Your search keyword '"Perucho, Juan"' showing total 18 results

1. Liver Growth Factor "LGF" as a Therapeutic Agent for Alzheimer's Disease.

Author

Gonzalo-Gobernado R, Perucho J, Vallejo-Muñoz M, Casarejos MJ, Reimers D, Jiménez-Escrig A, Gómez A, Ulzurrun de Asanza GM, and Bazán E

Subjects

Alzheimer Disease diagnosis, Alzheimer Disease drug therapy, Amyloid beta-Peptides genetics, Amyloid beta-Peptides metabolism, Animals, Behavior, Animal, Cerebral Cortex metabolism, Cerebral Cortex pathology, Disease Models, Animal, Gene Expression, Hippocampus metabolism, Hippocampus pathology, Humans, Memory, Short-Term, Mice, Mice, Transgenic, Microglia metabolism, Phosphorylation, Plaque, Amyloid etiology, Plaque, Amyloid metabolism, Plaque, Amyloid pathology, Ubiquitination, tau Proteins metabolism, Alzheimer Disease etiology, Alzheimer Disease metabolism, Bilirubin genetics, Bilirubin metabolism, Disease Susceptibility, Serum Albumin, Human genetics, Serum Albumin, Human metabolism

Abstract

Alzheimer's disease (AD) is a progressive degenerative disorder and the most common cause of dementia in aging populations. Although the pathological hallmarks of AD are well defined, currently no effective therapy exists. Liver growth factor (LGF) is a hepatic albumin-bilirubin complex with activity as a tissue regenerating factor in several neurodegenerative disorders such as Parkinson's disease and Friedreich's ataxia. Our aim here was to analyze the potential therapeutic effect of LGF on the APPswe mouse model of AD. Twenty-month-old mice received intraperitoneal (i.p.) injections of 1.6 µg LGF or saline, twice a week during three weeks. Mice were sacrificed one week later, and the hippocampus and dorsal cortex were prepared for immunohistochemical and biochemical studies. LGF treatment reduced amyloid-β (Aβ) content, phospho-Tau/Tau ratio and the number of Aβ plaques with diameter larger than 25 µm. LGF administration also modulated protein ubiquitination and HSP70 protein levels, reduced glial reactivity and inflammation, and the expression of the pro-apoptotic protein Bax. Because the administration of this factor also restored cognitive damage in APPswe mice, we propose LGF as a novel therapeutic tool that may be useful for the treatment of AD.

Published

2020

2. Singular Location and Signaling Profile of Adenosine A 2A -Cannabinoid CB 1 Receptor Heteromers in the Dorsal Striatum.

Author

Moreno E, Chiarlone A, Medrano M, Puigdellívol M, Bibic L, Howell LA, Resel E, Puente N, Casarejos MJ, Perucho J, Botta J, Suelves N, Ciruela F, Ginés S, Galve-Roperh I, Casadó V, Grandes P, Lutz B, Monory K, Canela EI, Lluís C, McCormick PJ, and Guzmán M

Subjects

Animals, Humans, Huntington Disease metabolism, Mice, Neural Pathways metabolism, Protein Subunits biosynthesis, Corpus Striatum metabolism, Protein Structure, Quaternary, Receptor, Adenosine A2A metabolism, Receptor, Cannabinoid, CB1 metabolism, Signal Transduction

Abstract

The dorsal striatum is a key node for many neurobiological processes such as motor activity, cognitive functions, and affective processes. The proper functioning of striatal neurons relies critically on metabotropic receptors. Specifically, the main adenosine and endocannabinoid receptors present in the striatum, ie, adenosine A 2A receptor (A 2A R) and cannabinoid CB 1 receptor (CB 1 R), are of pivotal importance in the control of neuronal excitability. Facilitatory and inhibitory functional interactions between striatal A 2A R and CB 1 R have been reported, and evidence supports that this cross-talk may rely, at least in part, on the formation of A 2A R-CB 1 R heteromeric complexes. However, the specific location and properties of these heteromers have remained largely unknown. Here, by using techniques that allowed a precise visualization of the heteromers in situ in combination with sophisticated genetically modified animal models, together with biochemical and pharmacological approaches, we provide a high-resolution expression map and a detailed functional characterization of A 2A R-CB 1 R heteromers in the dorsal striatum. Specifically, our data unveil that the A 2A R-CB 1 R heteromer (i) is essentially absent from corticostriatal projections and striatonigral neurons, and, instead, is largely present in striatopallidal neurons, (ii) displays a striking G protein-coupled signaling profile, where co-stimulation of both receptors leads to strongly reduced downstream signaling, and (iii) undergoes an unprecedented dysfunction in Huntington's disease, an archetypal disease that affects striatal neurons. Altogether, our findings may open a new conceptual framework to understand the role of coordinated adenosine-endocannabinoid signaling in the indirect striatal pathway, which may be relevant in motor function and neurodegenerative diseases.

Published

2018

3. Trehalose rescues glial cell dysfunction in striatal cultures from HD R6/1 mice at early postnatal development.

Author

Perucho J, Gómez A, Muñoz MP, de Yébenes JG, Mena MÁ, and Casarejos MJ

Subjects

Animals, Brain-Derived Neurotrophic Factor genetics, Brain-Derived Neurotrophic Factor metabolism, Cells, Cultured, Corpus Striatum growth & development, Cytoskeleton drug effects, Cytoskeleton metabolism, Female, Glial Cell Line-Derived Neurotrophic Factor genetics, Glial Cell Line-Derived Neurotrophic Factor metabolism, Gliosis metabolism, Humans, Huntingtin Protein genetics, Huntington Disease genetics, Male, Mice, Mice, Inbred C57BL, Neuroglia metabolism, Protein Transport, alpha-Synuclein genetics, alpha-Synuclein metabolism, Corpus Striatum cytology, Huntington Disease metabolism, Neuroglia drug effects, Neuroprotective Agents pharmacology, Trehalose pharmacology

Abstract

The pathological hallmark of Huntington disease (HD) is the intracellular aggregation of mutant huntingtin (mHTT) in striatal neurons and glia associated with the selective loss of striatal medium-sized spiny neurons. Up to the present, the role of glia in HD is poorly understood and has been classically considered secondary to neuronal disorder. Trehalose is a disaccharide known to possess many pharmacological properties, acting as an antioxidant, a chemical chaperone, and an inducer of autophagy. In this study, we analyzed at an early postnatal development stage the abnormalities observed in striatal glial cell cultures of postnatal R6/1 mice (HD glia), under baseline and stressing conditions and the protective effects of trehalose. Our data demonstrate that glial HD alterations already occur at early stages of postnatal development. After 20 postnatal days in vitro, striatal HD glia cultures showed more reactive astrocytes with increased expression of glial fibrillary acidic protein (GFAP) but with less replication capacity, less A2B5(+) glial progenitors and more microglia than wild-type (WT) cultures. HD glia had lower levels of intracellular glutathione (GSH) and was more susceptible to H2O2 and epoxomicin insults. The amount of expressed GDNF and secreted mature-BDNF by HD astrocytes were much lower than by WT astrocytes. In addition, HD glial cultures showed a deregulation of the major proteolytic systems, the ubiquitin-proteasomal system (UPS), and the autophagic pathway. This produces a defective protein quality control, indicated by the elevated levels of ubiquitination and p62 protein. Interestingly, we show that trehalose, through its capacity to induce autophagy, inhibited p62/SQSTM1 accumulation and facilitated the degradation of cytoplasmic aggregates from mHTT and α-synuclein proteins. Trehalose also reduced microglia activation and reversed the disrupted cytoskeleton of astrocytes accompanied with an increase in the replication capacity. In addition, trehalose up-regulated mature-BDNF neurotrophic factor expression and secretion, probably mediating cytoskeletal organization and helping in vesicular BDNF transport. Together, these findings indicate that glia suffers functional early changes in the disease process, changes that may contribute to HD neurodegeneration. Trehalose could be a very promising compound for treatment of HD and other diseases with abnormal protein aggregates. Furthermore our study identifies glial cells as a novel target for trehalose to induce neurotrophic and neuroprotective actions in HD., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

4. Trehalose improves human fibroblast deficits in a new CHIP-mutation related ataxia.

Author

Casarejos MJ, Perucho J, López-Sendón JL, García de Yébenes J, Bettencourt C, Gómez A, Ruiz C, Heutink P, Rizzu P, and Mena MA

Subjects

Ataxia drug therapy, Autophagy, Caspase 3 metabolism, Cell Proliferation, Cell Survival drug effects, Cells, Cultured, Free Radicals metabolism, Gene Expression, Glutathione metabolism, Humans, Mitochondria metabolism, Molecular Chaperones metabolism, Oligopeptides pharmacology, Reactive Oxygen Species metabolism, Trehalose therapeutic use, Ubiquitins metabolism, Ataxia genetics, Ataxia metabolism, Fibroblasts drug effects, Fibroblasts metabolism, Mutation, Trehalose pharmacology, Ubiquitin-Protein Ligases genetics

Abstract

In this work we investigate the role of CHIP in a new CHIP-mutation related ataxia and the therapeutic potential of trehalose. The patient's fibroblasts with a new form of hereditary ataxia, related to STUB1 gene (CHIP) mutations, and three age and sex-matched controls were treated with epoxomicin and trehalose. The effects on cell death, protein misfolding and proteostasis were evaluated. Recent studies have revealed that mutations in STUB-1 gene lead to a growing list of molecular defects as deregulation of protein quality, inhibition of proteasome, cell death, decreased autophagy and alteration in CHIP and HSP70 levels. In this CHIP-mutant patient fibroblasts the inhibition of proteasome with epoxomicin induced severe pathophysiological age-associated changes, cell death and protein ubiquitination. Additionally, treatment with epoxomicin produced a dose-dependent increase in the number of cleaved caspase-3 positive cells. However, co-treatment with trehalose, a disaccharide of glucose present in a wide variety of organisms and known as a autophagy enhancer, reduced these pathological events. Trehalose application also increased CHIP and HSP70 expression and GSH free radical levels. Furthermore, trehalose augmented macro and chaperone mediated autophagy (CMA), rising the levels of LC3, LAMP2, CD63 and increasing the expression of Beclin-1 and Atg5-Atg12. Trehalose treatment in addition increased the percentage of immunoreactive cells to HSC70 and LAMP2 and reduced the autophagic substrate, p62. Although this is an individual case based on only one patient and the statistical comparisons are not valid between controls and patient, the low variability among controls and the obvious differences with this patient allow us to conclude that trehalose, through its autophagy activation capacity, anti-aggregation properties, anti-oxidative effects and lack of toxicity, could be very promising for the treatment of CHIP-mutation related ataxia, and possibly a wide spectrum of neurodegenerative disorders related to protein disconformation.

Published

2014

5. Trehalose reverses cell malfunction in fibroblasts from normal and Huntington's disease patients caused by proteosome inhibition.

Author

Fernandez-Estevez MA, Casarejos MJ, López Sendon J, Garcia Caldentey J, Ruiz C, Gomez A, Perucho J, de Yebenes JG, and Mena MA

Subjects

Apoptosis drug effects, Autophagy drug effects, Cell Survival drug effects, Fibroblasts cytology, Fibroblasts pathology, HSP70 Heat-Shock Proteins metabolism, Humans, Huntington Disease metabolism, Huntington Disease prevention & control, Mitogen-Activated Protein Kinase 1 metabolism, Mitogen-Activated Protein Kinase 3 metabolism, Oligopeptides adverse effects, Proteasome Endopeptidase Complex metabolism, Reactive Oxygen Species metabolism, Ubiquitination drug effects, Fibroblasts drug effects, Huntington Disease chemically induced, Huntington Disease pathology, Proteasome Inhibitors adverse effects, Trehalose pharmacology

Abstract

Huntington's disease (HD) is a neurodegenerative disorder characterized by progressive motor, cognitive and psychiatric deficits, associated with predominant loss of striatal neurons and is caused by polyglutamine expansion in the huntingtin protein. Mutant huntingtin protein and its fragments are resistant to protein degradation and produce a blockade of the ubiquitin proteasome system (UPS). In HD models, the proteasome inhibitor epoxomicin aggravates protein accumulation and the inductor of autophagy, trehalose, diminishes it. We have investigated the effects of epoxomicin and trehalose in skin fibroblasts of control and HD patients. Untreated HD fibroblasts have increased the levels of ubiquitinized proteins and higher levels of reactive oxygen species (ROS), huntingtin and the autophagy marker LAMP2A. Baseline replication rates were higher in HD than in controls fibroblasts but that was reverted after 12 passages. Epoxomicin increases the activated caspase-3, HSP70, huntingtin, ubiquitinated proteins and ROS levels in both HD and controls. Treatment with trehalose counteracts the increase in ROS, ubiquitinated proteins, huntingtin and activated caspase-3 levels induced by epoxomicin, and also increases the LC3 levels more in HD fibroblast than controls. These results suggest that trehalose could revert protein processing abnormalities in patients with Huntington's Disease.

Published

2014

6. Liver growth factor as a tissue regenerating factor in neurodegenerative diseases.

Author

Gonzalo-Gobernado R, Calatrava-Ferreras L, Perucho J, Reimers D, Casarejos MJ, Herranz AS, Jimenez-Escrig A, Diaz-Gil JJ, and Bazan E

Subjects

Animals, Bilirubin pharmacology, Disease Models, Animal, Humans, Neurodegenerative Diseases physiopathology, Serum Albumin pharmacology, Serum Albumin, Human, Bilirubin therapeutic use, Nerve Regeneration drug effects, Neurodegenerative Diseases drug therapy, Serum Albumin therapeutic use

Abstract

Liver growth factor (LGF) is a hepatic mitogen purified by our group in 1986. In the following years we demonstrated its activity both in "in vivo" and "in vitro" systems, stimulating hepatocytes mitogenesis as well as liver regeneration in several models of liver injury. Furthermore, we established its chemical composition (albumin-bilirubin complex) and its mitogenic actions in liver. From 2000 onwards we used LGF as a tissue regenerating factor in several models of extrahepatic diseases. The use of Liver growth factor as a neural tissue regenerator has been recently protected (Patent No US 2014/8,642,551 B2). LGF administration stimulates neurogenesis and neuron survival, promotes migration of newly generated neurons, and induces the outgrowth of striatal dopaminergic terminals in 6-hidroxydopamine-lesioned rats. Furthermore, LGF treatment raises striatal dopamine levels and protects dopaminergic neurons in hemiparkinsonian animals. LGF also stimulates survival of grafted foetal neural stem cells in the damaged striatum, reduces rotational behaviour and improves motor coordination. Interestingly, LGF also exerts a neuroprotective role both in an experimental model of cerebellar ataxia and in a model of Friedrich´s ataxia. Microglia seem to be the cellular target of LGF in the CNS. Moreover, the activity of the factor could be mediated by the stimulation of MAPK´s signalling pathway and by regulating critical proteins for cell survival, such as Bcl-2 and phospho-CREB. Since the factor shows neuroprotective and neurorestorative effects we propose LGF as a patented novel therapeutic tool that may be useful for the treatment of Parkinson´s disease and cerebellar ataxias. Currently, our studies have been extended to other neurological disorders such as Alzheimer's disease (Patent No: US 2014/0113859 A1).

Published

2014

7. Striatal infusion of glial conditioned medium diminishes huntingtin pathology in r6/1 mice.

Author

Perucho J, Casarejos MJ, Gómez A, Ruíz C, Fernández-Estevez MÁ, Muñoz MP, de Yébenes JG, and Mena MÁ

Subjects

Animals, Brain-Derived Neurotrophic Factor metabolism, Cells, Cultured, Corpus Striatum drug effects, Corpus Striatum metabolism, Dopamine and cAMP-Regulated Phosphoprotein 32 genetics, Dopamine and cAMP-Regulated Phosphoprotein 32 metabolism, Genotype, Humans, Huntington Disease metabolism, Male, Mice, Neostriatum drug effects, Neostriatum metabolism, Culture Media, Conditioned chemistry, Huntington Disease drug therapy, Huntington Disease pathology, Neuroglia cytology

Abstract

Huntington's disease is a neurodegenerative disorder caused by an expansion of CAG repeats in the huntingtin gene which produces widespread neuronal and glial pathology. We here investigated the possible therapeutic role of glia or glial products in Huntington's disease using striatal glial conditioned medium (GCM) from fetus mice (E16) continuously infused for 15 and 30 days with osmotic minipumps into the left striatum of R6/1 mice. Animals infused with GCM had significantly less huntingtin inclusions in the ipsilateral cerebral cortex and in the ipsilateral and contralateral striata than mice infused with cerebrospinal fluid. The numbers of DARPP-32 and TH positive neurons were also greater in the ipsilateral but not contralateral striata and substantia nigra, respectively, suggesting a neuroprotective effect of GCM on efferent striatal and nigro-striatal dopamine neurons. GCM increases activity of the autophagic pathway, as shown by the reduction of autophagic substrate, p-62, and the augmentation of LC3 II, Beclin-1 and LAMP-2 protein levels, direct markers of autophagy, in GCM infused mice. GCM also increases BDNF levels. These results suggest that CGM should be further explored as a putative neuroprotective agent in Huntington's disease.

Published

2013

8. Natural cannabinoids improve dopamine neurotransmission and tau and amyloid pathology in a mouse model of tauopathy.

Author

Casarejos MJ, Perucho J, Gomez A, Muñoz MP, Fernandez-Estevez M, Sagredo O, Fernandez Ruiz J, Guzman M, de Yebenes JG, and Mena MA

Subjects

Amyloidosis pathology, Animals, Behavior, Animal drug effects, Behavior, Animal physiology, Biogenic Monoamines metabolism, Cannabidiol, Dronabinol, Drug Combinations, Frontotemporal Dementia pathology, Glutathione metabolism, Humans, Male, Mice, Mice, Neurologic Mutants, Mice, Transgenic, Tauopathies pathology, Amyloidosis physiopathology, Disease Models, Animal, Dopamine physiology, Frontotemporal Dementia physiopathology, Neuroprotective Agents pharmacology, Phytotherapy, Plant Extracts pharmacology, Synaptic Transmission drug effects, Synaptic Transmission physiology, Tauopathies physiopathology

Abstract

Cannabinoids are neuroprotective in models of neurodegenerative dementias. Their effects are mostly mediated through CB1 and CB2 receptor-dependent modulation of excitotoxicity, inflammation, oxidative stress, and other processes. We tested the effects of Sativex®, a mixture of Δ9-tetrahydrocannabinol and cannabidiol, acting on both CB1 and CB2 receptors, in parkin-null, human tau overexpressing (PK-/-/TauVLW) mice, a model of complex frontotemporal dementia, parkinsonism, and lower motor neuron disease. The animals received Sativex®, 4.63 mg/kg, ip, daily, for one month, at six months of age, at the onset of the clinical symptoms. We evaluated the effects of Sativex® on behavior, dopamine neurotransmission, glial activation, redox state, mitochondrial activity, and deposition of abnormal proteins. PK-/-/TauVLW mice developed the neurological deficits, but those treated with Sativex® showed less abnormal behaviors related to stress, less auto and hetero-aggression, and less stereotypy. Sativex® significantly reduced the intraneuronal, MAO-related free radicals produced during dopamine metabolism in the limbic system. Sativex® also decreased gliosis in cortex and hippocampus, increased the ratio reduced/oxidized glutathione in the limbic system, reduced the levels of iNOS, and increased those of complex IV in the cerebral cortex. With regard to tau and amyloid pathology, Sativex® reduced the deposition of both in the hippocampus and cerebral cortex of PK-/-/TauVLW mice and increased autophagy. Sativex®, even after a short administration in animals with present behavioral and pathological abnormalities, improves the phenotype, the oxidative stress, and the deposition of proteins in PK-/-/TauVLW mice, a model of complex neurodegenerative disorders.

Published

2013

9. Trehalose protects from aggravation of amyloid pathology induced by isoflurane anesthesia in APP(swe) mutant mice.

Author

Perucho J, Casarejos MJ, Gomez A, Solano RM, de Yébenes JG, and Mena MA

Subjects

Alzheimer Disease physiopathology, Anesthetics, Inhalation antagonists & inhibitors, Anesthetics, Inhalation toxicity, Animals, Disease Models, Animal, Female, Humans, Mice, Mice, Inbred C57BL, Mice, Transgenic, Neuroprotective Agents pharmacology, Plaque, Amyloid pathology, Treatment Outcome, Alzheimer Disease chemically induced, Alzheimer Disease drug therapy, Isoflurane antagonists & inhibitors, Isoflurane toxicity, Plaque, Amyloid drug therapy, Trehalose pharmacology

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

10. Parkin null cortical neuronal/glial cultures are resistant to amyloid-β1-42 toxicity: a role for autophagy?

Author

Solano RM, Casarejos MJ, Gómez A, Perucho J, de Yébenes JG, and Mena MA

Subjects

Animals, Blotting, Western, Cell Survival drug effects, Cells, Cultured, Cerebral Cortex cytology, Culture Media, Glutathione metabolism, Glutathione Peroxidase metabolism, Immunohistochemistry, Mice, Mice, Knockout, Molecular Chaperones, Proteasome Endopeptidase Complex metabolism, Ubiquitination, tau Proteins metabolism, Amyloid beta-Peptides toxicity, Autophagy physiology, Cerebral Cortex physiology, Neuroglia drug effects, Neurons drug effects, Peptide Fragments toxicity, Ubiquitin-Protein Ligases genetics

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

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

Author

Rodríguez-Navarro JA, Rodríguez L, Casarejos MJ, Solano RM, Gómez A, Perucho J, Cuervo AM, García de Yébenes J, and Mena MA

Subjects

Animals, Corpus Striatum drug effects, Corpus Striatum metabolism, Corpus Striatum pathology, Dopamine genetics, Genotype, Mesencephalon drug effects, Mesencephalon metabolism, Mesencephalon pathology, Mice, Mice, Transgenic, Neurofibrillary Tangles genetics, Neurofibrillary Tangles metabolism, Neurofibrillary Tangles pathology, Neurons metabolism, Neurons pathology, Parkinsonian Disorders genetics, Parkinsonian Disorders metabolism, Parkinsonian Disorders pathology, Polymerase Chain Reaction, Tauopathies genetics, Tauopathies metabolism, Tauopathies pathology, Trehalose pharmacology, Autophagy drug effects, Dopamine metabolism, Neurons drug effects, Parkinsonian Disorders drug therapy, Tauopathies drug therapy, Trehalose therapeutic use, Ubiquitin-Protein Ligases genetics, tau Proteins genetics

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

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

Author

Perucho J, Casarejos MJ, Rubio I, Rodriguez-Navarro JA, Gómez A, Ampuero I, Rodal I, Solano RM, Carro E, García de Yébenes J, and Mena MA

Subjects

Age Factors, Analysis of Variance, Animals, Brain metabolism, Brain pathology, Cognition Disorders genetics, Exploratory Behavior physiology, Glial Fibrillary Acidic Protein metabolism, Gliosis genetics, In Situ Nick-End Labeling methods, Interpersonal Relations, Maze Learning physiology, Mice, Mice, Inbred C57BL, Mice, Transgenic, Molecular Chaperones metabolism, Motor Activity genetics, Peptide Fragments metabolism, Rotarod Performance Test methods, Ubiquitin-Protein Ligases deficiency, tau Proteins metabolism, Amyloid beta-Peptides metabolism, Amyloid beta-Protein Precursor genetics, Apoptosis genetics, Behavior, Animal physiology, Mutation genetics, Ubiquitin-Protein Ligases metabolism

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

13. Anesthesia with isoflurane increases amyloid pathology in mice models of Alzheimer's disease.

Author

Perucho J, Rubio I, Casarejos MJ, Gomez A, Rodriguez-Navarro JA, Solano RM, De Yébenes JG, and Mena MA

Subjects

Alzheimer Disease metabolism, Amyloid beta-Peptides drug effects, Amyloid beta-Peptides metabolism, Animals, Apoptosis drug effects, Astrocytes drug effects, Behavior, Animal drug effects, Disease Models, Animal, Hippocampus drug effects, Hippocampus metabolism, Hippocampus pathology, Mice, Mice, Inbred C57BL, Nerve Degeneration pathology, Alzheimer Disease pathology, Anesthesia, General, Anesthetics, Inhalation pharmacology, Isoflurane pharmacology

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

14. Studies in animal models of the effects of anesthetics on behavior, biochemistry, and neuronal cell death.

Author

Mena MÁ, Perucho J, Rubio I, and de Yébenes JG

Subjects

Alzheimer Disease metabolism, Alzheimer Disease pathology, Alzheimer Disease psychology, Amyloid beta-Peptides metabolism, Anesthetics classification, Animals, Brain Chemistry drug effects, Cells, Cultured, Disease Models, Animal, Humans, Mutagens toxicity, Neurons drug effects, Alzheimer Disease complications, Anesthetics toxicity, Behavior, Animal drug effects, Cell Death drug effects, Neurons pathology

Abstract

Recent clinical studies have suggested that there is an increased risk of Alzheimer's disease (AD) in patients undergoing surgical interventions, but it is unknown whether this effect is related to anesthesia, cardiovascular complications of surgery, or associated conditions such as hypothermia. In addition, many patients, especially the elderly, present persistent post-operative cognitive deterioration after anesthesia, without clear complications during surgery. Experimental studies in animals may be helpful to dissect the pathogenic role of the different factors involved in surgery. Here, we review studies on the effects of anesthesia on neuronal function performed in tissue culture and in experimental animals. Several studies have shown that a small inhalation of anesthetics induces activation of caspases and cell toxicity on glioma and pheochromocitoma cells in culture, which is prevented by treatment with the metal chelating agent clioquinol. Exposure of old rodents to anesthesia produced memory deficits and increased levels of amyloid-β (Aβ) peptide and phosphorylated tau in brain. The effects of long term or short term repetitive exposure to small molecular weight anesthetics are more severe in transgenic AβPPswe than in wild type mice. In the former, low molecular weight increased the number of TUNEL(+) apoptotic cells and the ratio of pro-apoptotic proteins in hippocampus; reduced astroglial and increased microglial responses; increased Aβ aggregates and high molecular weight peptides; abnormal chaperone responses and reduced autophagy. In conclusion, anesthetic gases induce changes which may reproduce AD pathology in mice with mutations which produced AD. It would be interesting to know whether anesthetics are risky for subjects with special genetic risk factors.

Published

2010

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

Author

Casarejos MJ, Solano RM, Rodriguez-Navarro JA, Gómez A, Perucho J, Castaño JG, García de Yébenes J, and Mena MA

Subjects

Animals, Autophagy drug effects, Cell Line, Tumor, Cells, Cultured, Dose-Response Relationship, Drug, Glutathione drug effects, Homeostasis drug effects, Humans, Mesencephalon drug effects, Mesencephalon enzymology, Mesencephalon metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Neuroglia drug effects, Neuroglia enzymology, Neurons drug effects, Neurons enzymology, Oligopeptides pharmacology, Proteasome Endopeptidase Complex metabolism, Autophagy physiology, Glutathione physiology, Homeostasis physiology, Neuroglia metabolism, Neurons metabolism, Proteasome Inhibitors, Ubiquitin-Protein Ligases deficiency

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 naïve 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

16. Effects of partial suppression of parkin on huntingtin mutant R6/1 mice.

Author

Rubio I, Rodríguez-Navarro JA, Tomás-Zapico C, Ruíz C, Casarejos MJ, Perucho J, Gómez A, Rodal I, Lucas JJ, Mena MA, and de Yébenes JG

Subjects

Animals, Biogenic Monoamines metabolism, Brain metabolism, Cell Death genetics, Disease Models, Animal, Dopamine metabolism, HSP70 Heat-Shock Proteins metabolism, Humans, Huntingtin Protein, Huntington Disease physiopathology, Male, Mice, Mice, Knockout, Mice, Mutant Strains, Microtubule-Associated Proteins metabolism, Nerve Tissue Proteins genetics, Neurons drug effects, Neurons pathology, Nuclear Proteins genetics, Phenotype, Ubiquitin-Protein Ligases metabolism, Brain pathology, Exploratory Behavior, Huntington Disease genetics, Motor Activity genetics, Ubiquitin-Protein Ligases genetics

Abstract

Huntington's disease (HD) is a neurodegenerative disorder caused by an expansion of polyglutamines which makes huntingtin more resistant to degradation. Parkin is an ubiquitin ligase which promotes proteosomal degradation of abnormal proteins. We investigated whether partial suppression of parkin increases HD phenotype. We studied the behavior and brain histology and biochemistry of the mice produced by interbreeding of R6/1 (model of HD in mice) with Park-2(-/-) (parkin null mice): R6/1, WT (wild-type), PK(+/-) (hemizygotic deletion of Park-2) and R6/1/PK(+/-). R6/1 and R6/1/PK(+/-) mice had abnormal motor and exploratory behavior. R6/1/PK(+/-) mice were more akinetic. These two groups of mice had severe but similar loss of nigrostriatal dopamine neurons and monoamine levels in striatum. R6/1/PK(+/-) mice had fewer huntingtin inclusions and a greater number of TUNEL(+) cells than R6/1 in striatum but there were no differences in the hippocampus. DARPP-32 protein was equally reduced in striatum of R6/1 and R6/1/PK(+/-) mice. Striatal levels of GSH were increased, of HSP-70 reduced and of CHIP unchanged in both R6/1 and R6/1/PK(+/-) mice. LC-3 II/I ratios were significantly increased in striatum of R6/1/PK(+/-) mice. Partial suppression of parkin slightly aggravates the phenotype in R6/1 mice, confirming a pathogenic role of the UPS in the processing of mutant huntingtin. The absence of massive additional cellular lesions in R6/1/PK(+/-) mice suggests the existence of compensatory mechanisms, such as autophagy, for the processing of huntingtin.

Published

2009

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

Author

Rodríguez-Navarro JA, Gómez A, Rodal I, Perucho J, Martinez A, Furió V, Ampuero I, Casarejos MJ, Solano RM, de Yébenes JG, and Mena MA

Subjects

Alzheimer Disease etiology, Alzheimer Disease genetics, Alzheimer Disease metabolism, Alzheimer Disease pathology, Amyloid beta-Peptides metabolism, Amyloidosis, Familial etiology, Amyloidosis, Familial metabolism, Amyloidosis, Familial pathology, Animals, Astrocytes pathology, Behavior, Animal, Brain Diseases etiology, Brain Diseases metabolism, Brain Diseases pathology, Disease Models, Animal, Dopamine metabolism, Gene Deletion, HSP70 Heat-Shock Proteins metabolism, Humans, Limbic System metabolism, Liver metabolism, Liver pathology, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Microglia pathology, Neurons metabolism, Neurons pathology, Recombinant Proteins genetics, Amyloidosis, Familial genetics, Brain Diseases genetics, Mutation, Ubiquitin-Protein Ligases deficiency, Ubiquitin-Protein Ligases genetics, tau Proteins genetics

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

18. Gender differences and estrogen effects in parkin null mice.

Author

Rodríguez-Navarro JA, Solano RM, Casarejos MJ, Gomez A, Perucho J, de Yébenes JG, and Mena MA

Subjects

Animals, Apoptosis drug effects, Apoptosis physiology, Cells, Cultured, Cytoprotection drug effects, Cytoprotection physiology, Dopamine biosynthesis, Estradiol metabolism, Estradiol pharmacology, Estrogen Receptor alpha drug effects, Estrogens pharmacology, Female, Glial Fibrillary Acidic Protein drug effects, Glial Fibrillary Acidic Protein metabolism, Gliosis drug therapy, Gliosis metabolism, Gliosis physiopathology, Male, Mice, Mice, Knockout, Microglia drug effects, Microglia metabolism, Nerve Degeneration drug therapy, Nerve Degeneration genetics, Neurons drug effects, Neurons enzymology, Parkinson Disease drug therapy, Parkinson Disease genetics, Substantia Nigra drug effects, Substantia Nigra enzymology, Tyrosine 3-Monooxygenase metabolism, Estrogen Receptor alpha metabolism, Estrogens metabolism, Nerve Degeneration metabolism, Parkinson Disease metabolism, Sex Characteristics, Ubiquitin-Protein Ligases genetics

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