Review: Modelling the pathology and behaviour of frontotemporal dementia

Solomon, Daniel A.; Mitchell, Jacqueline C.; Salcher-Konrad, Marie-Therese; Vance, Caroline; Mizielinska, Sarah

doi:10.1111/nan.12536

Cited by 15 publications

(13 citation statements)

References 228 publications

(317 reference statements)

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“…In fact, knocking down PPIA affected the expression of a number of TDP-43 target genes involved in pathways leading to neurodegeneration, including GRN. GRN has been found mutated in familial forms of FTD and the disease mechanism seems to be linked to GRN haploinsufficiency, as also confirmed in mouse models (Solomon et al, 2019). In the cortex of PPIA-/-mice, we found that GRN was downregulated, indicating that a GRN loss-of-function probably contributes to the development of an FTD phenotype in PPIA-/-mice.…”

Section: Ftld-tdp Is the Most Common Neuropathologic Type Of Ftld Andsupporting

confidence: 79%

“…In previous work we demonstrated that PPIA deficiency affected the expression of a number of TDP-43 target genes, including GRN, which is a major mutated gene in familiar FTD (Lauranzano et al, 2015). GRN mutations in patients result in haplo-insufficiency and GRN knock-out mice present an FTD-like phenotype with mild TDP-43 pathology (Solomon et al, 2019). We verified whether knocking out PPIA influenced GRN expression in the brain cortex of the mice.…”

Section: Ppia Deficiency Downregulates Grn and Tardbp Expressionmentioning

confidence: 74%

“…Several mouse models of ALS/FTD have been generated targeting genes with known pathogenic roles but each one recapitulates only certain aspects of the human disease. For instance, TDP-43 pathology in mice is often absent or mild and is not always linked to neurodegeneration or behavioural phenotypes 62 . In TDP-43 mouse models overexpressing wild-type TDP-43 or diseaseassociated mutations, C-terminal TDP-43 fragments are detected at low levels or are absent 63 .…”

Section: Discussionmentioning

confidence: 99%

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Defective cyclophilin A induces TDP-43 proteinopathy: implications for amyotrophic lateral sclerosis and frontotemporal dementia

Pasetto

Grassano

Pozzi

et al. 2020

Preprint

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Frontotemporal dementia (FTD) is a common cause of early-onset dementia, characterized by frontotemporal lobar degeneration and considerable clinical, genetic and neuropathological heterogeneity. Several mouse models of FTD have been generated targeting genes with known pathogenic roles. However, each of these models recapitulates only certain aspects of the human disease. Cyclophilin A (PPIA) is a multifunctional protein abundantly expressed in the brain, with double-edged functions. Intracellularly, it is mainly protective as a foldase and molecular chaperone with scaffolding properties. Extracellularly, it behaves as a proinflammatory cytokine able to activate an aberrant inflammatory response. In a previous work, we found that PPIA governs TDP-43 functions and its deficiency exacerbates disease in a mouse model of ALS.Selective inhibition of extracellular PPIA rescued motor neurons and increased survival. To decipher PPIA's functions in the central nervous system, we planned a deep neuropathological and behavioral characterization of PPIA knock-out (PPIA-/-) mice throughout their lifespan. They develop a neurodegenerative disease that recapitulates key features of the behavioral variant of FTD associated with TDP-43 pathology. PPIA-/-mice present progressive hippocampal and cortex atrophy, with neuronal death and clear-cut TDP-43 pathology that include fragmentation, hyperphosphorylation, and cytoplasmic mislocalization/nuclear clearing. Mice exhibit increased disinhibition, defects in social behavior, but no memory and motor impairment. On a molecular level, our findings indicate that PPIA is involved in multiple genes and pathways that have a dominant protective effect in the brain, and is fundamental for TDP-43 function. Considering that an impaired interaction of TDP-43 with PPIA has been observed in ALS/FTD patients, the PPIA-/-mouse is a useful experimental model to investigate the mechanism at the basis of TDP-43 pathology and develop novel therapeutic approaches for ALS/FTD and possibly other TDP-43 proteinopathies.

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Section: Ftld-tdp Is the Most Common Neuropathologic Type Of Ftld Andsupporting

confidence: 79%

Section: Ppia Deficiency Downregulates Grn and Tardbp Expressionmentioning

confidence: 74%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Defective cyclophilin A induces TDP-43 proteinopathy: implications for amyotrophic lateral sclerosis and frontotemporal dementia

Pasetto

Grassano

Pozzi

et al. 2020

Preprint

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“…These findings have contributed to shed light on the major biological processes altered in ALS and FTD/FTLD pathologies (Table 1) [29]. On the other hand, as the genes associated with these diseases were fleshed out, it was apparent that ALS and FTD share pathophysiological processes.…”

mentioning

confidence: 94%

From basic research to the clinic: innovative therapies for ALS and FTD in the pipeline

Liščić

Alberici

Cairns

et al. 2020

Mol Neurodegeneration

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Amyotrophic lateral sclerosis (ALS) and Frontotemporal Degeneration (FTD) are neurodegenerative disorders, related by deterioration of motor and cognitive functions and short survival. Aside from cases with an inherited pathogenic mutation, the causes of the disorders are still largely unknown and no effective treatment currently exists. It has been shown that FTD may coexist with ALS and this overlap occurs at clinical, genetic, and molecular levels. In this work, we review the main pathological aspects of these complex diseases and discuss how the integration of the novel pathogenic molecular insights and the analysis of molecular interaction networks among all the genetic players represents a critical step to shed light on discovering novel therapeutic strategies and possibly tailoring personalized medicine approaches to specific ALS and FTD patients.

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“…Appropriate disease models are useful tools for testing hypotheses relevant for disease pathogenesis of FTLDs and will be essential for probing the efficacy of therapeutic approaches once they have become available. The article by Solomon, Mitchell, Konrad, Vance and Mizielinska provides a comprehensive and critical review of the in vivo models of distinct forms of FTLDs with an emphasis on disease models that replicate neuropathological and behavioural aspects of the human disease. It is particularly useful that the authors discuss separately two large groups of FTLD models, the genetic models ( GRN , C9orf72 , CHMP2B , VCP , UBQLN2 , SQSTM1 ) and models whose primary aim is to recapitulate directly the pathology of FTLD‐TDP or FTLD‐FUS.…”

mentioning

confidence: 99%

Frontotemporal lobar degenerations: from basic science to clinical manifestations

Révész

Mann

Lashley

2019

Neuropathology Appl Neurobio

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Review: Modelling the pathology and behaviour of frontotemporal dementia

Cited by 15 publications

References 228 publications

Defective cyclophilin A induces TDP-43 proteinopathy: implications for amyotrophic lateral sclerosis and frontotemporal dementia

Defective cyclophilin A induces TDP-43 proteinopathy: implications for amyotrophic lateral sclerosis and frontotemporal dementia

From basic research to the clinic: innovative therapies for ALS and FTD in the pipeline

Frontotemporal lobar degenerations: from basic science to clinical manifestations

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