FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2143488039> ?p ?o ?g. }

• W2143488039 endingPage "469" @default.
• W2143488039 startingPage "461" @default.
• W2143488039 abstract "Current histopathologic systems for classifying breast tumors require evaluation of multiple variables and are often associated with significant interobserver variability. Recent studies suggest that gene expression profiles may represent a promising alternative for clinical cancer classification. Here, we investigated the use of a customized microarray as a potential tool for clinical practice.We fabricated custom 188-gene microarrays containing expression signatures for three breast cancer molecular subtypes [luminal/estrogen receptor (ER) positive, human epidermal growth factor receptor 2 (HER2), and basaloid], the Nottingham prognostic index (NPI-ES), and low histologic grade (TuM1). The reliability of these multiple-signature arrays (MSA) was tested in a prospective cohort of 165 patients with primary breast cancer.The MSA-ER signature exhibited a high concordance of 90% with ER immunohistochemistry reported on diagnosis (P < 0.001). This remained unchanged at 89% (P < 0.001) when the immunohistochemistry was repeated using current laboratory standards. Expression of the HER2 signature showed a good correlation of 76% with HER2 fluorescence in situ hybridization (FISH; ratio > or =2.2; P < 0.001), which further improved to 89% when the ratio cutoff was raised to > or =5. A proportion of low-level FISH-amplified samples (ratio, 2.2-5) behaved comparably to FISH-negative samples by HER2 signature expression, HER2 quantitative reverse transcription-PCR, and HER2 immunohistochemistry. Luminal/ER+ tumors with high NPI-ES expression were associated with high NPI scores (P = 0.001), and luminal/ER+ TuM1-expressing tumors were significantly correlated with low histologic grade (P = 0.002) and improved survival outcome in an interim analysis (hazard ratio, 0.2; P = 0.019).The consistency of the MSA platform in an independent patient population suggests that custom microarrays could potentially function as an adjunct to standard immunohistochemistry and FISH in clinical practice." @default.
• W2143488039 created "2016-06-24" @default.
• W2143488039 creator A5001857515 @default.
• W2143488039 creator A5002658824 @default.
• W2143488039 creator A5014806180 @default.
• W2143488039 creator A5017591415 @default.
• W2143488039 creator A5018056806 @default.
• W2143488039 creator A5024386254 @default.
• W2143488039 creator A5028449420 @default.
• W2143488039 creator A5029035743 @default.
• W2143488039 creator A5036077922 @default.
• W2143488039 creator A5040036998 @default.
• W2143488039 creator A5053082742 @default.
• W2143488039 creator A5065389865 @default.
• W2143488039 creator A5069703207 @default.
• W2143488039 creator A5074190354 @default.
• W2143488039 creator A5090801100 @default.
• W2143488039 date "2008-01-15" @default.
• W2143488039 modified "2023-10-10" @default.
• W2143488039 title "Clinical Validation of a Customized Multiple Signature Microarray for Breast Cancer" @default.
• W2143488039 cites W1546709038 @default.
• W2143488039 cites W1829077072 @default.
• W2143488039 cites W1861891407 @default.
• W2143488039 cites W1924240366 @default.
• W2143488039 cites W1937618727 @default.
• W2143488039 cites W1942249117 @default.
• W2143488039 cites W1965427258 @default.
• W2143488039 cites W1967550860 @default.
• W2143488039 cites W1981313947 @default.
• W2143488039 cites W1995224853 @default.
• W2143488039 cites W1999463736 @default.
• W2143488039 cites W2000798782 @default.
• W2143488039 cites W2007161805 @default.
• W2143488039 cites W2010547484 @default.
• W2143488039 cites W2020830322 @default.
• W2143488039 cites W2064052354 @default.
• W2143488039 cites W2072648072 @default.
• W2143488039 cites W2096301110 @default.
• W2143488039 cites W2097255042 @default.
• W2143488039 cites W2098824829 @default.
• W2143488039 cites W2104872563 @default.
• W2143488039 cites W2105882193 @default.
• W2143488039 cites W2117495488 @default.
• W2143488039 cites W2117760677 @default.
• W2143488039 cites W2118135682 @default.
• W2143488039 cites W2118343282 @default.
• W2143488039 cites W2124972539 @default.
• W2143488039 cites W2128985829 @default.
• W2143488039 cites W2131994307 @default.
• W2143488039 cites W2134309775 @default.
• W2143488039 cites W2135598172 @default.
• W2143488039 cites W2139306864 @default.
• W2143488039 cites W2142495011 @default.
• W2143488039 cites W2144634511 @default.
• W2143488039 cites W2145238404 @default.
• W2143488039 cites W2150649458 @default.
• W2143488039 cites W2154976095 @default.
• W2143488039 cites W2156273110 @default.
• W2143488039 cites W2157840751 @default.
• W2143488039 cites W2160377567 @default.
• W2143488039 cites W2163563958 @default.
• W2143488039 cites W2165432902 @default.
• W2143488039 cites W2166609686 @default.
• W2143488039 cites W2167552083 @default.
• W2143488039 cites W2395461585 @default.
• W2143488039 doi "https://doi.org/10.1158/1078-0432.ccr-07-0999" @default.
• W2143488039 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/18223220" @default.
• W2143488039 hasPublicationYear "2008" @default.
• W2143488039 type Work @default.
• W2143488039 sameAs 2143488039 @default.
• W2143488039 citedByCount "13" @default.
• W2143488039 countsByYear W21434880392014 @default.
• W2143488039 countsByYear W21434880392015 @default.
• W2143488039 crossrefType "journal-article" @default.
• W2143488039 hasAuthorship W2143488039A5001857515 @default.
• W2143488039 hasAuthorship W2143488039A5002658824 @default.
• W2143488039 hasAuthorship W2143488039A5014806180 @default.
• W2143488039 hasAuthorship W2143488039A5017591415 @default.
• W2143488039 hasAuthorship W2143488039A5018056806 @default.
• W2143488039 hasAuthorship W2143488039A5024386254 @default.
• W2143488039 hasAuthorship W2143488039A5028449420 @default.
• W2143488039 hasAuthorship W2143488039A5029035743 @default.
• W2143488039 hasAuthorship W2143488039A5036077922 @default.
• W2143488039 hasAuthorship W2143488039A5040036998 @default.
• W2143488039 hasAuthorship W2143488039A5053082742 @default.
• W2143488039 hasAuthorship W2143488039A5065389865 @default.
• W2143488039 hasAuthorship W2143488039A5069703207 @default.
• W2143488039 hasAuthorship W2143488039A5074190354 @default.
• W2143488039 hasAuthorship W2143488039A5090801100 @default.
• W2143488039 hasBestOaLocation W21434880392 @default.
• W2143488039 hasConcept C104317684 @default.
• W2143488039 hasConcept C121608353 @default.
• W2143488039 hasConcept C126322002 @default.
• W2143488039 hasConcept C142724271 @default.
• W2143488039 hasConcept C143998085 @default.
• W2143488039 hasConcept C150194340 @default.
• W2143488039 hasConcept C160798450 @default.
• W2143488039 hasConcept C193270364 @default.

• next