Your search keyword '"tau aggregation"' showing total 258 results

1. A novel monoclonal antibody generated by immunization with granular tau oligomers binds to tau aggregates at 423-430 amino acid sequence

Author

Yoshiyuki Soeda, Emi Hayashi, Naoko Nakatani, Shinsuke Ishigaki, Yuta Takaichi, Taro Tachibana, Yuichi Riku, James K. Chambers, Riki Koike, Moniruzzaman Mohammad, and Akihiko Takashima

Subjects

Tau aggregation, Granular tau oligomers, Antibody, C-terminal regions of tau, Medicine, Science

Abstract

Abstract Prior to the formation of amyloid fibrils, the pathological hallmark in tau-related neurodegenerative disease, tau monomers aggregate into a diverse range of oligomers. Granular tau oligomers, consisting of approximately 40 tau protein molecules, are present in the prefrontal cortex of patients at Braak stages I-II, preclinical stages of Alzheimer’s disease (AD). Antibodies to granular tau oligomers as antigens have not been reported. Therefore, we generated new rat monoclonal antibodies by immunization with granular tau oligomers. Three antibodies from different hybridoma clones showed stronger immunoreactivity to granular tau oligomers and tau fibrils compared with monomeric tau. Of the three antibodies, 2D6-2C6 showed 3000-fold greater immunoreactivity in P301L-tau transgenic (rTg4510) mice than in non-transgenic mice, while MC1 antibody, which detects pathological conformations of tau, showed a 5.5-fold increase. These results suggest that 2D6-2C6 recognizes aggregates more specifically than MC1. In AD subjects, 2D6-2C6 recognized neurofibrillary tangles and pretangles, and co-localized within AT8-positive cells containing phosphorylated tau aggregates. The epitope of 2D6-2C6 is the 423–430 amino acid (AA) sequence of C-terminal regions. Taken together, a novel monoclonal antibody, 2D6-2C6, generated by immunization with granular tau oligomers binds to tau aggregates at the 423–430 AA sequence.

Published

2024

2. Biophysical Studies of Amyloid-Binding Fluorophores to Tau AD Core Fibrils Formed without Cofactors.

Author

Freitas, Daniela P., Saavedra, Joana, Cardoso, Isabel, and Gomes, Cláudio M.

Subjects

*TRANSMISSION electron microscopy, *FLUORESCENT probes, *TAU proteins, *YIELD curve (Finance), *MOLECULAR spectra

Abstract

Tau is an intrinsically disordered protein involved in several neurodegenerative diseases where a common hallmark is the appearance of tau aggregates in the brain. One common approach to elucidate the mechanisms behind the aggregation of tau has been to recapitulate in vitro the self-assembly process in a fast and reproducible manner. While the seeding of tau aggregation is prompted by negatively charged cofactors, the obtained fibrils are morphologically distinct from those found in vivo. The Tau AD core fragment (TADC, tau 306–378) has emerged as a new model and potential solution for the cofactor-free in vitro aggregation of tau. Here, we use TADC to further study this process combining multiple amyloid-detecting fluorophores and fibril bioimaging. We confirmed by transmission electron microscopy that this fragment forms fibrils after quiescent incubation at 37 °C. We then employed a panel of eight amyloid-binding fluorophores to query the formed species by acquiring their emission spectra. The results obtained showed that nearly all dyes detect TADC self-assembled species. However, the successful monitoring of TADC aggregation kinetics was limited to three fluorophores (X-34, Bis-ANS, and pFTAA) which yielded sigmoidal curves but different aggregation half-times, hinting to different species being detected. Altogether, this study highlights the potential of using multiple extrinsic fluorescent probes, alone or in combination, as tools to further clarify mechanisms behind the aggregation of amyloidogenic proteins. [ABSTRACT FROM AUTHOR]

Published

2024

3. Unlocking therapeutic potential: the role of adamantane in drug discovery.

Author

Dane, Chianna, Cumbers, Grace A., Allen, Beau, Montgomery, Andrew P., Danon, Jonathan J., and Kassiou, Michael

Subjects

*DRUG discovery, *PHARMACEUTICAL chemistry, *CANNABINOID receptors, *ADAMANTANE, *METHYL aspartate receptors

Abstract

The unique structural and physicochemical properties of adamantane and its derivatives have attracted considerable attention in the field of medicinal chemistry. Substituting phenyl rings for adamantane or its derivatives has provided a promising strategy to introduce lipophilicity and escape the 'flat land' of modern drug discovery. Additionally, the unique three-dimensional structure of adamantane facilitates the precise positioning of substituents allowing for a more effective exploration of drug targets. Evidently, we have seen an increased use of adamantane in pharmaceutically relevant molecules. The following Account highlights our group's research in five drug discovery programs over the past 15 years showcasing the use of adamantane and its analogues in these studies. Adamantyl-containing compounds have proven to be effective ligands at a range of therapeutic targets. Its unique structural and physicochemical properties provide a promising strategy to increase lipophilicity and introduce three-dimensionality to a structure. The following Account highlights our group's research in five drug discovery programs showcasing the use of adamantane. (Image credit: Chianna Dane.) This article belongs to the 10th Anniversary Collection of RACI and AAS Award papers. [ABSTRACT FROM AUTHOR]

Published

2024

4. A novel monoclonal antibody generated by immunization with granular tau oligomers binds to tau aggregates at 423-430 amino acid sequence.

Author

Soeda, Yoshiyuki, Hayashi, Emi, Nakatani, Naoko, Ishigaki, Shinsuke, Takaichi, Yuta, Tachibana, Taro, Riku, Yuichi, Chambers, James K., Koike, Riki, Mohammad, Moniruzzaman, and Takashima, Akihiko

Subjects

*TAU proteins, *MONOCLONAL antibodies, *AMINO acid sequence, *OLIGOMERS, *NEUROFIBRILLARY tangles, *ALZHEIMER'S disease, *IMMUNIZATION

Abstract

Prior to the formation of amyloid fibrils, the pathological hallmark in tau-related neurodegenerative disease, tau monomers aggregate into a diverse range of oligomers. Granular tau oligomers, consisting of approximately 40 tau protein molecules, are present in the prefrontal cortex of patients at Braak stages I-II, preclinical stages of Alzheimer's disease (AD). Antibodies to granular tau oligomers as antigens have not been reported. Therefore, we generated new rat monoclonal antibodies by immunization with granular tau oligomers. Three antibodies from different hybridoma clones showed stronger immunoreactivity to granular tau oligomers and tau fibrils compared with monomeric tau. Of the three antibodies, 2D6-2C6 showed 3000-fold greater immunoreactivity in P301L-tau transgenic (rTg4510) mice than in non-transgenic mice, while MC1 antibody, which detects pathological conformations of tau, showed a 5.5-fold increase. These results suggest that 2D6-2C6 recognizes aggregates more specifically than MC1. In AD subjects, 2D6-2C6 recognized neurofibrillary tangles and pretangles, and co-localized within AT8-positive cells containing phosphorylated tau aggregates. The epitope of 2D6-2C6 is the 423–430 amino acid (AA) sequence of C-terminal regions. Taken together, a novel monoclonal antibody, 2D6-2C6, generated by immunization with granular tau oligomers binds to tau aggregates at the 423–430 AA sequence. [ABSTRACT FROM AUTHOR]

Published

2024

5. Neurodegeneration risk factor, EIF2AK3 (PERK), influences tau protein aggregation

Author

Park, Goonho, Xu, Ke, Chea, Leon, Kim, Kyle, Safarta, Lance, Song, Keon-Hyoung, Wu, Jian, Park, Soyoung, Min, Hyejung, Hiramatsu, Nobuhiko, Han, Jaeseok, and Lin, Jonathan H

Subjects

Biochemistry and Cell Biology, Biological Sciences, Neurodegenerative, Alzheimer's Disease, Acquired Cognitive Impairment, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Genetics, Alzheimer's Disease Related Dementias (ADRD), Prevention, Neurosciences, Frontotemporal Dementia (FTD), Aging, Dementia, Brain Disorders, Aetiology, 2.1 Biological and endogenous factors, Neurological, Humans, Disease Susceptibility, eIF-2 Kinase, Mutation, Protein Aggregates, Protein Aggregation, Pathological, Risk Factors, tau Proteins, Tauopathies, EIF2AK3, ER stress, PERK, eIF2α phosphorylation, integrated stress response, neurodegeneration, tau aggregation, tauopathy, unfolded protein response, Chemical Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences

Abstract

Tauopathies are neurodegenerative diseases caused by pathologic misfolded tau protein aggregation in the nervous system. Population studies implicate EIF2AK3 (eukaryotic translation initiation factor 2 alpha kinase 3), better known as PERK (protein kinase R-like endoplasmic reticulum kinase), as a genetic risk factor in several tauopathies. PERK is a key regulator of intracellular proteostatic mechanisms-unfolded protein response and integrated stress response. Previous studies found that tauopathy-associated PERK variants encoded functional hypomorphs with reduced signaling in vitro. But, it remained unclear how altered PERK activity led to tauopathy. Here, we chemically or genetically modulated PERK signaling in cell culture models of tau aggregation and found that PERK pathway activation prevented tau aggregation, whereas inhibition exacerbated tau aggregation. In primary tauopathy patient brain tissues, we found that reduced PERK signaling correlated with increased tau neuropathology. We found that tauopathy-associated PERK variants targeted the endoplasmic reticulum luminal domain; and two of these variants damaged hydrogen bond formation. Our studies support that PERK activity protects against tau aggregation and pathology. This may explain why people carrying hypomorphic PERK variants have increased risk for developing tauopathies. Finally, our studies identify small-molecule augmentation of PERK signaling as an attractive therapeutic strategy to treat tauopathies by preventing tau pathology.

Published

2023

6. Tau truncation in the pathogenesis of Alzheimer's disease: a narrative review.

Author

Dandan Chu, Xingyue Yang, Jing Wang, Yan Zhou, Jin-Hua Gu, Jin Miao, Feng Wu, and Fei Liu

Published

2024

7. Codon Pattern and Context Analysis in Genes Triggering Alzheimer's Disease and Latent Tau Protein Aggregation Post-Anesthesia Exhibited Unique Molecular Patterns Associated with Functional Aspects.

Author

Jiao, Liyuan, Jing, Ziye, Zhang, Wenjie, Su, Xuesen, Yan, Hualei, and Tian, Shouyuan

Subjects

*ALZHEIMER'S disease, *TAU proteins, *LATENT infection, *MILD cognitive impairment, *GENES, *MEMORY loss

Abstract

Background: Previous reports have demonstrated post-operative dementia and Alzheimer's disease (AD), and increased amyloid-β levels and tau hyperphosphorylation have been observed in animal models post-anesthesia. Objective: After surgical interventions, loss in memory has been observed that has been found linked with genes modulated after anesthesia. Present study aimed to study molecular pattern present in genes modulated post anesthesia and involved in characters progressing towards AD. Methods: In the present study, 17 transcript variants belonging to eight genes, which have been found to modulate post-anesthesia and contribute to AD progression, were envisaged for their compositional features, molecular patterns, and codon and codon context-associated studies. Results: The sequences' composition was G/C rich, influencing dinucleotide preference, codon preference, codon usage, and codon context. The G/C nucleotides being highly occurring nucleotides, CpGdinucleotides were also preferred; however, CpG was highly disfavored at p3-1 at the codon junction. The nucleotide composition of Cytosine exhibited a unique feature, and unlike other nucleotides, it did not correlate with codon bias. Contrarily, it correlated with the sequence lengths. The sequences were leucine-rich, and multiple leucine repeats were present, exhibiting the functional role of neuroprotection from neuroinflammation post-anesthesia. Conclusions: The analysis pave the way to elucidate unique molecular patterns in genes modulated during anesthetic treatment and might help ameliorate the ill effects of anesthetics in the future. [ABSTRACT FROM AUTHOR]

Published

2024

8. Application of single-molecule analysis to singularity phenomenon of cells.

Author

Michio Hiroshima, Hiroko Bannai, Gen Matsumoto, and Masahiro Ueda

Subjects

*MOLECULAR clusters, *MOLECULAR kinetics, *IMAGING systems, *IMAGE analysis, *ARTIFICIAL intelligence

Abstract

Single-molecule imaging in living cells is an effective tool for elucidating the mechanisms of cellular phenomena at the molecular level. However, the analysis was not designed for throughput and requires high expertise, preventing it from reaching large scale, which is necessary when searching for rare cells that induce singularity phenomena. To overcome this limitation, we have automated the imaging procedures by combining our own focusing device, artificial intelligence, and robotics. The apparatus, called automated in-cell single-molecule imaging system (AiSIS), achieves a throughput that is a hundred-fold higher than conventional manual imaging operations, enabling the analysis of molecular events by individual cells across a large population. Here, using AiSIS, we demonstrate the single-molecule imaging of molecular behaviors and reactions related to tau protein aggregation, which is considered a singularity phenomenon in neurological disorders. Changes in the dynamics and kinetics of molecular events were observed inside and on the basal membrane of cells after the induction of aggregation. Additionally, to detect rare cells based on the molecular behavior, we developed a method to identify the state of individual cells defined by the quantitative distribution of molecular mobility and clustering. Using this method, cellular variations in receptor behavior were shown to decrease following ligand stimulation. This cell state analysis based on large-scale single-molecule imaging by AiSIS will advance the study of molecular mechanisms causing singularity phenomena. [ABSTRACT FROM AUTHOR]

Published

2024

9. Preclinical characterization and IND‐enabling safety studies for PNT001, an antibody that recognizes cis‐pT231 tau.

Author

Foster, Kelly, Manca, Matteo, McClure, Kim, Koivula, Pyry, Trojanowski, John Q., Havas, Daniel, Chancellor, Sarah, Goldstein, Lee, Brunden, Kurt R., Kraus, Allison, and Ahlijanian, Michael K.

Abstract

BACKGROUND: The cis‐conformer of tau phosphorylated at threonine‐231 (cis‐pT231 tau) is hypothesized to contribute to tauopathies. PNT001 is a humanized, monoclonal antibody that recognizes cis‐pT231 tau. PNT001 was characterized to assess clinical development readiness. METHODS: Affinity and selectivity were assessed by surface plasmon resonance and enzyme‐linked immunosorbent assay. Immunohistochemistry (IHC) was performed with brain sections from human tauopathy patients and controls. Real‐time quaking‐induced conversion (RT‐QuIC) was used to assess whether PNT001 reduced tau seeds from Tg4510 transgenic mouse brain. Murine PNT001 was evaluated in vivo in the Tg4510 mouse. RESULTS: The affinity of PNT001 for a cis‐pT231 peptide was 0.3 to 3 nM. IHC revealed neurofibrillary tangle‐like structures in tauopathy patients with no detectable staining in controls. Incubation of Tg4510 brain homogenates with PNT001 lowered seeding in RT‐QuIC. Multiple endpoints were improved in the Tg4510 mouse. No adverse findings attributable to PNT001 were detected in Good Laboratory Practice safety studies. DISCUSSION: The data support clinical development of PNT001 in human tauopathies. [ABSTRACT FROM AUTHOR]

Published

2023

10. Fluorescently Labelled Tau Protein

Author

Saurabh Awasthi, Liviana Mummolo, Yuanjie Li, Louise Bryan, Peter Niraj Nirmalraj, Sandor Balog, Jerry Yang, and Michael Mayer

Subjects

Alzheimer's disease, Sortase A, Tau aggregation, Chemistry, QD1-999

Published

2023

11. Effect of exogenous trivalent iron ions on tau phosphorylation and aggregation in SH-SY5Y cells

Author

Zhina ZHANG, Zhuoran WANG, Mingxuan YANG, Yanli ZHANG, Guowei LIU, Shu FANG, Qiang SU, Qiao NIU, and Junhong GUO

Subjects

sh-sy5y cell, exogenous trivalent iron ion, neurofibrillary tangle, tau hyperphosphorylation, tau aggregation, Medicine (General), R5-920, Toxicology. Poisons, RA1190-1270

Abstract

BackgroundA large amount of iron deposition in the brain can cause neuronal damage by inducing oxidative stress, neuroinflammation, and abnormal mitochondrial function. In addition, iron deposition is also reported to be closely related to the pathogenesis of Alzheimer's disease (AD). The neurofibrillary tangles aggregated by tau hyperphosphorylation are one of the important pathological features of AD. ObjectiveTo investigate potential effect of exogenous trivalent iron ions on neuronal activity in human neuroblastoma (SH-SY5Y) cells and tau hyperphosphorylation and aggregation. MethodsSH-SY5Y cells were treated with ferric chloride (FeCl3) at four concentrations (10, 100, 200, and 400 mg·L−1). Cell survival rate was then detected by CCK8 assay. Intracellular iron content was determined prussian blue (Perl's) by iron staining after 24 h exposure to FeCl3 at 10 or 200 mg·L−1. Transfection of tau-P301L plasmid was conducted to construct an AD-like cell model for tau overexpression. The differences in the expression of the phosphorylated tau (p-tau) protein in SH-SY5Y cells and SH-SY5Y cells with tau overexpression were detected by Western blotting after 24 h exposure to FeCl3 at 10 and 200 mg·L−1. After dilution with phosphate buffered saline (PBS), FeCl3, human tauR3, and FeCl3 + tauR3 were incubated at 37℃, and the fluorescence intensity reflecting tau aggregation level was measured by thioflavin T(ThT) method at 12, 24, 36, 48, 60, 72, 84, and 96 h, respectively. Meanwhile, after 96 h coincubation of FeCl3 and tauR3, the fibers formed by tau aggregation were observed under a transmission electron microscope (TEM). ResultsAfter 24 h of FeCl3 exposure, the cell survival rate of SH-SY5Y cells among all groups was statistically different (F=8.63, P

Published

2023

12. A 3D human co-culture to model neuron-astrocyte interactions in tauopathies

Author

Kevin L. Batenburg, Claudia Sestito, Paulien Cornelissen-Steijger, Jan R. T. van Weering, Leo S. Price, Vivi M. Heine, and Wiep Scheper

Subjects

hiPSC-derived neurons, Astrocytes, Neuron-astrocyte interaction, 3D co-culture, Tau aggregation, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Abstract Background Intraneuronal tau aggregation is the major pathological hallmark of neurodegenerative tauopathies. It is now generally acknowledged that tau aggregation also affects astrocytes in a cell non-autonomous manner. However, mechanisms involved are unclear, partly because of the lack of models that reflect the situation in the human tauopathy brain. To accurately model neuron-astrocyte interaction in tauopathies, there is a need for a model that contains both human neurons and human astrocytes, intraneuronal tau pathology and mimics the three-dimensional architecture of the brain. Results Here we established a novel 100–200 µm thick 3D human neuron/astrocyte co-culture model of tau pathology, comprising homogenous populations of hiPSC-derived neurons and primary human astrocytes in microwell format. Using confocal, electron and live microscopy, we validate the procedures by showing that neurons in the 3D co-culture form pre- and postsynapses and display spontaneous calcium transients within 4 weeks. Astrocytes in the 3D co-culture display bipolar and stellate morphologies with extensive processes that ensheath neuronal somas, spatially align with axons and dendrites and can be found perisynaptically. The complex morphology of astrocytes and the interaction with neurons in the 3D co-culture mirrors that in the human brain, indicating the model’s potential to study physiological and pathological neuron-astrocyte interaction in vitro. Finally, we successfully implemented a methodology to introduce seed-independent intraneuronal tau aggregation in the 3D co-culture, enabling study of neuron-astrocyte interaction in early tau pathogenesis. Conclusions Altogether, these data provide proof-of-concept for the utility of this rapid, miniaturized, and standardized 3D model for cell type-specific manipulations, such as the intraneuronal pathology that is associated with neurodegenerative disorders.

Published

2023

13. Development and Characterization of Mouse-Specific Anti-Tau Monoclonal Antibodies: Relevance for Analysis of Murine Tau in Cerebrospinal Fluid.

Author

Rodrigues Martins, Dina, Vandermeeren, Marc, Van Kolen, Kristof, Brepoels, Eddy, Borgers, Marianne, Wintmolders, Cindy, Delay, Charlotte, Bottelbergs, Astrid, Mercken, Marc, and Theunis, Clara

Subjects

*CEREBROSPINAL fluid, *MONOCLONAL antibodies, *TAU proteins, *ALZHEIMER'S disease, *TAUOPATHIES

Abstract

Background: Clearance of tau seeds by immunization with tau antibodies is currently evaluated as therapeutic strategy to block the spreading of tau pathology in Alzheimer's disease and other tauopathies. Preclinical evaluation of passive immunotherapy is performed in different cellular culture systems and in wild-type and human tau transgenic mouse models. Depending on the preclinical model used, tau seeds or induced aggregates can either be of mouse, human or mixed origin. Objective: We aimed to develop human and mouse tau-specific antibodies to discriminate between the endogenous tau and the introduced form in preclinical models. Methods: Using hybridoma technology, we developed human and mouse tau-specific antibodies that were then used to develop several assays to specifically detect mouse tau. Results: Four antibodies, mTau3, mTau5, mTau8, and mTau9, with a high degree of specificity for mouse tau were identified. Additionally, their potential application in highly sensitive immunoassays to measure tau in mouse brain homogenate and cerebrospinal fluid is illustrated, as well as their application for specific endogenous mouse tau aggregation detection. Conclusion: The antibodies reported here can be very important tools to better interpret the results obtained from different model systems as well as to study the role of endogenous tau in tau aggregation and pathology observed in the diverse mouse models available. [ABSTRACT FROM AUTHOR]

Published

2023

14. Human Tau Aggregates Are Permissive to Protein Synthesis-Dependent Memory in Drosophila Tauopathy Models.

Author

Vourkou, Ergina, Rouiz Ortega, Eva D., Mahajan, Sumeet, Mudher, Amrit, and Skoulakis, Efthimios M. C.

Subjects

*TAU proteins, *TAUOPATHIES, *DROSOPHILA, *ORAL drug administration, *METHYLENE blue, *ALZHEIMER'S disease

Abstract

Tauopathies including Alzheimer's disease, are characterized by progressive cognitive decline, neurodegeneration, and intraneuronal aggregates comprised largely of the axonal protein Tau. It has been unclear whether cognitive deficits are a consequence of aggregate accumulation thought to compromise neuronal health and eventually lead to neurodegeneration. We use the Drosophila tauopathy model and mixed-sex populations to reveal an adult onset pan-neuronal Tau accumulation-dependent decline in learning efficacy and a specific defect in protein synthesis-dependent memory (PSD-M), but not in its protein synthesis-independent variant. We demonstrate that these neuroplasticity defects are reversible on suppression of new transgenic human Tau expression and surprisingly correlate with an increase in Tau aggregates. Inhibition of aggregate formation via acute oral administration of methylene blue results in re-emergence of deficient memory in animals with suppressed human Tau (hTau)0N4R expression. Significantly, aggregate inhibition results in PSD-M deficits in hTau0N3R-expressing animals, which present elevated aggregates and normal memory if untreated with methylene blue. Moreover, methylene blue--dependent hTau0N4R aggregate suppression within adult mushroom body neurons also resulted in emergence of memory deficits. Therefore, deficient PSD-M on human Tau expression in the Drosophila CNS is not a consequence of toxicity and neuronal loss because it is reversible. Furthermore, PSD-M deficits do not result from aggregate accumulation, which appears permissive, if not protective of processes underlying this memory variant. [ABSTRACT FROM AUTHOR]

Published

2023

15. Photo-Excited Toluidine Blue Disaggregates the Repeat Tau and Modulates End-Binding Protein EB1, Cytoskeletal Structure in Neuronal Cells.

Author

Chinnathambi, Subashchandrabose, Dubey, Tushar, and Chandrashekar, Madhura

Subjects

*TOLUIDINE blue, *TAU proteins, *CELL anatomy, *ALZHEIMER'S disease, *ELECTRON spectroscopy, *CYTOSKELETON

Abstract

Background/Aims: Alzheimer's disease is a progressive neurological disorder characterized by the intracellular accumulation of Tau protein aggregates. In the present work, we studied the effect of Toluidine Blue and photo-excited Toluidine Blue on the aggregation of repeat Tau using in vitro assays. Methods: The in vitro experiments were carried out on recombinant repeat Tau which was purified by cation exchange chromatography. The ThS fluorescence analysis was used to study the aggregation kinetics of Tau. CD spectroscopy and electron microscopy were used to study the secondary structure and morphology of Tau respectively. The actin cytoskeleton modulation was studied in Neuro2a cells with help of immunofluorescent microscopy. Results: Results showed that Toluidine Blue efficiently inhibited the formation of higher-order aggregates, which was evidenced by Thioflavin S fluorescence assay, SDSPAGE, and TEM. Immunofluorescence studies on the cytoskeleton of Neuro2a cells showed that Toluidine Blue and photo-excited Toluidine Blue treatment at a non-toxic concentration of 0.5 µM stimulated the formation of actin-rich lamellipodia and filopodia structures. Tubulin networks were also differentially modulated after the treatment of Toluidine Blue and photoexcited Toluidine Blue. End-binding protein 1 (EB1) levels were observed to increase after Toluidine Blue and photo-excited Toluidine Blue treatment indicating accelerated microtubule polymerization. Conclusion: The overall study suggested that Toluidine Blue inhibited the aggregation of soluble Tau and photo-excited Toluidine Blue disaggregated the pre-formed Tau filaments. In our study, TB and PE-TB were observed to be potent against Tau aggregation. We observed a distinctive modulation of actin, tubulin networks, and EB1 levels after TB and PE-TB treatment, which suggested that TB and PE-TB have potency against cytoskeleton deformities. [ABSTRACT FROM AUTHOR]

Published

2023

16. A 3D human co-culture to model neuron-astrocyte interactions in tauopathies.

Author

Batenburg, Kevin L., Sestito, Claudia, Cornelissen-Steijger, Paulien, van Weering, Jan R. T., Price, Leo S., Heine, Vivi M., and Scheper, Wiep

Subjects

*TAUOPATHIES, *ASTROCYTES, *NEUROFIBRILLARY tangles, *NEURODEGENERATION, *TAU proteins, *ELECTRON microscopy, *DENDRITES

Abstract

Background: Intraneuronal tau aggregation is the major pathological hallmark of neurodegenerative tauopathies. It is now generally acknowledged that tau aggregation also affects astrocytes in a cell non-autonomous manner. However, mechanisms involved are unclear, partly because of the lack of models that reflect the situation in the human tauopathy brain. To accurately model neuron-astrocyte interaction in tauopathies, there is a need for a model that contains both human neurons and human astrocytes, intraneuronal tau pathology and mimics the three-dimensional architecture of the brain. Results: Here we established a novel 100–200 µm thick 3D human neuron/astrocyte co-culture model of tau pathology, comprising homogenous populations of hiPSC-derived neurons and primary human astrocytes in microwell format. Using confocal, electron and live microscopy, we validate the procedures by showing that neurons in the 3D co-culture form pre- and postsynapses and display spontaneous calcium transients within 4 weeks. Astrocytes in the 3D co-culture display bipolar and stellate morphologies with extensive processes that ensheath neuronal somas, spatially align with axons and dendrites and can be found perisynaptically. The complex morphology of astrocytes and the interaction with neurons in the 3D co-culture mirrors that in the human brain, indicating the model's potential to study physiological and pathological neuron-astrocyte interaction in vitro. Finally, we successfully implemented a methodology to introduce seed-independent intraneuronal tau aggregation in the 3D co-culture, enabling study of neuron-astrocyte interaction in early tau pathogenesis. Conclusions: Altogether, these data provide proof-of-concept for the utility of this rapid, miniaturized, and standardized 3D model for cell type-specific manipulations, such as the intraneuronal pathology that is associated with neurodegenerative disorders. [ABSTRACT FROM AUTHOR]

Published

2023

17. Stabilization of Monomeric Tau Protein by All D-Enantiomeric Peptide Ligands as Therapeutic Strategy for Alzheimer's Disease and Other Tauopathies.

Author

Altendorf, Tim, Gering, Ian, Santiago-Schübel, Beatrix, Aghabashlou Saisan, Selma, Tamgüney, Gültekin, Tusche, Markus, Honold, Dominik, Schemmert, Sarah, Hoyer, Wolfgang, Mohrlüder, Jeannine, and Willbold, Dieter

Subjects

*TAU proteins, *ALZHEIMER'S disease, *TAUOPATHIES, *PEPTIDES, *POST-translational modification, *NEURODEGENERATION

Abstract

Alzheimer's disease and other tauopathies are the world's leading causes of dementia and memory loss. These diseases are thought to be caused by the misfolding and aggregation of the intracellular tau protein, ultimately leading to neurodegeneration. The tau protein is involved in a multitude of different neurodegenerative diseases. During the onset of tauopathies, tau undergoes structural changes and posttranslational modifications and aggregates into amyloid fibrils that are able to spread with a prion-like behavior. Up to now, there is no therapeutic agent which effectively controls or reverses the disease. Most of the therapeutics that were developed and underwent clinical trials targeted misfolded or aggregated forms of tau. In the current manuscript, we present the selection and characterization of two all D-enantiomeric peptides that bind monomeric tau protein with a low nanomolar KD, stabilize tau in its monomeric intrinsically disordered conformation, and stop the conversion of monomers into aggregates. We show that the effect of the two all D-enantiomeric peptides is strong enough to stop ongoing tau aggregation in vitro and is able to significantly reduce tau fibril assembly in cell culture. Both compounds may serve as new lead components for the development of therapeutic agents against Alzheimer's disease and other tauopathies. [ABSTRACT FROM AUTHOR]

Published

2023

18. Macrocyclic peptides derived from AcPHF6* and AcPHF6 to selectively modulate the Tau aggregation.

Author

Dangi, Abha, Qureshi, Tazeen, Chinnathambi, Subashchandrabose, and Kiran Marelli, Udaya

Subjects

*CYCLIC peptides, *PEPTIDES, *AMINO acids, *TAU proteins, *DRUG design, *HEXAPEPTIDES

Abstract

[Display omitted] • Designed and synthesized 10 macrocyclic 14-mer peptides based on Tau PHF peptides. • NMR supported antiparallel β-sheet structure in all peptides, validating the design. • P3 and P8 showed the highest and lowest self-aggregation tendencies, respectively. • In cross-aggregation studies, P3 promoted PHF aggregation, P8 selectively reduced it. • P3 and P8 exhibited pro- and anti-aggregation effects even on Tau macromolecule. Ten macrocyclic peptides, each comprising 14 amino acids, were designed and synthesized based on the Tau aggregation model hexapeptides AcPHF6* and AcPHF6. The design took into account the aggregation tendencies of each residue in AcPHF6* and AcPHF6, their aggregation models, while employing peptide-based structural design principles including N- methylation to promote turns and to block hydrogen bond propagation and elongation of the aggregation chain. NMR analysis supported that all these peptides adopted an antiparallel β-sheet conformation. Self-aggregation studies characterized the aggregation properties of these peptides, identifying two peptides with the highest (P3) and lowest (P8) aggregation tendencies. In cross-aggregation studies with the parent peptides AcPHF6* and AcPHF6, P3 and P8 were found to promote and reduce aggregation, respectively. Furthermore, P3 and P8 demonstrated an enhancement and diminution effect on the aggregation of K18wt, indicating their capacity to modulate aggregation even at the macromolecular level. Thus, the two simple peptides, P3 and P8 selectively exhibit pro- or anti-aggregation effects on PHF peptides and Tau. This study, has thus developed structurally well-defined non-complex peptides, derived from AcPHF6* and AcPHF6, to modulate Tau aggregation as desired, offering applications in Tau model studies and the development of Tau aggregation inhibitors or promoters. [ABSTRACT FROM AUTHOR]

Published

2024

19. Liquid-liquid phase separation of protein tau: An emerging process in Alzheimer's disease pathogenesis

Author

Hassan Ainani, Najat Bouchmaa, Reda Ben Mrid, and Rachid El Fatimy

Subjects

Phase separation, Membrane-less organelle, Tau aggregation, Liquid droplet, Alzheimer's disease, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Metabolic reactions within cells occur in various isolated compartments with or without borders, the latter being known as membrane-less organelles (MLOs). The MLOs show liquid-like properties and are formed by a process known as liquid-liquid phase separation (LLPS). MLOs contribute to different molecules interactions such as protein-protein, protein-RNA, and RNA-RNA driven by various factors, such as multivalency of intrinsic disorders. MLOs are involved in several cell signaling pathways such as transcription, immune response, and cellular organization. However, disruption of these processes has been found in different pathologies. Recently, it has been demonstrated that protein aggregates, a characteristic of some neurodegenerative diseases, undergo similar phase separation. Tau protein is known as a major neurofibrillary tangles component in Alzheimer's disease (AD). This protein can undergo phase separation to form a MLO known as tau droplet in vitro and in vivo, and this process can be facilitated by several factors, including crowding agents, RNA, and phosphorylation. Tau droplet has been shown to mature into insoluble aggregates suggesting that this process may precede and induce neurodegeneration in AD. Here we review major factors involved in liquid droplet formation within a cell. Additionally, we highlight recent findings concerning tau aggregation following phase separation in AD, along with the potential therapeutic strategies that could be explored in this process against the progression of this pathology.

Published

2023

20. Hexameric Aggregation Nucleation Core Sequences and Diversity of Pathogenic Tau Strains.

Author

Wu, Ling, Madhavan, Sidharth S., Tan, Christopher, and Xu, Bin

Subjects

TAU proteins, PROGRESSIVE supranuclear palsy, ALZHEIMER'S disease, AMINO acid sequence, TAUOPATHIES, NUCLEATION

Abstract

Tau aggregation associates with multiple neurodegenerative diseases including Alzheimer's disease and rare tauopathies such as Pick's disease, progressive supranuclear palsy, and corticobasal degeneration. The molecular and structural basis of tau aggregation and related diverse misfolded tau strains are not fully understood. To further understand tau-protein aggregation mechanisms, we performed systematic truncation mutagenesis and mapped key segments of tau proteins that contribute to tau aggregation, where it was determined that microtubule binding domains R2 and R3 play critical roles. We validated that R2- or R3-related hexameric PHF6 and PHF6* peptide sequences are necessary sequences that render tau amyloidogenicity. We also determined that the consensus VQI peptide sequence is not sufficient for amyloidogenicity. We further proposed single- and dual-nucleation core-based strain classifications based on recent cryo-EM structures. We analyzed the structural environment of the hexameric peptide sequences in diverse tau strains in tauopathies that, in part, explains why the VQI consensus core sequence is not sufficient to induce tau aggregation. Our experimental work and complementary structural analysis highlighted the indispensible roles of the hexameric core sequences, and shed light on how the interaction environment of these core sequences contributes to diverse pathogenic tau-strains formation in various tauopathy brains. [ABSTRACT FROM AUTHOR]

Published

2022

21. Investigation of the role of prolines 232/233 in RTPPK motif in tau protein aggregation: An in vitro study.

Author

Akbari, Vali, Mohammadi, Soheila, Mehrabi, Masomeh, Ghobadi, Sirous, Farrokhi, Alireza, and Khodarahmi, Reza

Subjects

*TAU proteins, *ALZHEIMER'S disease, *CELL aggregation, *NEUROFIBRILLARY tangles, *IN vitro studies, *MUTANT proteins

Abstract

Disease-related tau protein in Alzheimer's disease is hyperphosphorylated and aggregates into neurofibrillary tangles. The cis -proline isomer of the pSer/Thr-Pro sequence has been proposed to act as a precursor of aggregation ('Cistauosis' hypothesis), but this aggregation scheme is not yet entirely accepted. Hence to investigate isomer-specific-aggregation of tau, proline residues at the RTPPK motif were replaced by alanine residues (with permanent trans configuration) employing genetic engineering methods. RTPAK, RTAPK, and RTAAK mutant variants of tau were generated, and their in vitro aggregation propensity was investigated using multi-spectroscopic techniques. Besides, the cell toxicity of oligomers/fibrils was analyzed and compared to those of the wild-type (WT) tau. Analyses of mutant variants have shown to be in agreement (to some degree) to the theory of the 'cistauosis' hypothesis. The results showed that the trans isomer in the 232-rd residue (P232A mutant rather than P233A) had reduced aggregation propensity. However, this study did not illustrate any statistically significant difference between the wild and the mutant protein aggregations concerning cell toxicity. [ABSTRACT FROM AUTHOR]

Published

2022

22. Intraneuronal tau aggregation induces the integrated stress response in astrocytes.

Author

Batenburg, Kevin L, Kasri, Nael N, Heine, Vivi M, and Scheper, Wiep

Abstract

Progressive aggregation of tau protein in neurons is associated with neurodegeneration in tauopathies. Cell non-autonomous disease mechanisms in astrocytes may be important drivers of the disease process but remain largely elusive. Here, we studied cell type-specific responses to intraneuronal tau aggregation prior to neurodegeneration. To this end, we developed a fully human co-culture model of seed-independent intraneuronal tau pathology, which shows no neuron and synapse loss. Using high-content microscopy, we show that intraneuronal tau aggregation induces oxidative stress accompanied by activation of the integrated stress response specifically in astrocytes. This requires the direct co-culture with neurons and is not related to neurodegeneration or extracellular tau levels. Tau-directed antisense therapy reduced intraneuronal tau levels and aggregation and prevented the cell non-autonomous responses in astrocytes. These data identify the astrocytic integrated stress response as a novel disease mechanism activated by intraneuronal tau aggregation. In addition, our data provide the first evidence for the efficacy of tau-directed antisense therapy to target cell autonomous and cell non-autonomous disease pathways in a fully human model of tau pathology. [ABSTRACT FROM AUTHOR]

Published

2022

23. The Chemical Features of Polyanions Modulate Tau Aggregation and Conformational States

Author

Montgomery, Kelly M

Subjects

Biochemistry, Neurodegeneration, Protein Folding, Tau Aggregation

Abstract

The aggregation of tau into insoluble fibrils is a defining feature of neurodegenerative tauopathies. However,tau has a positive overall charge and is highly soluble; so polyanions, such as heparin, are typically requiredto promote its aggregation in vitro. There are dozens of polyanions in living systems and it is not clear whichones might promote this process. Here, we systematically measure the ability of 37 diverse, anionicbiomolecules to initiate tau aggregation, using either wild type (WT) tau or the disease associated P301Smutant. We find that polyanions from many different structural classes can promote fibril formation and thatP301S tau is sensitive to a greater number of polyanions (28/37) than WT tau (21/37). We also find thatsome polyanions preferentially reduce the lag time of the aggregation reactions, while others enhance theelongation rate, suggesting that they act on partially distinct steps. From the resulting structure-activityrelationships, the valency of the polyanion seems to be an important chemical feature, such that anionswith low valency tend to be weaker aggregation inducers, even at the same overall charge. Finally, theidentity of the polyanion influences fibril morphology, based on electron microscopy and limited proteolysis.These results provide insight into the crucial role of polyanion—tau interactions in modulating tauconformational dynamics with implications for understanding the tau aggregation landscape in a complexcellular environment.

Published

2023

24. Tau R2 and R3 are essential regions for tau aggregation, seeding and propagation.

Author

Annadurai, Narendran, Malina, Lukáš, Malohlava, Jakub, Hajdúch, Marián, and Das, Viswanath

Subjects

*HEXAPEPTIDES, *TAU proteins, *NEUROFIBRILLARY tangles, *CELL aggregation, *TAUOPATHIES, *DRUG target

Abstract

Tauopathies are characterised by intracellular deposits of fibrillar tau tangles. However, the interneuronal spread of pathological tau species precedes the development of major tau burdens. Two amyloid motifs, VQIINK in repeat 2 and VQIVYK in repeat 3, of tau repeat domain, assemble into β-sheet-rich fibrils on their own but alone do not form seed-competent fibrils. In contrast, the entire R3 region self-aggregates and forms seed-competent fibrils. Our study aimed to identify the minimal regions in the tau repeat domain that define seeding and its impact on intracellular tau phosphorylation and aggregation. Using peptides of individual repeats, we show that R2, like R3, forms seed-competent fibrils when assembled in the presence of heparin. However, R3, but not R2, forms seed-competent fibrils when assembled without heparin, even though both R2 and R3 have identical N-terminal hexapeptide and cysteine residue sequences. Moreover, cysteine to alanine substitution in R3 abrogates its self-aggregation and seeding potency. Tau RD P301S biosensor cells and Tau P301L (0N4R)-expressing HEK293 cells seeded with R2 and R3 fibrils show the induction of pathological phosphorylation of tau at Ser262/Ser396/Ser404 positions and oligomerisation of native tau. Protein fractions of biosensor cells seeded with R2 and R3 fibrils reseed endogenous tau aggregation when introduced into a fresh set of biosensor cells. Our findings suggest that R3 may be the minimal region for pathological seed generation under physiological conditions, whereas R2 might need polyanionic cofactors to generate pathogenic seeds. Lastly, R2 and R3 fibrils induce template-induced misfolding and pathological hyperphosphorylation of intracellular tau, making intracellular tau seed-competent. [Display omitted] • R2 and R3 repeat regions of the tau microtubule-binding domain form β-sheet-rich fibrils. • R3 but not R2 self-assembles in the absence of heparin. • N-terminal hexapeptide and cysteine residue are essential for the self-assembly of seed-competent R3 fibrils. • Exogenous R2 and R3 fibrils seed intracellular tau aggregation in cells expressing aggregation-prone P301L/P301S tau. • R2 and R3 fibrils induce pathological hyperphosphorylation and oligomerisation of seeded endogenous tau. • The minimal regions, R2 and R3, are potential drug targets for developing anti-tau seeding therapeutics. [ABSTRACT FROM AUTHOR]

Published

2022

25. Season of birth and vulnerability to the pathology of Alzheimer's disease: an in vivo positron emission tomography study.

Author

Yasuno, Fumihiko and Minami, Hiroyuki

Subjects

*ALZHEIMER'S disease risk factors, *ALZHEIMER'S disease, *PSYCHOLOGICAL vulnerability, *TAU proteins, *MULTIPLE regression analysis, *COGNITION, *SEASONS, *RISK assessment, *AMYLOID beta-protein precursor, *POSITRON emission tomography, *ANALYSIS of covariance

Abstract

Background: This study used positron emission tomography to examine whether the seasonal birth effect as an exogenic indicator of early life environmental factors influenced vulnerability to Alzheimer's disease (AD) pathology in the elderly. Methods: We analysed datasets from the Alzheimer's Disease Neuroimaging Initiative, which included the data for 234 cognitively normal (CN) individuals and patients with mild cognitive impairment (MCI) (n = 114) and AD dementia (n = 38). As an index of amyloid β (Aβ)/tau accumulation, the 18F‐AV‐45‐ and 18F‐AV‐1451‐standardized uptake value ratios (SUVRs) were compared between groups of spring‐to‐summer births and fall‐to‐winter births by analysis of covariance. In addition, a multiple linear regression analysis was performed to determine whether the season of birth was a predictor of 18F‐AV‐45 and/or 18F‐AV‐1451 SUVRs, for which a difference was observed. Results: Seasonal birth difference was a good predictor of 18F‐AV‐1451 SUVR. We found that participants with a fall‐to‐winter birth showed lower 18F‐AV‐1451 SUVRs than those with a spring‐to‐summer birth in both the CN and MCI/AD groups, after correcting for the effect of age, sex, years of education, and Alzheimer's Disease Assessment Scale cognitive subscale score, that could possibly affect tau accumulation. Conclusions: Participants with a fall‐to‐winter birth showed less tau accumulation than those with a spring‐to‐summer birth after accounting for the factors that could affect tau accumulation. Our findings showed a vulnerability to tau pathology in participants with a fall‐to‐winter birth, which may be caused by perinatal or postnatal brain damage due to the risk factors associated with the cold season. [ABSTRACT FROM AUTHOR]

Published

2022

26. Structure-activity relationship of carbon nitride dots in inhibiting Tau aggregation.

Author

Zhou, Yiqun, Kandel, Nabin, Bartoli, Mattia, Serafim, Leonardo F., ElMetwally, Ahmed E., Falkenberg, Sophia M., Paredes, Xavier E., Nelson, Christopher J., Smith, Nathan, Padovano, Elisa, Zhang, Wei, Mintz, Keenan J., Ferreira, Braulio C.L.B., Cilingir, Emel Kirbas, Chen, Jiuyan, Shah, Sujit K., Prabhakar, Rajeev, Tagliaferro, Alberto, Wang, Chunyu, and Leblanc, Roger M.

Subjects

*CARBON nanodots, *STRUCTURE-activity relationships, *MOLECULAR dynamics, *REACTIVE oxygen species, *NITRIDES, *TUBULINS, *BLOOD-brain barrier

Abstract

Due to the numerous failed clinical trials of anti-amyloid drugs, microtubule associated protein tau (MAPT) now stands out as one of the most promising targets for AD therapy. In this study, we report for the first time the structure-dependent MAPT aggregation inhibition of carbon nitride dots (CNDs). CNDs have exhibited great promise as a potential treatment of Alzheimer's disease (AD) by inhibiting the aggregation of MAPT. In order to elucidate its structure-activity relationship, CNDs were separated via column chromatography and five fractions with different structures were obtained that were characterized by multiple spectroscopy methods. The increase of surface hydrophilic functional groups is consistent with the increase of polarity from fraction 1 to 5. Particle sizes (1–2 nm) and zeta potentials (∼-20 mV) are similar among five fractions. With the increase of polarity from fraction 1 to 5, their MAPT aggregation inhibition capacity was weakened. This suggests hydrophobic interactions between CNDs and MAPT, validated via molecular dynamics simulations. With a zebrafish blood-brain barrier (BBB) model, CNDs were observed to cross the BBB through passive diffusion. CNDs were also found to inhibit the generation of multiple reactive oxygen species, which is an important contributor to AD pathogenesis. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022

27. Design, Synthesis, and In Vitro, In Silico and In Cellulo Evaluation of New Pyrimidine and Pyridine Amide and Carbamate Derivatives as Multi-Functional Cholinesterase Inhibitors.

Author

Bortolami, Martina, Pandolfi, Fabiana, Tudino, Valeria, Messore, Antonella, Madia, Valentina Noemi, De Vita, Daniela, Di Santo, Roberto, Costi, Roberta, Romeo, Isabella, Alcaro, Stefano, Colone, Marisa, Stringaro, Annarita, Espargaró, Alba, Sabatè, Raimon, and Scipione, Luigi

Subjects

*CHOLINESTERASE inhibitors, *AMIDE derivatives, *CARBAMATE derivatives, *AMIDES, *PYRIDINE derivatives, *PYRIDINE, *MOLECULAR docking

Abstract

Alzheimer disease is an age-linked neurodegenerative disorder representing one of the greatest medical care challenges of our century. Several drugs are useful in ameliorating the symptoms, even if none could stop or reverse disease progression. The standard approach is represented by the cholinesterase inhibitors (ChEIs) that restore the levels of acetylcholine (ACh) by inhibiting the acetylcholinesterase (AChE). Still, their limited efficacy has prompted researchers to develop new ChEIs that could also reduce the oxidative stress by exhibiting antioxidant properties and by chelating the main metals involved in the disease. Recently, we developed some derivatives constituted by a 2-amino-pyrimidine or a 2-amino-pyridine moiety connected to various aromatic groups by a flexible amino-alkyl linker as new dual inhibitors of AChE and butyrylcholinesterase (BChE). Following our previous studies, in this work we explored the role of the flexible linker by replacing the amino group with an amide or a carbamic group. The most potent compounds showed higher selectivity against BChE in respect to AChE, proving also to possess a weak anti-aggregating activity toward Aβ42 and tau and to be able to chelate Cu2+ and Fe3+ ions. Molecular docking and molecular dynamic studies proposed possible binding modes with the enzymes. It is noteworthy that these compounds were predicted as BBB-permeable and showed low cytotoxicity on the human brain cell line. [ABSTRACT FROM AUTHOR]

Published

2022

28. Charge neutralization of lysine via carbamylation reveals hidden aggregation hot‐spots in tau protein flanking regions.

Author

Gadhavi, Joshna, Shah, Sumedha, Sinha, Tulika, Jain, Alok, and Gupta, Sharad

Subjects

*TAU proteins, *MOLECULAR dynamics, *LYSINE, *POST-translational modification, *PEPTIDES, *NEUROFIBRILLARY tangles

Abstract

Tau protein is found abundantly in neurofibrillary tangles in Alzheimer's disease (AD). The longest human tau isoform (2N4R) has 44 lysine residues. Several lysine‐based post‐translational modifications (PTMs) such as glycation, acetylation, ubiquitination, and sumoylation have been implicated not only in AD, but also in other tauopathies. Carbamylation is one such lysine neutralizing age‐related nonenzymatic PTM which can modulate the aggregation propensity of tau. In this work, we have studied the aggregation potential of lysine‐rich regions of tau upon carbamylation which do not aggregate in their native form. Using an array of biophysical and microscopic analyses, such as ThT kinetic assay, fluorescence microscopy, Congo red staining, and scanning electron microscopy, we demonstrate that peptides derived from four of five such regions exhibit robust fibrillar amyloid formation. These regions are found in the N‐terminal projection domain that encompasses proline‐rich domain (148–153 and 223–230), repeat domain R1 (253–260), as well as fibrillary core region (368–378), and can be described as hidden aggregation hot‐spots which become activated upon carbamylation. We have further compared the impact of carbamylation with acetylation on the aggregation propensity of lysine‐rich peptide (254KKVAVV259) using biophysical experiments and molecular dynamics simulations and deduced that carbamylation is a much stronger driver of aggregation than acetylation. Our findings may offer more insight into amyloid fibrils' interaction with hidden aggregation‐prone nucleating sequences that act as hot‐spots for inducing tau fibrillation. [ABSTRACT FROM AUTHOR]

Published

2022

29. Antitumour drugs targeting tau R3 VQIVYK and Cys322 prevent seeding of endogenous tau aggregates by exogenous seeds.

Author

Annadurai, Narendran, Malina, Lukáš, Salmona, Mario, Diomede, Luisa, Bastone, Antonio, Cagnotto, Alfredo, Romeo, Margherita, Šrejber, Martin, Berka, Karel, Otyepka, Michal, Hajdúch, Marián, and Das, Viswanath

Subjects

*NEUROFIBRILLARY tangles, *TAU proteins, *SEEDS, *ALZHEIMER'S disease, *ANTINEOPLASTIC agents, *CAENORHABDITIS elegans

Abstract

Emerging experimental evidence suggests tau pathology spreads between neuroanatomically connected brain regions in a prion‐like manner in Alzheimer's disease (AD). Tau seeding, the ability of prion‐like tau to recruit and misfold naïve tau to generate new seeds, is detected early in human AD brains before the development of major tau pathology. Many antitumour drugs have been reported to confer protection against neurodegeneration, supporting the repurposing of approved and experimental or investigational oncology drugs for AD therapy. In this study, we evaluated whether antitumour drugs that abrogate the generation of seed‐competent aggregates of tau Repeat 3 (R3) domain peptides can prevent tau seeding and toxicity in Tau‐RD P301S FRET Biosensor cells and Caenorhabditis elegans. We demonstrate that drugs that interact with the N‐terminal VQIVYK or the C‐terminal region housing the Cys322 prevent R3 dimerisation, abolishing the generation of prion‐like R3 seeds. Preformed R3 seeds (fibrils) capped with, or R3 seeds formed in the presence of VQIVYK‐ or Cys322‐targeting drugs have a reduced potency to cause aggregation of naïve tau in biosensor cells and protect worms from aggregate toxicity. These findings indicate that VQIVYK‐ or Cys322‐targeting drugs may act as prophylactic agents against tau seeding. [ABSTRACT FROM AUTHOR]

Published

2022

30. Comprehensive Characterization of CK1δ-Mediated Tau Phosphorylation in Alzheimer’s Disease

Author

Aileen Roth, Annabelle Sander, Marleen Silke Oswald, Fabian Gärtner, Uwe Knippschild, and Joachim Bischof

Subjects

Alzheimer’s disease, AD, casein kinase 1δ, CK1δ, tau phosphorylation, tau aggregation, Biology (General), QH301-705.5

Abstract

A main pathological event in Alzheimer’s disease is the generation of neurofibrillary tangles originating from hyperphosphorylated and subsequently aggregated tau proteins. Previous reports demonstrated the critical involvement of members of the protein kinase family CK1 in the pathogenesis of Alzheimer’s disease by hyperphosphorylation of tau. However, precise mechanisms and effects of CK1-mediated tau phosphorylation are still not fully understood. In this study, we analyzed recombinant tau441 phosphorylated by CK1δ in vitro via mass spectrometry and identified ten potential phosphorylation sites, five of them are associated to Alzheimer’s disease. To confirm these results, in vitro kinase assays and two-dimensional phosphopeptide analyses were performed with tau441 phosphomutants confirming Alzheimer’s disease-associated residues Ser68/Thr71 and Ser289 as CK1δ-specific phosphorylation sites. Treatment of differentiated human neural progenitor cells with PF-670462 and Western blot analysis identified Ser214 as CK1δ-targeted phosphorylation site. The use of an in vitro tau aggregation assay demonstrated a possible role of CK1δ in tau aggregation. Results obtained in this study highlight the potential of CK1δ to be a promising target in the treatment of Alzheimer’s disease.

Published

2022

31. Comparison of size distribution and (Pro249-Ser258) epitope exposure in in vitro and in vivo derived Tau fibrils

Author

André Marreiro, Kristof Van Kolen, Cristiano Sousa, Liesbet Temmerman, Bruno Vasconcelos, Rosa Crespo-Rodriguez, Jan R. T. van Weering, Debby Van Dam, Peter P. De Deyn, Adrian Apetri, Liliane Schoofs, and Marc H. Mercken

Subjects

Alzheimer’s disease, Tau, Tau aggregation, Aggregation, Seeding, Cytology, QH573-671

Abstract

Abstract Background Although several studies demonstrate prion-like properties of Tau fibrils, the effect of size in the seeding capacity of these aggregates is not fully understood. The aim of this study is to characterize Tau seeds by their size and seeding capacity. Methods Tau aggregates were isolated from postmortem AD brain tissue and separated from low molecular weight species by sucrose gradient ultracentrifugation. Biochemical characterization of the different fractions was done by non-reducing Western blotting and aggregate-specific immuno-assays using in house developed anti-Tau monoclonal antibodies, including PT76 which binds to an epitope close to the microtubule-binding domain and, hence, also to K18. Seeding efficiency was then assessed in HEK293 cells expressing K18 FRET sensors. Results We observed that upon sonication of Tau aggregates different size-distributed tau aggregates are obtained. In biochemical assays, these forms show higher signals than the non-sonicated material in some aggregation-specific Tau assays. This could be explained by an increased epitope exposure of the smaller aggregates created by the sonication. By analyzing human brain derived and recombinant (K18) Tau aggregates in a cellular FRET assay, it was observed that, in the absence of transfection reagent, sonicated aggregates showed higher aggregation induction. Preparations also showed altered profiles on native PAGE upon sonication and we could further separate different aggregate species based on their molecular weight via sucrose gradients. Conclusions This study further elucidates the molecular properties regarding relative aggregate size and seeding efficiency of sonicated vs. non-sonicated high molecular weight Tau species. This information will provide a better knowledge on how sonication, a commonly used technique in the field of study of Tau aggregation, impacts the aggregates. In addition, the description of PT76-based aggregation specific assay is a valuable tool to quantify K18 and human AD Tau fibrils.

Published

2020

32. Toxic tau: structural origins of tau aggregation in Alzheimer's disease

Author

Abdullah Al Mamun, Md Sahab Uddin, Bijo Mathew, and Ghulam Md Ashraf

Subjects

alzheimer’s disease, neurofibrillary tangles, shape-shifting nature of tau, tau aggregation, toxic tau, Neurology. Diseases of the nervous system, RC346-429

Abstract

Alzheimer’s disease is characterized by the extracellular accumulation of the amyloid β in the form of amyloid plaques and the intracellular deposition of the microtubule-associated protein tau in the form of neurofibrillary tangles. Most of the Alzheimer’s drugs targeting amyloid β have been failed in clinical trials. Particularly, tau pathology connects greatly in the pathogenesis of Alzheimer’s disease. Tau protein enhances the stabilization of microtubules that leads to the appropriate function of the neuron. Changes in the quantity or the conformation of tau protein could affect its function as a microtubules stabilizer and some of the processes wherein it is involved. The molecular mechanisms leading to the accumulation of tau are principally signified by numerous posttranslational modifications that change its conformation and structural state. Therefore, aberrant phosphorylation, as well as truncation of tau protein, has come into focus as significant mechanisms that make tau protein in a pathological entity. Furthermore, the shape-shifting nature of tau advocates to comprehend the progression of Alzheimer’s disease precisely. In this review, we emphasize the recent studies about the toxic and shape-shifting nature of tau in the pathogenesis of Alzheimer’s disease.

Published

2020

33. To target Tau pathologies, we must embrace and reconstruct their complexities

Author

Galina Limorenko and Hilal A. Lashuel

Subjects

Microtubule-associated protein Tau, Tau, Heparin, Tau aggregation, Tau fibrillization, PHF, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The accumulation of hyperphosphorylated fibrillar Tau aggregates in the brain is one of the defining hallmarks of Tauopathy diseases, including Alzheimer's disease. However, the primary events or molecules responsible for initiation of the pathological Tau aggregation and spreading remain unknown. The discovery of heparin as an effective inducer of Tau aggregation in vitro was instrumental to enabling different lines of research into the role of Tau aggregation in the pathogenesis of Tauopathies. However, recent proteomics and cryogenic electron microscopy (cryo-EM) studies have revealed that heparin-induced Tau fibrils generated in vitro do not reproduce the biochemical and ultrastructural properties of disease-associated brain-derived Tau fibrils. These observations demand that we reassess our current approaches for investigating the mechanisms underpinning Tau aggregation and pathology formation. Our review article presents an up-to-date survey and analyses of 1) the evolution of our understanding of the interactions between Tau and heparin, 2) the various structural and mechanistic models of the heparin-induced Tau aggregation, 3) the similarities and differences between brain-derived and heparin-induced Tau fibrils; and 4) emerging concepts on the biochemical and structural determinants underpinning Tau pathological heterogeneity in Tauopathies. Our analyses identify specific knowledge gaps and call for 1) embracing the complexities of Tau pathologies; 2) reassessment of current approaches to investigate, model and reproduce pathological Tau aggregation as it occurs in the brain; 3) more research towards a better understanding of the naturally-occurring cofactor molecules that are associated with Tau brain pathology initiation and propagation; and 4) developing improved approaches for in vitro production of the Tau aggregates and fibrils that recapitulate and/or amplify the biochemical and structural complexity and diversity of pathological Tau in Tauopathies. This will result in better and more relevant tools, assays, and mechanistic models, which could significantly improve translational research and the development of drugs and antibodies that have higher chances for success in the clinic.

Published

2021

34. Hexameric Aggregation Nucleation Core Sequences and Diversity of Pathogenic Tau Strains

Author

Ling Wu, Sidharth S. Madhavan, Christopher Tan, and Bin Xu

Subjects

tau aggregation, tauopathies, nucleation core sequences, amyloidogenicity, tau strains diversity, Medicine

Abstract

Tau aggregation associates with multiple neurodegenerative diseases including Alzheimer’s disease and rare tauopathies such as Pick’s disease, progressive supranuclear palsy, and corticobasal degeneration. The molecular and structural basis of tau aggregation and related diverse misfolded tau strains are not fully understood. To further understand tau-protein aggregation mechanisms, we performed systematic truncation mutagenesis and mapped key segments of tau proteins that contribute to tau aggregation, where it was determined that microtubule binding domains R2 and R3 play critical roles. We validated that R2- or R3-related hexameric PHF6 and PHF6* peptide sequences are necessary sequences that render tau amyloidogenicity. We also determined that the consensus VQI peptide sequence is not sufficient for amyloidogenicity. We further proposed single- and dual-nucleation core-based strain classifications based on recent cryo-EM structures. We analyzed the structural environment of the hexameric peptide sequences in diverse tau strains in tauopathies that, in part, explains why the VQI consensus core sequence is not sufficient to induce tau aggregation. Our experimental work and complementary structural analysis highlighted the indispensible roles of the hexameric core sequences, and shed light on how the interaction environment of these core sequences contributes to diverse pathogenic tau-strains formation in various tauopathy brains.

Published

2022

35. Computational Insights Into the Inhibition Mechanism of Proanthocyanidin B2 on Tau Hexapeptide (PHF6) Oligomer

Author

Qin Li, Chunmei Xiong, Hongli Liu, Huizhen Ge, Xiaojun Yao, and Huanxiang Liu

Subjects

PHF6, Tau aggregation, proanthocyanidin B2, molecular dynamics simulation, Alzheimer’s disease, Chemistry, QD1-999

Abstract

The formation of amyloid fibrils from Tau is a key pathogenic feature of Alzheimer’s disease (AD). To disturb the formation of Tau aggregates is considered as a promising therapeutic strategy for AD. Recently, a natural product proanthocyanidin B2 (PB2) was confirmed to not only inhibit Tau aggregation, but also disaggregate Tau fibrils. Herein, to explore the inhibition mechanism of PB2 against Tau fibril and to provide the useful information for drug design and discovery, all-atom molecular dynamics simulations were carried out for the ordered Tau hexapeptide PHF6 oligomer in the presence and absence of PB2. The obtained result shows that PB2 can transform PHF6 oligomer from the ordered β-sheet structure into disordered one. Moreover, the clustering analysis and binding free energy calculations identify that S3 site is the most potential binding site. At S3 site, by hydrophobic and hydrogen bond interactions, the residues V309, Y310 and K311 are essential for binding with PB2, especially K311. In a word, our study reveals the molecular mechanism of PB2 inhibiting PHF6 aggregation and it will provide some valuable information for the development of Tau aggregation inhibitors.

Published

2021

36. Significant effects of cholinesterase inhibitors on tau pathology in the Alzheimer's disease continuum: An in vivo positron emission tomography study.

Author

Fumihiko Yasuno, Hiroyuki Minami, Yasuno, Fumihiko, and Minami, Hiroyuki

Subjects

*POSITRON emission tomography, *TAU proteins, *ALZHEIMER'S disease, *CHOLINESTERASE inhibitors, *ACETYLCHOLINESTERASE, *ALZHEIMER'S patients

Abstract

Objectives: No prior study has assessed the effects of cholinesterase inhibitors (ChEIs) on tau pathology in the brains of patients with Alzheimer's disease (AD). Using positron emission tomography, this study aimed to investigate whether ChEIs reduce tau aggregation in amyloid-positive participants.Methods: We analyzed datasets from the Alzheimer's Disease Neuroimaging Initiative and included amyloid-positive participants who had undergone baseline and 1- or 2-year follow-up AV-1451 positron emission tomography scans. We included participants treated with and without ChEIs (ChEIs group: n = 15, No-ChEIs group, n = 45). The annual change in tau aggregation was calculated as the difference in AV-1451- standardized uptake value ratio (SUVR) between the two scans divided by the time between scans. Group differences in annual AV-1451-SUVR change were examined.Results: We found a significantly lower annual change in AV-1451-SUVR in the Braak 1/2 regions (entorhinal cortex and hippocampus) of participants taking ChEIs. Increased AV-1451-SUVR between the first and second examinations were observed in 22 of 45 participants not taking ChEIs and 2 of 15 participants taking ChEIs. Fisher's exact test showed a significant difference in the ratio of participants with increased AV-1451-SUVR between the groups.Conclusions: The findings of this positron emission tomography study suggest that the administration of ChEIs has some neuroprotective effects in patients of the AD continuum, at least in the early stage of the disease progression. This in vivo effect may be mediated via tau, preventing amyloid β-induced neurotoxicity. [ABSTRACT FROM AUTHOR]

Published

2021

37. The elusive tau molecular structures: can we translate the recent breakthroughs into new targets for intervention?

Author

Yann Fichou, Youssra K. Al-Hilaly, François Devred, Caroline Smet-Nocca, Philipp O. Tsvetkov, Joke Verelst, Joris Winderickx, Nick Geukens, Eugeen Vanmechelen, Audrey Perrotin, Louise Serpell, Bernard J Hanseeuw, Miguel Medina, Luc Buée, and Isabelle Landrieu

Subjects

Tauopathies, Alzheimer’s disease, tau structure, tau aggregation, Alzheimer’s disease diagnosis, Amyloid, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Insights into tau molecular structures have advanced significantly in recent years. This field has been the subject of recent breakthroughs, including the first cryo-electron microscopy structures of tau filaments from Alzheimer’s and Pick’s disease inclusions, as well as the structure of the repeat regions of tau bound to microtubules. Tau structure covers various species as the tau protein itself takes many forms. We will here address a range of studies that help to define the many facets of tau protein structures and how they translate into pathogenic forms. New results shed light on previous data that need now to be revisited in order to up-date our knowledge of tau molecular structure. Finally, we explore how these data can contribute the important medical aspects of this research - diagnosis and therapeutics.

Published

2019

38. Continuous Monitoring of Tau-Induced Neurotoxicity in Patient-Derived iPSC-Neurons.

Author

Oakley, Derek H., Klickstein, Naomi, Commins, Caitlin, Chung, Mirra, Dujardin, Simon, Bennett, Rachel E., Hyman, Bradley T., and Frosch, Matthew P.

Subjects

*NEUROFIBRILLARY tangles, *INDUCED pluripotent stem cells, *NEUROTOXICOLOGY, *FRONTOTEMPORAL lobar degeneration, *CELL aggregation, *ALZHEIMER'S disease

Abstract

Tau aggregation within neurons is a critical feature of Alzheimer's disease (AD) and related tauopathies. It is believed that soluble pathologic tau species seed the formation of tau aggregates in a prion-like manner and propagate through connected neurons during the progression of disease. Both soluble and aggregated forms of tau are thought to have neurotoxic properties. In addition, different strains of misfolded tau may cause differential neurotoxicity. In this work, we present an accelerated human neuronal model of tau-induced neurotoxicity that incorporates both soluble tau species and tau aggregation. Using patient-derived induced pluripotent stem cell (iPSC) neurons expressing a tau aggregation biosensor, we develop a cell culture system that allows continuous assessment of both induced tau aggregation and neuronal viability at single-cell resolution for periods of .1 week. We show that exogenous tau "seed" uptake, as measured by tau repeat domain (TauRD) reporter aggregation, increases the risk for subsequent neuronal death in vitro. These results are the first to directly visualize neuronal TauRD aggregation and subsequent cell death in single human iPSC neurons. Specific morphologic strains or patterns of TauRD aggregation are then identified and associated with differing neurotoxicity. Furthermore, we demonstrate that familial AD iPSC neurons expressing the PSEN1 L435F mutation exhibit accelerated TauRD aggregation kinetics and a tau strain propagation bias when compared with control iPSC neurons. [ABSTRACT FROM AUTHOR]

Published

2021

39. Relationship between neuropsychiatric symptoms and Alzheimer's disease pathology: An in vivo positron emission tomography study.

Author

Yasuno, Fumihiko, Minami, Hiroyuki, and Hattori, Hideyuki

Subjects

*POSITRON emission tomography, *PATHOLOGY, *ALZHEIMER'S disease, *SYMPTOMS, *RECEIVER operating characteristic curves, *CHRONIC traumatic encephalopathy, *CEREBRAL amyloid angiopathy

Abstract

Objectives: To investigate the relationship between amyloid‐β‐ and tau‐based Alzheimer's disease (AD) pathologies assessed using positron emission tomography imaging and neuropsychiatric symptoms (NPS) in a sample of AD continuum including clinically normal subjects and patients with mild cognitive impairment or AD. Methods: We analyzed datasets of the Alzheimer's disease Neuroimaging Initiative and included amyloid‐positive subjects who underwent an AV‐45 scan within 1 year of an AV‐1451 scan (n = 99). Correlation between standardized uptake value ratio (SUVR) of AV‐45 and AV‐1451 and the Neuropsychiatric Inventory (NPI) score (and its four domain subscores for hyperactivity, psychosis, affective, and apathy) was evaluated. Stepwise logistic regression analysis was used to examine the influence of SUVRs on the presence of NPS. SUVRs were also tested for their ability to discriminate the group with NPS using receiver operating characteristic (ROC) curve analyses. Results: Significant positive relationships were found between the total NPI score and affective symptoms and Braak 1&2 (transentorhinal region) AV‐1451 SUVR. Stepwise logistic regression analysis identified tau accumulation in the area of Braak 1&2 as a significant covariate discriminating the presence of affective symptoms. The area under the ROC curve analysis showed that subjects with affective symptoms were discriminated by AV‐1451 SUVR with an accuracy of 77.7%. Conclusions: Tau aggregation in the transentorhinal region, where neurodegeneration affected by tau pathology was seen in the early stage of AD, correlated with more severe NPS, especially affective symptoms. Therefore, tau pathology in the transentorhinal cortex might be associated with affective symptoms in the early stage of AD. [ABSTRACT FROM AUTHOR]

Published

2021

40. Design, Synthesis, and In Vitro, In Silico and In Cellulo Evaluation of New Pyrimidine and Pyridine Amide and Carbamate Derivatives as Multi-Functional Cholinesterase Inhibitors

Author

Martina Bortolami, Fabiana Pandolfi, Valeria Tudino, Antonella Messore, Valentina Noemi Madia, Daniela De Vita, Roberto Di Santo, Roberta Costi, Isabella Romeo, Stefano Alcaro, Marisa Colone, Annarita Stringaro, Alba Espargaró, Raimon Sabatè, and Luigi Scipione

Subjects

acetylcholinesterase inhibitors, butyrylcholinesterase inhibitors, multifunctional compounds, amyloid aggregation, tau aggregation, metal chelation, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Alzheimer disease is an age-linked neurodegenerative disorder representing one of the greatest medical care challenges of our century. Several drugs are useful in ameliorating the symptoms, even if none could stop or reverse disease progression. The standard approach is represented by the cholinesterase inhibitors (ChEIs) that restore the levels of acetylcholine (ACh) by inhibiting the acetylcholinesterase (AChE). Still, their limited efficacy has prompted researchers to develop new ChEIs that could also reduce the oxidative stress by exhibiting antioxidant properties and by chelating the main metals involved in the disease. Recently, we developed some derivatives constituted by a 2-amino-pyrimidine or a 2-amino-pyridine moiety connected to various aromatic groups by a flexible amino-alkyl linker as new dual inhibitors of AChE and butyrylcholinesterase (BChE). Following our previous studies, in this work we explored the role of the flexible linker by replacing the amino group with an amide or a carbamic group. The most potent compounds showed higher selectivity against BChE in respect to AChE, proving also to possess a weak anti-aggregating activity toward Aβ42 and tau and to be able to chelate Cu2+ and Fe3+ ions. Molecular docking and molecular dynamic studies proposed possible binding modes with the enzymes. It is noteworthy that these compounds were predicted as BBB-permeable and showed low cytotoxicity on the human brain cell line.

Published

2022

41. Application of single-molecule analysis to singularity phenomenon of cells.

Author

Hiroshima M, Bannai H, Matsumoto G, and Ueda M

Abstract

Single-molecule imaging in living cells is an effective tool for elucidating the mechanisms of cellular phenomena at the molecular level. However, the analysis was not designed for throughput and requires high expertise, preventing it from reaching large scale, which is necessary when searching for rare cells that induce singularity phenomena. To overcome this limitation, we have automated the imaging procedures by combining our own focusing device, artificial intelligence, and robotics. The apparatus, called automated in-cell single-molecule imaging system (AiSIS), achieves a throughput that is a hundred-fold higher than conventional manual imaging operations, enabling the analysis of molecular events by individual cells across a large population. Here, using AiSIS, we demonstrate the single-molecule imaging of molecular behaviors and reactions related to tau protein aggregation, which is considered a singularity phenomenon in neurological disorders. Changes in the dynamics and kinetics of molecular events were observed inside and on the basal membrane of cells after the induction of aggregation. Additionally, to detect rare cells based on the molecular behavior, we developed a method to identify the state of individual cells defined by the quantitative distribution of molecular mobility and clustering. Using this method, cellular variations in receptor behavior were shown to decrease following ligand stimulation. This cell state analysis based on large-scale single-molecule imaging by AiSIS will advance the study of molecular mechanisms causing singularity phenomena., Competing Interests: The authors declare no competing interests., (2024 THE BIOPHYSICAL SOCIETY OF JAPAN.)

Published

2024

42. Function of Protein Kinase RNA-like Endoplasmic Reticulum Kinase in regulating tau protein aggregation in Alzheimer’s Disease and Progressive Supranuclear Palsy

Author

Xu, Ke

Subjects

Biology, Alzheimer’s Disease, Endoplasmic reticulum, PERK, Progressive Supranuclear Palsy, Tau aggregation, Unfolded Protein Response

Abstract

Tauopathies, such as Alzheimer’s Disease (AD) and Progressive Supranuclear Palsy (PSP), are characterized by the central nervous system accumulation of misfolded tau protein. Endoplasmic reticulum (ER) stress and Unfolded Protein Response (UPR) may be cellular mechanisms that cause tauopathies. As one of three major branches of UPR, PERK was identified as a genetic risk factor for AD and PSP in several GWAS studies. Upon activation, PERK attenuates protein translation to restore ER homeostasis but prolonged PERK activation can induce apoptosis. Here, we studied the role of PERK in tau aggregation in human AD and PSP brain tissues and in a cell culture model. We prepared protein lysates from the hippocampus region of advanced AD patient brains (Braak 6) and normal brains (Braak 1). We found more tau aggregated protein in Braak 6 brains in comparison to Braak 1 brains by immunoblotting. We also found a statistically significant increase of phosphorylated PERK in Braak 1 brains in comparison to Braak 6 brains in AD patients. This finding suggests that PERK activity is inversely proportional to insoluble misfolded tau aggregation. We did not find any correlation between PERK-haplotype and PERK functional in AD brains. We also prepared protein lysates from 3 different anatomic regions from PSP patient brains (midbrain, frontal cortex, and occipital cortex). The PSP results were highly variable due to technical problems, and we did not identify any reproducible correlations between tau levels and phosphorylated PERK levels.We further studied how PERK and tau interact utilizing HEK293 cells stably expressing TauRD-YFP (Biosensor cells) developed by Marc Diamond’s group as a cellular model of tau protein aggregation. We activated or inhibited PERK activity in TauRD biosensor cells by treating them with pharmacochemical small molecule modulators (GSK2656157, GSK2606414, salubrinal, ISRIB). We monitored tau aggregation by the formation of YFP fluorescent puncta in the cells. We found an inverse association between PERK pathway activation and tau aggregation. In summary, our brain and cell culture findings implicate PERK as a regulator of tau protein accumulation. PERK pathway activation may have high therapeutic potential for tauopathy treatment.

Published

2021

43. Quirks of dye nomenclature. 15. Geranine — a simple name, with a less than straight forward identity.

Author

Cooksey, C. J.

Subjects

*CHEMICAL structure, *DYES & dyeing, *ISOMERS, *STAINS & staining (Microscopy)

Abstract

Geranines were manufactured initially as textile dyes; they were made by coupling diazotized aromatic amines with sulfonated 1-naphthols. Most commonly encountered was geranine G, which for more than fifty years was thought to be derived from 1-naphthol monosulfonic acid, but later was considered to be derived from a 1-naphthol disulfonic acid. Currently, geranine G is thought to be a mixture of two isomers derived from 1-naphthol disulfonic acids. This species and others are described here by chemical structure and by other reference names and numbers where available. The occasional uses of geranines as biological stains are documented. [ABSTRACT FROM AUTHOR]

Published

2020

44. Inhibition of Tau amyloid fibril formation by folic acid: In-vitro and theoretical studies.

Author

Ghasemzadeh, Samin and Riazi, Gholam Hossein

Subjects

*FOLIC acid, *MINERAL supplements, *TAU proteins, *PROTEIN-protein interactions, *NUCLEIC acids, *CELL division, *CELL growth

Abstract

Tauopathy belongs to a various class of neurodegenerative diseases in which insoluble Tau aggregates are formed, and cellular function is lost, leading to neuronal death. Various therapeutic strategies have been investigated, and many drugs have been proposed as a cure for these diseases but their toxicity and adverse side effects, limit their consumption by humans. Alternatively, the use of non-toxic medicine without any adverse or undesirable secondary effects like nutrients, vitamins, as well as herbal and mineral supplements is common and continues to increase each year. Folic acid is a form of vitamin B and plays a vital role in the synthesis of nucleic acid, methionine regeneration, and in shuttling one-carbon units essential for normal cell division and growth. We investigated the interaction between folic acid and Tau protein, then experimental and theoretical evidence were provided for the suppressing effects of folic acid on Tau fibril formation. The obtained results showed that folic acid could interact with Tau through a spontaneous binding process, mainly by hydrophobic forces, and this interaction leads to a decline in protein-protein interactions through stabilizing its native state, limiting successful Tau–seed oligomerization and consequently decelerating polymerization of Tau amyloid aggregates. [ABSTRACT FROM AUTHOR]

Published

2020

45. Cobalt-based metal complexes prevent Repeat Tau aggregation and nontoxic to neuronal cells.

Author

Gorantla, Nalini V., Balaraman, Ekambaram, and Chinnathambi, Subashchandrabose

Subjects

*TAU proteins, *METAL complexes, *CELL sheets (Biology), *COBALT, *MICROTUBULE-associated proteins, *MICROTUBULES, *ALZHEIMER'S disease, *DEATH rate

Abstract

Alzheimer's disease (AD) is a fatal neurodegenerative disorder with an alarming increase in the death rate every year. AD is characterised by an aberrant accumulation of proteins in the form of aggregates. The axonal microtubule-associated protein Tau and amyloid-β undergo structural transition to β-sheet rich structure and form aggregates in neuronal soma as well as in the extracellular region. The loss of Tau from microtubules leads to the disintegration of axon and causing neuronal degeneration. This led to the development of effective drugs against AD, to prevent Tau aggregation. Here, we synthesized and screen metal-based complexes to prevent Tau protein aggregation. ThS fluorescence and TEM suggested the role of synthetic cobalt complexes in inhibiting Tau aggregation. CD spectroscopy showed that these complexes prevented conformational changes in Tau to β-sheet. CBMCs were not toxic at lower concentrations and formed non-toxic Tau species. L1 and L2 prevented membrane leakage; whereas, higher concentrations of L3 caused membrane leakage as observed by LDH release assay. The overall results indicate the synthetic cobalt complexes to be a promising molecule against AD. [ABSTRACT FROM AUTHOR]

Published

2020

46. Traumatic Brain Injury Induces Tau Aggregation and Spreading.

Author

Edwards, George, Zhao, Jing, Dash, Pramod K., Soto, Claudio, and Moreno-Gonzalez, Ines

Subjects

*BRAIN injuries, *CHRONIC traumatic encephalopathy, *TRANSGENIC mice, *NEUROFIBRILLARY tangles, *TAU proteins

Abstract

The misfolding and aggregation of tau protein into neurofibrillary tangles is the main underlying hallmark of tauopathies. Most tauopathies have a sporadic origin and can be associated with multiple risk factors. Traumatic brain injury (TBI) has been suggested as a risk factor for tauopathies by triggering disease onset and facilitating its progression. Several studies indicate that TBI seems to be a risk factor to development of Alzheimer disease and chronic traumatic encephalopathy, because there is a relationship of TBI severity and propensity to development of these illnesses. In this study, we evaluated whether moderate to severe TBI can trigger the initial formation of pathological tau that would induce the development of the pathology throughout the brain. To this end, we subjected tau transgenic mice to TBI and assessed tau phosphorylation and aggregation pattern to create a spatial heat map of tau deposition and spreading in the brain. Our results suggest that brain injured tau transgenic mice have an accelerated tau pathology in different brain regions that increases over time compared with sham mice. The appearance of pathological tau occurs in regions distant to the injury area that are connected synaptically, suggesting dissemination of tau aggregates. Overall, this work posits TBI as a risk factor for tauopathies through the induction of tau hyperphosphorylation and aggregation. [ABSTRACT FROM AUTHOR]

Published

2020

47. Curcumin-Piperlongumine Hybrids with a Multitarget Profile Elicit Neuroprotection in In Vitro Models of Oxidative Stress and Hyperphosphorylation

Author

Ángel Cores, Noelia Carmona-Zafra, Olmo Martín-Cámara, Juan Domingo Sánchez, Pablo Duarte, Mercedes Villacampa, Paloma Bermejo-Bescós, Sagrario Martín-Aragón, Rafael León, and J. Carlos Menéndez

Subjects

oxidative stress, Tau aggregation, neuroinflammation, neuroprotection, Therapeutics. Pharmacology, RM1-950

Abstract

Curcumin shows a broad spectrum of activities of relevance in the treatment of Alzheimer’s disease (AD); however, it is poorly absorbed and is also chemically and metabolically unstable, leading to a very low oral bioavailability. A small library of hybrid compounds designed as curcumin analogues and incorporating the key structural fragment of piperlongumine, a natural neuroinflammation inhibitor, were synthesized by a two-step route that combines a three-component reaction between primary amines, β-ketoesters and α-haloesters and a base-promoted acylation with cinnamoyl chlorides. These compounds were predicted to have good oral absorption and CNS permeation, had good scavenging properties in the in vitro DPPH experiment and in a cellular assay based on the oxidation of dichlorofluorescin to a fluorescent species. The compounds showed low toxicity in two cellular models, were potent inductors of the Nrf2-ARE phase II antioxidant response, inhibited PHF6 peptide aggregation, closely related to Tau protein aggregation and were active against the LPS-induced inflammatory response. They also afforded neuroprotection against an oxidative insult induced by inhibition of the mitochondrial respiratory chain with the rotenone-oligomycin A combination and against Tau hyperphosphorylation induced by the phosphatase inhibitor okadaic acid. This multitarget pharmacological profile is highly promising in the development of treatments for AD and provides a good hit structure for future optimization efforts.

Published

2021

48. Insulin-Mediated Changes in Tau Hyperphosphorylation and Autophagy in a Drosophila Model of Tauopathy and Neuroblastoma Cells

Author

Shreyasi Chatterjee, Suren. S. Ambegaokar, George R. Jackson, and Amritpal Mudher

Subjects

Alzheimer’s disease, type 2 diabetes, tau aggregation, autophagy, tau hyper-phosphorylation, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Almost 50 million people in the world are affected by dementia; the most prevalent form of which is Alzheimer’s disease (AD). Although aging is considered to be the main risk factor for AD, growing evidence from epidemiological studies suggests that type 2 diabetes mellitus (T2DM) increases the risk of dementia including AD. Defective brain insulin signaling has been suggested as an early event in AD and other tauopathies but the mechanisms that link these diseases are largely unknown. Tau hyperphosphorylation is a hallmark of neurofibrillary pathology and insulin resistance increases the number of neuritic plaques particularly in AD. Utilizing a combination of our Drosophila models of tauopathy (expressing the 2N4R-Tau) and neuroblastoma cells, we have attempted to decipher the pathways downstream of the insulin signaling cascade that lead to tau hyperphosphorylation, aggregation and autophagic defects. Using cell-based, genetic, and biochemical approaches we have demonstrated that tau phosphorylation at AT8 and PHF1 residues is enhanced in an insulin-resistant environment. We also show that insulin-induced changes in total and phospho-tau are mediated by the crosstalk of AKT, glycogen synthase kinase-3β, and extracellular regulating kinase located downstream of the insulin receptor pathway. Finally, we demonstrate a significant change in the levels of the key proteins in the mammalian target of rapamycin/autophagy pathway, implying an increased impairment of aggregated protein clearance in our transgenic Drosophila models and cultured neuroblastoma cells.

Published

2019

49. Tau Inclusions in Alzheimer's, Chronic Traumatic Encephalopathy and Pick's Disease. A Speculation on How Differences in Backbone Polarization Underlie Divergent Pathways of Tau Aggregation

Author

Andrzej Stanisław Cieplak

Subjects

intrinsically disordered proteins, polypeptide backbone, tau aggregation, Alzheimer's disease, Pick's disease, chronic traumatic encephalopathy, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Tau-related dementias appear to involve specific to each disease aggregation pathways and morphologies of filamentous tau assemblies. To understand etiology of these differences, here we elucidate molecular mechanism of formation of tau PHFs based on the PMO theory of misfolding and aggregation of pleiomorphic proteins associated with neurodegenerative diseases. In this model, fibrillization of tau is initiated by the coupled binding and folding of the MTB domains that yields antiparallel homodimers, in analogy to folding of split inteins. The free energy of binding is minimized when the antiparallel alignment brings about backbone-backbone H-bonding between the MTBD segments of similar “strand” propensities. To assess these propensities, a function of the NMR shielding tensors of the Cα atoms is introduced as the folding potential function FPi; the Cα tensors are obtained by the quantum mechanical modeling of protein secondary structure (GIAO//B3LYP/D95**). The calculated FPi plots show that the “strand” propensities of the MBTD segments, and hence the homodimer's register, can be affected by the relatively small changes in the environment's pH, as a result of protonation of MBTD's conserved histidines. The assembly of the antiparallel tau dimers into granular aggregates and their subsequent conversion into the parallel cross-β structure of paired helical filaments is expected to follow the same path as the previously described fibrillization of Aβ. Consequently, the core structure of the nascent tau fibril is determined by the register of the tau homodimer. This model accounts for the reported differences in (i) fibril-core structure of in vivo and in vitro filaments, (ii) cross-seeding of isoforms, (iii) effects of reducing/non-reducing conditions, (iv) effects of PHF6 mutations, and (v) homologs' aggregation properties. The proposed model also suggests that in contrast to Alzheimer's and chronic traumatic encephalopathy disease, the assembly of tau prions in Pick's disease would be facilitated by a moderate drop in pH that accompanies e.g., transit in the endosomal system, inflammation response or an ischemic injury.

Published

2019

50. EB1 Increases the Dynamics of Tau Droplets and Inhibits Tau Aggregation: Implications in Tauopathies.

Author

Venkatramani A, Ashtam A, and Panda D

Subjects

Humans, Microtubule-Associated Proteins metabolism, Microtubules metabolism, Tubulin metabolism, tau Proteins metabolism, Neuroblastoma metabolism, Tauopathies metabolism

Abstract

EB1, a microtubule plus end-tracking protein (+TIP), regulates microtubule dynamics. Recent evidence indicates cross-talk between EB proteins and tau, a microtubule-associated neuronal protein that is important for the growth and stability of microtubules. We investigated the interaction between tau and EB1 and the effect of binding of EB1 on tau function and aggregation. EB1 colocalized with tau in SH-SY5Y cells and coimmunoprecipitated with tau. Further, purified EB1 impaired the ability of adult tau to induce tubulin polymerization in vitro . EB1 bound to tau with a dissociation constant of 2.5 ± 0.7 μM. EB1 reduced heparin-induced tau aggregation with a half-maximal inhibitory concentration of 4.3 ± 0.2 μM, and increased the dynamics of tau in phase-separated droplets. The fluorescence recovery rate in tau droplets increased from 0.02 ± 0.01 to 0.07 ± 0.03 s -1 , while the half-time of recovery decreased from 44.5 ± 14 to 13.5 ± 6 s in the presence of 8 μM EB1, suggesting a delay in the transition of tau from the soluble to aggregated form in tau liquid-liquid phase separation. EB1 decreased the rate of aggregation and increased the critical concentration of tau aggregation. Dynamic light scattering, atomic force microscopy, dot blot assays, and SDS-PAGE analysis showed that EB1 inhibited the formation of oligomers and higher-order aggregates of tau. The data suggest a novel role for EB1 as a regulator of tau function and aggregation, and the findings indicated the role of the EB family proteins in neuronal function and neurodegeneration.

Published

2024