FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4313478646> ?p ?o ?g. }

• W4313478646 endingPage "102597" @default.
• W4313478646 startingPage "102597" @default.
• W4313478646 abstract "Tauopathies are a major type of proteinopathies underlying neurodegenerative diseases. Mutations in the tau-encoding MAPT-gene lead to hereditary cases of frontotemporal lobar degeneration (FTLD)-tau, which span a wide phenotypic and pathological spectrum. Some of these mutations, such as the N279K mutation, result in a shift of the physiological 3R/4R ratio towards the more aggregation prone 4R isoform. Other mutations such as V337M cause a decrease in the in vitro affinity of tau to microtubules and a reduced ability to promote microtubule assembly. Whether both mutations address similar downstream signalling cascades remains unclear but is important for potential rescue strategies. Here, we developed a novel and optimised forward programming protocol for the rapid and highly efficient production of pure cultures of glutamatergic cortical neurons from hiPSCs. We apply this protocol to delineate mechanisms of neurodegeneration in an FTLD-tau hiPSC-model consisting of MAPTN279K- or MAPTV337M-mutants and wild-type or isogenic controls. The resulting cortical neurons express MAPT-genotype-dependent dominant proteome clusters regulating apoptosis, ROS homeostasis and mitochondrial function. Related pathways are significantly upregulated in MAPTN279K neurons but not in MAPTV337M neurons or controls. Live cell imaging demonstrates that both MAPT mutations affect excitability of membranes as reflected in spontaneous and stimulus evoked calcium signals when compared to controls, albeit more pronounced in MAPTN279K neurons. These spontaneous calcium oscillations in MAPTN279K neurons triggered mitochondrial hyperpolarisation and fission leading to mitochondrial ROS production, but also ROS production through NOX2 acting together to induce cell death. Importantly, we found that these mechanisms are MAPT mutation-specific and were observed in MAPTN279K neurons, but not in MAPTV337M neurons, supporting a pathological role of the 4R tau isoform in redox disbalance and highlighting MAPT-mutation specific clinicopathological-genetic correlations, which may inform rescue strategies in different MAPT mutations." @default.
• W4313478646 created "2023-01-06" @default.
• W4313478646 creator A5007880092 @default.
• W4313478646 creator A5012259669 @default.
• W4313478646 creator A5023953483 @default.
• W4313478646 creator A5029306578 @default.
• W4313478646 creator A5034872348 @default.
• W4313478646 creator A5038373894 @default.
• W4313478646 creator A5049216452 @default.
• W4313478646 creator A5059642763 @default.
• W4313478646 creator A5060778659 @default.
• W4313478646 creator A5060964395 @default.
• W4313478646 creator A5065525659 @default.
• W4313478646 creator A5071739030 @default.
• W4313478646 creator A5077244943 @default.
• W4313478646 creator A5082161323 @default.
• W4313478646 creator A5086688205 @default.
• W4313478646 creator A5089730879 @default.
• W4313478646 date "2023-02-01" @default.
• W4313478646 modified "2023-10-01" @default.
• W4313478646 title "MAPT genotype-dependent mitochondrial aberration and ROS production trigger dysfunction and death in cortical neurons of patients with hereditary FTLD" @default.
• W4313478646 cites W1465395011 @default.
• W4313478646 cites W1509571186 @default.
• W4313478646 cites W150987474 @default.
• W4313478646 cites W1511517753 @default.
• W4313478646 cites W1569078050 @default.
• W4313478646 cites W1764460837 @default.
• W4313478646 cites W1795598048 @default.
• W4313478646 cites W1848563179 @default.
• W4313478646 cites W1970308606 @default.
• W4313478646 cites W1972959301 @default.
• W4313478646 cites W1985730861 @default.
• W4313478646 cites W1988884999 @default.
• W4313478646 cites W2005311608 @default.
• W4313478646 cites W2011842392 @default.
• W4313478646 cites W2014033528 @default.
• W4313478646 cites W2023652080 @default.
• W4313478646 cites W2024627685 @default.
• W4313478646 cites W2030775222 @default.
• W4313478646 cites W2035462700 @default.
• W4313478646 cites W2040027262 @default.
• W4313478646 cites W2043478432 @default.
• W4313478646 cites W2052742260 @default.
• W4313478646 cites W2059501379 @default.
• W4313478646 cites W2066459208 @default.
• W4313478646 cites W2082388312 @default.
• W4313478646 cites W2124317694 @default.
• W4313478646 cites W2129390057 @default.
• W4313478646 cites W2133603940 @default.
• W4313478646 cites W2147718170 @default.
• W4313478646 cites W2153206087 @default.
• W4313478646 cites W2155893343 @default.
• W4313478646 cites W2172007938 @default.
• W4313478646 cites W2415373443 @default.
• W4313478646 cites W2511608637 @default.
• W4313478646 cites W2516117108 @default.
• W4313478646 cites W2529866404 @default.
• W4313478646 cites W2558758033 @default.
• W4313478646 cites W2570634615 @default.
• W4313478646 cites W2592476914 @default.
• W4313478646 cites W2594390960 @default.
• W4313478646 cites W2599676012 @default.
• W4313478646 cites W2605465471 @default.
• W4313478646 cites W2775738646 @default.
• W4313478646 cites W2883093512 @default.
• W4313478646 cites W2886265612 @default.
• W4313478646 cites W2899760200 @default.
• W4313478646 cites W2928352487 @default.
• W4313478646 cites W2998669529 @default.
• W4313478646 cites W3017944168 @default.
• W4313478646 cites W3095251182 @default.
• W4313478646 cites W3165842025 @default.
• W4313478646 cites W3175499610 @default.
• W4313478646 cites W3195151239 @default.
• W4313478646 cites W4284895216 @default.
• W4313478646 cites W4362221370 @default.
• W4313478646 cites W47608607 @default.
• W4313478646 doi "https://doi.org/10.1016/j.redox.2022.102597" @default.
• W4313478646 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/36599286" @default.
• W4313478646 hasPublicationYear "2023" @default.
• W4313478646 type Work @default.
• W4313478646 citedByCount "4" @default.
• W4313478646 countsByYear W43134786462023 @default.
• W4313478646 crossrefType "journal-article" @default.
• W4313478646 hasAuthorship W4313478646A5007880092 @default.
• W4313478646 hasAuthorship W4313478646A5012259669 @default.
• W4313478646 hasAuthorship W4313478646A5023953483 @default.
• W4313478646 hasAuthorship W4313478646A5029306578 @default.
• W4313478646 hasAuthorship W4313478646A5034872348 @default.
• W4313478646 hasAuthorship W4313478646A5038373894 @default.
• W4313478646 hasAuthorship W4313478646A5049216452 @default.
• W4313478646 hasAuthorship W4313478646A5059642763 @default.
• W4313478646 hasAuthorship W4313478646A5060778659 @default.
• W4313478646 hasAuthorship W4313478646A5060964395 @default.
• W4313478646 hasAuthorship W4313478646A5065525659 @default.
• W4313478646 hasAuthorship W4313478646A5071739030 @default.
• W4313478646 hasAuthorship W4313478646A5077244943 @default.
• W4313478646 hasAuthorship W4313478646A5082161323 @default.

• next