein 70, but PK-KO did not. Glia conditioned medium (GCM) from PK-KO was less neuroprotective and had lower levels of GSH than WT. GCM from WT increased the levels of dopamine markers in midbrain neuronal cultures transferred to EF12 more efficiently than GCM from PK-KO, and the difference was corrected by supplementation with GSH. PK-KO-GCM was a less powerful suppressor of apoptosis and microglia in neuronal cultures. Our data prove that abnormal glial function is critical in parkin mutations, and its role increases with aging.

Published

2008

9. Differential effects of l-DOPA on monoamine metabolism, cell survival and glutathione production in midbrain neuronal-enriched cultures from parkin knockout and wild-type mice

Author

J. Menéndez, Jose A. Rodriguez-Navarro, J. García de Yébenes, Maria Angeles Mena, C. Correa, María José Casarejos, and Rosa M. Solano

Subjects

medicine.medical_specialty, Tyrosine hydroxylase, Monoamine oxidase, Biology, Biochemistry, Parkin, nervous system diseases, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Endocrinology, chemistry, Dopamine, Internal medicine, medicine, Catecholamine, Neurotoxin, Neurotransmitter, Intracellular, medicine.drug

Abstract

l-DOPA is the most effective treatment for Parkinson's disease but in isolated neuronal cultures it is neurotoxic for dopamine (DA) neurones. Experiments in vivo and clinical studies have failed to show toxicity of l-DOPA in animals or patients but that does not exclude the possibility of a toxic effect of l-DOPA on patients with certain genetic risk factors. Mutations of the parkin gene are the most frequent cause of hereditary parkinsonism. Parkin null mice have a mild phenotype that could be modified by different neurotoxins. The aim of this study was to investigate whether the toxic effects of l-DOPA on DA neurones are amplified in parkin null mice. We have measured the effects of l-DOPA on cell viability, tyrosine hydroxylase (TH) expression, DA metabolism and glutathione levels of parkin knockout (PK-KO) midbrain cultures. Neuronal-enriched cultures from PK-KO mice have similar proportions of the different cell types with the exception of a significant increment of microglial cells. l-DOPA (400 µm for 24 h) reduced the number of TH-immunoreactive cells to 50% of baseline and increased twofold the percentage of apoptotic cells in cultures of wild-type (WT) animals. The PK-KO mice, however, are not only resistant to the l-DOPA-induced pro-apoptotic effects but they have an increased number of TH-immunoreactive neurones after treatment with l-DOPA, suggesting that l-DOPA is toxic for neurones of WT mice but not those of parkin null mice. MAPK and phosphatidylinositol-3 kinase signalling pathways are not involved in the differential l-DOPA effects in WT and PK-KO cultures. Intracellular levels of l-DOPA were not different in WT and parkin null mice but the intracellular and extracellular levels of DA and 3-4-dihydroxyphenylacetic acid, however, were significantly increased in parkin null animals. Furthermore, monoamine oxidase activity was significantly increased in parkin null mice, suggesting that these animals have an increased metabolism of DA. The levels of glutathione were further increased in parkin null mice than in controls both with and without treatment with l-DOPA, suggesting that a compensatory mechanism may protect DA neurones from neuronal death. This study opens new avenues for understanding the mechanisms of action of l-DOPA on DA neurones in patients with Park-2 mutations.

Published

2005

10. Role of extracellular signal-regulated protein kinase in neuronal cell death induced by glutathione depletion in neuron/glia mesencephalic cultures

Author

Maria Angeles Mena, Santiago Canals, Rosa M. Solano, J. Menéndez, María José Casarejos, and S de Bernardo

Subjects

MAPK/ERK pathway, medicine.medical_specialty, Programmed cell death, Dopamine, p38 mitogen-activated protein kinases, MAP Kinase Kinase 2, MAP Kinase Kinase 1, Ascorbic Acid, Biology, Biochemistry, Cellular and Molecular Neuroscience, Mesencephalon, Internal medicine, Nitriles, Butadienes, medicine, Animals, Lipoxygenase Inhibitors, Enzyme Inhibitors, Extracellular Signal-Regulated MAP Kinases, Protein kinase A, Buthionine Sulfoximine, Cells, Cultured, Flavonoids, Neurons, Cell Death, Dose-Response Relationship, Drug, Kinase, Ascorbic acid, Glutathione, Coculture Techniques, Rats, Cell biology, Enzyme Activation, medicine.anatomical_structure, Endocrinology, nervous system, Neuroglia, Neuron, Nitric Oxide Synthase, Reactive Oxygen Species

Abstract

To date, glutathione (GSH) depletion is the earliest biochemical alteration shown in brains of Parkinson's disease patients, but the role of GSH in dopamine cell survival is debated. In this study we show that GSH depletion, produced with GSH synthesis inhibitor, L-buthionine-(S,R)-sulfoximine (BSO), induces selectively neuronal cell death in neuron/glia, but not in neuronal-enriched midbrain cultures and that cell death occurs with characteristics of necrosis and apoptosis. BSO produces a dose- and time-dependent generation of reactive oxygen species (ROS) in neurons. BSO activates extracellular signal-regulated kinases (ERK-1/2), 4 and 6 h after treatment. MEK-1/2 and lipoxygenase (LOX) inhibitors, as well as ascorbic acid, prevent ERK-1/2 activation and neuronal loss, but the inhibition of nitric oxide sintase (NOS), cyclo-oxygenase (COX), c-Jun N-terminal kinase (JNK) and p38 mitogen-activated protein kinase (p38 MAPK) does not have protective effects. Co-localization studies show that p-ERK-1/2 expression after BSO treatment increased in astrocytes and microglial cells, but not in neurons. Selective metabolic impairment of glial cells with fluoroacetate decreased ERK activation. However, blockade of microglial activation with minocycline did not. Our results indicate that neuronal death induced by GSH depletion is due to ROS-dependent activation of the ERK-1/2 signalling pathway in glial cells. These data may be of relevance in Parkinson's disease, where GSH depletion and glial dysfunction have been documented.

Published

2004

11. Parkin gene inactivation alters behaviour and dopamine neurotransmission in the mouse

Author

Nacer Abbas, Patrice Denefle, Jeremy Pratt, Maria Angeles Mena, Gunter Tremp, Thomas Rooney, Eva Gallego, Marina P. Sánchez, Gwénnäelle Ret, Francisco Araujo, Chantal Joubert, Justo García de Yébenes, Pablo Ibanez, Alexis Brice, Rosa M. Solano, Olga Corti, Charles Cohen-Salmon, Jean Michel Itier, Laurent Pradier, Michel Laville, Magali Periquet, Santiago Canals, Alba Serrano, María José Casarejos, Julia Negroni, Georg Andrees Bohme, and Jesus Benavides

Subjects

Male, medicine.medical_specialty, Dopamine, Ubiquitin-Protein Ligases, Mice, Transgenic, Striatum, Biology, Neuroprotection, Parkin, Body Temperature, Mice, Catecholamines, Dopamine receptor D3, Internal medicine, Genetics, medicine, Animals, Neurotransmitter Uptake Inhibitors, Gene Silencing, Enzyme Inhibitors, Monoamine Oxidase, Molecular Biology, Alleles, Cells, Cultured, Genetics (clinical), Sequence Deletion, Dopamine transporter, Neurons, Base Sequence, Behavior, Animal, Body Weight, Homozygote, Dopaminergic, Glutamate receptor, Exons, General Medicine, Introns, nervous system diseases, alpha-Methyltyrosine, Endocrinology, biology.protein, Female, medicine.drug

Abstract

Mutations of the parkin gene are the most frequent cause of early onset autosomal recessive parkinsonism (EO-AR). Here we show that inactivation of the parkin gene in mice results in motor and cognitive deficits, inhibition of amphetamine-induced dopamine release and inhibition of glutamate neurotransmission. The levels of dopamine are increased in the limbic brain areas of parkin mutant mice and there is a shift towards increased metabolism of dopamine by MAO. Although there was no evidence for a reduction of nigrostriatal dopamine neurons in the parkin mutant mice, the level of dopamine transporter protein was reduced in these animals, suggesting a decreased density of dopamine terminals, or adaptative changes in the nigrostriatal dopamine system. GSH levels were increased in the striatum and fetal mesencephalic neurons from parkin mutant mice, suggesting that a compensatory mechanism may protect dopamine neurons from neuronal death. These parkin mutant mice provide a valuable tool to better understand the preclinical deficits observed in patients with PD and to characterize the mechanisms leading to the degeneration of dopamine neurons that could provide new strategies for neuroprotection.

Published

2003

12. LOW EXPRESSION OF G?? PROTEIN SUBUNITS IN HUMAN PROSTATE CANCER

Author

M. OLGA GARC??A-FERN??NDEZ, ROSA M. SOLANO, MANUEL S??NCHEZ-CHAPADO, ANTONIO RUIZ-VILLAESPESA, JUAN C. PRIETO, and MAR??A J. CARMENA

Subjects

Urology

Published

2001

13. P3‐026: Effects of amyloid (1‐42) peptide on cortical neuron/glia cultures from parkin null mice. Role of autophagy and glutathione homeostasis

Author

Ana M. Gómez, Rosa M. Solano, Maria Angeles Mena, María José Casarejos, Justo García de Yébenes, and Juan Perucho

Subjects

Null mice, chemistry.chemical_classification, Amyloid, Epidemiology, Cortical neuron, Health Policy, Autophagy, Peptide, Glutathione, Biology, Parkin, Cell biology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Developmental Neuroscience, chemistry, Neurology (clinical), Geriatrics and Gerontology, Neuroscience, Homeostasis

Published

2011

14. P3‐027: Trehalose protects from aggravation of amyloid pathology induced by isoflurane anesthesia in APPswe mutant mice

Author

Ana M. Gómez, Juan Perucho, Rosa M. Solano, Justo García de Yébenes, Maria Angeles Mena, and María José Casarejos

Subjects

Amyloid pathology, Epidemiology, business.industry, Health Policy, Mutant, Trehalose, Psychiatry and Mental health, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Developmental Neuroscience, chemistry, Isoflurane, Anesthesia, Medicine, Neurology (clinical), Geriatrics and Gerontology, business, medicine.drug

Published

2011

15. The accumulation of neurotoxic proteins, induced by proteasome inhibition, is reverted by trehalose, an enhancer of autophagy, in human neuroblastoma cells

Author

Juan Perucho, Maria Angeles Mena, Rosa M. Solano, Ana M. Gómez, María José Casarejos, and J.G. de Yebenes

Subjects

Programmed cell death, Cell Survival, Blotting, Western, Biology, Neuroprotection, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Neuroblastoma, Epoxomicin, GSK-3, Cell Line, Tumor, medicine, Autophagy, Humans, Enzyme Inhibitors, Cell Proliferation, Proteins, Trehalose, Cell Biology, Immunohistochemistry, Proteasome, chemistry, Biochemistry, Proteasome inhibitor, Oligopeptides, Proteasome Inhibitors, medicine.drug

Abstract

Neurodegenerative diseases like Parkinson's disease, Alzheimer's disease, Huntington's disease and others are due to accumulation of abnormal proteins which fold improperly and impair neuronal function. Accumulation of these proteins could be achieved by several mechanisms including mutation, overproduction or impairment of its degradation. Inhibition of the normal protein degradation is produced by blockade of the ubiquitin proteasome system. We have shown that epoxomicin, a proteasome inhibitor, increases the levels of proteins involved in neurodegenerative disorders such as α-synuclein and hyper phosphorylated tau in NB69 human neuroblastoma cells and that such increase correlates with an enhanced rate of cell death. We then investigated whether the stimulation of autophagy, an alternative mechanism for elimination of abnormal proteins, by treatment with trehalose, counteracts the effects of proteasomal blockade. Trehalose, a disaccharide present in many non-mammalian species, known to enhance autophagy, protects cells against various environmental stresses. Treatment with trehalose produced a dose and time-dependent increase in the number of autophagosomes and markers of autophagy in NB69 cells. Trehalose did not change the number of total neither the number of dividing cells in the culture but it completely prevented the necrosis of NB69 induced by epoxomicin. In addition, the treatment with trehalose reverted the accumulation, induced by epoxomicin, of polyubiquitinated proteins, total and phosphorylated tau, p-GSK-3, and α-synuclein, as well as the α-synuclein intracellular aggregates. The effects of trehalose were not mediated through activation of free radical scavenging compounds, like GSH, or mitochondrial proteins, like DJ1, but trehalose reduced the activation of ERK and chaperone HSP-70 induced by epoxomicin. Inhibition of ERK phosphorylation prevented the epoxomicin-induced cell death. Inhibition of autophagy reverted the neuroprotective effects of trehalose in epoxomicin-induced cell death. These results suggest that trehalose is a powerful modifier of abnormal protein accumulation in neurodegenerative diseases.

Published

2010

16. Trehalose ameliorates dopaminergic and tau pathology in parkin deleted/tau overexpressing mice through autophagy activation

Author

Justo García de Yébenes, Maria Angeles Mena, Jose A. Rodriguez-Navarro, María José Casarejos, Laura Zúñiga Rodríguez, Juan Perucho, Rosa M. Solano, Ana Maria Cuervo, and Ana Gómez

Subjects

medicine.medical_specialty, Pathology, Genotype, Parkinson's disease, Dopamine, Ubiquitin-Protein Ligases, Tau protein, Mice, Transgenic, tau Proteins, Biology, Polymerase Chain Reaction, Parkin, lcsh:RC321-571, chemistry.chemical_compound, Mice, Parkinsonian Disorders, Mesencephalon, Internal medicine, medicine, Autophagy, Animals, Senile plaques, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Neurons, Dopaminergic, Trehalose, Neurofibrillary Tangles, medicine.disease, Corpus Striatum, Astrogliosis, Endocrinology, Neurology, chemistry, Tauopathies, biology.protein, Tauopathy, Tau, medicine.drug

Abstract

Tauopathies are neurodegenerative diseases, sporadic or familial, mainly characterized by dementia and parkinsonism associated to atrophy of the frontotemporal cortex and the basal ganglia, with deposition of abnormal tau in brain. Hereditary tauopathies are related with mutations of the tau gene. Up to the present, these diseases have not been helped by any disease-modifying treatment, and patients die a few years after the onset of symptoms. We have developed and characterized a mouse model of tauopathy with parkinsonism, overexpressing human mutated tau protein with deletion of parkin (PK(-/-)/Tau(VLW)). At 3 months of age, these mice present abnormal dopamine-related behavior, severe dropout of dopamine neurons in the ventral midbrain, reduced dopamine levels in the striatum and abundant phosphorylated tau-positive neuritic plaques, neurofibrillary tangles, astrogliosis, and, at 12 months old, plaques of murine beta-amyloid in the hippocampus. Trehalose is a natural disaccharide that increases the removal of abnormal proteins through enhancement of autophagy. In this work, we tested if 1% trehalose in the drinking water reverts the PK(-/-)/Tau(VLW) phenotype. The treatment with trehalose of 3-month-old PK(-/-)/Tau(VLW) mice for 2.5 months reverted the dropout of dopamine neurons, which takes place in the ventral midbrain of vehicle treated PK(-/-)/Tau(VLW) and the reduced dopamine-related proteins levels in the midbrain and striatum. The number of phosphorylated tau-positive neuritic plaques and the levels of phosphorylated tau decreased, as well as astrogliosis in brain regions. The autophagy markers in the brain, the autophagic vacuoles isolated from the liver, and the electron microscopy data indicate that these effects of trehalose are mediated by autophagy. The treatment with trehalose for 4 months of 3-month-old PK(-/-)/Tau(VLW) mice maintained the amelioration of the tau pathology and astrogliosis but failed to revert DA-related pathology in the striatum. Furthermore, the 3-week treatment with trehalose of 14-month-old PK(-/-)/Tau(VLW) mice, at the limit of their life expectancy, improved the motor behavior and anxiety of these animals, and reduced their levels of phosphorylated tau and the number of murine beta-amyloid plaques. Trehalose is neuroprotective in this model of tauopathy. Since trehalose is free of toxic effects at high concentrations, this study opens the way for clinical studies of the effects of trehalose in human tauopathies.

Published

2010

17. Parkin deficiency increases the resistance of midbrain neurons and glia to mild proteasome inhibition: the role of autophagy and glutathione homeostasis

Author

Ana Gómez, Rosa M. Solano, Jose A. Rodriguez-Navarro, Juan Perucho, Maria Angeles Mena, José G. Castaño, Justo García de Yébenes, and María José Casarejos

Subjects

Programmed cell death, medicine.medical_specialty, Proteasome Endopeptidase Complex, Ubiquitin-Protein Ligases, Mice, Transgenic, Protein degradation, Biochemistry, Parkin, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Mice, Epoxomicin, Ubiquitin, Mesencephalon, Internal medicine, Cell Line, Tumor, medicine, Autophagy, Animals, Homeostasis, Humans, Cells, Cultured, Mice, Knockout, Neurons, biology, Dose-Response Relationship, Drug, Glutathione, Mice, Inbred C57BL, Endocrinology, chemistry, Proteasome, biology.protein, Signal transduction, Neuroglia, Oligopeptides, Proteasome Inhibitors

Abstract

Parkin mutations in humans produce parkinsonism whose pathogenesis is related to impaired protein degradation, increased free radicals and abnormal neurotransmitter release. In this study, we have investigated whether partial proteasomal inhibition by epoxomicin, an ubiquitin proteasomal system (UPS) irreversible inhibitor, further aggravates the cellular effects of parkin suppression in midbrain neurons and glia. We observed that parkin null (PK-KO) midbrain neuronal cultures are resistant to epoxomicin-induced cell death. This resistance is due to increased GSH and DJ-1 protein levels in PK-KO mice. The treatment with epoxomicin increases, in wild type (WT) cultures, the pro-apoptotic Bax/Bcl-2 ratio, the phosphorylation of tau, and the levels of chaperones heat-shock protein 70 and C-terminal Hsc-interacting protein, but none of these effects took place in epoxomicin-treated PK-KO cultures. Poly-ubiquitinated proteins increased more in WT than in PK-KO-treated neuronal cultures. Parkin accumulated in WT neuronal cultures treated with epoxomicin. Markers of autophagy, such as LC3II/I, were increased in naive PK-KO cultures, and further increased after treatment with epoxomicin, implying that the blockade of the proteasome in PK-KO neurons triggers the enhancement of autophagy. The treatment with l-buthionine-S,R-sulfoximine and the inhibition of autophagy, however, reverted the increase resistance to epoxomicin of the PK-KO cultures. We also found that PK-KO glial cells, stressed by growth in defined medium and depleted of GSH, were more susceptible to epoxomicin induced cell death than WT glia treated similarly. This susceptibility was linked to reduced GSH levels and less heat-shock protein 70 response, and to activation of p-serine/threonine kinase protein signaling pathway as well as to increased poly-ubiquitinated proteins. These data suggest that mild UPS inhibition is compensated by other mechanisms in PK-KO midbrain neurons. However the depletion of GSH, as happens in stressed glia, suppresses the protection against UPS inhibition-induced cell death. Furthermore, GSH inhibition regulated differentially UPS activity and in old PK-KO mice, which have depletion of GSH, UPS activity is decreased in comparison with that of old-WT.

Published

2009

18. Parkin deletion causes cerebral and systemic amyloidosis in human mutated tau over-expressing mice

Author

Israel Ampuero, Maria Angeles Mena, Rosa M. Solano, Ana Gómez, Armando Martínez, Jose A. Rodriguez-Navarro, Justo García de Yébenes, Juan Perucho, María José Casarejos, Izaskun Rodal, and Vicente Furió

Subjects

Amyloid, Dopamine, Ubiquitin-Protein Ligases, Tau protein, Mice, Transgenic, tau Proteins, Parkin, Presenilin, Mice, Alzheimer Disease, mental disorders, Genetics, Amyloid precursor protein, medicine, Limbic System, Animals, Humans, HSP70 Heat-Shock Proteins, Senile plaques, Molecular Biology, Genetics (clinical), Mice, Knockout, Neurons, Brain Diseases, Amyloid beta-Peptides, biology, Behavior, Animal, General Medicine, medicine.disease, Molecular biology, Recombinant Proteins, Mice, Inbred C57BL, Disease Models, Animal, Liver, Astrocytes, Mutation, biology.protein, Microglia, Alzheimer's disease, Amyloid precursor protein secretase, Amyloidosis, Familial, Gene Deletion

Abstract

Deposition of proteins leading to amyloid takes place in some neurodegenerative diseases such as Alzheimer's disease and Huntington's disease. Mutations of tau and parkin proteins produce neurofibrillary abnormalities without deposition of amyloid. Here we report that mature, parkin null, over-expressing human mutated tau (PK(-/-)/Tau(VLW)) mice have altered behaviour and dopamine neurotransmission, tau pathology in brain and amyloid deposition in brain and peripheral organs. PK(-/-)/Tau(VLW) mice have abnormal behaviour and severe drop out of dopamine neurons in the ventral midbrain, up to 70%, at 12 months and abundant phosphorylated tau positive neuritic plaques, neuro-fibrillary tangles, astrogliosis, microgliosis and plaques of murine beta-amyloid in the hippocampus. PK(-/-)/Tau(VLW) mice have organomegaly of the liver, spleen and kidneys. The electron microscopy of the liver confirmed the presence of a fibrillary protein deposits with amyloid characteristics. There is also accumulation of mouse tau in hepatocytes. These mice have lower levels of CHIP-HSP70, involved in the proteosomal degradation of tau, increased oxidative stress, measured as depletion of glutathione which, added to lack of parkin, could trigger tau accumulation and amyloidogenesis. This model is the first that demonstrates beta-amyloid deposits caused by over-expression of tau and without modification of the amyloid precursor protein, presenilins or secretases. PK(-/-)/Tau(VLW) mice provide a link between the two proteins more important for the pathogenesis of Alzheimer disease.

Published

2008

19. Mortality, oxidative stress and tau accumulation during ageing in parkin null mice

Author

Justo García de Yébenes, Izaskun Rodal, Jose A. Rodriguez-Navarro, Maria Angeles Mena, Ana Gómez, Rosa M. Solano, M. José Casarejos, and J. Menéndez

Subjects

Male, medicine.medical_specialty, Aging, Parkinson's disease, Dopamine, Ubiquitin-Protein Ligases, Glutathione reductase, Posture, Substantia nigra, Cell Count, tau Proteins, Striatum, Biology, Motor Activity, medicine.disease_cause, Biochemistry, Parkin, Cellular and Molecular Neuroscience, Mice, Mice, Neurologic Mutants, Parkinsonian Disorders, Mesencephalon, Internal medicine, medicine, Animals, chemistry.chemical_classification, Mice, Knockout, Glutathione peroxidase, medicine.disease, Substantia Nigra, Survival Rate, Disease Models, Animal, Oxidative Stress, Endocrinology, chemistry, Ageing, Disease Progression, Exploratory Behavior, Oxidative stress

Abstract

Young parkin null (pk-/-) mice have subtle abnormalities of behaviour, dopamine (DA) neurotransmission and free radical production, but no massive loss of DA neurons. We investigated whether these findings are maintained while ageing. Pk-/- mice have reduced life span and age-related reduced exploratory behaviour, abnormal walking and posture, and behaviours similar to those of early Parkinson's disease (PD), reduced number of nigrostriatal DA neurons and proapoptotic shifts in the survival/death proteins in midbrain and striatum. Contrary to young pk-/- animals 24-month-old pk-/- mice do not have compensatory elevation of GSH in striatum, glutathione reductase (GR) and glutathione peroxidase (GPx) activities are increased and catalase unchanged. Aged pk-/- mice accumulate high levels of tau and fail to up-regulate CHIP and HSP70. Our results suggest that aged pk-/- mice lack of the compensatory mechanisms that maintain a relatively normal DA function in early adulthood. This study could help to explain the effects of ageing in patients with genetic risks for Parkinson's disease.

Published

2007

20. Suppression of Parkin enhances nigrostriatal and motor neuron lesion in mice over-expressing human-mutated tau protein

Author

Jesús Avila, J.G. de Yebenes, Rosa Guerrero, J. Menéndez, María José Casarejos, Maria Angeles Mena, Jose A. Rodriguez-Navarro, Izaskun Rodal, Rosa M. Solano, Marina P. Sánchez, and Instituto de Salud Carlos III

Subjects

Genetically modified mouse, Male, medicine.medical_specialty, Genotype, Ubiquitin-Protein Ligases, Tau protein, Blotting, Western, Mice, Transgenic, tau Proteins, Motor Activity, medicine.disease_cause, Parkin, Progressive supranuclear palsy, Glycogen Synthase Kinase 3, Mice, Internal medicine, mental disorders, Genetics, medicine, Animals, Humans, Biogenic Monoamines, Molecular Biology, Genetics (clinical), Mice, Knockout, Motor Neurons, Mutation, Glycogen Synthase Kinase 3 beta, biology, Parkinsonism, HSC70 Heat-Shock Proteins, Brain, General Medicine, medicine.disease, Glutathione, Corpus Striatum, nervous system diseases, Mice, Inbred C57BL, Substantia Nigra, Endocrinology, Spinal Cord, biology.protein, Female, Mutant Proteins, Tauopathy, Frontotemporal dementia

Abstract

Abnormal deposition of protein tau takes place in the brain of patients with several neurodegenerative diseases. Few of these patients present frontotemporal dementia with parkinsonism and amyotrophy (FTDPA-17), an autosomal dominant tauopathy related to mutations of the gene that codes for protein tau, localized in chromosome 17. The great majority of patients with tauopathies such as Alzheimer's disease, sporadic frontotemporal dementia or progressive supranuclear palsy do not show a Mendelian pattern of inheritance. We have occasionally seen tauopathies in patients with parkin mutations and, therefore, hypothesized that the protein tau interacts with parkin. We have tested that hypothesis in mice with combined genetic modifications of tau (over-expression of human tau with three mutations known to produce FTDPA-17) and parkin (deleted) proteins. Homozygote parkin null or over-expressing mutated-human tau mice have subtle behavioral and molecular abnormalities but do not express a clinical phenotype of neurodegenerative disease. Mice with combined homozygous mutations of these two genes show progressively abnormal walking already noticeable at 3 months of age, loss of dopamine and dopamine markers in striatum, nuclear tau immunoreactive deposits in motor neurons of the spinal cord, abnormal expression of glial markers and enhanced levels of pro-apoptotic proteins; findings that were absent or less pronounced in homozygote animals with deletions of parkin or over-expression of tau. The double transgenic mice do not express normal mechanisms of adaptation to stress such as increased levels of GSH and Hsp-70. In addition, they have reduced levels of CHIP–Hsc70, a complex known to attenuate aggregation of tau and to enhance ubiquitination of phosphorylated tau. We have found high levels of phosphorylated tau in parkin−/−+tauVLW mice and a relative decrease of the inactivated pSer9 to total GSK-3 levels. Our data reveal that there are interactions between tau and parkin that could be relevant for the pathogenesis and treatment of tauopathies. Similarly, we hope that the double transgenic parkin−/−+tauVLW mice could be useful for testing of compounds with putative therapeutic value in human tauopathies., This work was supported by the Spanish Government Grants, FIS 2002/PI20265, 2004/PI40360 and RED CIEN 03/06. J.M. and J.A.R. are recipients of FIS predoctoral fellowships.

Published

2006

21. Susceptibility to rotenone is increased in neurons from parkin null mice and is reduced by minocycline

Author

Maria Angeles Mena, J. Menéndez, Rosa M. Solano, Jose A. Rodriguez-Navarro, J. García de Yébenes, and María José Casarejos

Subjects

Male, medicine.medical_specialty, Programmed cell death, Tyrosine 3-Monooxygenase, Dopamine, Ubiquitin-Protein Ligases, Apoptosis, Mice, Transgenic, Minocycline, Biology, complex mixtures, Biochemistry, Parkin, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Mice, Internal medicine, Rotenone, medicine, Animals, Genetic Predisposition to Disease, Tyrosine, Enzyme Inhibitors, Cells, Cultured, Mice, Knockout, Neurons, Glial fibrillary acidic protein, Microglia, Tyrosine hydroxylase, Dose-Response Relationship, Drug, Uncoupling Agents, food and beverages, NADPH Oxidases, Parkinson Disease, Immunity, Innate, Anti-Bacterial Agents, Substantia Nigra, Disease Models, Animal, medicine.anatomical_structure, Endocrinology, Neuroprotective Agents, chemistry, biology.protein, Neuroglia, Female

Abstract

Parkinson's disease is a neurodegenerative disorder which is in most cases of unknown etiology. Mutations of the Park-2 gene are the most frequent cause of familial parkinsonism and parkin knockout (PK-KO) mice have abnormalities that resemble the clinical syndrome. We investigated the interaction of genetic and environmental factors, treating midbrain neuronal cultures from PK-KO and wild-type (WT) mice with rotenone (ROT). ROT (0.025-0.1 microm) produced a dose-dependent selective reduction of tyrosine hydroxylase-immunoreactive cells and of other neurons, as shown by the immunoreactivity to microtubule-associated protein 2 in PK-KO cultures, suggesting that the toxic effect of ROT involved dopamine and other types of neurons. Neuronal death was mainly apoptotic and suppressible by the caspase inhibitor t-butoxycarbonyl-Asp(OMe)-fluoromethyl ketone (Boc-D-FMK). PK-KO cultures were more susceptible to apoptosis induced by low doses of ROT than those from WT. ROT increased the proportion of astroglia and microglia more in PK-KO than in WT cultures. Indomethacin, a cyclo-oxygenase inhibitor, worsened the effects of ROT on tyrosine hydroxylase cells, apoptosis and astroglial (glial fibrillary acidic protein) cells. N-nitro-L-arginine methyl ester, an inhibitor of nitric oxide synthase, increased ROT-induced apoptosis but did not change tyrosine hydroxylase-immunoreactive or glial fibrillary acidic protein area. Neither indomethacin nor N-nitro-L-arginine methyl ester had any effect on the reduction by ROT of the mitochondrial potential as measured by 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide. Microglial NADPH oxidase inhibition, however, protected against ROT. The roles of p38 MAPK and extracellular signal-regulated kinase signaling pathways were tested by treatment with SB20358 and PD98059, respectively. These compounds were inactive in ROT-naive cultures but PD98059 slightly increased cellular necrosis, as measured by lactate dehydrogenase levels, caused by ROT, without changing mitochondrial activity. SB20358 increased the mitochondrial failure and lactate dehydrogenase elevation induced by ROT. Minocycline, an inhibitor of microglia, prevented the dropout of tyrosine hydroxylase and apoptosis by ROT; the addition of microglia from PK-KO to WT neuronal cultures increased the sensitivity of dopaminergic neurons to ROT. PK-KO mice were more susceptible than WT to ROT and the combined effects of Park-2 suppression and ROT reproduced the cellular events observed in Parkinson's disease. These events were prevented by minocycline.

Published

2006

22. Neuroprotective and Neurotoxic Effects of L-DOPA in Rat Midbrain Dopaminergic Neurons in Culture

Author

J. Menéndez, Maria Angeles Mena, María José Casarejos, Rosa M. Solano, E. Rodríguez‐Martín, and Justo García de Yébenes

Subjects

Midbrain, Chemistry, Dopaminergic, Neuroscience, Neuroprotection

Published

2005

23. Midbrain neuronal cultures from parkin mutant mice are resistant to nitric oxide-induced toxicity

Author

J. Menéndez, J. García de Yébenes, Jose A. Rodriguez-Navarro, Maria Angeles Mena, Rosa M. Solano, and María José Casarejos

Subjects

medicine.medical_specialty, Ubiquitin-Protein Ligases, Biology, Nitric Oxide, Parkin, Nitric oxide, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Mice, Dopamine, Mesencephalon, Internal medicine, medicine, Animals, Nitric Oxide Donors, Cells, Cultured, Pharmacology, Mice, Knockout, Neurons, Tyrosine hydroxylase, Cell Death, Neurotoxicity, Glutathione, medicine.disease, nervous system diseases, Endocrinology, Hydrazines, chemistry, Knockout mouse, S-Nitrosoglutathione, biology.protein, medicine.drug, Neurotrophin

Abstract

Nitric oxide (NO) is a modulator of differentiation and survival of dopamine (DA) neurons. NO may play a role in the pathogenesis of Parkinson's disease (PD) since its levels are increased in parkinsonian brains and it can nitrosylate and alter the function of key proteins involved in the pathogenesis of PD. NO producing neurons are spared in parkinsonian brains suggesting that toxicity by NO can be compensated. Furthermore, the neurotoxic or neurotrophic effects of NO on DA neurons depend on the balance between NO levels and the intracellular levels of glutathione (GSH). We have investigated the effects of NO-donating agents on midbrain neuronal cultures from parkin-deficient mice. Parkin mutations are the most common genetic deficit observed in hereditary parkinsonism. These mice have abnormal DA release and metabolism, increased production of free radicals and a compensatory elevation of GSH. Cultures from parkin knockout (PK-KO) mice were more resistant than those of wild type (WT) to the neurotoxicity by NO, and the difference of susceptibility applied equally to DA, GABA and total number of neurons, and to astrocytes. NO-induced cell death was mainly apoptotic and could be reduced by caspase inhibitors. Cultures from PK-KO had greater levels of GSH than WT and, after treatment with NO, greater levels of S-nitrosoglutathione. The differences in susceptibility disappear when the synthesis of GSH is inhibited or the GSH chelated with diethyl maleate. Our data show that, contrary to the expectations, and related to the enhanced production of GSH in parkin knockout mice, parkin-deficient dopamine neurons are less susceptible to toxicity by NO.

Published

2005

24. Selective and persistent activation of extracellular signal-regulated protein kinase by nitric oxide in glial cells induces neuronal degeneration in glutathione-depleted midbrain cultures

Author

Rosa M. Solano, Maria Angeles Mena, Sonsoles de Bernardo, Santiago Canals, and María José Casarejos

Subjects

MAPK/ERK pathway, Programmed cell death, Biology, Nitric Oxide, Nitric oxide, Rats, Sprague-Dawley, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Mesencephalon, medicine, Animals, Protein kinase A, Molecular Biology, Cells, Cultured, Mitogen-Activated Protein Kinase 1, Mitogen-Activated Protein Kinase 3, Dose-Response Relationship, Drug, Neurotoxicity, Cell Biology, Glutathione, medicine.disease, Cell biology, Rats, Enzyme Activation, medicine.anatomical_structure, chemistry, Nerve Degeneration, Neuroglia, Signal transduction, Mitogen-Activated Protein Kinases

Abstract

Intracellular glutathione (GSH) levels determine whether nitric oxide (NO) is neurotrophic for dopamine neurons or triggers a cell death cascade in primary midbrain cultures. We have investigated herein the role of the extracellular-signal regulated protein kinase (ERK) 1/2 pathway in this GSH switching effect. The short-lived NO donor DEA/NO induces a transient activation of ERK-1/2 that totally disappears 2 h after NO administration. The depletion of GSH increases and the supplementation of GSH suppresses ERK-1/2 activation in response to NO treatment. More interestingly, GSH depletion changes the kinetic of phosphorylation leading to a second prolonged phase of ERK-1/2 activation from 2 to 16 h after NO addition. This change of kinetic is ultimately responsible for NO toxicity under GSH-depleted conditions, because selective blockade of the second and persistent phase of activation prevents cell death. In addition, the only transient ERK activation, induced by NO under normal GSH conditions, did not cause ERK-dependent cell death. Immunocytochemical colocalization studies demonstrate that ERK activation takes place exclusively in glial cells, mainly in astrocytes and less frequently in oligodendrocytes and glial progenitors. Furthermore, glial cell elimination or inactivation in the culture, by gliotoxic drugs, abrogates NO-induced ERK activation. Our results indicate that neurotrophism of NO switches into neurotoxicity after GSH depletion due to persistent activation of the ERK-1/2 signaling pathway in glial cells. The implication of these results in pathological conditions like Parkinson's disease, where GSH depletion and NO overproduction have been documented, are discussed.

Published

2003

25. Protection by glia-conditioned medium in a cell model of Huntington disease

Author

Maria Angeles Mena, Ana M. Gómez, María José Casarejos, Justo García de Yébenes, Rosa M. Solano, and Carolina Ruiz

Subjects

Programmed cell death, Huntingtin, biology, Glutamate receptor, Excitotoxicity, Medicine (miscellaneous), Molecular/Cellular, medicine.disease_cause, Neuroprotection, Cell biology, nervous system, Biochemistry, Neurotrophic factors, Glial cell line-derived neurotrophic factor, biology.protein, medicine, Neurotrophin

Abstract

The physiological role of huntingtin and the pathogenic mechanisms that produce the disease are unknown. Mutant huntingtin changes its normal localization and produces cytoplasmic and intranuclear inclusions, changes gene transcription, alters synaptic transmission, impairs mitochondrial activity and activates caspases and other pro-apoptotic molecules, promotes excitotoxicity, energy deficits, synthesis and release reduction of neurotrophic factors and oxidative stress. Previous studies confirm that the mutant huntingtin difficult neurotrophic function of astrocytes leading to neuronal dysfunction in Huntingtons disease. Our objective was to study the neuroprotective potential role of glia-conditioned medium (GCM) in an in vitro model of Huntingtons disease. We used conditionally-immortalized striatal neuronal progenitor cell lines (STHdhQ7/Q7 and STHdhQ111/Q111) expressing endogenous levels of normal and mutant huntingtin with 7 and 111 glutamines, respectively. We studied the protection of fetal and postnatal glia conditioned medium (GCM) on H2O2 (2 µM), glutamate (5 mM) and 3-nitropropionic acid (2.5 mM) related toxicity. We also compared the neuroprotective effects of GCM versus that of the growth factors bFGF, BDNF and GDNF. Fetal GCM protects from every toxin, reducing the cell death and increasing the cell survival. Fetal GCM reduces the caspases fragmentation of the protein PARP, the expression of chaperone Hsp70 and the accumulation of ROS and polyubiquitinated proteins. In addition, in Q111 striatal cells treated with H2O2 (2 µM) for 24 hours, the intracellular GSH levels are higher in the presence of GCM. Notably, the 13-day and 2-month postnatal GCM, totally protects from H2O2 induced cell death in mutant striatal cells. GCM neuroprotective effects are more potent than those of the already identified neurotrophic factors. We conclude that GCM protects Q111 cells from neuronal neurotoxins and the effects of GCM are more potent than those of any known neurotrophic factor. GCM may contain new and more potent, as yet unidentified, neurotrophic molecules, potentially useful in patients with Huntingtons disease. Abstract The physiological role of huntingtin and the pathogenic mechanisms that produce the disease are unknown. Mutant huntingtin changes its normal localization and produces cytoplasmic and intranuclear inclusions, changes gene transcription, alters synaptic transmission, impairs mitochondrial activity and activates caspases and other pro-apoptotic molecules, promotes excitotoxicity, energy deficits, synthesis and release reduction of neurotrophic factors and oxidative stress. Previous studies confirm that the mutant huntingtin difficult neurotrophic function of astrocytes leading to neuronal dysfunction in Huntingtons disease. Our objective was to study the neuroprotective potential role of glia-conditioned medium (GCM) in an in vitro model of Huntingtons disease. We used conditionally-immortalized striatal neuronal progenitor cell lines (STHdhQ7/Q7 and STHdhQ111/Q111) expressing endogenous levels of normal and mutant huntingtin with 7 and 111 glutamines, respectively. We studied the protection of fetal and postnatal glia conditioned medium (GCM) on H2O2 (2 µM), glutamate (5 mM) and 3-nitropropionic acid (2.5 mM) related toxicity. We also compared the neuroprotective effects of GCM versus that of the growth factors bFGF, BDNF and GDNF. Fetal GCM protects from every toxin, reducing the cell death and increasing the cell survival. Fetal GCM reduces the caspases fragmentation of the protein PARP, the expression of chaperone Hsp70 and the accumulation of ROS and polyubiquitinated proteins. In addition, in Q111 striatal cells treated with H2O2 (2 µM) for 24 hours, the intracellular GSH levels are higher in the presence of GCM. Notably, the 13-day and 2-month postnatal GCM, totally protects from H2O2 induced cell death in mutant striatal cells. GCM neuroprotective effects are more potent than those of the already identified neurotrophic factors. We conclude that GCM protects Q111 cells from neuronal neurotoxins and the effects of GCM are more potent than those of any known neurotrophic factor. GCM may contain new and more potent, as yet unidentified, neurotrophic molecules, potentially useful in patients with Huntingtons disease. Abstract The physiological role of huntingtin and the pathogenic mechanisms that produce the disease are unknown. Mutant huntingtin changes its normal localization and produces cytoplasmic and intranuclear inclusions, changes gene transcription, alters synaptic transmission, impairs mitochondrial activity and activates caspases and other pro-apoptotic molecules, promotes excitotoxicity, energy deficits, synthesis and release reduction of neurotrophic factors and oxidative stress. Previous studies confirm that the mutant huntingtin difficult neurotrophic function of astrocytes leading to neuronal dysfunction in Huntingtons disease. Our objective was to study the neuroprotective potential role of glia-conditioned medium (GCM) in an in vitro model of Huntingtons disease. We used conditionally-immortalized striatal neuronal progenitor cell lines (STHdhQ7/Q7 and STHdhQ111/Q111) expressing endogenous levels of normal and mutant huntingtin with 7 and 111 glutamines, respectively. We studied the protection of fetal and postnatal glia conditioned medium (GCM) on H2O2 (2 µM), glutamate (5 mM) and 3-nitropropionic acid (2.5 mM) related toxicity. We also compared the neuroprotective effects of GCM versus that of the growth factors bFGF, BDNF and GDNF. Fetal GCM protects from every toxin, reducing the cell death and increasing the cell survival. Fetal GCM reduces the caspases fragmentation of the protein PARP, the expression of chaperone Hsp70 and the accumulation of ROS and polyubiquitinated proteins. In addition, in Q111 striatal cells treated with H2O2 (2 µM) for 24 hours, the intracellular GSH levels are higher in the presence of GCM. Notably, the 13-day and 2-month postnatal GCM, totally protects from H2O2 induced cell death in mutant striatal cells. GCM neuroprotective effects are more potent than those of the already identified neurotrophic factors. We conclude that GCM protects Q111 cells from neuronal neurotoxins and the effects of GCM are more potent than those of any known neurotrophic factor. GCM may contain new and more potent, as yet unidentified, neurotrophic molecules, potentially useful in patients with Huntingtons disease.

Published

2012

26. Response

Author

Juan Perucho, Isabel Rubio, Maria J. Casarejos, Ana Gomez, Jose A. Rodriguez-Navarro, Rosa M. Solano, Justo Garcia De Yébenes, and Maria A. Mena

Subjects

Psychiatry and Mental health, Clinical Psychology, General Neuroscience, General Medicine, Geriatrics and Gerontology

Published

2010