Early Microglial Activation Precedes Neuronal Loss in the Brain of theCstb−/−Mouse Model of Progressive Myoclonus Epilepsy, EPM1

Stefin B (cystatin B) is an inhibitor of endo-lysosomal cysteine cathepsin, and the loss-of-function mutations in the stefin B gene were reported in patients with Unverricht–Lundborg disease (EPM1), a form of progressive myoclonus epilepsy. Stefin B-deficient mice, a mouse model of the disease, display key features of EPM1, including myoclonic seizures. Although the underlying mechanism is not yet completely clear, it was reported that the impaired redox homeostasis and inflammation in the brain contribute to the progression of the disease. In the present study, we investigated if lipopolysaccharide (LPS)-triggered neuroinflammation affected the protein levels of redox-sensitive proteins: thioredoxin (Trx1), thioredoxin reductase (TrxR), peroxiredoxins (Prxs) in brain and cerebella of stefin B-deficient mice. LPS challenge was found to result in a marked elevation of Trx1 and TrxR in the brain and cerebella of stefin B deficient mice, while Prx1 was upregulated only in cerebella after LPS challenge. Mitochondrial peroxiredoxin 3 (Prx3), was upregulated also in the cerebellar tissue lysates prepared from unchallenged stefin B deficient mice, while after LPS challenge Prx3 was upregulated in stefin B deficient brain and cerebella. Our results imply the role of oxidative stress in the progression of the disease.

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Abnormal microglial activation in theCstb−/−mouse, a model for progressive myoclonus epilepsy, EPM1

Glia ◽

10.1002/glia.22760 ◽

2014 ◽

Vol 63 (3) ◽

pp. 400-411 ◽

Cited By ~ 35

Author(s):

Olesya Okuneva ◽

Inken Körber ◽

Zhilin Li ◽

Li Tian ◽

Tarja Joensuu ◽

...

Keyword(s):

Microglial Activation ◽

Progressive Myoclonus Epilepsy ◽

Myoclonus Epilepsy

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AAD-2004 Attenuates Progressive Neuronal Loss in the Brain of Tg-betaCTF99/B6 Mouse Model of Alzheimer Disease

Experimental Neurobiology ◽

10.5607/en.2013.22.1.31 ◽

2013 ◽

Vol 22 (1) ◽

pp. 31-37 ◽

Cited By ~ 7

Author(s):

In-Sun Baek ◽

Tae-Kyung Kim ◽

Ji-Seon Seo ◽

Kang-Woo Lee ◽

Young Ae Lee ◽

...

Keyword(s):

Alzheimer Disease ◽

Mouse Model ◽

Neuronal Loss ◽

The Brain

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Impaired osteoclast homeostasis in the cystatin B-deficient mouse model of progressive myoclonus epilepsy

Bone Reports ◽

10.1016/j.bonr.2015.10.002 ◽

2015 ◽

Vol 3 ◽

pp. 76-82 ◽

Cited By ~ 3

Author(s):

Otto Manninen ◽

Tero Puolakkainen ◽

Jemina Lehto ◽

Elina Harittu ◽

Aki Kallonen ◽

...

Keyword(s):

Mouse Model ◽

Deficient Mouse ◽

Cystatin B ◽

Progressive Myoclonus Epilepsy ◽

Myoclonus Epilepsy

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Altered Tryptophan Metabolism in the Brain of Cystatin B-Deficient Mice: A Model System for Progressive Myoclonus Epilepsy

Epilepsia ◽

10.1111/j.1528-1167.2006.00638.x ◽

2006 ◽

Vol 47 (10) ◽

pp. 1650-1654 ◽

Cited By ~ 9

Author(s):

Annika Vaarmann ◽

Allen Kaasik ◽

Alexander Zharkovsky

Keyword(s):

Model System ◽

Tryptophan Metabolism ◽

Cystatin B ◽

Progressive Myoclonus Epilepsy ◽

Myoclonus Epilepsy ◽

The Brain ◽

Deficient Mice

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Cystatin C Rescues Degenerating Neurons in a Cystatin B-Knockout Mouse Model of Progressive Myoclonus Epilepsy

American Journal Of Pathology ◽

10.2353/ajpath.2010.100461 ◽

2010 ◽

Vol 177 (5) ◽

pp. 2256-2267 ◽

Cited By ~ 30

Author(s):

Gurjinder Kaur ◽

Panaiyur Mohan ◽

Monika Pawlik ◽

Steven DeRosa ◽

Jay Fajiculay ◽

...

Keyword(s):

Mouse Model ◽

Cystatin C ◽

Knockout Mouse ◽

Knockout Mouse Model ◽

Cystatin B ◽

Progressive Myoclonus Epilepsy ◽

Myoclonus Epilepsy

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Targeting α-synuclein by PD03 AFFITOPE® and Anle138b rescues neurodegenerative pathology in a model of multiple system atrophy: clinical relevance

Translational Neurodegeneration ◽

10.1186/s40035-020-00217-y ◽

2020 ◽

Vol 9 (1) ◽

Author(s):

Miguel Lemos ◽

Serena Venezia ◽

Violetta Refolo ◽

Antonio Heras-Garvin ◽

Sabine Schmidhuber ◽

...

Keyword(s):

Multiple System Atrophy ◽

Dopaminergic Neurons ◽

Microglial Activation ◽

Combined Therapy ◽

Neuronal Loss ◽

Substantia Nigra Pars Compacta ◽

Vehicle Group ◽

Treatment Groups ◽

Igg Binding ◽

The Brain

Abstract Background Misfolded oligomeric α-synuclein plays a pivotal role in the pathogenesis of α-synucleinopathies including Parkinson’s disease and multiple system atrophy, and its detection parallels activation of microglia and a loss of neurons in the substantia nigra pars compacta. Here we aimed to analyze the therapeutic efficacy of PD03, a new AFFITOPE® immunotherapy approach, either alone or in combination with Anle138b, in a PLP-α-syn mouse model. Methods The PLP-α-syn mice were treated with PD03 immunotherapy, Anle138b, or a combination of two. Five months after study initiation, the mice underwent behavioral testing and were sacrificed for neuropathological analysis. The treatment groups were compared to the vehicle group with regard to motor performance, nigral neuronal loss, microglial activation and α-synuclein pathology. Results The PLP-α-syn mice receiving the PD03 or Anle138b single therapy showed improvement of gait deficits and preservation of nigral dopaminergic neurons associated with the reduced α-synuclein oligomer levels and decreased microglial activation. The combined therapy with Anle138b and PD03 resulted in lower IgG binding in the brain as compared to the single immunotherapy with PD03. Conclusions PD03 and Anle138b can selectively target oligomeric α-synuclein, resulting in attenuation of neurodegeneration in the PLP-α-syn mice. Both approaches are potential therapies that should be developed further for disease modification in α-synucleinopathies.

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Inhibition of microglia overactivation restores neuronal survival in a mouse model of CDKL5 deficiency disorder

Journal of Neuroinflammation ◽

10.1186/s12974-021-02204-0 ◽

2021 ◽

Vol 18 (1) ◽

Author(s):

Giuseppe Galvani ◽

Nicola Mottolese ◽

Laura Gennaccaro ◽

Manuela Loi ◽

Giorgio Medici ◽

...

Keyword(s):

Mouse Model ◽

Hippocampal Neurons ◽

Microglial Activation ◽

Neuronal Survival ◽

Day Treatment ◽

Neurodevelopmental Disorder ◽

Stat3 Signaling ◽

Inflammatory Status ◽

The Brain ◽

Increased Susceptibility

Abstract Background CDKL5 deficiency disorder (CDD), a severe neurodevelopmental disorder characterized by early onset epilepsy, intellectual disability, and autistic features, is caused by mutations in the CDKL5 gene. Evidence in animal models of CDD showed that absence of CDKL5 negatively affects neuronal survival, as well as neuronal maturation and dendritic outgrowth; however, knowledge of the substrates underlying these alterations is still limited. Neuroinflammatory processes are known to contribute to neuronal dysfunction and death. Recent evidence shows a subclinical chronic inflammatory status in plasma from CDD patients. However, to date, it is unknown whether a similar inflammatory status is present in the brain of CDD patients and, if so, whether this plays a causative or exacerbating role in the pathophysiology of CDD. Methods We evaluated microglia activation using AIF-1 immunofluorescence, proinflammatory cytokine expression, and signaling in the brain of a mouse model of CDD, the Cdkl5 KO mouse, which is characterized by an impaired survival of hippocampal neurons that worsens with age. Hippocampal neuron survival was determined by DCX, NeuN, and cleaved caspase-3 immunostaining in Cdkl5 KO mice treated with luteolin (10 mg/kg), a natural anti-inflammatory flavonoid. Since hippocampal neurons of Cdkl5 KO mice exhibit increased susceptibility to excitotoxic stress, we evaluated neuronal survival in Cdkl5 KO mice injected with NMDA (60 mg/kg) after a 7-day treatment with luteolin. Results We found increased microglial activation in the brain of the Cdkl5 KO mouse. We found alterations in microglial cell morphology and number, increased levels of AIF-1 and proinflammatory cytokines, and activation of STAT3 signaling. Remarkably, treatment with luteolin recovers microglia alterations as well as neuronal survival and maturation in Cdkl5 KO mice, and prevents the increase in NMDA-induced cell death in the hippocampus. Conclusions Our results suggest that neuroinflammatory processes contribute to the pathogenesis of CDD and imply the potential usefulness of luteolin as a treatment option in CDD patients.

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Divergent metabolic substrate utilization in brain during epileptogenesis precedes chronic hypometabolism

Journal of Cerebral Blood Flow & Metabolism ◽

10.1177/0271678x18809886 ◽

2018 ◽

Vol 40 (1) ◽

pp. 204-213 ◽

Cited By ~ 5

Author(s):

Pablo Bascuñana ◽

Mirjam Brackhan ◽

Ina Leiter ◽

Heike Keller ◽

Ina Jahreis ◽

...

Keyword(s):

Amino Acid ◽

Microglial Activation ◽

Neuronal Loss ◽

Volume Of Distribution ◽

Substrate Utilization ◽

Translocator Protein ◽

Positron Emission ◽

Amino Acid Turnover ◽

Therapy Target ◽

The Brain

Alterations in metabolism during epileptogenesis may be a therapy target. Recently, an increase in amino acid transport into the brain was proposed to play a role in epileptogenesis. We aimed to characterize alterations of substrate utilization during epileptogenesis and in chronic epilepsy. The lithium-pilocarpine post status epilepticus (SE) rat model was used. We performed longitudinal O-(2-[(18)F]fluoroethyl)-l-tyrosine (18F-FET) and 18F-fluorodeoxyglucose (18F-FDG) positron emission tomography (PET) and calculated 18F-FET volume of distribution (Vt) and 18F-FDG uptake. Correlation analyses were performed with translocator protein-PET defined neuroinflammation from previously acquired data. We found reduced 18F-FET Vt at 48 h after SE (amygdala: −30.2%, p = 0.014), whereas 18F-FDG showed increased glucose uptake 4 and 24 h after SE (hippocampus: + 43.6% and +42.5%, respectively; p < 0.001) returning to baseline levels thereafter. In chronic epileptic animals, we found a reduction in 18F-FET and 18F-FDG in the hippocampus. No correlation was found for 18F-FET or 18F-FDG to microglial activation at seven days post SE. Whereas metabolic alterations do not reflect higher metabolism associated to activated microglia, they might be partially driven by chronic neuronal loss. However, both metabolisms diverge during early epileptogenesis, pointing to amino acid turnover as a possible biomarker and/or therapeutic target for epileptogenesis.

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