FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4281777148> ?p ?o ?g. }

• W4281777148 endingPage "110913" @default.
• W4281777148 startingPage "110913" @default.
• W4281777148 abstract "An intronic (G4C2)n expansion in C9orf72 causes amyotrophic lateral sclerosis and frontotemporal dementia primarily through gain-of-function mechanisms: the accumulation of sense and antisense repeat RNA foci and dipeptide repeat (DPR) proteins (poly-GA/GP/GR/PA/PR) translated from repeat RNA. To therapeutically block this pathway, we screen a library of 1,430 approved drugs and known bioactive compounds in patient-derived induced pluripotent stem cell-derived neurons (iPSC-Neurons) for inhibitors of DPR expression. The clinically used guanosine/cytidine analogs decitabine, entecavir, and nelarabine reduce poly-GA/GP expression, with decitabine being the most potent. Hit compounds nearly abolish sense and antisense RNA foci and reduce expression of the repeat-containing nascent C9orf72 RNA transcript and its mature mRNA with minimal effects on global gene expression, suggesting that they specifically act on repeat transcription. Importantly, decitabine treatment reduces (G4C2)n foci and DPRs in C9orf72 BAC transgenic mice. Our findings suggest that nucleoside analogs are a promising compound class for therapeutic development in C9orf72 repeat-expansion-associated disorders." @default.
• W4281777148 created "2022-06-13" @default.
• W4281777148 creator A5002343259 @default.
• W4281777148 creator A5006191068 @default.
• W4281777148 creator A5014535603 @default.
• W4281777148 creator A5014982696 @default.
• W4281777148 creator A5015542289 @default.
• W4281777148 creator A5026032684 @default.
• W4281777148 creator A5034936279 @default.
• W4281777148 creator A5037187581 @default.
• W4281777148 creator A5037719541 @default.
• W4281777148 creator A5040670619 @default.
• W4281777148 creator A5040749566 @default.
• W4281777148 creator A5042914162 @default.
• W4281777148 creator A5051305145 @default.
• W4281777148 creator A5054217973 @default.
• W4281777148 creator A5054997255 @default.
• W4281777148 creator A5057989264 @default.
• W4281777148 creator A5067385624 @default.
• W4281777148 creator A5080670617 @default.
• W4281777148 creator A5082317538 @default.
• W4281777148 creator A5083784674 @default.
• W4281777148 creator A5091747176 @default.
• W4281777148 date "2022-06-01" @default.
• W4281777148 modified "2023-09-25" @default.
• W4281777148 title "Drug screen in iPSC-Neurons identifies nucleoside analogs as inhibitors of (G4C2)n expression in C9orf72 ALS/FTD" @default.
• W4281777148 cites W1504564486 @default.
• W4281777148 cites W1533438796 @default.
• W4281777148 cites W1982725145 @default.
• W4281777148 cites W1984538960 @default.
• W4281777148 cites W1985010554 @default.
• W4281777148 cites W2001604203 @default.
• W4281777148 cites W2007568107 @default.
• W4281777148 cites W2013488820 @default.
• W4281777148 cites W2016195040 @default.
• W4281777148 cites W2035618305 @default.
• W4281777148 cites W2039901186 @default.
• W4281777148 cites W2040027262 @default.
• W4281777148 cites W2054068057 @default.
• W4281777148 cites W2054542675 @default.
• W4281777148 cites W2061981717 @default.
• W4281777148 cites W2066173903 @default.
• W4281777148 cites W2069171272 @default.
• W4281777148 cites W2072947354 @default.
• W4281777148 cites W2095855829 @default.
• W4281777148 cites W2099232044 @default.
• W4281777148 cites W2113534011 @default.
• W4281777148 cites W2114872355 @default.
• W4281777148 cites W2119679922 @default.
• W4281777148 cites W2123193865 @default.
• W4281777148 cites W2131551315 @default.
• W4281777148 cites W2132814495 @default.
• W4281777148 cites W2137039075 @default.
• W4281777148 cites W2137592631 @default.
• W4281777148 cites W2138977668 @default.
• W4281777148 cites W2139264742 @default.
• W4281777148 cites W2150523249 @default.
• W4281777148 cites W2154945114 @default.
• W4281777148 cites W2160995259 @default.
• W4281777148 cites W2161413262 @default.
• W4281777148 cites W2170098894 @default.
• W4281777148 cites W2170711824 @default.
• W4281777148 cites W2304886140 @default.
• W4281777148 cites W2337901090 @default.
• W4281777148 cites W2338545563 @default.
• W4281777148 cites W2603984147 @default.
• W4281777148 cites W2606980242 @default.
• W4281777148 cites W2751645476 @default.
• W4281777148 cites W2767664549 @default.
• W4281777148 cites W2773167564 @default.
• W4281777148 cites W2782523843 @default.
• W4281777148 cites W2787027993 @default.
• W4281777148 cites W2902982722 @default.
• W4281777148 cites W2905196328 @default.
• W4281777148 cites W2908795173 @default.
• W4281777148 cites W2921042490 @default.
• W4281777148 cites W2949082553 @default.
• W4281777148 cites W2973039076 @default.
• W4281777148 cites W2981085933 @default.
• W4281777148 cites W2981866831 @default.
• W4281777148 cites W2987949299 @default.
• W4281777148 cites W2995882197 @default.
• W4281777148 cites W3005905327 @default.
• W4281777148 cites W3015984203 @default.
• W4281777148 cites W3021436433 @default.
• W4281777148 cites W3036311811 @default.
• W4281777148 cites W3045265801 @default.
• W4281777148 cites W3047793391 @default.
• W4281777148 cites W3062227316 @default.
• W4281777148 cites W3193479599 @default.
• W4281777148 cites W3208479311 @default.
• W4281777148 cites W4298878794 @default.
• W4281777148 doi "https://doi.org/10.1016/j.celrep.2022.110913" @default.
• W4281777148 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/35675776" @default.
• W4281777148 hasPublicationYear "2022" @default.
• W4281777148 type Work @default.
• W4281777148 citedByCount "5" @default.
• W4281777148 countsByYear W42817771482022 @default.

• next