FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W3043443561> ?p ?o ?g. }

• W3043443561 endingPage "14" @default.
• W3043443561 startingPage "1" @default.
• W3043443561 abstract "The formation of neurofibrillary tangles has been implicated as an important pathological marker for Alzheimer’s disease (AD). Studies have revealed that the inhibition of abnormal hyperphosphorylation and aggregation of tau in the AD brain might serve as an important drug target. Using in vitro and in vivo experimental models, such as the AD mouse model (5xFAD mice), we investigated the inhibition of hyperphosphorylation of tau using the human umbilical cord blood-derived mesenchymal stem cells (hUCB-MSCs). Administration of hUCB-MSCs not only ameliorated the spatial learning and memory impairments but also mitigated the hyperphosphorylation of tau in 5xFAD mice. Furthermore, in vivo experiments in mice and in vitro ThT fluorescence assay validated galectin-3 (GAL-3) as an essential factor of hUCB-MSC. Moreover, GAL-3 was observed to be involved in the removal of aberrant forms of tau, by reducing hyperphosphorylation through decrements in the glycogen synthase kinase 3 beta (GSK-3 β ). Our results confirm that GAL-3, secreted by hUCB-MSC, regulates the abnormal accumulation of tau by protein-protein interactions. This study suggests that hUCB-MSCs mitigate hyperphosphorylation of tau through GAL-3 secretion. These findings highlight the potential role of hUCB-MSCs as a therapeutic agent for aberrant tau in AD." @default.
• W3043443561 created "2020-07-23" @default.
• W3043443561 creator A5023915332 @default.
• W3043443561 creator A5058515910 @default.
• W3043443561 creator A5059760054 @default.
• W3043443561 creator A5059976643 @default.
• W3043443561 creator A5062049299 @default.
• W3043443561 creator A5063112254 @default.
• W3043443561 date "2020-07-18" @default.
• W3043443561 modified "2023-09-23" @default.
• W3043443561 title "Galectin-3 Secreted by Human Umbilical Cord Blood-Derived Mesenchymal Stem Cells Reduces Aberrant Tau Phosphorylation in an Alzheimer Disease Model" @default.
• W3043443561 cites W1530520327 @default.
• W3043443561 cites W1600934558 @default.
• W3043443561 cites W162803433 @default.
• W3043443561 cites W1733847523 @default.
• W3043443561 cites W1942922429 @default.
• W3043443561 cites W1969615032 @default.
• W3043443561 cites W1972493045 @default.
• W3043443561 cites W1975040221 @default.
• W3043443561 cites W1976602187 @default.
• W3043443561 cites W1993327095 @default.
• W3043443561 cites W1998282284 @default.
• W3043443561 cites W2001127699 @default.
• W3043443561 cites W2009799196 @default.
• W3043443561 cites W2011197454 @default.
• W3043443561 cites W2011803642 @default.
• W3043443561 cites W2013308243 @default.
• W3043443561 cites W2014222652 @default.
• W3043443561 cites W2015948653 @default.
• W3043443561 cites W2021734242 @default.
• W3043443561 cites W2031507955 @default.
• W3043443561 cites W2035470211 @default.
• W3043443561 cites W2044513730 @default.
• W3043443561 cites W2050463440 @default.
• W3043443561 cites W2057193931 @default.
• W3043443561 cites W2059809766 @default.
• W3043443561 cites W2060490044 @default.
• W3043443561 cites W2061953902 @default.
• W3043443561 cites W2062106032 @default.
• W3043443561 cites W2070929003 @default.
• W3043443561 cites W2070991505 @default.
• W3043443561 cites W2073128231 @default.
• W3043443561 cites W2077631696 @default.
• W3043443561 cites W2080415606 @default.
• W3043443561 cites W2082429191 @default.
• W3043443561 cites W2095066614 @default.
• W3043443561 cites W2097801964 @default.
• W3043443561 cites W2121214202 @default.
• W3043443561 cites W2124121545 @default.
• W3043443561 cites W2128932095 @default.
• W3043443561 cites W2144091853 @default.
• W3043443561 cites W2144949842 @default.
• W3043443561 cites W2147954894 @default.
• W3043443561 cites W2156093068 @default.
• W3043443561 cites W2159377066 @default.
• W3043443561 cites W2170644095 @default.
• W3043443561 cites W2226005455 @default.
• W3043443561 cites W2272060897 @default.
• W3043443561 cites W2302116106 @default.
• W3043443561 cites W2462234872 @default.
• W3043443561 cites W2463434945 @default.
• W3043443561 cites W2548586067 @default.
• W3043443561 cites W2552728987 @default.
• W3043443561 cites W2578655793 @default.
• W3043443561 cites W2613267922 @default.
• W3043443561 cites W2615732360 @default.
• W3043443561 cites W2615798278 @default.
• W3043443561 cites W2744402516 @default.
• W3043443561 cites W2776868171 @default.
• W3043443561 cites W2781937491 @default.
• W3043443561 cites W2789752648 @default.
• W3043443561 cites W2797727149 @default.
• W3043443561 cites W2808028315 @default.
• W3043443561 cites W2892215859 @default.
• W3043443561 cites W2922142848 @default.
• W3043443561 cites W2938377166 @default.
• W3043443561 cites W2944988109 @default.
• W3043443561 cites W2981221281 @default.
• W3043443561 doi "https://doi.org/10.1155/2020/8878412" @default.
• W3043443561 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/7383310" @default.
• W3043443561 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/32733573" @default.
• W3043443561 hasPublicationYear "2020" @default.
• W3043443561 type Work @default.
• W3043443561 sameAs 3043443561 @default.
• W3043443561 citedByCount "16" @default.
• W3043443561 countsByYear W30434435612021 @default.
• W3043443561 countsByYear W30434435612022 @default.
• W3043443561 countsByYear W30434435612023 @default.
• W3043443561 crossrefType "journal-article" @default.
• W3043443561 hasAuthorship W3043443561A5023915332 @default.
• W3043443561 hasAuthorship W3043443561A5058515910 @default.
• W3043443561 hasAuthorship W3043443561A5059760054 @default.
• W3043443561 hasAuthorship W3043443561A5059976643 @default.
• W3043443561 hasAuthorship W3043443561A5062049299 @default.
• W3043443561 hasAuthorship W3043443561A5063112254 @default.
• W3043443561 hasBestOaLocation W30434435611 @default.
• W3043443561 hasConcept C11960822 @default.
• W3043443561 hasConcept C142724271 @default.

• next