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W4284971024 abstract "Alzheimer's disease (AD) is the most common cause of mental dementia in the aged population. AD is characterized by the progressive decline of memory and multiple cognitive functions, and changes in behavior and personality. Recent research has revealed age-dependent increased levels of VDAC1 in postmortem AD brains and cerebral cortices of APP, APPxPS1, and 3xAD.Tg mice. Further, we found abnormal interaction between VDAC1 and P-Tau in the AD brains, leading to mitochondrial structural and functional defects. Our current study aimed to understand the impact of a partial reduction of voltage-dependent anion channel 1 (VDAC1) protein on mitophagy/autophagy, mitochondrial and synaptic activities, and behavior changes in transgenic TAU mice in Alzheimer's disease. To determine if a partial reduction of VDAC1 reduces mitochondrial and synaptic toxicities in transgenic Tau (P301L) mice, we crossed heterozygote VDAC1 knockout (VDAC1+/- ) mice with TAU mice and generated double mutant (VDAC1+/- /TAU) mice. We assessed phenotypic behavior, protein levels of mitophagy, autophagy, synaptic, other key proteins, mitochondrial morphology, and dendritic spines in TAU mice relative to double mutant mice. Partial reduction of VDAC1 rescued the TAU-induced behavioral impairments such as motor coordination and exploratory behavioral changes, and learning and spatial memory impairments in VDAC1+/- /TAU mice. Protein levels of mitophagy, autophagy, and synaptic proteins were significantly increased in double mutant mice compared with TAU mice. In addition, dendritic spines were significantly increased; the mitochondrial number was significantly reduced, and mitochondrial length was increased in double mutant mice. Based on these observations, we conclude that reduced VDAC1 is beneficial in symptomatic-transgenic TAU mice." @default.
W4284971024 created "2022-07-10" @default.
W4284971024 creator A5042058638 @default.
W4284971024 creator A5053127310 @default.
W4284971024 creator A5062197554 @default.
W4284971024 creator A5067956284 @default.
W4284971024 creator A5083946168 @default.
W4284971024 creator A5084673116 @default.
W4284971024 date "2022-07-07" @default.
W4284971024 modified "2023-10-15" @default.
W4284971024 title "A partial reduction of <scp>VDAC1</scp> enhances mitophagy, autophagy, synaptic activities in a transgenic Tau mouse model" @default.
W4284971024 cites W112421516 @default.
W4284971024 cites W1480786153 @default.
W4284971024 cites W1564001101 @default.
W4284971024 cites W1564336783 @default.
W4284971024 cites W1573153072 @default.
W4284971024 cites W1601030123 @default.
W4284971024 cites W1602771322 @default.
W4284971024 cites W1912085582 @default.
W4284971024 cites W1968362444 @default.
W4284971024 cites W1975910482 @default.
W4284971024 cites W1979489548 @default.
W4284971024 cites W1979645469 @default.
W4284971024 cites W1993160420 @default.
W4284971024 cites W1996981671 @default.
W4284971024 cites W2000742321 @default.
W4284971024 cites W2001389093 @default.
W4284971024 cites W2002930469 @default.
W4284971024 cites W2007047564 @default.
W4284971024 cites W2011353108 @default.
W4284971024 cites W2017462929 @default.
W4284971024 cites W2024108470 @default.
W4284971024 cites W2025872915 @default.
W4284971024 cites W2034087770 @default.
W4284971024 cites W2042508628 @default.
W4284971024 cites W2049016912 @default.
W4284971024 cites W2053273794 @default.
W4284971024 cites W2054645758 @default.
W4284971024 cites W2061404811 @default.
W4284971024 cites W2082841638 @default.
W4284971024 cites W2087240799 @default.
W4284971024 cites W2089141103 @default.
W4284971024 cites W2090217381 @default.
W4284971024 cites W2094162211 @default.
W4284971024 cites W2098676436 @default.
W4284971024 cites W2099860718 @default.
W4284971024 cites W2100084621 @default.
W4284971024 cites W2100262552 @default.
W4284971024 cites W2103024032 @default.
W4284971024 cites W2105442740 @default.
W4284971024 cites W2106296386 @default.
W4284971024 cites W2115466888 @default.
W4284971024 cites W2121077787 @default.
W4284971024 cites W2129739398 @default.
W4284971024 cites W2131952786 @default.
W4284971024 cites W2133103790 @default.
W4284971024 cites W2135986226 @default.
W4284971024 cites W2136937485 @default.
W4284971024 cites W2142350129 @default.
W4284971024 cites W21428969 @default.
W4284971024 cites W2144096576 @default.
W4284971024 cites W2144956444 @default.
W4284971024 cites W2146282250 @default.
W4284971024 cites W2146885685 @default.
W4284971024 cites W2149090315 @default.
W4284971024 cites W2151283457 @default.
W4284971024 cites W2152165298 @default.
W4284971024 cites W2156313819 @default.
W4284971024 cites W2157751043 @default.
W4284971024 cites W2158328957 @default.
W4284971024 cites W2163859059 @default.
W4284971024 cites W2165427528 @default.
W4284971024 cites W2169152986 @default.
W4284971024 cites W2172204522 @default.
W4284971024 cites W2229190653 @default.
W4284971024 cites W2257218554 @default.
W4284971024 cites W2311380696 @default.
W4284971024 cites W2516368667 @default.
W4284971024 cites W2519570594 @default.
W4284971024 cites W2536701740 @default.
W4284971024 cites W2583298501 @default.
W4284971024 cites W2584608383 @default.
W4284971024 cites W2586594127 @default.
W4284971024 cites W2733951407 @default.
W4284971024 cites W2761011647 @default.
W4284971024 cites W2764071986 @default.
W4284971024 cites W2789405288 @default.
W4284971024 cites W2790161245 @default.
W4284971024 cites W2790842992 @default.
W4284971024 cites W2796906206 @default.
W4284971024 cites W2802911313 @default.
W4284971024 cites W2891635110 @default.
W4284971024 cites W2900998599 @default.
W4284971024 cites W2911248861 @default.
W4284971024 cites W2913440408 @default.
W4284971024 cites W2945779890 @default.
W4284971024 cites W2966592848 @default.
W4284971024 cites W2980025301 @default.
W4284971024 cites W2999771085 @default.
W4284971024 cites W3005606800 @default.