Genetic Background Influences the Propagation of Tau Pathology in Transgenic Rodent Models of Tauopathy

Smolek, Tomáš; Cubinkova, Veronika; Brezováková, Veronika; Valachova, Bernadeta; Szalay, Peter; Žilka, Norbert; Jadhav, Santosh

doi:10.3389/fnagi.2019.00343

Cited by 10 publications

(12 citation statements)

References 38 publications

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“…A large number of pieces of evidence support a prion-like model for tau spreading, consisting of abnormal proteins with the capacity to convert normal proteins into a pathological form. The inoculation of brain extracts from mice or humans with tauopathy into the brain of wild-type animals induced tau pathology in recipient animals and its propagation from the site of injection along neuronal connections (Clavaguera et al, 2009 , 2013 ; Lasagna-Reeves et al, 2012 ; Ahmed et al, 2014 ; Guo et al, 2016 ; Gibbons et al, 2017 ; Narasimhan et al, 2017 ; Smolek et al, 2019a , b ). Similar results were obtained when synthetic tau fibrils were injected into young mice overexpressing mutant human tau (P301S) which resulted as well in the formation of NFT-like inclusions that propagated from the injected sites to connected brain regions in a time-dependent manner (Iba et al, 2013 ).…”

Section: The Spread Of Taumentioning

confidence: 99%

Mechanisms of Pathogenic Tau and Aβ Protein Spreading in Alzheimer’s Disease

d’Errico

Meyer‐Luehmann

2020

Front. Aging Neurosci.

115

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Alzheimer's disease (AD) is pathologically defined by extracellular accumulation of amyloid-β (Aβ) peptides generated by the cleavage of amyloid precursor protein (APP), strings of hyperphosphorylated Tau proteins accumulating inside neurons known as neurofibrillary tangles (NFTs) and neuronal loss. The association between the two hallmarks and cognitive decline has been known since the beginning of the 20th century when the first description of the disease was carried out by Alois Alzheimer. Today, more than 40 million people worldwide are affected by AD that represents the most common cause of dementia and there is still no effective treatment available to cure the disease. In general, the aggregation of Aβ is considered an essential trigger in AD pathogenesis that gives rise to NFTs, neuronal dysfunction and dementia. During the process leading to AD, tau and Aβ first misfold and form aggregates in one brain region, from where they spread to interconnected areas of the brain thereby inducing its gradual morphological and functional deterioration. In this mini-review article, we present an overview of the current literature on the spreading mechanisms of Aβ and tau pathology in AD since a more profound understanding is necessary to design therapeutic approaches aimed at preventing or halting disease progression.

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Section: The Spread Of Taumentioning

confidence: 99%

Mechanisms of Pathogenic Tau and Aβ Protein Spreading in Alzheimer’s Disease

d’Errico

Meyer‐Luehmann

2020

Front. Aging Neurosci.

115

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“…Nevertheless, the increasing use of patient-derived brain lysates and the recent emergence of humanized tauopathy mouse models may be decisive in the search for a treatment capable of slowing disease progression or reversing its detrimental effects. Additionally, patient-derived tau seeding in rat models could also be further explored, as their larger brain size may make them better research models for characterizing tau PET tracers compared to mice [ 178 , 179 ]. Of note, robust cognitive deficits have thus far not been reported in seeding models.…”

Section: Discussionmentioning

confidence: 99%

Tau Seeding Mouse Models with Patient Brain-Derived Aggregates

Robert

Schöll

Vogels

2021

IJMS

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Tauopathies are a heterogeneous class of neurodegenerative diseases characterized by intracellular inclusions of aggregated tau proteins. Tau aggregates in different tauopathies have distinct structural features and can be found in different cell types. Transgenic animal models overexpressing human tau have been used for over two decades in the research of tau pathology. However, these models poorly recapitulate the heterogeneity of tauopathies found in human brains. Recent findings demonstrate that injection of purified tau aggregates from the brains of human tauopathy patients recapitulates both the structural features and cell-type specificity of the tau pathology of the donor tauopathy. These models may therefore have unique translational value in the study of functional consequences of tau pathology, tau-based diagnostics, and tau targeting therapeutics. This review provides an update of the literature relating to seeding-based tauopathy and their potential applications.

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“…It has been shown that these abnormalities and aggregation of tau proteins are along with impairment in autophagy process (Ando et al, 2020). A newly published article has demonstrated that genetic background is a candidate involved in spread of tauopathy (Smolek et al, 2019). The aggregations of tau proteins are found in temporal, ventral, lateral, and primary cortical areas of brain.…”

Section: Tau Protein and Pathological Eventsmentioning

confidence: 99%

Resveratrol targeting tau proteins, amyloid‐beta aggregations, and their adverse effects: An updated review

Ashrafizadeh

Zarrabi

Najafi

et al. 2020

Phytotherapy Research

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Resveratrol (Res) is a non-flavonoid compound with pharmacological actions such as antioxidant, antiinflammatory, hepatoprotective, antidiabetes, and antitumor. This plant-derived chemical has a long history usage in treatment of diseases. The excellent therapeutic impacts of Res and its capability in penetration into blood-brain barrier have made it an appropriate candidate in the treatment of neurological disorders (NDs). Tau protein aggregations and amyloid-beta (Aβ) deposits are responsible for the induction of NDs. A variety of studies have elucidated the role of these aggregations in NDs and the underlying molecular pathways in their development. In the present review, based on the recently published articles, we describe that how Res administration could inhibit amyloidogenic pathway and stimulate processes such as autophagy to degrade Aβ aggregations. Besides, we demonstrate that Res supplementation is beneficial in dephosphorylation of tau proteins and suppressing their aggregations. Then, we discuss molecular pathways and relate them to the treatment of NDs.

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Genetic Background Influences the Propagation of Tau Pathology in Transgenic Rodent Models of Tauopathy

Cited by 10 publications

References 38 publications

Mechanisms of Pathogenic Tau and Aβ Protein Spreading in Alzheimer’s Disease

Mechanisms of Pathogenic Tau and Aβ Protein Spreading in Alzheimer’s Disease

Tau Seeding Mouse Models with Patient Brain-Derived Aggregates

Resveratrol targeting tau proteins, amyloid‐beta aggregations, and their adverse effects: An updated review

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