Apoptosis in Transgenic Mice Expressing the P301L Mutated Form of Human Tau

Ramalho, Rita M.; Viana, Ricardo J.S.; Castro, Rui E.; Steer, Clifford J.; Low, Walter C.; Rodrigues, Cecília M. P.

doi:10.2119/2007-00133.ramalho

Cited by 29 publications

(15 citation statements)

References 38 publications

(52 reference statements)

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“…It has been suggested that activation of caspase-3 in the frontal cortex and hippocampus resulted in cleavage of tau in rTg4510 mice at 2.5 months (22), but the present study showed that amount of caspase-cleaved tau is very sparse in 2.5-month-old rTg4510 mouse neurons. Although Riesman et al demonstrated caspase-cleaved tau in early, tangle-like structures within neuronal somata and a myelinated axon in AD brain using IEM (5), TauC3 immunogold labeling was not observed in a 4-month-old rTg4510 mouse brain that had similar early tangle structures positive with MC1 and CP13 antibodies.…”

Section: Discussioncontrasting

confidence: 88%

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Immunoelectron Microscopic and Biochemical Studies of Caspase-Cleaved Tau in a Mouse Model of Tauopathy

Lin¹,

Dickson²,

Sahara³

2011

J Neuropathol Exp Neurol

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Neurofibrillary tangles (NFTs) have been implicated in mediating neuronal death and disease progression in human tauopathies; however, mounting in vivo data suggest that NFTs may not be the primary initiators of neurotoxicity. Caspase activity has been implicated in processes associated with the development of tauopathy, but the position that caspase activation holds in neurodegenerative cascades remains uncertain. Using multiphoton real time imaging microscopy, de Calignon et al recently demonstrated that caspase activation precedes and leads to tangle formation within 24 hours in the rTg4510 mouse model of tauopathy. Here, we used immunoelectron microscopy to determine whether caspase-cleaved tau was present in NFTs of rTg4510 mice. Using a caspase-cleaved-tau-specific antibody (TauC3), we found very little immunogold labeling in NFTs in the brains of rTg4510 mice. By immunohistochemistry, the number of TauC3-positive neurons was far less than the numbers of neurons stained with the MC1 antibody, which recognizes abnormal conformations of tau. Biochemically, caspase-cleaved tau was barely detectable in fractions of rTg4510 mouse brain extracts. Our data suggest that caspase activation might be one of multiple routes through which NFT formation occurs, rather than an obligatory initiation step in pathological tau production in rTg4510 mice.

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Section: Discussioncontrasting

confidence: 88%

“…Because TauC3-positive neurons have been shown in both AD brains and those of rTg4510 mice (4, 6, 11, 21, 22), we also performed immunohistochemistry on rTg4510 mouse brains following formalin fixation and paraffin embedding. We first observed early changes of tau phosphorylation detected with the CP13 antibody at 2.5 months of age (Fig.…”

Section: Resultsmentioning

confidence: 99%

Immunoelectron Microscopic and Biochemical Studies of Caspase-Cleaved Tau in a Mouse Model of Tauopathy

Lin¹,

Dickson²,

Sahara³

2011

J Neuropathol Exp Neurol

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“…Studies on htau mice indicated that tau pathology may trigger an age-dependent learning impairment via disruption of synaptic function ( Figure 1) (Polydoro, Acker, Duff, Castillo, & Davies, 2009). Studies on rTg4510 tau transgenic mouse demonstrate caspase-3 activation, which substantiates the evidence linking caspase-3 and tau-mediated neurodegeneration (Calissano, Matrone, & Amadoro, 2009, Ramalho et al, 2008. A triple transgenic Alzheimer mouse model consisting PS1(M146V), APP(Swe), and tau(P301L) transgenes curbs caspase-9 activation, and attenuates the processing of APP and tau, thus decreasing the number of NFTs and extracellular deposits of Aβ entailed with the progression of this disease (Calissano et al, 2009, Rohn et al, 2008.…”

Section: Neuropathology In Animal Modelsmentioning

confidence: 54%

Animal Models of Alzheimer's Disease: An Understanding of Pathology and Therapeutic Avenues

Obulesu

Rao

2010

International Journal of Neuroscience

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Alzheimer's disease is a neurodegenerative disorder with unclear etiology for a few decades. Many animal models employed to study the etiology of the disease and test the efficacy of a drug could give limited understanding of these events. Introduction of aluminum salts into aged New Zealand rabbit brain could demonstrate neurofibrillary tangle formation in 1965. This outstanding contribution substantiated the role of aluminum in Alzheimer's disease in turn becoming the basis further molecular studies in rabbits. In this review, various animal models (transgenic mice, rats, rabbits, zebrafish) used to study the pathology of the disease and to test the efficacy of a drug have been summarized. It also focuses on the growing need to unravel the molecular underpinnings of the disease progression.

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“…For example, overexpressing human mutant tau P301L in mice results in apoptosis, caspase-3 activation, and appearance of caspase truncated tau (de Calignon et al , 2010; Ramalho et al , 2008). Similarly, overexpression of human 4R tau results in caspase activation, although total numbers of caspase bearing neurons are low (de Calignon et al , 2010).…”

Section: The Role Of Tau In Cellular Dysfunctionmentioning

confidence: 99%

“…However, similar to human studies, transgenic animal models of tauopathy suggest that formation of caspase truncated tau occurs prior to tau aggregation and correlates with cognitive decline. In fact, in P301L mice, caspase cleavage of tau proceeds neurofibrillary tangle formation (de Calignon et al , 2010; Ramalho et al , 2008), and is coincident with the beginnings of cognitive impairment (Ramalho et al , 2008). Furthermore, animal models confirm in-vitro findings that caspase truncated tau can seed filament formation of full length tau (Gamblin et al , 2003; Rissman et al , 2004).…”

Section: The Role Of Tau In Cellular Dysfunctionmentioning

confidence: 99%

Chronic traumatic encephalopathy-integration of canonical traumatic brain injury secondary injury mechanisms with tau pathology

Kulbe

Hall

2017

Progress in Neurobiology

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In recent years, a new neurodegenerative tauopathy labeled Chronic Traumatic Encephalopathy (CTE), has been identified that is believed to be primarily a sequela of repeated mild traumatic brain injury (TBI), often referred to as concussion, that occurs in athletes participating in contact sports (e.g. boxing, football, football, rugby, soccer, ice hockey) or in military combatants, especially after blast-induced injuries. Since the identification of CTE, and its neuropathological finding of deposits of hyperphosphorylated tau protein, mechanistic attention has been on lumping the disorder together with various other non-traumatic neurodegenerative tauopathies. Indeed, brains from suspected CTE cases that have come to autopsy have been confirmed to have deposits of hyperphosphorylated tau in locations that make its anatomical distribution distinct for other tauopathies. The fact that these individuals experienced repetitive TBI episodes during their athletic or military careers suggests that the secondary injury mechanisms that have been extensively characterized in acute TBI preclinical models, and in TBI patients, including glutamate excitotoxicity, intracellular calcium overload, mitochondrial dysfunction, free radical-induced oxidative damage and neuroinflammation, may contribute to the brain damage associated with CTE. Thus, the current review begins with an in depth analysis of what is known about the tau protein and its functions and dysfunctions followed by a discussion of the major TBI secondary injury mechanisms, and how the latter have been shown to contribute to tau pathology. The value of this review is that it might lead to improved neuroprotective strategies for either prophylactically attenuating the development of CTE or slowing its progression.

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Apoptosis in Transgenic Mice Expressing the P301L Mutated Form of Human Tau

Cited by 29 publications

References 38 publications

Immunoelectron Microscopic and Biochemical Studies of Caspase-Cleaved Tau in a Mouse Model of Tauopathy

Immunoelectron Microscopic and Biochemical Studies of Caspase-Cleaved Tau in a Mouse Model of Tauopathy

Animal Models of Alzheimer's Disease: An Understanding of Pathology and Therapeutic Avenues

Chronic traumatic encephalopathy-integration of canonical traumatic brain injury secondary injury mechanisms with tau pathology

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