Your search keyword '"Mar, Puigdellívol"' showing total 10 results

1. Inflammatory neuronal loss in the substantia nigra induced by systemic lipopolysaccharide is prevented by knockout of the P2Y6 receptor in mice

Author

Stefan Milde, Francesca W. van Tartwijk, Anna Vilalta, Tamara C. Hornik, Jacob M. Dundee, Mar Puigdellívol, and Guy C. Brown

Subjects

Microglia, Phagocytosis, Neuroinflammation, Cell death, Parkinson’s disease, Neurodegeneration, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Inflammation may contribute to multiple brain pathologies. One cause of inflammation is lipopolysaccharide/endotoxin (LPS), the levels of which are elevated in blood and/or brain during bacterial infections, gut dysfunction and neurodegenerative diseases, such as Parkinson’s disease. How inflammation causes neuronal loss is unclear, but one potential mechanism is microglial phagocytosis of neurons, which is dependent on the microglial P2Y6 receptor. We investigated here whether the P2Y6 receptor was required for inflammatory neuronal loss. Intraperitoneal injection of LPS on 4 successive days resulted in specific loss of dopaminergic neurons (measured as cells staining with tyrosine hydroxylase or NeuN) in the substantia nigra of wild-type mice, but no neuronal loss in cortex or hippocampus. This supports the hypothesis that neuronal loss in Parkinson’s disease may be driven by peripheral LPS. By contrast, there was no LPS-induced neuronal loss in P2Y6 receptor knockout mice. In vitro, LPS-induced microglial phagocytosis of cells was prevented by inhibition of the P2Y6 receptor, and LPS-induced neuronal loss was reduced in mixed glial–neuronal cultures from P2Y6 receptor knockout mice. This supports the hypothesis that microglial phagocytosis contributes to inflammatory neuronal loss, and can be prevented by blocking the P2Y6 receptor, suggesting that P2Y6 receptor antagonists might be used to prevent inflammatory neuronal loss in Parkinson’s disease and other brain pathologies involving inflammatory neuronal loss.

Published

2021

2. Sialylation and Galectin-3 in Microglia-Mediated Neuroinflammation and Neurodegeneration

Author

Mar Puigdellívol, David H. Allendorf, and Guy C. Brown

Subjects

sialic acid, desialylation, galectin-3, phagocytosis, microglia, neurodegeneration, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Microglia are brain macrophages that mediate neuroinflammation and contribute to and protect against neurodegeneration. The terminal sugar residue of all glycoproteins and glycolipids on the surface of mammalian cells is normally sialic acid, and addition of this negatively charged residue is known as “sialylation,” whereas removal by sialidases is known as “desialylation.” High sialylation of the neuronal cell surface inhibits microglial phagocytosis of such neurons, via: (i) activating sialic acid receptors (Siglecs) on microglia that inhibit phagocytosis and (ii) inhibiting binding of opsonins C1q, C3, and galectin-3. Microglial sialylation inhibits inflammatory activation of microglia via: (i) activating Siglec receptors CD22 and CD33 on microglia that inhibit phagocytosis and (ii) inhibiting Toll-like receptor 4 (TLR4), complement receptor 3 (CR3), and other microglial receptors. When activated, microglia release a sialidase activity that desialylates both microglia and neurons, activating the microglia and rendering the neurons susceptible to phagocytosis. Activated microglia also release galectin-3 (Gal-3), which: (i) further activates microglia via binding to TLR4 and TREM2, (ii) binds to desialylated neurons opsonizing them for phagocytosis via Mer tyrosine kinase, and (iii) promotes Aβ aggregation and toxicity in vivo. Gal-3 and desialylation may increase in a variety of brain pathologies. Thus, Gal-3 and sialidases are potential treatment targets to prevent neuroinflammation and neurodegeneration.

Published

2020

3. Modulation of dopamine D1 receptors via histamine H3 receptors is a novel therapeutic target for Huntington's disease

Author

David Moreno-Delgado, Mar Puigdellívol, Estefanía Moreno, Mar Rodríguez-Ruiz, Joaquín Botta, Paola Gasperini, Anna Chiarlone, Lesley A Howell, Marco Scarselli, Vicent Casadó, Antoni Cortés, Sergi Ferré, Manuel Guzmán, Carmen Lluís, Jordi Alberch, Enric I Canela, Silvia Ginés, and Peter J McCormick

Subjects

huntington's disease, dopamine, histamine, g-protein coupled receptors, Medicine, Science, Biology (General), QH301-705.5

Abstract

Early Huntington’s disease (HD) include over-activation of dopamine D1 receptors (D1R), producing an imbalance in dopaminergic neurotransmission and cell death. To reduce D1R over-activation, we present a strategy based on targeting complexes of D1R and histamine H3 receptors (H3R). Using an HD mouse striatal cell model and HD mouse organotypic brain slices we found that D1R-induced cell death signaling and neuronal degeneration, are mitigated by an H3R antagonist. We demonstrate that the D1R-H3R heteromer is expressed in HD mice at early but not late stages of HD, correlating with HD progression. In accordance, we found this target expressed in human control subjects and low-grade HD patients. Finally, treatment of HD mice with an H3R antagonist prevented cognitive and motor learning deficits and the loss of heteromer expression. Taken together, our results indicate that D1R - H3R heteromers play a pivotal role in dopamine signaling and represent novel targets for treating HD.

Published

2020

4. Calreticulin and Galectin-3 Opsonise Bacteria for Phagocytosis by Microglia

Author

Tom O. J. Cockram, Mar Puigdellívol, and Guy C. Brown

Subjects

calreticulin, galectin-3, opsonin, MerTK, LRP1, microglia, Immunologic diseases. Allergy, RC581-607

Abstract

Opsonins are soluble, extracellular proteins, released by activated immune cells, and when bound to a target cell, can induce phagocytes to phagocytose the target cell. There are three known classes of opsonin: antibodies, complement factors and secreted pattern recognition receptors, but these have limited access to the brain. We identify here two novel opsonins of bacteria, calreticulin, and galectin-3 (both lectins that can bind lipopolysaccharide), which were released by microglia (brain-resident macrophages) when activated by bacterial lipopolysaccharide. Calreticulin and galectin-3 both bound to Escherichia coli, and when bound increased phagocytosis of these bacteria by microglia. Furthermore, lipopolysaccharide-induced microglial phagocytosis of E. coli bacteria was partially inhibited by: sugars, an anti-calreticulin antibody, a blocker of the calreticulin phagocytic receptor LRP1, a blocker of the galectin-3 phagocytic receptor MerTK, or simply removing factors released from the microglia, indicating this phagocytosis is dependent on extracellular calreticulin and galectin-3. Thus, calreticulin and galectin-3 are opsonins, released by activated microglia to promote clearance of bacteria. This innate immune response of microglia may help clear bacterial infections of the brain.

Published

2019

5. Effective Knockdown of Gene Expression in Primary Microglia With siRNA and Magnetic Nanoparticles Without Cell Death or Inflammation

Author

Alejandro Carrillo-Jimenez, Mar Puigdellívol, Anna Vilalta, Jose Luis Venero, Guy Charles Brown, Peter StGeorge-Hyslop, and Miguel Angel Burguillos

Subjects

microglia, siRNA, transfection, TREM2, CD33, CGC, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Microglia, the resident immune cells of the brain, have multiple functions in physiological and pathological conditions, including Alzheimer’s disease (AD). The use of primary microglial cell cultures has proved to be a valuable tool to study microglial biology under various conditions. However, more advanced transfection methodologies for primary cultured microglia are still needed, as current methodologies provide low transfection efficiency and induce cell death and/or inflammatory activation of the microglia. Here, we describe an easy, and effective method based on the Glial-Mag method (OZ Biosciences) using magnetic nanoparticles and a magnet to successfully transfect primary microglia cells with different small interfering RNAs (siRNAs). This method does not require specialist facilities or specific training and does not induce cell toxicity or inflammatory activation. We demonstrate that this protocol successfully decreases the expression of two key genes associated with AD, the triggering receptor expressed in myeloid cells 2 (TREM2) and CD33, in primary microglia cell cultures.

Published

2018

6. The microglial P2Y6 receptor mediates neuronal loss and memory deficits in neurodegeneration

Author

Mar Puigdellívol, Stefan Milde, Anna Vilalta, Tom O.J. Cockram, David H. Allendorf, Jeffrey Y. Lee, Jacob M. Dundee, Katryna Pampuščenko, Vilmante Borutaite, Hugh N. Nuthall, Jack H. Brelstaff, Maria Grazia Spillantini, and Guy C. Brown

Subjects

Male, Mice, Knockout, Memory Disorders, Amyloid beta-Peptides, Receptors, Purinergic P2, neurodegeneration, memory deficits, microglia, phagocytosis, Neurodegenerative Diseases, tau Proteins, P2Y6 receptor, General Biochemistry, Genetics and Molecular Biology, Mice, Inbred C57BL, Mice, cell death, nervous system, Report, Animals, Female, Alzheimer’s disease

Abstract

Summary Microglia are implicated in neurodegeneration, potentially by phagocytosing neurons, but it is unclear how to block the detrimental effects of microglia while preserving their beneficial roles. The microglial P2Y6 receptor (P2Y6R) – activated by extracellular UDP released by stressed neurons – is required for microglial phagocytosis of neurons. We show here that injection of amyloid beta (Aβ) into mouse brain induces microglial phagocytosis of neurons, followed by neuronal and memory loss, and this is all prevented by knockout of P2Y6R. In a chronic tau model of neurodegeneration (P301S TAU mice), P2Y6R knockout prevented TAU-induced neuronal and memory loss. In vitro, P2Y6R knockout blocked microglial phagocytosis of live but not dead targets and reduced tau-, Aβ-, and UDP-induced neuronal loss in glial-neuronal cultures. Thus, the P2Y6 receptor appears to mediate Aβ- and tau-induced neuronal and memory loss via microglial phagocytosis of neurons, suggesting that blocking this receptor may be beneficial in the treatment of neurodegenerative diseases., Graphical abstract, Highlights • P2Y6R knockout prevents microglial phagocytosis of stressed-but-viable cells • P2Y6R knockout does not alter microglial phagocytosis of healthy or dead cells • P2Y6R knockout prevents microglial phagocytosis of neurons induced by Aβ in vivo • P2Y6R knockout reduces neuronal loss and memory deficits induced by Aβ or Tau in mice, Puigdellívol et al. find that the knockout of the microglial P2Y6 receptor, required for microglial engulfment of neurons, prevents neuronal and memory loss in two different mouse models of neurodegeneration, suggesting that neuronal loss in neurodegeneration is due to microglia eating neurons, which may be prevented by blocking the P2Y6 receptor.

Published

2021

7. Modulation of dopamine D1 receptors via histamine H3 receptors is a novel therapeutic target for Huntington’s disease

Author

Peter J. McCormick, Manuel Guzmán, Marco Scarselli, Anna Chiarlone, Carmen Lluis, Sergi Ferré, Antoni Cortés, Enric I. Canela, Joaquin Botta, David Moreno, Paola Gasperini, Silvia Ginés, Lesley A. Howell, Vicent Casadó, Jordi Alberch, Mar Puigdellívol, Mar Rodríguez-Ruiz, and Estefanía Moreno

Subjects

Bioquímica, Programmed cell death, huntington's disease, QH301-705.5, Dopamine, Science, Neurociencias, Heteromer, Dopamina, Huntington's chorea, General Biochemistry, Genetics and Molecular Biology, neuroscience, chemistry.chemical_compound, Huntington's disease, Corea de Huntington, medicine, Biology (General), Receptor, mouse, G protein-coupled receptor, General Immunology and Microbiology, business.industry, General Neuroscience, Antagonist, General Medicine, medicine.disease, histamine, dopamine, g-protein coupled receptors, chemistry, Histamina, Medicine, Histamine H3 receptor, Motor learning, business, Neuroscience, Histamine, medicine.drug

Abstract

Early Huntington’s disease (HD) include over-activation of dopamine D1 receptors (D1R), producing an imbalance in dopaminergic neurotransmission and cell death. To reduce D1R over-activation, we present a strategy based on targeting complexes of D1R and histamine H3 receptors (H3R). Using an HD striatal cell model and HD organotypic brain slices we found that D1R-induced cell death signaling and neuronal degeneration, are mitigated by an H3R antagonist. We demonstrate that the D1R-H3R heteromer is expressed in HD animal models at early but not late stages of HD, correlating with HD progression. In accordance, we found this target expressed in human control subjects and low-grade HD patients. Finally, treatment of HD mice with an H3R antagonist prevented cognitive and motor learning deficits, as well as the loss of heteromer expression. Taken together, our results indicate that D1R - H3R heteromers play a pivotal role in dopamine signaling and represent novel targets for treating HD.Impact StatementProgression of Huntington’s disease can be slowed by altering dopamine signalling through the Dopamine 1 receptor - Histamine 3 receptor heteromer.

Published

2020

8. BDNF Induces Striatal-Enriched Protein Tyrosine Phosphatase 61 Degradation Through the Proteasome

Author

Shiraz Tyebji, Esther Pérez-Navarro, Pradeep Kurup, Mar Puigdellívol, Jordi Alberch, Silvia Ginés, Paul J. Lombroso, Jian Xu, and Ana Saavedra

Subjects

0301 basic medicine, medicine.medical_specialty, Proteasome Endopeptidase Complex, Phosphatase, Neuroscience (miscellaneous), Neurones, Neurotrophin-3, Protein tyrosine phosphatase, Hippocampus, Receptors, N-Methyl-D-Aspartate, Article, Membrane Potentials, Proteïna-tirosina-fosfatasa, 03 medical and health sciences, Cellular and Molecular Neuroscience, Mice, 0302 clinical medicine, Neurotrophin 3, Neurotrophic factors, Internal medicine, Nerve Growth Factor, medicine, Animals, Phosphorylation, Extracellular Signal-Regulated MAP Kinases, Protein-tyrosine phosphatase, Brain-derived neurotrophic factor, Cerebral Cortex, Neurons, biology, Phospholipase C gamma, Brain-Derived Neurotrophic Factor, Ubiquitination, Proteins, Protein Tyrosine Phosphatases, Non-Receptor, Neostriatum, 030104 developmental biology, Endocrinology, Nerve growth factor, Neurology, nervous system, Sinapsi, Synapses, Proteolysis, biology.protein, Proteïnes, Tyrosine kinase, 030217 neurology & neurosurgery

Abstract

Brain-derived neurotrophic factor (BDNF) promotes synaptic strengthening through the regulation of kinase and phosphatase activity. Conversely, striatal-enriched protein tyrosine phosphatase (STEP) opposes synaptic strengthening through inactivation or internalization of signaling molecules. Here, we investigated whether BDNF regulates STEP levels/activity. BDNF induced a reduction of STEP61 levels in primary cortical neurons, an effect that was prevented by inhibition of tyrosine kinases, phospholipase C gamma, or the ubiquitin-proteasome system (UPS). The levels of pGluN2B(Tyr1472) and pERK1/2(Thr202/Tyr204), two STEP substrates, increased in BDNF-treated cultures, and blockade of the UPS prevented STEP61 degradation and reduced BDNF-induced GluN2B and ERK1/2 phosphorylation. Moreover, brief or sustained cell depolarization reduced STEP61 levels in cortical neurons by different mechanisms. BDNF also promoted UPS-mediated STEP61 degradation in cultured striatal and hippocampal neurons. In contrast, nerve growth factor and neurotrophin-3 had no effect on STEP61 levels. Our results thus indicate that STEP61 degradation is an important event in BDNF-mediated effects.

Published

2015

9. Imbalance of p75(NTR)/TrkB protein expression in Huntington's disease: implication for neuroprotective therapies

Author

Verónica Brito, Daniel del Toro, Mar Puigdellívol, Jordi Alberch, Albert Giralt, and Silvia Ginés

Subjects

Cancer Research, Huntingtin, Excitotoxicity, Apoptosis, Tropomyosin receptor kinase B, medicine.disease_cause, Receptor, Nerve Growth Factor, Mice, Genètica mèdica, Protein Phosphatase 1, Low-affinity nerve growth factor receptor, Gene Knock-In Techniques, Enzyme Inhibitors, Phosphorylation, RNA, Small Interfering, Huntingtin Protein, biology, Neurodegeneration, Medical genetics, Putamen, neurodegeneration, Nuclear Proteins, Huntington Disease, embryonic structures, RNA Interference, Original Article, neuroprotection, excitotoxicity, Neurotrophin, Protein Binding, Signal Transduction, N-Methylaspartate, huntingtin, Immunology, Nerve Tissue Proteins, Huntington's chorea, Neuroprotection, Cell Line, Cellular and Molecular Neuroscience, Corea de Huntington, Okadaic Acid, medicine, Animals, Humans, Receptor, trkB, BDNF receptors, Brain-Derived Neurotrophic Factor, JNK Mitogen-Activated Protein Kinases, Cell Biology, medicine.disease, Corpus Striatum, Disease Models, Animal, nervous system, biology.protein, Cancer research, sense organs, Proto-Oncogene Proteins c-akt

Abstract

Neuroprotective therapies based on brain-derived neurotrophic factor (BDNF) administration have been proposed for Huntington's disease (HD) treatment. However, our group has recently reported reduced levels of TrkB in HD mouse models and HD human brain suggesting that besides a decrease on BDNF levels a reduction of TrkB expression could also contribute to diminished neurotrophic support in HD. BDNF can also bind to p75 neurotrophin receptor (p75(NTR)) modulating TrkB signaling. Therefore, in this study we have analyzed the levels of p75(NTR) in several HD models, as well as in HD human brain. Our data demonstrates a p75(NTR)/TrkB imbalance in the striatum of two different HD mouse models, Hdh(Q111/111) homozygous knockin mice and R6/1 mice that was also manifested in the putamen of HD patients. The imbalance between TrkB and p75(NTR) levels in a HD cellular model did not affect BDNF-mediated TrkB activation of prosurvival pathways but induced activation of apoptotic cascades as demonstrated by increased JNK phosphorylation. Moreover, BDNF failed to protect mutant huntingtin striatal cells transfected with p75(NTR) against NMDA-mediated excitotoxicity, which was associated with decreased Akt phosphorylation. Interestingly, lack of Akt activation following BDNF and NMDA treatment correlated with increased PP1 levels. Accordingly, pharmacological inhibition of PP1 by okadaic acid (OA) prevented mutant huntingtin striatal cell death induced by NMDA and BDNF. Altogether, our findings demonstrate that the p75(NTR)/TrkB imbalance induced by mutant huntingtin in striatal cells associated with the aberrant activity of PP1 disturbs BDNF neuroprotection likely contributing to increasing striatal vulnerability in HD. On the basis of this data we hypothesize that normalization of p75(NTR) and/or TrkB expression or their signaling will improve BDNF neuroprotective therapies in HD. Cell Death and Disease (2013) 4, e595; doi:10.1038/cddis.2013.116; published online 18 April 2013

Published

2013

10. Microglial phagocytosis of neurons in neurodegeneration, and its regulation

Author

Mar Puigdellívol, Guy C. Brown, Alma S. Popescu, Claire Ann Butler, Emily J. A. Kitchener, David H. Allendorf, Butler, Claire A [0000-0001-9320-8297], Popescu, Alma S [0000-0001-9459-6754], Allendorf, David H [0000-0003-0161-7056], Puigdellívol, Mar [0000-0002-9955-3558], Brown, Guy C [0000-0002-3610-1730], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Apolipoprotein E, Retinal degeneration, Phagocytosis, Parkinson's disease, Biology, Biochemistry, neuroinflammation, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, medicine, Animals, Humans, Receptor, Neuroinflammation, Neurons, Microglia, Neurodegeneration, neurodegeneration, SIGLEC, Brain, Neurodegenerative Diseases, Alzheimer's disease, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, ageing, Neuroscience, 030217 neurology & neurosurgery, Signal Transduction

Abstract

There is growing evidence that excessive microglial phagocytosis of neurons and synapses contributes to multiple brain pathologies. RNA-seq and genome-wide association (GWAS) studies have linked multiple phagocytic genes to neurodegenerative diseases, and knock-out of phagocytic genes has been found to protect against neurodegeneration in animal models, suggesting that excessive microglial phagocytosis contributes to neurodegeneration. Here, we review recent evidence that microglial phagocytosis of live neurons and synapses causes neurodegeneration in animal models of Alzheimer's disease and other tauopathies, Parkinson's disease, frontotemporal dementias, multiple sclerosis, retinal degeneration and neurodegeneration induced by ischaemia, infection or ageing. We also review factors regulating microglial phagocytosis of neurons, including: nucleotides, frackalkine, phosphatidylserine, calreticulin, UDP, CD47, sialylation, complement, galectin-3, Apolipoprotein E, phagocytic receptors, Siglec receptors, cytokines, microglial epigenetics and expression profile. Some of these factors may be potential treatment targets to prevent neurodegeneration mediated by excessive microglial phagocytosis of live neurons and synapses.