Early Cognitive/Social Deficits and Late Motor Phenotype in Conditional Wild-Type TDP-43 Transgenic Mice

Alfieri, Julio Armando; Silva, Pablo R.; Igaz, Lionel M.

doi:10.3389/fnagi.2016.00310

Cited by 24 publications

(39 citation statements)

References 51 publications

(98 reference statements)

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“…The presence of ubiquitinated and phosphorylated cytoplasmic inclusions of TDP-43 in the CNS of patients with ALS and FTLD [ 119 ], and the subsequent identification of TARDBP mutations in the sporadic and familial forms of these diseases [ 57 , 79 , 160 , 175 , 192 ], have led to the rapid development of TDP-43 transgenic models. Mutant Tardbp mice manifest some key features of human ALS and FTLD, including motor neuron loss, gliosis, motor and cognitive deficits, and early mortality [ 4 , 5 , 8 , 18 , 73 , 162 , 186 , 188 , 194 ].…”

Section: Metabolic Dysfunction In Animal Models Of Als/ftldmentioning

confidence: 99%

Disease-modifying effects of metabolic perturbations in ALS/FTLD

Jawaid

Khan

Polymenidou

et al. 2018

Mol Neurodegeneration

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Amyotrophic lateral sclerosis (ALS) and frontotemporal lobar degeneration (FTLD) are two fatal neurodegenerative disorders with considerable clinical, pathological and genetic overlap. Both disorders are characterized by the accumulation of pathological protein aggregates that contain a number of proteins, most notably TAR DNA binding protein 43 kDa (TDP-43). Surprisingly, recent clinical studies suggest that dyslipidemia, high body mass index, and type 2 diabetes mellitus are associated with better clinical outcomes in ALS. Moreover, ALS and FTLD patients have a significantly lower incidence of cardiovascular disease, supporting the idea that an unfavorable metabolic profile may be beneficial in ALS and FTLD. The two most widely studied ALS/FTLD models, super-oxide dismutase 1 (SOD1) and TAR DNA binding protein of 43 kDA (TDP-43), reveal metabolic dysfunction and a positive effect of metabolic strategies on disease onset and/or progression. In addition, molecular studies reveal a role for ALS/FTLD-associated proteins in the regulation of cellular and whole-body metabolism. Here, we systematically evaluate these observations and discuss how changes in cellular glucose/lipid metabolism may result in abnormal protein aggregations in ALS and FTLD, which may have important implications for new treatment strategies for ALS/FTLD and possibly other neurodegenerative conditions.

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Section: Metabolic Dysfunction In Animal Models Of Als/ftldmentioning

confidence: 99%

Disease-modifying effects of metabolic perturbations in ALS/FTLD

Jawaid

Khan

Polymenidou

et al. 2018

Mol Neurodegeneration

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“…They found that embryogenesis was impaired in homozygous knockout mice, suggesting that TDP43 played a part in disease pathogenesis (106). Conversely, there was evidence that TDP43 synthesis was autoregulated, as heterozygous knockout mice did not have symptoms of neuromuscular disease and had normal protein expression (106)(107)(108). Symptoms typical of ALS were not exhibited in any of the generated knockout models.…”

Section: The Tardbp Mutationmentioning

confidence: 99%

“…Furthermore, in order to study the nature of GOF toxicity in ALS and the nature of GOF toxicity in ALS in which high levels of TARDBP mRNA and protein in defected neurons have been reported, researchers generated transgenic mice overexpressing human wild-type TDP43 carried by exogenous promoters such as Cre, Thy1.2, Prp and Camkllα (108,110). The mice in this model exhibited phenotypes similar to those observed in Camkllα mice.…”

Section: The Tardbp Mutationmentioning

confidence: 99%

From Mouse Models to Human Disease: An Approach for Amyotrophic Lateral Sclerosis

Alrafiah

2018

In Vivo

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Amyotrophic lateral sclerosis (ALS) is a fatal adult-onset neurodegenerative disorder. There are several genetic mutations that lead to ALS development, such as chromosome 9 hexanucleotide repeat 72 (C9ORF72), transactive response DNA-binding protein (TARDBP), superoxide dismutase 1 (SOD1) and fused in sarcoma (FUS). ALS is associated with disrupted gene homeostasis causing aberrant RNA processing or toxic pathology. Several animal models of ALS disease have been developed to understand whether TARDBP-mediated neurodegeneration results from a gain or a loss of function of the protein, however, none exactly mimic the pathophysiology and the phenotype of human ALS. Here, the pathophysiology of specific ALS-linked gene mutations is discussed. Furthermore, some of the generated mouse models, as well as the similarities and differences between these models, are comprehensively reviewed. Further refinement of mouse models will likely aid the development of a better form of model that mimics human ALS. However, disrupted gene homeostasis that causes mutation can result in an ALS-like syndrome, increasing concerns about whether neurodegeneration and other effects in these models are due to the mutation or to gene overexpression. Research on the pleiotropic role of different proteins present in motor neurons is also summarized. The development of better mouse models that closely mimic human ALS will help identify potential therapeutic targets for this disease.

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“…Using a mouse model of TDP-43 proteinopathies that conditionally overexpresses the wild-type human TDP-43 protein (hTDP-43-WT) in forebrain neurons and reproduces neuropathological changes of the FTD/ALS spectrum (Igaz et al., 2011), we have recently shown that they display early behavioral phenotypes in the cognitive and social domains (Alfieri et al., 2016). Interestingly, these animals also exhibit progressive motor abnormalities after prolonged transgene expression (Alfieri et al., 2016). These behavioral features provide an interesting correlate to human disease, starting with a more “pure” FTD-like phenotype and later evolving into a FTD with motor neuron disease presentation (expressing some ALS-like features).…”

Section: Introductionmentioning

confidence: 99%

“…In this work, we aimed to investigate how short-term transgene suppression affects the early behavioral phenotypes displayed by conditional TDP-43-WT mice (Alfieri et al., 2016). In particular, we studied (1) if the cognitive and social phenotypes previously described were present after a shorter period (0.5 month) of transgene expression, and (2) the effect of the suppression on both affected domains and in motor behaviors, which were preserved after 1 month of transgene expression.…”

Section: Introductionmentioning

confidence: 99%

Suppression of Conditional TDP-43 Transgene Expression Differentially Affects Early Cognitive and Social Phenotypes in TDP-43 Mice

2019

Self Cite

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Dysregulation of TAR DNA-binding protein 43 (TDP-43) is a hallmark feature of frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS), two fatal neurodegenerative diseases. TDP-43 is a ubiquitously expressed RNA-binding protein with many physiological functions, playing a role in multiple aspects of RNA metabolism. We developed transgenic mice conditionally overexpressing human wild-type TDP-43 protein (hTDP-43-WT) in forebrain neurons, a model that recapitulates several key features of FTD. After post-weaning transgene (TG) induction during 1 month, these mice display an early behavioral phenotype, including impaired cognitive and social function with no substantial motor abnormalities. In order to expand the analysis of this model, we took advantage of the temporal and regional control of TG expression possible in these mice. We behaviorally evaluated mice at two different times: after 2 weeks of post-weaning TG induction (0.5 month group) and after subsequent TG suppression for 2 weeks following that time point [1 month (sup) group]. We found no cognitive abnormalities after 0.5 month of hTDP-43 expression, evaluated with a spatial working memory task (Y-maze test). Suppression of TG expression with doxycycline (Dox) at this time point prevented the development of cognitive deficits previously observed at 1 month post-induction, as revealed by the performance of the 1 month (sup) group. On the other hand, sociability deficits (assessed through the social interaction test) appeared very rapidly after Dox removal (0.5 month) and TG suppression was not sufficient to reverse this phenotype, indicating differential vulnerability to hTDP-43 expression and suppression. Animals evaluated at the early time point (0.5 month) post-induction do not display a motor phenotype, in agreement with the results obtained after 1 month of TG expression. Moreover, all motor tests (open field, accelerated rotarod, limb clasping, hanging wire grip) showed identical responses in both control and bigenic animals in the suppressed group, demonstrating that this protocol and treatment do not cause non-specific effects in motor behavior, which could potentially mask the phenotypes in other domains. Our results show that TDP-43-WT mice have a phenotype that qualifies them as a useful model of FTD and provide valuable information for susceptibility windows in therapeutic strategies for TDP-43 proteinopathies.

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Early Cognitive/Social Deficits and Late Motor Phenotype in Conditional Wild-Type TDP-43 Transgenic Mice

Cited by 24 publications

References 51 publications

Disease-modifying effects of metabolic perturbations in ALS/FTLD

Disease-modifying effects of metabolic perturbations in ALS/FTLD

From Mouse Models to Human Disease: An Approach for Amyotrophic Lateral Sclerosis

Suppression of Conditional TDP-43 Transgene Expression Differentially Affects Early Cognitive and Social Phenotypes in TDP-43 Mice

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