FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1991309446> ?p ?o ?g. }

• W1991309446 endingPage "e56308" @default.
• W1991309446 startingPage "e56308" @default.
• W1991309446 abstract "Overexpression of ecotropic viral integration site 1 (EVI1) is associated with aggressive disease in acute myeloid leukemia (AML). Despite of its clinical importance, little is known about the mechanism through which EVI1 confers resistance to antileukemic drugs. Here, we show that a human myeloid cell line constitutively overexpressing EVI1 after infection with a retroviral vector (U937_EVI1) was partially resistant to etoposide and daunorubicin as compared to empty vector infected control cells (U937_vec). Similarly, inducible expression of EVI1 in HL-60 cells decreased their sensitivity to daunorubicin. Gene expression microarray analyses of U937_EVI1 and U937_vec cells cultured in the absence or presence of etoposide showed that 77 and 419 genes were regulated by EVI1 and etoposide, respectively. Notably, mRNA levels of 26 of these genes were altered by both stimuli, indicating that EVI1 regulated genes were strongly enriched among etoposide regulated genes and vice versa. One of the genes that were induced by both EVI1 and etoposide was CDKN1A/p21/WAF, which in addition to its function as a cell cycle regulator plays an important role in conferring chemotherapy resistance in various tumor types. Indeed, overexpression of CDKN1A in U937 cells mimicked the phenotype of EVI1 overexpression, similarly conferring partial resistance to antileukemic drugs." @default.
• W1991309446 created "2016-06-24" @default.
• W1991309446 creator A5001469388 @default.
• W1991309446 creator A5024089455 @default.
• W1991309446 creator A5030453966 @default.
• W1991309446 creator A5033593586 @default.
• W1991309446 creator A5035726155 @default.
• W1991309446 creator A5036993972 @default.
• W1991309446 creator A5038021708 @default.
• W1991309446 creator A5041101614 @default.
• W1991309446 creator A5043913136 @default.
• W1991309446 creator A5050637640 @default.
• W1991309446 creator A5052246323 @default.
• W1991309446 creator A5056993090 @default.
• W1991309446 creator A5061578149 @default.
• W1991309446 creator A5072208578 @default.
• W1991309446 creator A5077200888 @default.
• W1991309446 creator A5078452627 @default.
• W1991309446 creator A5081811379 @default.
• W1991309446 creator A5084733300 @default.
• W1991309446 date "2013-02-14" @default.
• W1991309446 modified "2023-10-09" @default.
• W1991309446 title "EVI1 Inhibits Apoptosis Induced by Antileukemic Drugs via Upregulation of CDKN1A/p21/WAF in Human Myeloid Cells" @default.
• W1991309446 cites W1495123612 @default.
• W1991309446 cites W1566969252 @default.
• W1991309446 cites W1966960697 @default.
• W1991309446 cites W1967865921 @default.
• W1991309446 cites W1968028322 @default.
• W1991309446 cites W1969004055 @default.
• W1991309446 cites W1973019785 @default.
• W1991309446 cites W1981937563 @default.
• W1991309446 cites W1985161949 @default.
• W1991309446 cites W2000639048 @default.
• W1991309446 cites W2001103347 @default.
• W1991309446 cites W2006355147 @default.
• W1991309446 cites W2007978249 @default.
• W1991309446 cites W2009085603 @default.
• W1991309446 cites W2009837903 @default.
• W1991309446 cites W2011103777 @default.
• W1991309446 cites W2011723750 @default.
• W1991309446 cites W2016771132 @default.
• W1991309446 cites W2017337160 @default.
• W1991309446 cites W2040006901 @default.
• W1991309446 cites W2040128687 @default.
• W1991309446 cites W2041418254 @default.
• W1991309446 cites W2042152044 @default.
• W1991309446 cites W2047632128 @default.
• W1991309446 cites W2048789245 @default.
• W1991309446 cites W2052600649 @default.
• W1991309446 cites W2053290453 @default.
• W1991309446 cites W2055462720 @default.
• W1991309446 cites W2056960087 @default.
• W1991309446 cites W2057685763 @default.
• W1991309446 cites W2059589294 @default.
• W1991309446 cites W2061480425 @default.
• W1991309446 cites W2065552179 @default.
• W1991309446 cites W2071151794 @default.
• W1991309446 cites W2072904998 @default.
• W1991309446 cites W2073437758 @default.
• W1991309446 cites W2074320863 @default.
• W1991309446 cites W2075016284 @default.
• W1991309446 cites W2075810792 @default.
• W1991309446 cites W2076814104 @default.
• W1991309446 cites W2078936160 @default.
• W1991309446 cites W2081712810 @default.
• W1991309446 cites W2082510362 @default.
• W1991309446 cites W2083663096 @default.
• W1991309446 cites W2094734927 @default.
• W1991309446 cites W2104683328 @default.
• W1991309446 cites W2105232554 @default.
• W1991309446 cites W2106194243 @default.
• W1991309446 cites W2107277218 @default.
• W1991309446 cites W2110502951 @default.
• W1991309446 cites W2112362958 @default.
• W1991309446 cites W2125597344 @default.
• W1991309446 cites W2130410032 @default.
• W1991309446 cites W2133764756 @default.
• W1991309446 cites W2136139751 @default.
• W1991309446 cites W2137248525 @default.
• W1991309446 cites W2144395887 @default.
• W1991309446 cites W2155147356 @default.
• W1991309446 cites W2155836153 @default.
• W1991309446 cites W2157721629 @default.
• W1991309446 cites W2161027618 @default.
• W1991309446 cites W2162262059 @default.
• W1991309446 cites W2167571277 @default.
• W1991309446 cites W2170510628 @default.
• W1991309446 cites W90182880 @default.
• W1991309446 doi "https://doi.org/10.1371/journal.pone.0056308" @default.
• W1991309446 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/3572987" @default.
• W1991309446 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/23457546" @default.
• W1991309446 hasPublicationYear "2013" @default.
• W1991309446 type Work @default.
• W1991309446 sameAs 1991309446 @default.
• W1991309446 citedByCount "21" @default.
• W1991309446 countsByYear W19913094462013 @default.
• W1991309446 countsByYear W19913094462014 @default.
• W1991309446 countsByYear W19913094462015 @default.

• next