FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4377019664> ?p ?o ?g. }

• W4377019664 endingPage "2719" @default.
• W4377019664 startingPage "2711" @default.
• W4377019664 abstract "The cumulative damage caused by repetitive mild traumatic brain injury can cause long-term neurodegeneration leading to cognitive impairment. This cognitive impairment is thought to result specifically from damage to the hippocampus. In this study, we detected cognitive impairment in mice 6 weeks after repetitive mild traumatic brain injury using the novel object recognition test and the Morris water maze test. Immunofluorescence staining showed that p-tau expression was increased in the hippocampus after repetitive mild traumatic brain injury. Golgi staining showed a significant decrease in the total density of neuronal dendritic spines in the hippocampus, as well as in the density of mature dendritic spines. To investigate the specific molecular mechanisms underlying cognitive impairment due to hippocampal damage, we performed proteomic and phosphoproteomic analyses of the hippocampus with and without repetitive mild traumatic brain injury. The differentially expressed proteins were mainly enriched in inflammation, immunity, and coagulation, suggesting that non-neuronal cells are involved in the pathological changes that occur in the hippocampus in the chronic stage after repetitive mild traumatic brain injury. In contrast, differentially expressed phosphorylated proteins were mainly enriched in pathways related to neuronal function and structure, which is more consistent with neurodegeneration. We identified N-methyl-D-aspartate receptor 1 as a hub molecule involved in the response to repetitive mild traumatic brain injury , and western blotting showed that, while N-methyl-D-aspartate receptor 1 expression was not altered in the hippocampus after repetitive mild traumatic brain injury, its phosphorylation level was significantly increased, which is consistent with the omics results. Administration of GRP78608, an N-methyl-D-aspartate receptor 1 antagonist, to the hippocampus markedly improved repetitive mild traumatic brain injury-induced cognitive impairment. In conclusion, our findings suggest that N-methyl-D-aspartate receptor 1 signaling in the hippocampus is involved in cognitive impairment in the chronic stage after repetitive mild traumatic brain injury and may be a potential target for intervention and treatment." @default.
• W4377019664 created "2023-05-19" @default.
• W4377019664 creator A5006012404 @default.
• W4377019664 creator A5008427935 @default.
• W4377019664 creator A5019349493 @default.
• W4377019664 creator A5029420268 @default.
• W4377019664 creator A5029538512 @default.
• W4377019664 creator A5033231648 @default.
• W4377019664 creator A5043876952 @default.
• W4377019664 creator A5050393948 @default.
• W4377019664 creator A5065288562 @default.
• W4377019664 creator A5077508570 @default.
• W4377019664 creator A5079870659 @default.
• W4377019664 creator A5086529957 @default.
• W4377019664 date "2023-05-12" @default.
• W4377019664 modified "2023-10-18" @default.
• W4377019664 title "Quantitative proteomic and phosphoproteomic analyses of the hippocampus reveal the involvement of NMDAR1 signaling in repetitive mild traumatic brain injury" @default.
• W4377019664 cites W1509460845 @default.
• W4377019664 cites W1781730610 @default.
• W4377019664 cites W1970802518 @default.
• W4377019664 cites W1973404434 @default.
• W4377019664 cites W1989879415 @default.
• W4377019664 cites W1991909451 @default.
• W4377019664 cites W1992414754 @default.
• W4377019664 cites W2005758956 @default.
• W4377019664 cites W2009662334 @default.
• W4377019664 cites W2012491213 @default.
• W4377019664 cites W2014756302 @default.
• W4377019664 cites W2016748026 @default.
• W4377019664 cites W2019416392 @default.
• W4377019664 cites W2031222456 @default.
• W4377019664 cites W2031704980 @default.
• W4377019664 cites W2037138754 @default.
• W4377019664 cites W2047363376 @default.
• W4377019664 cites W2060612467 @default.
• W4377019664 cites W2062223404 @default.
• W4377019664 cites W2067966687 @default.
• W4377019664 cites W2077100662 @default.
• W4377019664 cites W2081874117 @default.
• W4377019664 cites W2106261678 @default.
• W4377019664 cites W2109946226 @default.
• W4377019664 cites W2137938185 @default.
• W4377019664 cites W2159482845 @default.
• W4377019664 cites W2314970270 @default.
• W4377019664 cites W2462917668 @default.
• W4377019664 cites W2509240827 @default.
• W4377019664 cites W2516703534 @default.
• W4377019664 cites W2586877771 @default.
• W4377019664 cites W2594653909 @default.
• W4377019664 cites W2606173963 @default.
• W4377019664 cites W2606478035 @default.
• W4377019664 cites W2610621727 @default.
• W4377019664 cites W2766268933 @default.
• W4377019664 cites W2770830089 @default.
• W4377019664 cites W2898505717 @default.
• W4377019664 cites W2902125374 @default.
• W4377019664 cites W2907341743 @default.
• W4377019664 cites W2914947612 @default.
• W4377019664 cites W2950951682 @default.
• W4377019664 cites W2954418115 @default.
• W4377019664 cites W2955184815 @default.
• W4377019664 cites W2964824489 @default.
• W4377019664 cites W2967222948 @default.
• W4377019664 cites W2975048791 @default.
• W4377019664 cites W2980016890 @default.
• W4377019664 cites W2990254633 @default.
• W4377019664 cites W3000080966 @default.
• W4377019664 cites W3005742140 @default.
• W4377019664 cites W3014474568 @default.
• W4377019664 cites W3015042576 @default.
• W4377019664 cites W3044340453 @default.
• W4377019664 cites W3093476080 @default.
• W4377019664 cites W3117024003 @default.
• W4377019664 cites W3126902774 @default.
• W4377019664 cites W3128428002 @default.
• W4377019664 cites W3147199143 @default.
• W4377019664 cites W3153773701 @default.
• W4377019664 cites W3173778575 @default.
• W4377019664 cites W3185882388 @default.
• W4377019664 cites W3202909993 @default.
• W4377019664 cites W4206361268 @default.
• W4377019664 cites W4210733870 @default.
• W4377019664 cites W4220854722 @default.
• W4377019664 cites W4229012524 @default.
• W4377019664 cites W4283269902 @default.
• W4377019664 cites W4285801091 @default.
• W4377019664 cites W4294216483 @default.
• W4377019664 doi "https://doi.org/10.4103/1673-5374.374654" @default.
• W4377019664 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/37449635" @default.
• W4377019664 hasPublicationYear "2023" @default.
• W4377019664 type Work @default.
• W4377019664 citedByCount "0" @default.
• W4377019664 crossrefType "journal-article" @default.
• W4377019664 hasAuthorship W4377019664A5006012404 @default.
• W4377019664 hasAuthorship W4377019664A5008427935 @default.
• W4377019664 hasAuthorship W4377019664A5019349493 @default.
• W4377019664 hasAuthorship W4377019664A5029420268 @default.
• W4377019664 hasAuthorship W4377019664A5029538512 @default.

• next