FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2580077891> ?p ?o ?g. }

• W2580077891 endingPage "444" @default.
• W2580077891 startingPage "431" @default.
• W2580077891 abstract "Meningioma is the most common primary brain tumor and carries a substantial risk of local recurrence. Methylation profiles of meningioma and their clinical implications are not well understood. We hypothesized that aggressive meningiomas have unique DNA methylation patterns that could be used to better stratify patient management. Samples (n = 140) were profiled using the Illumina HumanMethylation450BeadChip. Unsupervised modeling on a training set (n = 89) identified 2 molecular methylation subgroups of meningioma (MM) with significantly different recurrence-free survival (RFS) times between the groups: a prognostically unfavorable subgroup (MM-UNFAV) and a prognostically favorable subgroup (MM-FAV). This finding was validated in the remaining 51 samples and led to a baseline meningioma methylation classifier (bMMC) defined by 283 CpG loci (283-bMMC). To further optimize a recurrence predictor, probes subsumed within the baseline classifier were subject to additional modeling using a similar training/validation approach, leading to a 64-CpG loci meningioma methylation predictor (64-MMP). After adjustment for relevant clinical variables [WHO grade, mitotic index, Simpson grade, sex, location, and copy number aberrations (CNAs)] multivariable analyses for RFS showed that the baseline methylation classifier was not significant (p = 0.0793). The methylation predictor, however, was significantly associated with tumor recurrence (p < 0.0001). CNAs were extracted from the 450k intensity profiles. Tumor samples in the MM-UNFAV subgroup showed an overall higher proportion of CNAs compared to the MM-FAV subgroup tumors and the CNAs were complex in nature. CNAs in the MM-UNFAV subgroup included recurrent losses of 1p, 6q, 14q and 18q, and gain of 1q, all of which were previously identified as indicators of poor outcome. In conclusion, our analyses demonstrate robust DNA methylation signatures in meningioma that correlate with CNAs and stratify patients by recurrence risk." @default.
• W2580077891 created "2017-02-03" @default.
• W2580077891 creator A5006827524 @default.
• W2580077891 creator A5032190194 @default.
• W2580077891 creator A5041096535 @default.
• W2580077891 creator A5054809773 @default.
• W2580077891 creator A5060829987 @default.
• W2580077891 creator A5063290790 @default.
• W2580077891 creator A5064456190 @default.
• W2580077891 creator A5072584423 @default.
• W2580077891 creator A5081212023 @default.
• W2580077891 date "2017-01-27" @default.
• W2580077891 modified "2023-10-01" @default.
• W2580077891 title "Global epigenetic profiling identifies methylation subgroups associated with recurrence-free survival in meningioma" @default.
• W2580077891 cites W1501449679 @default.
• W2580077891 cites W1562381964 @default.
• W2580077891 cites W1815159282 @default.
• W2580077891 cites W1893588436 @default.
• W2580077891 cites W1928158719 @default.
• W2580077891 cites W1973888912 @default.
• W2580077891 cites W1975735086 @default.
• W2580077891 cites W1978813254 @default.
• W2580077891 cites W1988756388 @default.
• W2580077891 cites W1990505672 @default.
• W2580077891 cites W2000381516 @default.
• W2580077891 cites W2001470466 @default.
• W2580077891 cites W2001915960 @default.
• W2580077891 cites W2001944063 @default.
• W2580077891 cites W2002973959 @default.
• W2580077891 cites W2003122802 @default.
• W2580077891 cites W2004342375 @default.
• W2580077891 cites W2007163549 @default.
• W2580077891 cites W2016757970 @default.
• W2580077891 cites W2023606058 @default.
• W2580077891 cites W2025169227 @default.
• W2580077891 cites W2026642573 @default.
• W2580077891 cites W2032800329 @default.
• W2580077891 cites W2037160755 @default.
• W2580077891 cites W2038690678 @default.
• W2580077891 cites W2040473070 @default.
• W2580077891 cites W2041025015 @default.
• W2580077891 cites W2044702943 @default.
• W2580077891 cites W2047265377 @default.
• W2580077891 cites W2057642694 @default.
• W2580077891 cites W205979824 @default.
• W2580077891 cites W2066446775 @default.
• W2580077891 cites W2074838987 @default.
• W2580077891 cites W2082671989 @default.
• W2580077891 cites W2084139018 @default.
• W2580077891 cites W2085791754 @default.
• W2580077891 cites W2088766333 @default.
• W2580077891 cites W2094638688 @default.
• W2580077891 cites W2096189743 @default.
• W2580077891 cites W2096283970 @default.
• W2580077891 cites W2097626332 @default.
• W2580077891 cites W2105528101 @default.
• W2580077891 cites W2107813326 @default.
• W2580077891 cites W2109364195 @default.
• W2580077891 cites W2111298900 @default.
• W2580077891 cites W2113160553 @default.
• W2580077891 cites W2113432767 @default.
• W2580077891 cites W2116401585 @default.
• W2580077891 cites W2118882840 @default.
• W2580077891 cites W2120816877 @default.
• W2580077891 cites W2122404743 @default.
• W2580077891 cites W2123297118 @default.
• W2580077891 cites W2127431419 @default.
• W2580077891 cites W2136787567 @default.
• W2580077891 cites W2137147070 @default.
• W2580077891 cites W2142279946 @default.
• W2580077891 cites W2142635246 @default.
• W2580077891 cites W2142942500 @default.
• W2580077891 cites W2145489645 @default.
• W2580077891 cites W2146302353 @default.
• W2580077891 cites W2148528280 @default.
• W2580077891 cites W2148977460 @default.
• W2580077891 cites W2149031002 @default.
• W2580077891 cites W2149802344 @default.
• W2580077891 cites W2154170543 @default.
• W2580077891 cites W2160382843 @default.
• W2580077891 cites W2162108296 @default.
• W2580077891 cites W2210813576 @default.
• W2580077891 cites W2270206867 @default.
• W2580077891 cites W2286322195 @default.
• W2580077891 cites W2292921380 @default.
• W2580077891 cites W2328930886 @default.
• W2580077891 cites W2392819176 @default.
• W2580077891 cites W2460673340 @default.
• W2580077891 cites W2473952297 @default.
• W2580077891 cites W4245392732 @default.
• W2580077891 doi "https://doi.org/10.1007/s00401-017-1678-x" @default.
• W2580077891 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/5600514" @default.
• W2580077891 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/28130639" @default.
• W2580077891 hasPublicationYear "2017" @default.
• W2580077891 type Work @default.
• W2580077891 sameAs 2580077891 @default.
• W2580077891 citedByCount "126" @default.
• W2580077891 countsByYear W25800778912017 @default.

• next