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30 results
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TDP-43 involvement. Biomarker strategies, including cerebrospinal fluid TDP-43
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TDP-43. The TDP-43 protein contains multiple arginine-rich
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TDP-43 pathology, and p38α inhibition reduces pathological TDP-43
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TDP-43-Aβ and TDP-43-tau interaction complexes in CSF, with
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TDP-43). Under physiological conditions, TDP-43 functions as a nuclear
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TDP-43 localization and normalized expression of TDP-43-regulated
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TDP-43 functionality. TDP-43 (TAR DNA-binding protein 43) is a predominantly
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- Hypothesis HSPB1 Phosphorylation Mimetics to Promote Protective TDP-43 Liquid-Liquid Phase Separation
TDP-43 Liquid-Liquid Phase Separation ## Scientific Rationale TDP-43
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TDP-43 Mitochondrial Import starts from the claim that modulating
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TDP-43 encephalopathy (LATE). Under physiological conditions, TDP-43 functions
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TDP-43. The low complexity domain of TDP-43, spanning
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TDP-43 encephalopathy (LATE), and other TDP-43 proteinopathies affecting
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TDP-43. Under physiological conditions, circPDS5B maintains homeostatic levels of TDP
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TDP-43 proteinopathy in neurodegenerative diseases. The central hypothesis revolves
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TDP-43 function and microtubule dynamics regulation. TDP-43 (TAR DNA-binding
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TDP-43 Depletion Drives Synaptic Splicing Dysregulation in ALS-FTD starts
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TDP-43 starts from the claim that Pathological TDP-43
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TDP-43 fragments—reliable biomarkers of TDP-43 cleavage and aggregation
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TDP-43 and tau aggregation pathways, as phosphorylated TDP-43
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TDP-43 in motor neurons, with approximately 70-80% of TDP
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TDP-43 truncation (cTDP-43 fragments) that lose normal DNA repair
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TDP-43 aggregation sequesters SNAP29 and syntaxin-17, blocking autophagosome
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TDP-43 Proteinopathy Neuroinflammation in ALS/FTD starts from the claim
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TDP-43 Toxicity starts from the claim that modulating MCU, CK1D
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TDP-43 localization by 4-6 weeks. Phosphorylated TDP-43
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TDP-43 Traps TRIM21 Into Inactive Complexes starts from the claim
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TDP-43 models, maintaining normal mitochondrial aspect ratios (3.2±0.4 vs 1.8±0.3 in TDP
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TDP-43 clearance co-localization data from FTLD, not AD-TDP
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TDP-43 pathology. The proposed pathway connects astrocytic APOE4 to GLT-1 glutamate
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TDP-43 accumulation in AD neurons disrupts normal nuclear function
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