Your search keyword '"MAPT"' showing total 100 results

1. Severe neurodegeneration in brains of transgenic rats producing human tau prions

Author

Ayers, Jacob, Lopez, T Peter, Steele, Ian T, Oehler, Abby, Roman-Albarran, Rigo, Cleveland, Elisa, Chong, Alex, Carlson, George A, Condello, Carlo, and Prusiner, Stanley B

Subjects

Biomedical and Clinical Sciences, Neurosciences, Acquired Cognitive Impairment, Neurodegenerative, Alzheimer's Disease Related Dementias (ADRD), Alzheimer's Disease, Infectious Diseases, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Dementia, Brain Disorders, Aging, Genetics, Rare Diseases, Transmissible Spongiform Encephalopathy (TSE), Emerging Infectious Diseases, Frontotemporal Dementia (FTD), 2.1 Biological and endogenous factors, Neurological, Animals, tau Proteins, Rats, Transgenic, Humans, Rats, Brain, Disease Models, Animal, Prions, Tauopathies, Nerve Degeneration, Mutation, Tauopathy, MAPT, Hyperphosphorylation, Misfolding, Transgenic rat, Clinical Sciences, Neurology & Neurosurgery

Abstract

Both wild-type and mutant tau proteins can misfold into prions and self-propagate in the central nervous system of animals and people. To extend the work of others, we investigated the molecular basis of tau prion-mediated neurodegeneration in transgenic (Tg) rats expressing mutant human tau (P301S); this line of Tg rats is denoted Tg12099. We used the rat Prnp promoter to drive the overexpression of mutant tau (P301S) in the human 0N4R isoform. In Tg12099(+/+) rats homozygous for the transgene, ubiquitous expression of mutant human tau resulted in the progressive accumulation of phosphorylated tau inclusions, including silver-positive tangles in the frontal cortices and limbic system. Signs of central nervous system dysfunction were found in terminal Tg12099(+/+) rats exhibiting severe neurodegeneration and profound atrophy of the amygdala and piriform cortex. The greatest increases in tau prion activity were found in the corticolimbic structures. In contrast to the homozygous Tg12099(+/+) rats, we found lower levels of mutant tau in the hemizygous rats, resulting in few neuropathologic changes up to 2 years of age. Notably, these hemizygous rats could be infected by intracerebral inoculation with recombinant tau fibrils or precipitated tau prions from the brain homogenates of sick, aged homozygous Tg12099(+/+) rats. Our studies argue that the regional propagation of tau prions and neurodegeneration in the Tg12099 rats resembles that found in human primary tauopathies. These findings seem likely to advance our understanding of human tauopathies and may lead to effective therapeutics for Alzheimer's disease and other tau prion disorders.

Published

2024

2. Development and characterization of novel anti-acetylated tau monoclonal antibodies to probe pathogenic tau species in Alzheimer's disease.

Author

Bryan III, Miles R., Tian, Xu, Tseng, Jui-Heng, Evangelista, Baggio A., Ragusa, Joey V., Bryan, Audra F., Trotman, Winifred, Irwin, David, and Cohen, Todd J.

Subjects

*MONOCLONAL antibody probes, *ALZHEIMER'S disease, *AMYLOID plaque, *POST-translational modification, *NEUROFIBRILLARY tangles

Abstract

Tauopathies, including Alzheimer's disease (AD), are a class of neurodegenerative diseases characterized by the presence of insoluble tau inclusions. Tau phosphorylation has traditionally been viewed as the dominant post-translational modification (PTM) controlling tau function and pathogenesis in tauopathies. However, we and others have identified tau acetylation as a primary PTM regulating both normal tau function as well as abnormal pathogenic features including aggregation. Prior work showed robust tau acetylation in aggregation hotspots located within the 2nd and 3rd repeat regions of tau (residues K280 and K311) in tauopathy brains, including AD, compared to non-tauopathy controls. By screening thousands of hybridoma clones, we generated site-specific and modification-specific monoclonal antibodies targeting acetylated tau at residues K280 or K311. To validate these antibodies in a bona fide neuronal system, we targeted the acetyltransferase CBP to the cytoplasm of neurons to promote tau acetylation. Several antibody clones specifically detected CBP-acetylated tau and co-localized with ac-tau in neurons. Additionally, our lead optimal anti-acetylated-tau monoclonal antibodies detected robust tau pathology in tangles and neuritic plaques of human AD brains. Given the now emerging interest in acetylated tau as critical regulator of tau functions, these sensitive and highly specific tools will allow us to further unravel the tau PTM code and, importantly, could be deployed as diagnostic or disease-modifying agents. [ABSTRACT FROM AUTHOR]

Published

2024

3. The cellular prion protein does not affect tau seeding and spreading of sarkosyl-insoluble fractions from Alzheimer's disease.

Author

Sala-Jarque, Julia, Gil, Vanessa, Andrés-Benito, Pol, Martínez-Soria, Inés, Picón-Pagès, Pol, Hernández, Félix, Ávila, Jesús, Lanciego, José Luis, Nuvolone, Mario, Aguzzi, Adriano, Gavín, Rosalina, Ferrer, Isidro, and del Río, José Antonio

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *ALZHEIMER'S disease, *TAU proteins, *AMYLOID, *PRIONS

Abstract

The cellular prion protein (PrPC) plays many roles in the developing and adult brain. In addition, PrPC binds to several amyloids in oligomeric and prefibrillar forms and may act as a putative receptor of abnormal misfolded protein species. The role of PrPC in tau seeding and spreading is not known. In the present study, we have inoculated well-characterized sarkosyl-insoluble fractions of sporadic Alzheimer's disease (sAD) into the brain of adult wild-type mice (Prnp+/+), Prnp0/0 (ZH3 strain) mice, and mice over-expressing the secreted form of PrPC lacking their GPI anchor (Tg44 strain). Phospho-tau (ptau) seeding and spreading involving neurons and oligodendrocytes were observed three and six months after inoculation. 3Rtau and 4Rtau deposits from the host tau, as revealed by inoculating Mapt0/0 mice and by using specific anti-mouse and anti-human tau antibodies suggest modulation of exon 10 splicing of the host mouse Mapt gene elicited by exogenous sAD-tau. However, no tau seeding and spreading differences were observed among Prnp genotypes. Our results show that PrPC does not affect tau seeding and spreading in vivo. [ABSTRACT FROM AUTHOR]

Published

2024

4. CircSLC4A7 in resistant‐cells‐derived exosomes promotes docetaxel resistance via the miR‐1205/MAPT axis in prostate cancer.

Author

Lin, Anhua, Li, Junhe, and He, Wenjing

Subjects

*WESTERN immunoblotting, *ANIMAL experimentation, *REPORTER genes, *BINDING sites, *TAU proteins

Abstract

Prostate cancer (PCa) is a high‐mortality cancer. Docetaxel (DCT) combined with second‐generation anti‐androgens is considered the golden standard therapy for PCa, whose application is limited for DCT resistance (DR). Therefore, exploring the mechanism of DR is of great importance. In this study, PCa cell lines of PC3 and DU145 were employed, and DR cells were constructed by treatment with graded DCT. CircSLC4A7, miR‐1205, and microtubule‐associated protein tau (MAPT) transfections were established. Cell counting kit‐8 assay was performed to evaluate the cell activity and IC50 of DCT. After being treated with DCT, DR was assessed by colony formation assay, flow cytometry analysis, and terminal transferase‐mediated UTP nick end‐labeling assay. Real‐time quantitative PCR and western blotting analysis evaluated the expression levels of genes. The dual‐luciferase reporter gene assay verified the miR‐1205 binding sites with circSLC4A7 and MAPT. An animal experiment was performed to assess the tumor growth influenced by circSLC4A7. After conducting DR cells and isolated exosomes, we found that not only co‐culture with DR cells but also treatment with DR cells' exosomes would promote the DR of normal cells. Moreover, circSLC4A7 was highly expressed in DR cells and their exosomes. CircSLC4A7 overexpression enhanced DR, represented as raised IC50 of DCT, increased colony formation, and decreased cell apoptosis after DCT treatment, while circSLC4A7 knockdown had the opposite effect. MiR‐1205 was confirmed as a circSLC4A7‐sponged miRNA and miR‐1205 inhibitor reversed the effect of sh‐circSLC4A7. MAPT was further identified as a target of miR‐1205 and had a similar effect with circSLC4A7. The effect of circSLC4A7 on DR was also confirmed by xenograft experiments. Collectively, circSLC4A7 in resistant‐cells‐derived exosomes promotes DCT resistance of PCa via miR‐1205/MAPT axis, which may provide a new treatment strategy for DR of PCa. [ABSTRACT FROM AUTHOR]

Published

2024

5. MAPT mutations associated with familial tauopathies lead to formation of conformationally distinct oligomers that have cross‐seeding ability.

Author

Bhopatkar, Anukool A., Bhatt, Nemil, Haque, Md Anzarul, Xavier, Rhea, Fung, Leiana, Jerez, Cynthia, and Kayed, Rakez

Abstract

The microtubule associated protein, tau, is implicated in a multitude of neurodegenerative disorders that are collectively termed as tauopathies. These disorders are characterized by the presence of tau aggregates within the brain of afflicted individuals. Mutations within the MAPT gene that encodes the tau protein form the genetic backdrop for familial forms of tauopathies, such as frontotemporal dementia (FTD), but the molecular consequences of such alterations and their pathological effects are unclear. We sought to investigate the conformational properties of the aggregates of three tau mutants: A152T, P301L, and R406W, all implicated within FTD, and compare them to those of the native form (WT‐Tau 2N4R). Our immunochemical analysis reveals that mutants and WT tau oligomers exhibit similar affinity for conformation‐specific antibodies but have distinct morphology and secondary structure. Additionally, these oligomers possess different dye‐binding properties and varying sensitivity to proteolytic processing. These results point to conformational variety among them. We then tested the ability of the mutant oligomers to cross‐seed the aggregation of WT tau monomer. Using similar array of experiments, we found that cross‐seeding with mutant aggregates leads to the formation of conformationally unique WT oligomers. The results discussed in this paper provide a novel perspective on the structural properties of oligomeric forms of WT tau 2N4R and its mutant, along with shedding some light on their cross‐seeding behavior. [ABSTRACT FROM AUTHOR]

Published

2024

6. Development and characterization of novel anti-acetylated tau monoclonal antibodies to probe pathogenic tau species in Alzheimer’s disease

Author

Miles R. Bryan III, Xu Tian, Jui-Heng Tseng, Baggio A. Evangelista, Joey V. Ragusa, Audra F. Bryan, Winifred Trotman, David Irwin, and Todd J. Cohen

Subjects

Alzheimer’s disease (AD), MAPT, Posttranslational modification (PTM), Acetylation, Tau, Neurodegeneration, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Tauopathies, including Alzheimer’s disease (AD), are a class of neurodegenerative diseases characterized by the presence of insoluble tau inclusions. Tau phosphorylation has traditionally been viewed as the dominant post-translational modification (PTM) controlling tau function and pathogenesis in tauopathies. However, we and others have identified tau acetylation as a primary PTM regulating both normal tau function as well as abnormal pathogenic features including aggregation. Prior work showed robust tau acetylation in aggregation hotspots located within the 2nd and 3rd repeat regions of tau (residues K280 and K311) in tauopathy brains, including AD, compared to non-tauopathy controls. By screening thousands of hybridoma clones, we generated site-specific and modification-specific monoclonal antibodies targeting acetylated tau at residues K280 or K311. To validate these antibodies in a bona fide neuronal system, we targeted the acetyltransferase CBP to the cytoplasm of neurons to promote tau acetylation. Several antibody clones specifically detected CBP-acetylated tau and co-localized with ac-tau in neurons. Additionally, our lead optimal anti-acetylated-tau monoclonal antibodies detected robust tau pathology in tangles and neuritic plaques of human AD brains. Given the now emerging interest in acetylated tau as critical regulator of tau functions, these sensitive and highly specific tools will allow us to further unravel the tau PTM code and, importantly, could be deployed as diagnostic or disease-modifying agents.

Published

2024

7. The cellular prion protein does not affect tau seeding and spreading of sarkosyl-insoluble fractions from Alzheimer’s disease

Author

Julia Sala-Jarque, Vanessa Gil, Pol Andrés-Benito, Inés Martínez-Soria, Pol Picón-Pagès, Félix Hernández, Jesús Ávila, José Luis Lanciego, Mario Nuvolone, Adriano Aguzzi, Rosalina Gavín, Isidro Ferrer, and José Antonio del Río

Subjects

PrPC, Prnp, Tau, Mapt, Alzheimer’s disease, Seeding, Medicine, Science

Abstract

Abstract The cellular prion protein (PrPC) plays many roles in the developing and adult brain. In addition, PrPC binds to several amyloids in oligomeric and prefibrillar forms and may act as a putative receptor of abnormal misfolded protein species. The role of PrPC in tau seeding and spreading is not known. In the present study, we have inoculated well-characterized sarkosyl-insoluble fractions of sporadic Alzheimer’s disease (sAD) into the brain of adult wild-type mice (Prnp +/+), Prnp 0/0 (ZH3 strain) mice, and mice over-expressing the secreted form of PrPC lacking their GPI anchor (Tg44 strain). Phospho-tau (ptau) seeding and spreading involving neurons and oligodendrocytes were observed three and six months after inoculation. 3Rtau and 4Rtau deposits from the host tau, as revealed by inoculating Mapt 0/0 mice and by using specific anti-mouse and anti-human tau antibodies suggest modulation of exon 10 splicing of the host mouse Mapt gene elicited by exogenous sAD-tau. However, no tau seeding and spreading differences were observed among Prnp genotypes. Our results show that PrPC does not affect tau seeding and spreading in vivo.

Published

2024

8. Astrocyte tau deposition in progressive supranuclear palsy is associated with dysregulation of MAPT transcription

Author

Rosemary J. Jackson, Alexandra Melloni, Dustin P. Fykstra, Alberto Serrano-Pozo, Leslie Shinobu, and Bradley T. Hyman

Subjects

Progressive supranuclear palsy, Astrocytes, MAPT, Tufted astrocytes, Tau, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Progressive supranuclear palsy (PSP) is a neurodegenerative disease characterized by 4R tau deposition in neurons as well as in astrocytes and oligodendrocytes. While astrocytic tau deposits are rarely observed in normal aging (so-called aging-related tau astrogliopathy, ARTAG) and Alzheimer’s disease (AD), astrocytic tau in the form of tufted astrocytes is a pathognomonic hallmark of PSP. Classical biochemical experiments emphasized tau synthesis in neurons in the central nervous system, suggesting that astrocytic tau inclusions might be derived from uptake of extracellular neuronal-derived tau. However, recent single-nucleus RNAseq experiments highlight the fact that MAPT, the gene encoding tau, is also expressed by astrocytes, albeit in lower amounts. We, therefore, revisited the question of whether astrocyte-driven expression of tau might contribute to astrocytic tau aggregates in PSP by performing fluorescent in situ hybridization/immunohistochemical co-localization in human postmortem brain specimens from individuals with PSP and AD with ARTAG as well as normal controls. We find that, in PSP but not in AD, tau-immunoreactive astrocytes have higher levels of MAPT mRNA compared to astrocytes that do not have tau aggregates. These results suggest that astrocytic responses in PSP are unique to this tauopathy and support the possibility that fundamental changes in PSP astrocyte-endogenous mRNA biology contribute to increased synthesis of tau protein and underlies the formation of the astrocytic tau deposits characteristic of PSP.

Published

2024

9. Astrocyte tau deposition in progressive supranuclear palsy is associated with dysregulation of MAPT transcription.

Author

Jackson, Rosemary J., Melloni, Alexandra, Fykstra, Dustin P., Serrano-Pozo, Alberto, Shinobu, Leslie, and Hyman, Bradley T.

Subjects

*PROGRESSIVE supranuclear palsy, *FLUORESCENCE in situ hybridization, *ALZHEIMER'S disease, *TAU proteins, *TAUOPATHIES

Abstract

Progressive supranuclear palsy (PSP) is a neurodegenerative disease characterized by 4R tau deposition in neurons as well as in astrocytes and oligodendrocytes. While astrocytic tau deposits are rarely observed in normal aging (so-called aging-related tau astrogliopathy, ARTAG) and Alzheimer's disease (AD), astrocytic tau in the form of tufted astrocytes is a pathognomonic hallmark of PSP. Classical biochemical experiments emphasized tau synthesis in neurons in the central nervous system, suggesting that astrocytic tau inclusions might be derived from uptake of extracellular neuronal-derived tau. However, recent single-nucleus RNAseq experiments highlight the fact that MAPT, the gene encoding tau, is also expressed by astrocytes, albeit in lower amounts. We, therefore, revisited the question of whether astrocyte-driven expression of tau might contribute to astrocytic tau aggregates in PSP by performing fluorescent in situ hybridization/immunohistochemical co-localization in human postmortem brain specimens from individuals with PSP and AD with ARTAG as well as normal controls. We find that, in PSP but not in AD, tau-immunoreactive astrocytes have higher levels of MAPT mRNA compared to astrocytes that do not have tau aggregates. These results suggest that astrocytic responses in PSP are unique to this tauopathy and support the possibility that fundamental changes in PSP astrocyte-endogenous mRNA biology contribute to increased synthesis of tau protein and underlies the formation of the astrocytic tau deposits characteristic of PSP. [ABSTRACT FROM AUTHOR]

Published

2024

10. Genetic background of cognitive decline in Parkinson's disease.

Author

Blazekovic, Antonela, Jercic, Kristina Gotovac, Devedija, Sabina, and Borovecki, Fran

Subjects

*PARKINSON'S disease, *COGNITION disorders, *DARDARIN, *DEMENTIA, *APOLIPOPROTEIN E

Abstract

Parkinson's disease (PD) is a complex disorder that is influenced by multiple genetic risk factors. There is a significant heterogeneity in PD presentation, both pathologically and clinically. Some of the most common and important symptoms affecting the patient are cognitive impairment and dementia. However, the genetic and biological basis underlying the differences in cognitive profiles, including the development of dementia in PD, is not yet well understood. Understanding the role of genes in cognitive outcomes is crucial for effective patient counseling and treatment. Research on familial PD has discovered more than 20 genes that can cause the disease. The identified genes responsible for familial cases of PD are LRRK2, PARK7, PINK1, PRKN, or SNCA gene, although theremay be other genes that also contribute. Additionally, some of these genes may also play a role in cases that were previously thought to be sporadic. Currently, numerous well-described genes increase the risk of cognitive decline in PD, each with varying levels of penetrance. The aim of this review is to identify the relevant genetic factors that contribute to differences in cognition. We discuss the genes thatmay affect cognition and the challenges in establishing a clear genetic diagnostic and prognostic assessment. This article aims to demonstrate the complexity of the genetic background of cognition in PD and to present the different types of genotype changes that can impact cognition through various neurobiological mechanisms. [ABSTRACT FROM AUTHOR]

Published

2024

11. Rescue Stenting of Isolated Middle Cerebral Artery (MCA) Dissections (MCAD) with Antithrombogenic Coated Stents and Mono-Antiplatelet Therapy (MAPT).

Author

Pedowski, Piotr, Fedorko, Jakub, Pataky, Stefan, and Gdovinova, Zuzana

Subjects

*ISCHEMIC stroke, *INTRACRANIAL hemorrhage, *STROKE, *ENDOVASCULAR surgery, *CEREBRAL arteries

Abstract

Objective: Acute ischemic stroke (AIS) is a leading cause of death, but isolated middle cerebral artery dissection (MCAD) is rarely reported. The aim of this article is to sum up the current information on this pathology and to explore the technical aspects of its endovascular treatment with emphasis on novel coated, antithrombogenic stents and antiplatelet management. Another part of this article offers our experience with the problematics represented by a small sample group of patients with an MCAD diagnosis who were treated in our center. Methods: We conducted literature research and a retrospective review of patients treated for anterior circulation AIS at our comprehensive stroke center from January 2022 to March 2024. The cohort included 16 patients diagnosed with isolated MCAD, 9 received antithrombogenic coated stents, while 7 received bare metal stents. Pharmacological management of coated stents involved the use of Cangrelor for acute antiplatelet therapy, transitioning to oral Ticagrelor. Results: Among the 16 patients treated, those with antithrombogenic coated stents showed no major complications and had a lower incidence of intracranial hemorrhage compared to the bare metal stent group. The average National Institutes of Health Stroke Scale (NIHSS) score at discharge improved in both groups. Functional outcomes and mortality rates were slightly better in the coated stent group, but no statistical significance was proven. Conclusions: Antithrombogenic coated stents, in conjunction with MAPT, demonstrated a safe and effective option for treating isolated MCAD. These stents offer promising potential for improved outcomes and reduced complications compared to traditional treatments. Further multicentric studies with larger cohorts are recommended to validate these findings. [ABSTRACT FROM AUTHOR]

Published

2024

12. Oligodendrocyte Dysfunction in Tauopathy: A Less Explored Area in Tau-Mediated Neurodegeneration.

Author

Majumder, Moumita and Dutta, Debashis

Subjects

*PROGRESSIVE supranuclear palsy, *TAU proteins, *TAUOPATHIES, *AXONAL transport, *MICROTUBULE-associated proteins

Abstract

Aggregation of the microtubule-associated protein tau (MAPT) is the hallmark pathology in a spectrum of neurodegenerative disorders collectively called tauopathies. Physiologically, tau is an inherent neuronal protein that plays an important role in the assembly of microtubules and axonal transport. However, disease-associated mutations of this protein reduce its binding to the microtubule components and promote self-aggregation, leading to formation of tangles in neurons. Tau is also expressed in oligodendrocytes, where it has significant developmental roles in oligodendrocyte maturation and myelin synthesis. Oligodendrocyte-specific tau pathology, in the form of fibrils and coiled coils, is evident in major tauopathies including progressive supranuclear palsy (PSP), corticobasal degeneration (CBD), and Pick's disease (PiD). Multiple animal models of tauopathy expressing mutant forms of MAPT recapitulate oligodendroglial tau inclusions with potential to cause degeneration/malfunction of oligodendrocytes and affecting the neuronal myelin sheath. Till now, mechanistic studies heavily concentrated on elucidating neuronal tau pathology. Therefore, more investigations are warranted to comprehensively address tau-induced pathologies in oligodendrocytes. The present review provides the current knowledge available in the literature about the intricate relations between tau and oligodendrocytes in health and diseases. [ABSTRACT FROM AUTHOR]

Published

2024

13. Clinical and neuroimaging characterization of the first frontotemporal dementia family carrying the MAPT p.K298E mutation.

Author

Pozzi, Federico Emanuele, Aprea, Vittoria, Giovannelli, Ginevra, Lattuada, Francesca, Crivellaro, Cinzia, Bertola, Francesca, Castelnovo, Veronica, Canu, Elisa, Filippi, Massimo, Appollonio, Ildebrando, Ferrarese, Carlo, Agosta, Federica, and Tremolizzo, Lucio

Subjects

FRONTOTEMPORAL dementia, BRAIN imaging, MEMORY disorders, SYMPTOMS, COGNITION disorders

Abstract

We present an in-depth clinical and neuroimaging analysis of a family carrying the MAPT K298E mutation associated with frontotemporal dementia (FTD). Initial identification of this mutation in a single clinical case led to a comprehensive investigation involving four affected siblings allowing to elucidate the mutation's phenotypic expression. A 60-year-old male presented with significant behavioral changes and progressed rapidly, exhibiting speech difficulties and cognitive decline. Neuroimaging via FDG-PET revealed asymmetrical frontotemporal hypometabolism. Three siblings subsequently showed varied but consistent clinical manifestations, including abnormal behavior, speech impairments, memory deficits, and motor symptoms correlating with asymmetric frontotemporal atrophy observed in MRI scans. Based on the genotype–phenotype correlation, we propose that the p.K298E mutation results in early-onset behavioral variant FTD, accompanied by a various constellation of speech and motor impairment. This detailed characterization expands the understanding of the p.K298E mutation's clinical and neuroimaging features, underlining its role in the pathogenesis of FTD. Further research is crucial to comprehensively delineate the clinical and epidemiological implications of the MAPT p.K298E mutation. [ABSTRACT FROM AUTHOR]

Published

2024

14. A Systematic Review of Empirical Mobile-Assisted Pronunciation Studies through a Perception–Production Lens.

Author

Stoughton, Anne M. and Kang, Okim

Subjects

VERBAL behavior, PRONUNCIATION, PHONEME (Linguistics), TEACHING methods, EXPERIMENTAL groups, INTELLIGIBILITY of speech

Abstract

The communicative approach to language learning, a teaching method commonly used in second language (L2) classrooms, places little to no emphasis on pronunciation training. As a result, mobile-assisted pronunciation training (MAPT) platforms provide an alternative to classroom-based pronunciation training. To date, there have been several meta-analyses and systematic reviews of mobile-assisted language learning (MALL) studies, but only a few of these meta-analyses have concentrated on pronunciation. To better understand MAPT's impact on L2 learners' perceptions and production of targeted pronunciation features, this study conducted a systematic review of the MAPT literature following PRISMA 2020 guidelines. Potential mobile-assisted articles were identified through searches of the ERIC, Educational Full Text, Linguistics and Language Behavior Abstract, MLI International, and Scopus databases and specific journal searches. Criteria for article inclusion in this study included the following: the article must be a peer-reviewed empirical or quasi-empirical research study using both experimental and control groups to assess the impact of pronunciation training. Pronunciation training must have been conducted via MALL or MAPT technologies, and the studies must have been published between 2014 and 2024. A total of 232 papers were identified; however, only ten articles with a total of 524 participants met the established criteria. Data pertaining to the participants used in the study (nationality and education level), the MPAT applications and platforms used, the pronunciation features targeted, the concentration on perception and/or production of these features, and the methods used for training and assessments were collected and discussed. Effect sizes using Cohen's d were also calculated for each study. The findings of this review reveal that only two of the articles assessed the impact of MAPT on L2 learners' perceptions of targeted features, with results indicating that the use of MPAT did not significantly improve L2 learners' abilities to perceive segmental features. In terms of production, all ten articles assessed MPAT's impact on L2 learners' production of the targeted features. The results of these assessments varied greatly, with some studies indicating a significant and large effect of MAPT and others citing non-significant gains and negligible effect sizes. The variation in these results, in addition to differences in the types of participants, the targeted pronunciation features, and MAPT apps and platforms used, makes it difficult to conclude that MAPT has a significant impact on L2 learners' production. Furthermore, the selected studies' concentration on mostly segmental features (i.e., phoneme and word pronunciation) is likely to have had only a limited impact on participants' intelligibility. This paper provides suggestions for further MAPT research, including increased emphasis on suprasegmental features and perception assessments, to further our understanding of the effectiveness of MAPT for pronunciation training. [ABSTRACT FROM AUTHOR]

Published

2024

15. Genetic forms of tauopathies: inherited causes and implications of Alzheimer's disease-like TAU pathology in primary and secondary tauopathies.

Author

Langerscheidt, Felix, Wied, Tamara, Al Kabbani, Mohamed Aghyad, van Eimeren, Thilo, Wunderlich, Gilbert, and Zempel, Hans

Subjects

*ALZHEIMER'S disease, *TAUOPATHIES, *PROGRESSIVE supranuclear palsy, *TAU proteins, *HUNTINGTON disease

Abstract

Tauopathies are a heterogeneous group of neurologic diseases characterized by pathological axodendritic distribution, ectopic expression, and/or phosphorylation and aggregation of the microtubule-associated protein TAU, encoded by the gene MAPT. Neuronal dysfunction, dementia, and neurodegeneration are common features of these often detrimental diseases. A neurodegenerative disease is considered a primary tauopathy when MAPT mutations/haplotypes are its primary cause and/or TAU is the main pathological feature. In case TAU pathology is observed but superimposed by another pathological hallmark, the condition is classified as a secondary tauopathy. In some tauopathies (e.g. MAPT-associated frontotemporal dementia (FTD), progressive supranuclear palsy (PSP), corticobasal degeneration (CBD), and Alzheimer's disease (AD)) TAU is recognized as a significant pathogenic driver of the disease. In many secondary tauopathies, including Parkinson's disease (PD) and Huntington's disease (HD), TAU is suggested to contribute to the development of dementia, but in others (e.g. Niemann-Pick disease (NPC)) TAU may only be a bystander. The genetic and pathological mechanisms underlying TAU pathology are often not fully understood. In this review, the genetic predispositions and variants associated with both primary and secondary tauopathies are examined in detail, assessing evidence for the role of TAU in these conditions. We highlight less common genetic forms of tauopathies to increase awareness for these disorders and the involvement of TAU in their pathology. This approach not only contributes to a deeper understanding of these conditions but may also lay the groundwork for potential TAU-based therapeutic interventions for various tauopathies. [ABSTRACT FROM AUTHOR]

Published

2024

16. Clinical and Pathological Features of FTDP‐17 with MAPT p.K298_H299insQ Mutation.

Author

Morino, Hiroyuki, Kurashige, Takashi, Matsuda, Yukiko, Ono, Maiko, Sahara, Naruhiko, Miyasaka, Tomohiro, Soeda, Yoshiyuki, Shimada, Hitoshi, Yamazaki, Yu, Takahashi, Tetsuya, Izumi, Yuishin, Ito, Hidefumi, Maruyama, Hirofumi, Higuchi, Makoto, Arihiro, Koji, Suhara, Tetsuya, Takashima, Akihiko, and Kawakami, Hideshi

Subjects

*PROGRESSIVE supranuclear palsy, *FRONTOTEMPORAL dementia, *TAU proteins, *PARKINSON'S disease, *TUBULINS, *GENETIC disorders

Abstract

Background: MAPT is a causative gene in frontotemporal dementia with parkinsonism linked to chromosome 17 (FTDP‐17), a hereditary degenerative disease with various clinical manifestations, including progressive supranuclear palsy, corticobasal syndrome, Parkinson's disease, and frontotemporal dementia. Objectives: To analyze genetically, biochemically, and pathologically multiple members of two families who exhibited various phenotypes of the disease. Methods: Genetic analysis included linkage analysis, homozygosity haplotyping, and exome sequencing. We conducted tau protein microtubule polymerization assay, heparin‐induced tau aggregation, and western blotting with brain lysate from an autopsy case. We also evaluated abnormal tau aggregation by using anti‐tau antibody and PM‐PBB3. Results: We identified a variant, c.896_897insACA, p.K298_H299insQ, in the MAPT gene of affected patients. Similar to previous reports, most patients presented with atypical parkinsonism. Biochemical analysis revealed that the mutant tau protein had a reduced ability to polymerize microtubules and formed abnormal fibrous aggregates. Pathological study revealed frontotemporal lobe atrophy, midbrain atrophy, depigmentation of the substantia nigra, and four‐repeat tau‐positive inclusions in the hippocampus, brainstem, and spinal cord neurons. The inclusion bodies also stained positively with PM‐PBB3. Conclusions: This study confirmed that the insACA mutation caused FTDP‐17. The affected patients showed symptoms resembling Parkinson's disease initially and symptoms of progressive supranuclear palsy later. Despite the initial clinical diagnosis of frontotemporal dementia in the autopsy case, the spread of lesions could explain the process of progressive supranuclear palsy. The study of more cases in the future will help clarify the common pathogenesis of MAPT mutations or specific pathogeneses of each mutation. [ABSTRACT FROM AUTHOR]

Published

2024

17. LRRK2 kinase inhibition reverses G2019S mutation-dependent effects on tau pathology progression

Author

Noah Lubben, Julia K. Brynildsen, Connor M. Webb, Howard L. Li, Cheryl E. G. Leyns, Lakshmi Changolkar, Bin Zhang, Emily S. Meymand, Mia O’Reilly, Zach Madaj, Daniella DeWeerd, Matthew J. Fell, Virginia M. Y. Lee, Dani S. Bassett, and Michael X. Henderson

Subjects

G2019S, MLi-2, Cell-to-cell spread, Transmission, Genetic risk, Mapt, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Mutations in leucine-rich repeat kinase 2 (LRRK2) are the most common cause of familial Parkinson’s disease (PD). These mutations elevate the LRRK2 kinase activity, making LRRK2 kinase inhibitors an attractive therapeutic. LRRK2 kinase activity has been consistently linked to specific cell signaling pathways, mostly related to organelle trafficking and homeostasis, but its relationship to PD pathogenesis has been more difficult to define. LRRK2-PD patients consistently present with loss of dopaminergic neurons in the substantia nigra but show variable development of Lewy body or tau tangle pathology. Animal models carrying LRRK2 mutations do not develop robust PD-related phenotypes spontaneously, hampering the assessment of the efficacy of LRRK2 inhibitors against disease processes. We hypothesized that mutations in LRRK2 may not be directly related to a single disease pathway, but instead may elevate the susceptibility to multiple disease processes, depending on the disease trigger. To test this hypothesis, we have previously evaluated progression of α-synuclein and tau pathologies following injection of proteopathic seeds. We demonstrated that transgenic mice overexpressing mutant LRRK2 show alterations in the brain-wide progression of pathology, especially at older ages. Methods Here, we assess tau pathology progression in relation to long-term LRRK2 kinase inhibition. Wild-type or LRRK2G2019S knock-in mice were injected with tau fibrils and treated with control diet or diet containing LRRK2 kinase inhibitor MLi-2 targeting the IC50 or IC90 of LRRK2 for 3–6 months. Mice were evaluated for tau pathology by brain-wide quantitative pathology in 844 brain regions and subsequent linear diffusion modeling of progression. Results Consistent with our previous work, we found systemic alterations in the progression of tau pathology in LRRK2G2019S mice, which were most pronounced at 6 months. Importantly, LRRK2 kinase inhibition reversed these effects in LRRK2G2019S mice, but had minimal effect in wild-type mice, suggesting that LRRK2 kinase inhibition is likely to reverse specific disease processes in G2019S mutation carriers. Additional work may be necessary to determine the potential effect in non-carriers. Conclusions This work supports a protective role of LRRK2 kinase inhibition in G2019S carriers and provides a rational workflow for systematic evaluation of brain-wide phenotypes in therapeutic development.

Published

2024

18. Unraveling the complex role of MAPT-containing H1 and H2 haplotypes in neurodegenerative diseases.

Author

Pedicone, Chiara, Weitzman, Sarah A., Renton, Alan E., and Goate, Alison M.

Subjects

*SINGLE nucleotide polymorphisms, *HAPLOTYPES, *NEURODEGENERATION, *GENETIC variation, *CHROMOSOME inversions, *22Q11 deletion syndrome, *DNA copy number variations

Abstract

A ~ 1 Mb inversion polymorphism exists within the 17q21.31 locus of the human genome as direct (H1) and inverted (H2) haplotype clades. This inversion region demonstrates high linkage disequilibrium, but the frequency of each haplotype differs across ancestries. While the H1 haplotype exists in all populations and shows a normal pattern of genetic variability and recombination, the H2 haplotype is enriched in European ancestry populations, is less frequent in African ancestry populations, and nearly absent in East Asian ancestry populations. H1 is a known risk factor for several neurodegenerative diseases, and has been associated with many other traits, suggesting its importance in cellular phenotypes of the brain and entire body. Conversely, H2 is protective for these diseases, but is associated with predisposition to recurrent microdeletion syndromes and neurodevelopmental disorders such as autism. Many single nucleotide variants and copy number variants define H1/H2 haplotypes and sub-haplotypes, but identifying the causal variant(s) for specific diseases and phenotypes is complex due to the extended linkage equilibrium. In this review, we assess the current knowledge of this inversion region regarding genomic structure, gene expression, cellular phenotypes, and disease association. We discuss recent discoveries and challenges, evaluate gaps in knowledge, and highlight the importance of understanding the effect of the 17q21.31 haplotypes to promote advances in precision medicine and drug discovery for several diseases. [ABSTRACT FROM AUTHOR]

Published

2024

19. The six brain‐specific TAU isoforms and their role in Alzheimer's disease and related neurodegenerative dementia syndromes.

Author

Buchholz, Sarah and Zempel, Hans

Abstract

INTRODUCTION: Alternative splicing of the human MAPT gene generates six brain‐specific TAU isoforms. Imbalances in the TAU isoform ratio can lead to neurodegenerative diseases, underscoring the need for precise control over TAU isoform balance. Tauopathies, characterized by intracellular aggregates of hyperphosphorylated TAU, exhibit extensive neurodegeneration and can be classified by the TAU isoforms present in pathological accumulations. METHODS: A comprehensive review of TAU and related dementia syndromes literature was conducted using PubMed, Google Scholar, and preprint server. RESULTS: While TAU is recognized as key driver of neurodegeneration in specific tauopathies, the contribution of the isoforms to neuronal function and disease development remains largely elusive. DISCUSSION: In this review we describe the role of TAU isoforms in health and disease, and stress the importance of comprehending and studying TAU isoforms in both, physiological and pathological context, in order to develop targeted therapeutic interventions for TAU‐associated diseases. Highlights: MAPT splicing is tightly regulated during neuronal maturation and throughout life.TAU isoform expression is development‐, cell‐type and brain region specific.The contribution of TAU to neurodegeneration might be isoform‐specific.Ineffective TAU‐based therapies highlight the need for specific targeting strategies. [ABSTRACT FROM AUTHOR]

Published

2024

20. Changes in Oxidised Phospholipids in Response to Oxidative Stress in Microtubule-Associated Protein Tau (MAPT) Mutant Dopamine Neurons.

Author

Bradford, Xanthe, Fernandes, Hugo J. R., and Snowden, Stuart G.

Subjects

TAU proteins, MICROTUBULE-associated proteins, DOPAMINE receptors, HEAT shock proteins, OXIDATIVE stress, LYSIS, DOPAMINERGIC neurons

Abstract

Microtubule-associated protein Tau (MAPT) is strongly associated with the development of neurodegenerative diseases. In addition to driving the formation of neurofibrillary tangles (NFT), mutations in the MAPT gene can also cause oxidative stress through hyperpolarisation of the mitochondria. This study explores the impact that MAPT mutation is having on phospholipid metabolism in iPSC-derived dopamine neurons, and to determine if these effects are exacerbated by mitochondrial and endoplasmic reticulum stress. Neurons that possessed a mutated copy of MAPT were shown to have significantly higher levels of oxo-phospholipids (Oxo-PL) than wild-type neurons. Oxidation of the hydrophobic fatty acid side chains changes the chemistry of the phospholipid leading to disruption of membrane function and potential cell lysis. In wild-type neurons, both mitochondrial and endoplasmic reticulum stress increased Oxo-PL abundance; however, in MAPT mutant neurons mitochondrial stress appeared to have a minimal effect. Endoplasmic reticulum stress, surprisingly, reduced the abundance of Oxo-PL in MAPT mutant dopamine neurons, and we postulate that this reduction could be modulated through hyperactivation of the unfolded protein response and X-box binding protein 1. Overall, the results of this study contribute to furthering our understanding of the regulation and impact of oxidative stress in Parkinson's disease pathology. [ABSTRACT FROM AUTHOR]

Published

2024

21. Person‐specific differences in ubiquitin‐proteasome mediated proteostasis in human neurons.

Author

Hsieh, Yi‐Chen, Augur, Zachary M., Arbery, Mason, Ashour, Nancy, Barrett, Katharine, Pearse, Richard V., Tio, Earvin S., Duong, Duc M., Felsky, Daniel, De Jager, Philip L., Bennett, David A., Seyfried, Nicholas T., and Young‐Pearse, Tracy L.

Abstract

BACKGROUND: Impairment of the ubiquitin‐proteasome system (UPS) has been implicated in abnormal protein accumulation in Alzheimer's disease. It remains unclear if genetic variation affects the intrinsic properties of neurons that render some individuals more vulnerable to UPS impairment. METHODS: Induced pluripotent stem cell (iPSC)‐derived neurons were generated from over 50 genetically variant and highly characterized participants of cohorts of aging. Proteomic profiling, proteasome activity assays, and Western blotting were employed to examine neurons at baseline and in response to UPS perturbation. RESULTS: Neurons with lower basal UPS activity were more vulnerable to tau accumulation following mild UPS inhibition. Chronic reduction in proteasome activity in human neurons induced compensatory elevation of regulatory proteins involved in proteostasis and several proteasome subunits. DISCUSSION: These findings reveal that genetic variation influences basal UPS activity in human neurons and differentially sensitizes them to external factors perturbing the UPS, leading to the accumulation of aggregation‐prone proteins such as tau. Highlights: Polygenic risk score for AD is associated with the ubiquitin‐proteasome system (UPS) in neurons.Basal proteasome activity correlates with aggregation‐prone protein levels in neurons.Genetic variation affects the response to proteasome inhibition in neurons.Neuronal proteasome perturbation induces an elevation in specific proteins involved in proteostasis.Low basal proteasome activity leads to enhanced tau accumulation with UPS challenge. [ABSTRACT FROM AUTHOR]

Published

2024

22. LRRK2 kinase inhibition reverses G2019S mutation-dependent effects on tau pathology progression.

Author

Lubben, Noah, Brynildsen, Julia K., Webb, Connor M., Li, Howard L., Leyns, Cheryl E. G., Changolkar, Lakshmi, Zhang, Bin, Meymand, Emily S., O'Reilly, Mia, Madaj, Zach, DeWeerd, Daniella, Fell, Matthew J., Lee, Virginia M. Y., Bassett, Dani S., and Henderson, Michael X.

Subjects

*DARDARIN, *NEUROFIBRILLARY tangles, *CHRONIC traumatic encephalopathy, *PROGRESSIVE supranuclear palsy, *PARKINSON'S disease, *SUBSTANTIA nigra

Abstract

Background: Mutations in leucine-rich repeat kinase 2 (LRRK2) are the most common cause of familial Parkinson's disease (PD). These mutations elevate the LRRK2 kinase activity, making LRRK2 kinase inhibitors an attractive therapeutic. LRRK2 kinase activity has been consistently linked to specific cell signaling pathways, mostly related to organelle trafficking and homeostasis, but its relationship to PD pathogenesis has been more difficult to define. LRRK2-PD patients consistently present with loss of dopaminergic neurons in the substantia nigra but show variable development of Lewy body or tau tangle pathology. Animal models carrying LRRK2 mutations do not develop robust PD-related phenotypes spontaneously, hampering the assessment of the efficacy of LRRK2 inhibitors against disease processes. We hypothesized that mutations in LRRK2 may not be directly related to a single disease pathway, but instead may elevate the susceptibility to multiple disease processes, depending on the disease trigger. To test this hypothesis, we have previously evaluated progression of α-synuclein and tau pathologies following injection of proteopathic seeds. We demonstrated that transgenic mice overexpressing mutant LRRK2 show alterations in the brain-wide progression of pathology, especially at older ages. Methods: Here, we assess tau pathology progression in relation to long-term LRRK2 kinase inhibition. Wild-type or LRRK2G2019S knock-in mice were injected with tau fibrils and treated with control diet or diet containing LRRK2 kinase inhibitor MLi-2 targeting the IC50 or IC90 of LRRK2 for 3–6 months. Mice were evaluated for tau pathology by brain-wide quantitative pathology in 844 brain regions and subsequent linear diffusion modeling of progression. Results: Consistent with our previous work, we found systemic alterations in the progression of tau pathology in LRRK2G2019S mice, which were most pronounced at 6 months. Importantly, LRRK2 kinase inhibition reversed these effects in LRRK2G2019S mice, but had minimal effect in wild-type mice, suggesting that LRRK2 kinase inhibition is likely to reverse specific disease processes in G2019S mutation carriers. Additional work may be necessary to determine the potential effect in non-carriers. Conclusions: This work supports a protective role of LRRK2 kinase inhibition in G2019S carriers and provides a rational workflow for systematic evaluation of brain-wide phenotypes in therapeutic development. [ABSTRACT FROM AUTHOR]

Published

2024

23. Exploring SVA Insertion Polymorphisms in Shaping Differential Gene Expressions in the Central Nervous System.

Author

Hughes, Lauren S., Fröhlich, Alexander, Pfaff, Abigail L., Bubb, Vivien J., Quinn, John P., and Kõks, Sulev

Subjects

*GENE expression, *CENTRAL nervous system, *WHOLE genome sequencing, *LOCUS (Genetics), *GENETIC regulation, *AMYOTROPHIC lateral sclerosis

Abstract

Transposable elements (TEs) are repetitive elements which make up around 45% of the human genome. A class of TEs, known as SINE-VNTR-Alu (SVA), demonstrate the capacity to mobilise throughout the genome, resulting in SVA polymorphisms for their presence or absence within the population. Although studies have previously highlighted the involvement of TEs within neurodegenerative diseases, such as Parkinson's disease and amyotrophic lateral sclerosis (ALS), the exact mechanism has yet to be identified. In this study, we used whole-genome sequencing and RNA sequencing data of ALS patients and healthy controls from the New York Genome Centre ALS Consortium to elucidate the influence of reference SVA elements on gene expressions genome-wide within central nervous system (CNS) tissues. To investigate this, we applied a matrix expression quantitative trait loci analysis and demonstrate that reference SVA insertion polymorphisms can significantly modulate the expression of numerous genes, preferentially in the trans position and in a tissue-specific manner. We also highlight that SVAs significantly regulate mitochondrial genes as well as genes within the HLA and MAPT loci, previously associated within neurodegenerative diseases. In conclusion, this study continues to bring to light the effects of polymorphic SVAs on gene regulation and further highlights the importance of TEs within disease pathology. [ABSTRACT FROM AUTHOR]

Published

2024

24. Parkinson-ALS with a novel MAPT variant.

Author

Ferrari, Camilla, Ingannato, Assunta, Matà, Sabrina, Ramat, Silvia, Caremani, Luca, Bagnoli, Silvia, Bessi, Valentina, Sorbi, Sandro, and Nacmias, Benedetta

Subjects

*PROGRESSIVE supranuclear palsy, *TAU proteins, *AMYOTROPHIC lateral sclerosis, *TUBULINS, *NEUROFIBRILLARY tangles, *FRONTOTEMPORAL dementia

Abstract

The mutations on microtubule associated protein tau (MAPT) gene manifest clinically with behavioural frontotemporal dementia (FTD), parkinsonism, such as progressive supranuclear palsy and corticobasal degeneration, and rarely with amyotrophic lateral sclerosis (ALS). FTD-parkinsonism and FTD-ALS are clinical overlaps included in the spectrum of MAPT mutation's phenotypes. The mutations on MAPT gene cause the dysfunction of tau protein determining its accumulation in neurofibrillary tangles. Recent data describe frequently the co-occurrence of the aggregation of tau protein and α-synuclein in patients with parkinsonism and Parkinson disease (PD), suggesting an interaction of the two proteins in determining neurodegenerative process. The sporadic description of PD-ALS clinical complex, known as Brait–Fahn–Schwarz disease, supports the hypothesis of common neuropathological pathways between different disorders. Here we report the case of a 54-year-old Italian woman with idiopathic PD later complicated by ALS carrying a novel MAPT variant (Pro494Leu). The variant is characterized by an amino acid substitution and is classified as damaging for MAPT functions. The case supports the hypothesis of tau dysfunction as the basis of multiple neurodegenerative disorders. [ABSTRACT FROM AUTHOR]

Published

2024

25. Galectin‐3 is upregulated in frontotemporal dementia patients with subtype specificity.

Author

Borrego–Écija, Sergi, Pérez‐Millan, Agnès, Antonell, Anna, Fort‐Aznar, Laura, Kaya‐Tilki, Elif, León‐Halcón, Alberto, Lladó, Albert, Molina‐Porcel, Laura, Balasa, Mircea, Juncà‐Parella, Jordi, Vitorica, Javier, Venero, Jose Luis, Deierborg, Tomas, Boza‐Serrano, Antonio, and Sánchez‐Valle, Raquel

Abstract

INTRODUCTION: Neuroinflammation is a major contributor to the progression of frontotemporal dementia (FTD). Galectin‐3 (Gal‐3), a microglial activation regulator, holds promise as a therapeutic target and potential biomarker. Our study aimed to investigate Gal‐3 levels in patients with FTD and assess its diagnostic potential. METHODS: We examined Gal‐3 levels in brain, serum, and cerebrospinal fluid (CSF) samples of patients with FTD and controls. Multiple linear regressions between Gal‐3 levels and other FTD markers were explored. RESULTS: Gal‐3 levels were increased significantly in patients with FTD, mainly across brain tissue and CSF, compared to controls. Remarkably, Gal‐3 levels were higher in cases with tau pathology than TAR‐DNA Binding Protein 43 (TDP‐43) pathology. Only MAPT mutation carriers displayed increased Gal‐3 levels in CSF samples, which correlated with total tau and 14‐3‐3. DISCUSSION: Our findings underscore the potential of Gal‐3 as a diagnostic marker for FTD, particularly in MAPT cases, and highlights the relation of Gal‐3 with neuronal injury markers. [ABSTRACT FROM AUTHOR]

Published

2024

26. BAG3 regulates the specificity of the recognition of specific MAPT species by NBR1 and SQSTM1.

Author

Lin, Heng, Sandkuhler, Sarah, Dunlea, Colleen, Rodwell-Bullock, Joel, King, Darron H, and Johnson, Gail V. W.

Subjects

BINDING site assay, ALZHEIMER'S disease, TAU proteins, POSTMORTEM changes, NEUROFIBRILLARY tangles, MICROTUBULE-associated proteins, COATED vesicles

Abstract

Macroautophagy/autophagy receptors are essential for the recognition and clearance of specific cargos by selective autophagy, which is essential for maintaining MAPT proteostasis. Previous studies have implicated different autophagy receptors in directing distinct species of MAPT to autophagy, but the underlying mechanisms have not been fully investigated. Here we examine how the autophagy receptors NBR1 and SQSTM1 differentially associate with specific forms of MAPT. In primary neurons depletion of NBR1, unlike depletion of SQSTM1, significantly increased phosphorylated MAPT levels. The specificity of the interactions was confirmed using in vitro binding assays with purified proteins. We provide direct evidence that the co-chaperone BAG3 promotes the preferential association of NBR1 with monomeric MAPT and SQSTM1 with oligomeric MAPT. Using an in vitro affinity-isolation assay, we show that SQSTM1 only binds to monomeric MAPT when BAG3 is absent and fails to bind when BAG3 is present. The opposite is true of NBR1; its association with monomeric MAPT was dependent on the presence of BAG3. Interestingly, in Alzheimer disease brain the association of NBR1 with BAG3 was significantly decreased. In a mouse model, ablation of BAG3 in neural cells disrupted the association of NBR1 with phosphorylated MAPT and led to increased levels of phosphorylated and oligomeric MAPT. Overall, our results uncover a novel role for BAG3 in regulating the specificity of selective autophagy receptors in targeting different species of MAPT and provide compelling evidence that BAG3 plays a key role in maintaining MAPT proteostasis. Abbreviations: AD: Alzheimer disease; BAG3: BCL2-associated athanogene 3; BSA: bovine serum albumin; CERAD: Consortium to Establish a Registry for Alzheimer's Disease; ESCRT: endosomal sorting complexes required for transport; GST: glutathione S-transferases; MAPT: microtubule-associated protein tau; NBR1: NBR1, autophagy cargo receptor; NFT: neurofibrillary tangles; PMI: postmortem interval; SQSTM1: sequestosome 1. [ABSTRACT FROM AUTHOR]

Published

2024

27. MAPT Mutations V337M and N297K Alter Organelle Trafficking in Frontotemporal Dementia Patient-Specific Motor Neurons.

Author

Hartmann, Christiane, Anskat, Marie, Ehrlich, Marc, Sterneckert, Jared, Pal, Arun, and Hermann, Andreas

Subjects

MOTOR neurons, FRONTOTEMPORAL dementia, CELL physiology, TAU proteins, MICROTUBULE-associated proteins, GLYCOGEN storage disease type II

Abstract

Frontotemporal dementia (FTD) is a neurodegenerative disease characterized by the progressive loss of neurons mainly in the frontal and temporal lobes of the brain. Mutations (e.g., V337M, N297K) in the microtubule-associated protein TAU (MAPT) are responsible 5–20% of familial FTD cases and have been associated with defects in organelle trafficking that plays a critical role in the proper function of cells, including transport of essential molecules and degradation of waste products. Due to the critical role of TAU mutations in microtubule stabilization and organelle transportation, it is of great interest to study these molecular mechanisms to develop effective therapeutic strategies. Therefore, herein, we analyzed mitochondrial and lysosomal trafficking in disease-specific spinal motor neurons by using live cell imaging in undirected (uncompartmentalized) and directed (compartmentalized) cell culture systems. While V337M neurons only expressed 3R TAU, the N297K mutant neurons expressed both 3R and 4R TAU. Axonal trafficking was affected differentially in V337M and N297 MAPT mutated neurons. These findings suggest that the MAPT mutations V337M and N297K impaired axon physiology differentially, which highlights the need for mutation- and/or 3R/4R TAU-specific therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2024

28. Rapid Phenotypic Antibiotic Susceptibility Profiling of Clinical Escherichia coli and Klebsiella pneumoniae Blood Cultures.

Author

Hefetz, Idan, Bardenstein, Rita, Rotem, Shahar, Zaide, Galia, Bilinsky, Gal, Shifman, Ohad, Zimhony, Oren, and Aloni-Grinstein, Ronit

Subjects

KLEBSIELLA pneumoniae, ESCHERICHIA coli, FRANCISELLA tularensis, ANTIBIOTICS, MICROBIAL sensitivity tests, YERSINIA pestis

Abstract

Bloodstream infections (BSI) are defined by the presence of viable bacteria or fungi, accompanied by systemic signs of infection. Choosing empirical therapy based solely on patient risk factors and prior antibiotic susceptibility test (AST) may lead to either ineffective treatment or unnecessarily broad-spectrum antibiotic exposure. In general, Clinical & Laboratory Standards Institute guideline-approved ASTs have a turnaround time of 48–72 h from sample to answer, a period that may result in a critical delay in the appropriate selection of therapy. Therefore, reducing the time required for AST is highly advantageous. We have previously shown that our novel rapid AST method, MAPt (Micro-Agar-PCR-test), accurately identifies susceptibility profiles for spiked bioterrorism agents like Bacillus anthracis, Yersinia pestis and Francisella tularensis directly from whole-blood and blood culture samples, even at low bacterial levels (500 CFU/mL). This study evaluated the performance of MAPt on routine bloodstream infection (BSI), focusing on Escherichia coli and Klebsiella pneumoniae isolates from clinical cultures, including resistant strains to some of the six tested antibiotics. Notably, MAPt yielded results exceeding 95% agreement with the standard hospital method within a significantly shorter timeframe of 6 h. These findings suggest significant potential for MAPt as a rapid and reliable BSI management tool. [ABSTRACT FROM AUTHOR]

Published

2024

29. Genetic background of cognitive decline in Parkinson's disease

Author

Antonela Blazekovic, Kristina Gotovac Jercic, Sabina Devedija, and Fran Borovecki

Subjects

Parkinson's disease, genes, cognition, polygenic score, MAPT, SNCA, Consciousness. Cognition, BF309-499

Abstract

Parkinson's disease (PD) is a complex disorder that is influenced by multiple genetic risk factors. There is a significant heterogeneity in PD presentation, both pathologically and clinically. Some of the most common and important symptoms affecting the patient are cognitive impairment and dementia. However, the genetic and biological basis underlying the differences in cognitive profiles, including the development of dementia in PD, is not yet well understood. Understanding the role of genes in cognitive outcomes is crucial for effective patient counseling and treatment. Research on familial PD has discovered more than 20 genes that can cause the disease. The identified genes responsible for familial cases of PD are LRRK2, PARK7, PINK1, PRKN, or SNCA gene, although there may be other genes that also contribute. Additionally, some of these genes may also play a role in cases that were previously thought to be sporadic. Currently, numerous well-described genes increase the risk of cognitive decline in PD, each with varying levels of penetrance. The aim of this review is to identify the relevant genetic factors that contribute to differences in cognition. We discuss the genes that may affect cognition and the challenges in establishing a clear genetic diagnostic and prognostic assessment. This article aims to demonstrate the complexity of the genetic background of cognition in PD and to present the different types of genotype changes that can impact cognition through various neurobiological mechanisms.

Published

2024

30. Neuronal MAPT expression is mediated by long-range interactions with cis-regulatory elements.

Author

Rogers, Brianne B., Anderson, Ashlyn G., Lauzon, Shelby N., Davis, M. Natalie, Hauser, Rebecca M., Roberts, Sydney C., Rodriguez-Nunez, Ivan, Trausch-Lowther, Katie, Barinaga, Erin A., Hall, Paige I., Knuesel, Matthew T., Taylor, Jared W., Mackiewicz, Mark, Roberts, Brian S., Cooper, Sara J., Rizzardi, Lindsay F., Myers, Richard M., and Cochran, J. Nicholas

Subjects

*GENE expression, *GENETIC variation, *FUNCTIONAL genomics, *MICROTUBULE-associated proteins, *TAUOPATHIES

Abstract

Tauopathies are a group of neurodegenerative diseases defined by abnormal aggregates of tau, a microtubule-associated protein encoded by MAPT. MAPT expression is near absent in neural progenitor cells (NPCs) and increases during differentiation. This temporally dynamic expression pattern suggests that MAPT expression could be controlled by transcription factors and cis -regulatory elements specific to differentiated cell types. Given the relevance of MAPT expression to neurodegeneration pathogenesis, identification of such elements is relevant to understanding disease risk and pathogenesis. Here, we performed chromatin conformation assays (HiC & Capture-C), single-nucleus multiomics (RNA-seq+ATAC-seq), bulk ATAC-seq, and ChIP-seq for H3K27ac and CTCF in NPCs and differentiated neurons to nominate candidate cis -regulatory elements (cCREs). We assayed these cCREs using luciferase assays and CRISPR interference (CRISPRi) experiments to measure their effects on MAPT expression. Finally, we integrated cCRE annotations into an analysis of genetic variation in neurodegeneration-affected individuals and control subjects. We identified both proximal and distal regulatory elements for MAPT and confirmed the regulatory function for several regions, including three regions centromeric to MAPT beyond the H1/H2 haplotype inversion breakpoint. We also found that rare and predicted damaging genetic variation in nominated CREs was nominally depleted in dementia-affected individuals relative to control subjects, consistent with the hypothesis that variants that disrupt MAPT enhancer activity, and thereby reduced MAPT expression, may be protective against neurodegenerative disease. Overall, this study provides compelling evidence for pursuing detailed knowledge of CREs for genes of interest to permit better understanding of disease risk. This study uses functional genomics approaches to assess candidate cis -regulatory elements (cCREs) for MAPT in neurons. The study suggests that impactful rare non-coding variants in MAPT cCREs (hypothesized to result in lower tau expression) may be protective against neurodegeneration, emphasizing the potential importance of rare non-coding variants in disease risk. [ABSTRACT FROM AUTHOR]

Published

2024

31. Association between Alzheimer’s disease, <italic>MAPT</italic> gene mutation and some biochemical biomarkers.

Author

Sen, Aysenur, Avsar, Orcun, Eliacik, Sinan, and Uysal Tan, Funda

Abstract

AbstractAlzheimer’s Disease (AD) is a multifactorial neurodegenerative disease and there is still no definitive treatment today. Early diagnosis of the disease is important, but there are almost no biomarkers that can be used in early diagnosis. The cerebrospinal fluid used in the diagnosis of the disease is not sufficient and is very difficult to obtain. Therefore, blood biomarkers that are less costly, less invasive, easily accessible, and can be used in long-term studies would be a better alternative. The aim of this study is to determine the relationship between Alzheimer’s Disease and P301L MAPT gene mutation, homocysteine, folate and uric acid. 101 Alzheimer’s patients and 101 healthy individuals were included in this study. Mutation analysis was performed using the Polymerase Chain Reaction-Restriction Fragment Length Polymorphism (PCR-RFLP) method with blood samples taken from the subjects. There was no significant difference between the patient and control groups in terms of homocysteine (p = 0.771), folate (p = 0.366) and uric acid (p = 0.860). When the genotypes were compared between the patient and control groups in terms of MAPT gene mutation (P301L), no statistically significant difference was detected (p = 0.081). There are very few studies in the literature investigating the relationship between Alzheimer’s disease and P301L MAPT gene mutation. Additionally, there is no study investigating the relationship between Alzheimer’s disease and homocysteine, folate, uric acid and P301L MAPT mutation in the Turkish population. We believe that this study has shed light on future studies. [ABSTRACT FROM AUTHOR]

Published

2024

32. MAPT Locus in Parkinson's Disease Patients of Ashkenazi Origin: A Stratified Analysis.

Author

Shani, Shachar, Gana-Weisz, Mali, Bar-Shira, Anat, Thaler, Avner, Gurevich, Tanya, Mirelman, Anat, Giladi, Nir, Alcalay, Roy N., Goldstein, Orly, and Orr-Urtreger, Avi

Subjects

*GENE expression, *PARKINSON'S disease, *LOCUS (Genetics), *MISSENSE mutation, *GENETIC variation, *WHOLE genome sequencing

Abstract

Introduction: MAPT locus is associated with Parkinson's disease (PD), which is located within a large inversion region of high linkage disequilibrium (LD). We aimed to determine whether the H2-haplotype protective effect and its effect size depends on the GBA1 or LRRK2 risk allele carrier status, and to further characterize genetic alterations that might contribute to its effect. Methods: LD analysis was performed using whole-genome sequencing data of 202 unrelated Ashkenazi Jewish (AJ) PDs. A haplotype-divergent variant was genotyped in a cohort of 1200 consecutively recruited AJ-PDs. The odd ratios were calculated using AJ-non-neuro cases from the gnomAD database as the controls in an un-stratified and a stratified manner according to the mutation carrier status, and the effect on the Age at Motor Symptom Onset (AMSO) was examined. Expression and splicing quantitative trait locus (eQTL and sQTL) analyses were carried out using brain tissues from a database. Results: The H2 haplotype exhibited significant association with PD protection, with a similar effect size in GBA1 carriers, LRRK2-G2019S carriers, and non-carriers (OR = 0.77, 0.69, and 0.82, respectively), and there was no effect on AMSO. The LD interval was narrowed to approximately 1.2 Mb. The H2 haplotype carried potential variants in candidate genes (MAPT and SPPL2C); structural deletions and segmental duplication (KANSL1); and variants affecting gene expression and intron excision ratio in brain tissues (LRRC37A/2). Conclusions: Our results demonstrate that H2 is associated with PD and its protective effect is not influenced by the GBA1/LRRK2 risk allele carrier status. This effect may be genetically complex, resulting from different levels of variations such as missense mutations in relevant genes, structural variations, epigenetic modifications, and RNA expression changes, which may operate independently or in synergy. [ABSTRACT FROM AUTHOR]

Published

2024

33. A Systematic Review of Empirical Mobile-Assisted Pronunciation Studies through a Perception–Production Lens

Author

Anne M. Stoughton and Okim Kang

Subjects

mobile-assisted pronunciation training, mobile-assisted language learning, MALL, MAPT, perception, production, Language and Literature

Abstract

The communicative approach to language learning, a teaching method commonly used in second language (L2) classrooms, places little to no emphasis on pronunciation training. As a result, mobile-assisted pronunciation training (MAPT) platforms provide an alternative to classroom-based pronunciation training. To date, there have been several meta-analyses and systematic reviews of mobile-assisted language learning (MALL) studies, but only a few of these meta-analyses have concentrated on pronunciation. To better understand MAPT’s impact on L2 learners’ perceptions and production of targeted pronunciation features, this study conducted a systematic review of the MAPT literature following PRISMA 2020 guidelines. Potential mobile-assisted articles were identified through searches of the ERIC, Educational Full Text, Linguistics and Language Behavior Abstract, MLI International, and Scopus databases and specific journal searches. Criteria for article inclusion in this study included the following: the article must be a peer-reviewed empirical or quasi-empirical research study using both experimental and control groups to assess the impact of pronunciation training. Pronunciation training must have been conducted via MALL or MAPT technologies, and the studies must have been published between 2014 and 2024. A total of 232 papers were identified; however, only ten articles with a total of 524 participants met the established criteria. Data pertaining to the participants used in the study (nationality and education level), the MPAT applications and platforms used, the pronunciation features targeted, the concentration on perception and/or production of these features, and the methods used for training and assessments were collected and discussed. Effect sizes using Cohen’s d were also calculated for each study. The findings of this review reveal that only two of the articles assessed the impact of MAPT on L2 learners’ perceptions of targeted features, with results indicating that the use of MPAT did not significantly improve L2 learners’ abilities to perceive segmental features. In terms of production, all ten articles assessed MPAT’s impact on L2 learners’ production of the targeted features. The results of these assessments varied greatly, with some studies indicating a significant and large effect of MAPT and others citing non-significant gains and negligible effect sizes. The variation in these results, in addition to differences in the types of participants, the targeted pronunciation features, and MAPT apps and platforms used, makes it difficult to conclude that MAPT has a significant impact on L2 learners’ production. Furthermore, the selected studies’ concentration on mostly segmental features (i.e., phoneme and word pronunciation) is likely to have had only a limited impact on participants’ intelligibility. This paper provides suggestions for further MAPT research, including increased emphasis on suprasegmental features and perception assessments, to further our understanding of the effectiveness of MAPT for pronunciation training.

Published

2024

34. Oligodendrocyte Dysfunction in Tauopathy: A Less Explored Area in Tau-Mediated Neurodegeneration

Author

Moumita Majumder and Debashis Dutta

Subjects

MAPT, oligodendrocytes, myelin, tauopathy, neurodegeneration, Cytology, QH573-671

Abstract

Aggregation of the microtubule-associated protein tau (MAPT) is the hallmark pathology in a spectrum of neurodegenerative disorders collectively called tauopathies. Physiologically, tau is an inherent neuronal protein that plays an important role in the assembly of microtubules and axonal transport. However, disease-associated mutations of this protein reduce its binding to the microtubule components and promote self-aggregation, leading to formation of tangles in neurons. Tau is also expressed in oligodendrocytes, where it has significant developmental roles in oligodendrocyte maturation and myelin synthesis. Oligodendrocyte-specific tau pathology, in the form of fibrils and coiled coils, is evident in major tauopathies including progressive supranuclear palsy (PSP), corticobasal degeneration (CBD), and Pick’s disease (PiD). Multiple animal models of tauopathy expressing mutant forms of MAPT recapitulate oligodendroglial tau inclusions with potential to cause degeneration/malfunction of oligodendrocytes and affecting the neuronal myelin sheath. Till now, mechanistic studies heavily concentrated on elucidating neuronal tau pathology. Therefore, more investigations are warranted to comprehensively address tau-induced pathologies in oligodendrocytes. The present review provides the current knowledge available in the literature about the intricate relations between tau and oligodendrocytes in health and diseases.

Published

2024

35. Pathologic correlates of aging-related tau astrogliopathy: ARTAG is associated with LATE-NC and cerebrovascular pathologies, but not with ADNC

Author

Yuriko Katsumata, Xian Wu, Khine Zin Aung, Kathryn Gauthreaux, Charles Mock, Shelley L. Forrest, Gabor G. Kovacs, and Peter T. Nelson

Subjects

Astrocytes, MAPT, Aging, Tauopathy, Amygdala, Small vessel disease, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Age-related tau astrogliopathy (ARTAG) is detectable in the brains of over one-third of autopsied persons beyond age 80, but the pathoetiology of ARTAG is poorly understood. Insights can be gained by analyzing risk factors and comorbid pathologies. Here we addressed the question of which prevalent co-pathologies are observed with increased frequency in brains with ARTAG. The study sample was the National Alzheimer's Coordinating Center (NACC) data set, derived from multiple Alzheimer's disease research centers (ADRCs) in the United States. Data from persons with unusual conditions (e.g. frontotemporal dementia) were excluded leaving 504 individual autopsied research participants, clustering from 20 different ADRCs, autopsied since 2020; ARTAG was reported in 222 (44.0%) of included participants. As has been shown previously, ARTAG was increasingly frequent with older age and in males. The presence and severity of other common subtypes of pathology that were previously linked to dementia were analyzed, stratifying for the presence of ARTAG. In logistical regression-based statistical models that included age and sex as covariates, ARTAG was relatively more likely to be found in brains with limbic-predominant age-related TDP-43 encephalopathy neuropathologic change (LATE-NC), and in brains with comorbid cerebrovascular pathology (arteriolosclerosis and/or brain infarcts). However, ARTAG was not associated with severe Alzheimer's disease neuropathologic change (ADNC), or primary age-related tauopathy (PART). In a subset analysis of 167 participants with neurocognitive testing data, there was a marginal trend for ARTAG pathology to be associated with cognitive impairment as assessed with MMSE scores (P = 0.07, adjusting for age, sex, interval between final clinic visit and death, and ADNC severity). A limitation of the study was that there were missing data about ARTAG pathologies, with incomplete operationalization of ARTAG according to anatomic region and pathologic subtypes (e.g., thorn-shaped or granular-fuzzy astrocytes). In summary, ARTAG was not associated with ADNC, whereas prior observations about ARTAG occurring with increased frequency in aging, males, and brains with LATE-NC were replicated. It remains to be determined whether the increased frequency of ARTAG in brains with comorbid cerebrovascular pathology is related to local infarctions or neuroinflammatory signaling, or with some other set of correlated factors including blood-brain barrier dysfunction.

Published

2024

36. Changes in Oxidised Phospholipids in Response to Oxidative Stress in Microtubule-Associated Protein Tau (MAPT) Mutant Dopamine Neurons

Author

Xanthe Bradford, Hugo J. R. Fernandes, and Stuart G. Snowden

Subjects

microtubule-associated protein tau, MAPT, oxidised phospholipids, oxidative stress, XBP1, unfolded protein response, Therapeutics. Pharmacology, RM1-950

Abstract

Microtubule-associated protein Tau (MAPT) is strongly associated with the development of neurodegenerative diseases. In addition to driving the formation of neurofibrillary tangles (NFT), mutations in the MAPT gene can also cause oxidative stress through hyperpolarisation of the mitochondria. This study explores the impact that MAPT mutation is having on phospholipid metabolism in iPSC-derived dopamine neurons, and to determine if these effects are exacerbated by mitochondrial and endoplasmic reticulum stress. Neurons that possessed a mutated copy of MAPT were shown to have significantly higher levels of oxo-phospholipids (Oxo-PL) than wild-type neurons. Oxidation of the hydrophobic fatty acid side chains changes the chemistry of the phospholipid leading to disruption of membrane function and potential cell lysis. In wild-type neurons, both mitochondrial and endoplasmic reticulum stress increased Oxo-PL abundance; however, in MAPT mutant neurons mitochondrial stress appeared to have a minimal effect. Endoplasmic reticulum stress, surprisingly, reduced the abundance of Oxo-PL in MAPT mutant dopamine neurons, and we postulate that this reduction could be modulated through hyperactivation of the unfolded protein response and X-box binding protein 1. Overall, the results of this study contribute to furthering our understanding of the regulation and impact of oxidative stress in Parkinson’s disease pathology.

Published

2024

37. MAPT Mutations V337M and N297K Alter Organelle Trafficking in Frontotemporal Dementia Patient-Specific Motor Neurons

Author

Christiane Hartmann, Marie Anskat, Marc Ehrlich, Jared Sterneckert, Arun Pal, and Andreas Hermann

Subjects

FTD, MAPT, TAU, organelle trafficking, mitochondria, lysosome, Biology (General), QH301-705.5

Abstract

Frontotemporal dementia (FTD) is a neurodegenerative disease characterized by the progressive loss of neurons mainly in the frontal and temporal lobes of the brain. Mutations (e.g., V337M, N297K) in the microtubule-associated protein TAU (MAPT) are responsible 5–20% of familial FTD cases and have been associated with defects in organelle trafficking that plays a critical role in the proper function of cells, including transport of essential molecules and degradation of waste products. Due to the critical role of TAU mutations in microtubule stabilization and organelle transportation, it is of great interest to study these molecular mechanisms to develop effective therapeutic strategies. Therefore, herein, we analyzed mitochondrial and lysosomal trafficking in disease-specific spinal motor neurons by using live cell imaging in undirected (uncompartmentalized) and directed (compartmentalized) cell culture systems. While V337M neurons only expressed 3R TAU, the N297K mutant neurons expressed both 3R and 4R TAU. Axonal trafficking was affected differentially in V337M and N297 MAPT mutated neurons. These findings suggest that the MAPT mutations V337M and N297K impaired axon physiology differentially, which highlights the need for mutation- and/or 3R/4R TAU-specific therapeutic approaches.

Published

2024

38. Rapid Phenotypic Antibiotic Susceptibility Profiling of Clinical Escherichia coli and Klebsiella pneumoniae Blood Cultures

Author

Idan Hefetz, Rita Bardenstein, Shahar Rotem, Galia Zaide, Gal Bilinsky, Ohad Shifman, Oren Zimhony, and Ronit Aloni-Grinstein

Subjects

bloodstream infection, Escherichia coli, Klebsiella pneumoniae, MAPt, antibiotic susceptibility, Therapeutics. Pharmacology, RM1-950

Abstract

Bloodstream infections (BSI) are defined by the presence of viable bacteria or fungi, accompanied by systemic signs of infection. Choosing empirical therapy based solely on patient risk factors and prior antibiotic susceptibility test (AST) may lead to either ineffective treatment or unnecessarily broad-spectrum antibiotic exposure. In general, Clinical & Laboratory Standards Institute guideline-approved ASTs have a turnaround time of 48–72 h from sample to answer, a period that may result in a critical delay in the appropriate selection of therapy. Therefore, reducing the time required for AST is highly advantageous. We have previously shown that our novel rapid AST method, MAPt (Micro-Agar-PCR-test), accurately identifies susceptibility profiles for spiked bioterrorism agents like Bacillus anthracis, Yersinia pestis and Francisella tularensis directly from whole-blood and blood culture samples, even at low bacterial levels (500 CFU/mL). This study evaluated the performance of MAPt on routine bloodstream infection (BSI), focusing on Escherichia coli and Klebsiella pneumoniae isolates from clinical cultures, including resistant strains to some of the six tested antibiotics. Notably, MAPt yielded results exceeding 95% agreement with the standard hospital method within a significantly shorter timeframe of 6 h. These findings suggest significant potential for MAPt as a rapid and reliable BSI management tool.

Published

2024

39. Dissecting the Clinical Heterogeneity and Genotype-Phenotype Correlations of MAPT Mutations: A Systematic Review

Author

Cristina Villa, Elisa Pellencin, Aurora Romeo, Giorgio Giaccone, Giacomina Rossi, Sara Prioni, and Paola Caroppo

Subjects

mapt, ftd, primary progressive aphasia, ad, cbs, psp, phenotypes, Biochemistry, QD415-436, Biology (General), QH301-705.5

Abstract

Background: Microtubule-associated protein tau (MAPT) mutations are one of the main causes of genetic Frontotemporal dementia (FTD) and are characterised by high clinical heterogeneity. A behavioural variant of FTD is the principal phenotype, but other rarer phenotypes are described, mostly reported as single cases. In this review, we provide an overview of the clinical phenotypes associated with MAPT mutations in order to define their characteristics and explore genotype-phenotype correlations. Methods: We performed systematic bibliographic research on the Pubmed database, focusing on articles published between 1998 and 2022. We analysed the clinical phenotype of 177 patients carrying MAPT mutations, focusing on the rarest ones. We performed a narrative synthesis of the results. Results: Regarding language phenotypes, the most frequent were the non-fluent variant and the semantic variant of Primary Progressive Aphasia (nfvPPA, svPPA), approximately in the same proportion. Almost 20% of the whole group of patients present a clinical phenotype belonging to the corticobasal syndrome-progressive supranuclear palsy (CBS-PSP) spectrum. While no clear genotype-phenotype correlation could be identified, some mutations were associated with a specific phenotype, while others gave origin to multiple clinical pictures and mixed phenotypes. Conclusions: A high clinical heterogeneity exists in FTD associated with MAPT mutations without a clear phenotype-genotype correlation in most cases. However, some characteristics can be helpful to drive genetic testing. Deep phenotyping of patients, together with functional studies of single mutations, particularly those associated with atypical phenotypes, are necessary to better understand the biological mechanisms underlying this clinical variability.

Published

2024

40. Clinical and molecular predictors of survival among atypical parkinsonian syndromes in a North African tertiary referral center.

Author

Sghaier, Ikram, Nasri, Amina, Atrous, Amal, Abida, Youssef, Gharbi, Alya, Souissi, Amira, Mrabet, Saloua, Ben Djebara, Mouna, Kacem, Imen, Gargouri-Berrechid, Amina, and Gouider, Riadh

Subjects

*GENETIC profile, *PARKINSONIAN disorders, *SURVIVAL rate, *HAPLOTYPES, *PATIENTS' families

Abstract

Atypical Parkinsonian Syndromes(APS) are challenging neurodegenerative disorders due to their heterogeneous phenotypic overlaps.So far,there are no validated biomarkers that can accurately predict disease progression,and survival studies were highly different and contradictory. To investigate clinical and molecular survival factors among Tunisian APS patients. A retrospective study included Tunisian APS-patients.Using clinical and molecular parameters,survival was explored by Kaplan-Meier analysis. We included 409-APS patients divided into 166-DLB,112-PSP,81-MSA and 50-CBS.Survival rate was similar in synucleinopathies, while it differed in tauopathies,being shorter in PSP compared to CBS.Median survival in DLB was different according to gender(p = 0.0048),early parkinsonism and cognitive disorders. Among MSA, prognosis was worse in MSA-C-patients(p = 0.012) and those with stridor(p = 0.0049),oculomotor and neuropsychiatric disorders. For tauopathies, survival was shorter in PSP-RS(p = 0.027),cerebellar phenotype, those with tremor and swallowing problems at onset, early parkinsonism and memory impairment. For CBS,prognosis was worse in patients with tremor,swallowing and cognitive problems.Significant differences were noted in terms of survival across APS non-carriers of APOE- ε4(p < 0.001) as well APS patients carriers of MAPT- H1.PSP patients had lower survival rate according to MAPT haplotype carriage. Moreover, the number of copies had an influence as patients with H1/H2- MAPT profile had better prognosis than those with H1/H1. This study determined survival rates in APS subgroups,which were comparable across synucleinopathies but shorter in PSP and longer in CBS.It also characterized demographic,phenotypic,and genetic profiles identifying more aggressive forms within APS subgroups.These findings address clinical gaps,aiding counseling for patients and families and guiding clinical management.Furthermore,they could facilitate patient stratification in clinical trials where mortality is an outcome measure. • Survival rates are similar in both synucleinopathies; PSP has a shorter median survival, while CBS has a longer one. • RBD in synucleinopathies, tremor and FOG in tauopathies, memory deficits, levodopa-resistance, APOE-ε4, and MAPT-H1 are linked to shorter survival rates in APS. • Tau expression is associated with decreased survival, and the MAPT H1 haplotype is linked to higher gene expression. [ABSTRACT FROM AUTHOR]

Published

2024

41. Galectin-3 is upregulated in frontotemporal dementia patients with subtype specificity

Author

Instituto de Salud Carlos III, European Commission, Generalitat de Catalunya, Fundación BBVA, Ministerio de Ciencia e Innovación (España), Lund University, Swedish Brain Foundation, Crafoord Foundation, Swedish Dementia Association, Greta and Johan Kocks Foundation, Olle Engkvist Foundation, Gamla Tjänarinnor Foundation, Swedish Medical Research Council, Swedish Parkinson Foundation, Anna och Edwin Bergers Stiftelse, Consejo Superior de Investigaciones Científicas [https://ror.org/02gfc7t72], Borrego-Écija, Sergi, Pérez-Millan, Agnès, Antonell, Anna, Fort-Aznar, Laura, Kaya-Tilki, Elif, León-Halcón, Alberto, Lladó, Albert, Molina-Porcel, Laura, Balasa, Mircea, Juncà-Parella, Jordi, Vitorica, Javier, Venero, Jose Luis, Deierborg, Tomas, Boza-Serrano, Antonio, Sánchez-Valle, Raquel, Instituto de Salud Carlos III, European Commission, Generalitat de Catalunya, Fundación BBVA, Ministerio de Ciencia e Innovación (España), Lund University, Swedish Brain Foundation, Crafoord Foundation, Swedish Dementia Association, Greta and Johan Kocks Foundation, Olle Engkvist Foundation, Gamla Tjänarinnor Foundation, Swedish Medical Research Council, Swedish Parkinson Foundation, Anna och Edwin Bergers Stiftelse, Consejo Superior de Investigaciones Científicas [https://ror.org/02gfc7t72], Borrego-Écija, Sergi, Pérez-Millan, Agnès, Antonell, Anna, Fort-Aznar, Laura, Kaya-Tilki, Elif, León-Halcón, Alberto, Lladó, Albert, Molina-Porcel, Laura, Balasa, Mircea, Juncà-Parella, Jordi, Vitorica, Javier, Venero, Jose Luis, Deierborg, Tomas, Boza-Serrano, Antonio, and Sánchez-Valle, Raquel

Abstract

Neuroinflammation is a major contributor to the progression of frontotemporal dementia (FTD). Galectin-3 (Gal-3), a microglial activation regulator, holds promise as a therapeutic target and potential biomarker. Our study aimed to investigate Gal-3 levels in patients with FTD and assess its diagnostic potential.

Published

2024

42. Clinical and neuroimaging characterization of the first frontotemporal dementia family carrying the MAPT p.K298E mutation

Author

Pozzi, F, Aprea, V, Giovannelli, G, Lattuada, F, Crivellaro, C, Bertola, F, Castelnovo, V, Canu, E, Filippi, M, Appollonio, I, Ferrarese, C, Agosta, F, Tremolizzo, L, Pozzi, Federico Emanuele, Aprea, Vittoria, Giovannelli, Ginevra, Lattuada, Francesca, Crivellaro, Cinzia, Bertola, Francesca, Castelnovo, Veronica, Canu, Elisa, Filippi, Massimo, Appollonio, Ildebrando, Ferrarese, Carlo, Agosta, Federica, Tremolizzo, Lucio, Pozzi, F, Aprea, V, Giovannelli, G, Lattuada, F, Crivellaro, C, Bertola, F, Castelnovo, V, Canu, E, Filippi, M, Appollonio, I, Ferrarese, C, Agosta, F, Tremolizzo, L, Pozzi, Federico Emanuele, Aprea, Vittoria, Giovannelli, Ginevra, Lattuada, Francesca, Crivellaro, Cinzia, Bertola, Francesca, Castelnovo, Veronica, Canu, Elisa, Filippi, Massimo, Appollonio, Ildebrando, Ferrarese, Carlo, Agosta, Federica, and Tremolizzo, Lucio

Abstract

We present an in-depth clinical and neuroimaging analysis of a family carrying the MAPT K298E mutation associated with frontotemporal dementia (FTD). Initial identification of this mutation in a single clinical case led to a comprehensive investigation involving four affected siblings allowing to elucidate the mutation's phenotypic expression. A 60-year-old male presented with significant behavioral changes and progressed rapidly, exhibiting speech difficulties and cognitive decline. Neuroimaging via FDG-PET revealed asymmetrical frontotemporal hypometabolism. Three siblings subsequently showed varied but consistent clinical manifestations, including abnormal behavior, speech impairments, memory deficits, and motor symptoms correlating with asymmetric frontotemporal atrophy observed in MRI scans. Based on the genotype–phenotype correlation, we propose that the p.K298E mutation results in early-onset behavioral variant FTD, accompanied by a various constellation of speech and motor impairment. This detailed characterization expands the understanding of the p.K298E mutation's clinical and neuroimaging features, underlining its role in the pathogenesis of FTD. Further research is crucial to comprehensively delineate the clinical and epidemiological implications of the MAPT p.K298E mutation.

Published

2024

43. Proximity labeling reveals dynamic changes in the SQSTM1 protein network.

Author

Rondón-Ortiz AN, Zhang L, Ash PEA, Basu A, Puri S, van der Spek SJF, Wang Z, Dorrian L, Emili A, and Wolozin B

Subjects

Humans, Protein Interaction Maps, tau Proteins metabolism, tau Proteins genetics, tau Proteins chemistry, Adaptor Proteins, Signal Transducing metabolism, Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing chemistry, Protein Binding, HEK293 Cells, Recombinant Fusion Proteins metabolism, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins chemistry, Sequestosome-1 Protein metabolism, Sequestosome-1 Protein genetics, Sequestosome-1 Protein chemistry

Abstract

Sequestosome1 (SQSTM1) is an autophagy receptor that mediates the degradation of intracellular cargo, including protein aggregates, through multiple protein interactions. These interactions form the SQSTM1 protein network, and these interactions are mediated by SQSTM1 functional interaction domains, which include LIR, PB1, UBA, and KIR. Technological advances in cell biology continue to expand our knowledge of the SQSTM1 protein network and the relationship between the actions of the SQSTM1 protein network in cellular physiology and disease states. Here we apply proximity profile labeling to investigate the SQSTM1 protein interaction network by fusing TurboID with the human protein SQSTM1 (TurboID::SQSTM1). This chimeric protein displayed well-established SQSTM1 features including production of SQSTM1 intracellular bodies, binding to known SQSTM1 interacting partners, and capture of novel SQSTM1 protein interactors. Strikingly, aggregated tau protein altered the protein interaction network of SQSTM1 to include many stress-associated proteins. We demonstrate the importance of the PB1 and/or UBA domains for binding network members, including the K18 domain of tau. Overall, our work reveals the dynamic landscape of the SQSTM1 protein network and offers a resource to study SQSTM1 function in cellular physiology and disease state., Competing Interests: Conflict of interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: BW is Co-Founder and CSO for Aquinnah Pharmaceuticals Inc., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

44. MAPT mutations associated with familial tauopathies lead to formation of conformationally distinct oligomers that have cross-seeding ability.

Author

Bhopatkar AA, Bhatt N, Haque MA, Xavier R, Fung L, Jerez C, and Kayed R

Subjects

Humans, Mutation, Protein Conformation, Protein Multimerization, Frontotemporal Dementia genetics, Frontotemporal Dementia metabolism, tau Proteins chemistry, tau Proteins genetics, tau Proteins metabolism, Tauopathies genetics, Tauopathies metabolism

Abstract

The microtubule associated protein, tau, is implicated in a multitude of neurodegenerative disorders that are collectively termed as tauopathies. These disorders are characterized by the presence of tau aggregates within the brain of afflicted individuals. Mutations within the MAPT gene that encodes the tau protein form the genetic backdrop for familial forms of tauopathies, such as frontotemporal dementia (FTD), but the molecular consequences of such alterations and their pathological effects are unclear. We sought to investigate the conformational properties of the aggregates of three tau mutants: A152T, P301L, and R406W, all implicated within FTD, and compare them to those of the native form (WT-Tau 2N4R). Our immunochemical analysis reveals that mutants and WT tau oligomers exhibit similar affinity for conformation-specific antibodies but have distinct morphology and secondary structure. Additionally, these oligomers possess different dye-binding properties and varying sensitivity to proteolytic processing. These results point to conformational variety among them. We then tested the ability of the mutant oligomers to cross-seed the aggregation of WT tau monomer. Using similar array of experiments, we found that cross-seeding with mutant aggregates leads to the formation of conformationally unique WT oligomers. The results discussed in this paper provide a novel perspective on the structural properties of oligomeric forms of WT tau 2N4R and its mutant, along with shedding some light on their cross-seeding behavior., (© 2024 The Author(s). Protein Science published by Wiley Periodicals LLC on behalf of The Protein Society.)

Published

2024

45. Mutational Landscape of Alzheimer's Disease and Frontotemporal Dementia: Regional Variances in Northern, Central, and Southern Italy.

Author

Saraceno C, Pagano L, Laganà V, Geviti A, Bagnoli S, Ingannato A, Mazzeo S, Longobardi A, Fostinelli S, Bellini S, Montesanto A, Binetti G, Maletta R, Nacmias B, and Ghidoni R

Subjects

Humans, Italy epidemiology, Female, Male, Middle Aged, Aged, Age of Onset, C9orf72 Protein genetics, Presenilin-2 genetics, Retrospective Studies, Amyloid beta-Protein Precursor genetics, Presenilin-1 genetics, Progranulins genetics, Adult, Aged, 80 and over, Genetic Predisposition to Disease, Alzheimer Disease genetics, Alzheimer Disease epidemiology, Frontotemporal Dementia genetics, Frontotemporal Dementia epidemiology, Frontotemporal Dementia pathology, Mutation, tau Proteins genetics

Abstract

Alzheimer's Disease (AD) and Frontotemporal Dementia (FTD) are the two major neurodegenerative diseases with distinct clinical and neuropathological profiles. The aim of this report is to conduct a population-based investigation in well-characterized APP , PSEN1 , PSEN2 , MAPT , GRN , and C9orf72 mutation carriers/pedigrees from the north, the center, and the south of Italy. We retrospectively analyzed the data of 467 Italian individuals. We identified 21 different GRN mutations, 20 PSEN1 , 11 MAPT , 9 PSEN2 , and 4 APP . Moreover, we observed geographical variability in mutation frequencies by looking at each cohort of participants, and we observed a significant difference in age at onset among the genetic groups. Our study provides evidence that age at onset is influenced by the genetic group. Further work in identifying both genetic and environmental factors that modify the phenotypes in all groups is needed. Our study reveals Italian regional differences among the most relevant AD/FTD causative genes and emphasizes how the collaborative studies in rare diseases can provide new insights to expand knowledge on genetic/epigenetic modulators of age at onset.

Published

2024

46. Proximity labeling reveals dynamic changes in the SQSTM1 protein network.

Author

Ortiz ANR, Zhang L, Ash PEA, Basu A, Puri S, van der Spek SJF, Wang Z, Dorrian L, Emili A, and Wolozin B

Abstract

Sequestosome1 (SQSTM1) is an autophagy receptor that mediates degradation of intracellular cargo, including protein aggregates, through multiple protein interactions. These interactions form the SQSTM1 protein network, and these interactions are mediated by SQSTM1 functional interaction domains, which include LIR, PB1, UBA and KIR. Technological advances in cell biology continue to expand our knowledge of the SQSTM1 protein network and of the relationship of the actions of the SQSTM1 protein network in cellular physiology and disease states. Here we apply proximity profile labeling to investigate the SQSTM1 protein interaction network by fusing TurboID with the human protein SQSTM1 (TurboID::SQSTM1). This chimeric protein displayed well-established SQSTM1 features including production of SQSTM1 intracellular bodies, binding to known SQSTM1 interacting partners, and capture of novel SQSTM1 protein interactors. Strikingly, aggregated tau protein altered the protein interaction network of SQSTM1 to include many stress-associated proteins. We demonstrate the importance of the PB1 and/or UBA domains for binding network members, including the K18 domain of tau. Overall, our work reveals the dynamic landscape of the SQSTM1 protein network and offers a resource to study SQSTM1 function in cellular physiology and disease state., Competing Interests: CONFLICT OF INTEREST BW is Co-Founder and CSO for Aquinnah Pharmaceuticals Inc.

Published

2024

47. Role of autophagy-related genes in liver cancer prognosis.

Author

Zhou, Yuling, Shan, Rong, Xie, Wangti, Zhou, Qiang, Yin, Qinghua, Su, Yuqi, Xiao, Jia, Luo, Pan, Yao, Xiang, Fang, Jianlong, Wen, Fang, Shen, Erdong, and Weng, Jie

Subjects

*LIVER cancer, *CANCER genes, *CANCER prognosis, *CANCER cell proliferation, *PROGNOSIS, *LIVER regeneration

Abstract

Autophagy, a highly conserved process of protein and organelle degradation, has emerged as a critical regulator in various diseases, including cancer progression. In the context of liver cancer, the predictive value of autophagy-related genes remains ambiguous. Leveraging chip datasets from the TCGA and GTEx databases, we identified 23 differentially expressed autophagy-related genes in liver cancer. Notably, five key autophagy genes, PRKAA2, BIRC5, MAPT, IGF1, and SPNS1, were highlighted as potential prognostic markers, with MAPT showing significant overexpression in clinical samples. In vitro cellular assays further demonstrated that MAPT promotes liver cancer cell proliferation, migration, and invasion by inhibiting autophagy and suppressing apoptosis. Subsequent in vivo studies further corroborated the pro-tumorigenic role of MAPT by suppressing autophagy. Collectively, our model based on the five key genes provides a promising tool for predicting liver cancer prognosis, with MAPT emerging as a pivotal factor in tumor progression through autophagy modulation. • Differential gene analysis identified 23 differentially expressed autophagy-related genes. • LASSO regression analysis selected five key autophagy-related genes associated with the prognosis of liver cancer patients. • These five key autophagy-related genes can accurately predict the prognosis of liver cancer patients. • MAPT can promote the growth of liver cancer in vivo by inhibiting autophagy. • This study provides a new theoretical basis for the early diagnosis and prognostic prediction of liver cancer. [ABSTRACT FROM AUTHOR]

Published

2024

48. Nobiletin, an active component of Wenyang Yiqi formula, alleviates constipation associated depression through targeting MAPT to inhibit the MAPK signaling pathway.

Author

Zhou, Qing, He, Zongqi, Yan, Shuai, Wang, Xiaopeng, and Wu, Bensheng

Abstract

Slow transit constipation (STC) is a common gastrointestinal disorder that is often accompanied by depression. Nobiletin is a natural compound that has been shown to have anti-inflammatory and anti-depressant effects. To study the effects of nobiletin extracted from Wenyang Yiqi Formula 19 (WYF) on STC accompanied by depression and the related mechanism in STC mouse models. In this study, the effects of nobiletin on STC accompanied by depression were investigated in both an STC animal model and an in vitro study. The animal model was induced by loperamide, and the in vitro study used Interstitial cells of Cajal (ICCs) isolated from STC mice. The efficacy of nobiletin was assessed by comparing various parameters, including stool particle counts, moisture content, intestinal propulsive rate, colon histopathology, microtubule-associated protein-tau (MAPT) expression in colon tissue, serum levels of TNF-α, IL-1β, IL-6, IFN-γ, and the levels of MAPK pathway-related proteins among three experimental groups. Nobiletin treatment significantly improved stool particle counts, moisture content, intestinal propulsive rate, and colon histopathology in the STC animal model. Nobiletin also decreased MAPT expression in colon tissue and serum levels of TNF-α, IL-1β, IL-6, IFN-γ, and the levels of MAPK pathway-related proteins. In the in vitro study, nobiletin treatment reversed the increased cell proliferation and cell apoptosis observed in ICC isolated from the STC model. The findings of this study indicate that nobiletin exhibits promising therapeutic potential in addressing STC accompanied by depression. This potential may be attributed to its ability to regulate the function of ICC by targeting MAPT. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

49. The six brain-specific TAU isoforms and their role in Alzheimer's disease and related neurodegenerative dementia syndromes.

Author

Buchholz S and Zempel H

Subjects

Humans, Tauopathies genetics, Tauopathies metabolism, Alternative Splicing, Neurodegenerative Diseases genetics, Neurodegenerative Diseases metabolism, Animals, Dementia genetics, Dementia metabolism, tau Proteins metabolism, Protein Isoforms, Alzheimer Disease metabolism, Alzheimer Disease genetics, Brain metabolism, Brain pathology

Abstract

Introduction: Alternative splicing of the human MAPT gene generates six brain-specific TAU isoforms. Imbalances in the TAU isoform ratio can lead to neurodegenerative diseases, underscoring the need for precise control over TAU isoform balance. Tauopathies, characterized by intracellular aggregates of hyperphosphorylated TAU, exhibit extensive neurodegeneration and can be classified by the TAU isoforms present in pathological accumulations., Methods: A comprehensive review of TAU and related dementia syndromes literature was conducted using PubMed, Google Scholar, and preprint server., Results: While TAU is recognized as key driver of neurodegeneration in specific tauopathies, the contribution of the isoforms to neuronal function and disease development remains largely elusive., Discussion: In this review we describe the role of TAU isoforms in health and disease, and stress the importance of comprehending and studying TAU isoforms in both, physiological and pathological context, in order to develop targeted therapeutic interventions for TAU-associated diseases., Highlights: MAPT splicing is tightly regulated during neuronal maturation and throughout life. TAU isoform expression is development-, cell-type and brain region specific. The contribution of TAU to neurodegeneration might be isoform-specific. Ineffective TAU-based therapies highlight the need for specific targeting strategies., (© 2024 The Authors. Alzheimer's & Dementia published by Wiley Periodicals LLC on behalf of Alzheimer's Association.)

Published

2024

50. Person-specific differences in ubiquitin-proteasome mediated proteostasis in human neurons.

Author

Hsieh YC, Augur ZM, Arbery M, Ashour N, Barrett K, Pearse RV 2nd, Tio ES, Duong DM, Felsky D, De Jager PL, Bennett DA, Seyfried NT, and Young-Pearse TL

Subjects

Humans, Proteostasis, Proteomics, Neurons metabolism, Proteasome Endopeptidase Complex metabolism, Ubiquitin metabolism

Abstract

Background: Impairment of the ubiquitin-proteasome system (UPS) has been implicated in abnormal protein accumulation in Alzheimer's disease. It remains unclear if genetic variation affects the intrinsic properties of neurons that render some individuals more vulnerable to UPS impairment., Methods: Induced pluripotent stem cell (iPSC)-derived neurons were generated from over 50 genetically variant and highly characterized participants of cohorts of aging. Proteomic profiling, proteasome activity assays, and Western blotting were employed to examine neurons at baseline and in response to UPS perturbation., Results: Neurons with lower basal UPS activity were more vulnerable to tau accumulation following mild UPS inhibition. Chronic reduction in proteasome activity in human neurons induced compensatory elevation of regulatory proteins involved in proteostasis and several proteasome subunits., Discussion: These findings reveal that genetic variation influences basal UPS activity in human neurons and differentially sensitizes them to external factors perturbing the UPS, leading to the accumulation of aggregation-prone proteins such as tau., Highlights: Polygenic risk score for AD is associated with the ubiquitin-proteasome system (UPS) in neurons. Basal proteasome activity correlates with aggregation-prone protein levels in neurons. Genetic variation affects the response to proteasome inhibition in neurons. Neuronal proteasome perturbation induces an elevation in specific proteins involved in proteostasis. Low basal proteasome activity leads to enhanced tau accumulation with UPS challenge., (© 2024 The Authors. Alzheimer's & Dementia published by Wiley Periodicals LLC on behalf of Alzheimer's Association.)

Published

2024