FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1837429296> ?p ?o ?g. }

• W1837429296 endingPage "876" @default.
• W1837429296 startingPage "863" @default.
• W1837429296 abstract "The loss of chromosome 9 open reading frame 72 (C9ORF72) expression, associated with C9ORF72 repeat expansions, has not been examined systematically. Three C9ORF72 transcript variants have been described thus far; the GGGGCC repeat is located between two non-coding exons (exon 1a and exon 1b) in the promoter region of transcript variant 2 (NM_018325.4) or in the first intron of variant 1 (NM_145005.6) and variant 3 (NM_001256054.2). We studied C9ORF72 expression in expansion carriers (n = 56) for whom cerebellum and/or frontal cortex was available. Using quantitative real-time PCR and digital molecular barcoding techniques, we assessed total C9ORF72 transcripts, variant 1, variant 2, variant 3, and intron containing transcripts [upstream of the expansion (intron 1a) and downstream of the expansion (intron 1b)]; the latter were correlated with levels of poly(GP) and poly(GA) proteins aberrantly translated from the expansion as measured by immunoassay (n = 50). We detected a decrease in expansion carriers as compared to controls for total C9ORF72 transcripts, variant 1, and variant 2: the strongest association was observed for variant 2 (quantitative real-time PCR cerebellum: median 43 %, p = 1.26e-06, and frontal cortex: median 58 %, p = 1.11e-05; digital molecular barcoding cerebellum: median 31 %, p = 5.23e-10, and frontal cortex: median 53 %, p = 5.07e-10). Importantly, we revealed that variant 1 levels greater than the 25th percentile conferred a survival advantage [digital molecular barcoding cerebellum: hazard ratio (HR) 0.31, p = 0.003, and frontal cortex: HR 0.23, p = 0.0001]. When focusing on intron containing transcripts, analysis of the frontal cortex revealed an increase of potentially truncated transcripts in expansion carriers as compared to controls [digital molecular barcoding frontal cortex (intron 1a): median 272 %, p = 0.003], with the highest levels in patients pathologically diagnosed with frontotemporal lobar degeneration. In the cerebellum, our analysis suggested that transcripts were less likely to be truncated and, excitingly, we discovered that intron containing transcripts were associated with poly(GP) levels [digital molecular barcoding cerebellum (intron 1a): r = 0.33, p = 0.02, and (intron 1b): r = 0.49, p = 0.0004] and poly(GA) levels [digital molecular barcoding cerebellum (intron 1a): r = 0.34, p = 0.02, and (intron 1b): r = 0.38, p = 0.007]. In summary, we report decreased expression of specific C9ORF72 transcripts and provide support for the presence of truncated transcripts as well as pre-mRNAs that may serve as templates for RAN translation. We further show that higher C9ORF72 levels may have beneficial effects, which warrants caution in the development of new therapeutic approaches." @default.
• W1837429296 created "2016-06-24" @default.
• W1837429296 creator A5004201320 @default.
• W1837429296 creator A5006098963 @default.
• W1837429296 creator A5007824103 @default.
• W1837429296 creator A5009533777 @default.
• W1837429296 creator A5014535603 @default.
• W1837429296 creator A5030913073 @default.
• W1837429296 creator A5031027678 @default.
• W1837429296 creator A5033998542 @default.
• W1837429296 creator A5045246745 @default.
• W1837429296 creator A5046761674 @default.
• W1837429296 creator A5048217446 @default.
• W1837429296 creator A5048408999 @default.
• W1837429296 creator A5048437199 @default.
• W1837429296 creator A5053463417 @default.
• W1837429296 creator A5058278504 @default.
• W1837429296 creator A5059027860 @default.
• W1837429296 creator A5064561010 @default.
• W1837429296 creator A5066352714 @default.
• W1837429296 creator A5076687967 @default.
• W1837429296 creator A5077126324 @default.
• W1837429296 creator A5086394733 @default.
• W1837429296 creator A5090281014 @default.
• W1837429296 creator A5091046259 @default.
• W1837429296 date "2015-10-05" @default.
• W1837429296 modified "2023-10-17" @default.
• W1837429296 title "Novel clinical associations with specific C9ORF72 transcripts in patients with repeat expansions in C9ORF72" @default.
• W1837429296 cites W1137678651 @default.
• W1837429296 cites W1533438796 @default.
• W1837429296 cites W1646693466 @default.
• W1837429296 cites W1796096082 @default.
• W1837429296 cites W1797572428 @default.
• W1837429296 cites W1878242548 @default.
• W1837429296 cites W1982725145 @default.
• W1837429296 cites W1984538960 @default.
• W1837429296 cites W2007568107 @default.
• W1837429296 cites W2013488820 @default.
• W1837429296 cites W2013846239 @default.
• W1837429296 cites W2039279752 @default.
• W1837429296 cites W2041964860 @default.
• W1837429296 cites W2045151039 @default.
• W1837429296 cites W2054542675 @default.
• W1837429296 cites W2063996210 @default.
• W1837429296 cites W2065219073 @default.
• W1837429296 cites W2069171272 @default.
• W1837429296 cites W2092145129 @default.
• W1837429296 cites W2099232044 @default.
• W1837429296 cites W2109274553 @default.
• W1837429296 cites W2110308292 @default.
• W1837429296 cites W2113670539 @default.
• W1837429296 cites W2114872355 @default.
• W1837429296 cites W2128739333 @default.
• W1837429296 cites W2138004525 @default.
• W1837429296 cites W2139264742 @default.
• W1837429296 cites W2150523249 @default.
• W1837429296 cites W2154945114 @default.
• W1837429296 cites W2158949580 @default.
• W1837429296 cites W2165213609 @default.
• W1837429296 doi "https://doi.org/10.1007/s00401-015-1480-6" @default.
• W1837429296 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4655160" @default.
• W1837429296 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/26437865" @default.
• W1837429296 hasPublicationYear "2015" @default.
• W1837429296 type Work @default.
• W1837429296 sameAs 1837429296 @default.
• W1837429296 citedByCount "100" @default.
• W1837429296 countsByYear W18374292962015 @default.
• W1837429296 countsByYear W18374292962016 @default.
• W1837429296 countsByYear W18374292962017 @default.
• W1837429296 countsByYear W18374292962018 @default.
• W1837429296 countsByYear W18374292962019 @default.
• W1837429296 countsByYear W18374292962020 @default.
• W1837429296 countsByYear W18374292962021 @default.
• W1837429296 countsByYear W18374292962022 @default.
• W1837429296 countsByYear W18374292962023 @default.
• W1837429296 crossrefType "journal-article" @default.
• W1837429296 hasAuthorship W1837429296A5004201320 @default.
• W1837429296 hasAuthorship W1837429296A5006098963 @default.
• W1837429296 hasAuthorship W1837429296A5007824103 @default.
• W1837429296 hasAuthorship W1837429296A5009533777 @default.
• W1837429296 hasAuthorship W1837429296A5014535603 @default.
• W1837429296 hasAuthorship W1837429296A5030913073 @default.
• W1837429296 hasAuthorship W1837429296A5031027678 @default.
• W1837429296 hasAuthorship W1837429296A5033998542 @default.
• W1837429296 hasAuthorship W1837429296A5045246745 @default.
• W1837429296 hasAuthorship W1837429296A5046761674 @default.
• W1837429296 hasAuthorship W1837429296A5048217446 @default.
• W1837429296 hasAuthorship W1837429296A5048408999 @default.
• W1837429296 hasAuthorship W1837429296A5048437199 @default.
• W1837429296 hasAuthorship W1837429296A5053463417 @default.
• W1837429296 hasAuthorship W1837429296A5058278504 @default.
• W1837429296 hasAuthorship W1837429296A5059027860 @default.
• W1837429296 hasAuthorship W1837429296A5064561010 @default.
• W1837429296 hasAuthorship W1837429296A5066352714 @default.
• W1837429296 hasAuthorship W1837429296A5076687967 @default.
• W1837429296 hasAuthorship W1837429296A5077126324 @default.
• W1837429296 hasAuthorship W1837429296A5086394733 @default.
• W1837429296 hasAuthorship W1837429296A5090281014 @default.

• next