FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1569359062> ?p ?o ?g. }

• W1569359062 endingPage "364" @default.
• W1569359062 startingPage "347" @default.
• W1569359062 abstract "Tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) is known to induce apoptosis, otherwise known as programmed cell death, in many malignant cells without any known detrimental effects to normal cells. These aspects of TRAIL indicate the potential of TRAIL as a therapeutic agent in cancer. Ovarian cancer remains the deadliest gynecologic malignancy and is the fourth leading cause of death due to cancer in women. However, it has been shown in studies that ovarian cancer cells are sensitive to TRAIL-induced cell death when treated with TRAIL alone or in combination with chemotherapeutic agents. TRAIL signals through two death receptors, TRAIL-R1 and TRAIL-R2, to induce apoptosis. TRAIL also binds to two other cell surface receptors, TRAIL-R3 and TRAIL-R4, which do not have intracellular death domains and therefore do not transmit the apoptotic signal upon ligation with TRAIL. It has been shown that a chemokine, interleukin-8 (IL-8), may play a role in ovarian tumor progression due to its elevated presence in the fluid surrounding ovarian cancer tissues. Possible roles for IL-8 in ovarian tumorigenesis include angiogenesis and metastasis. Because the mechanism of regulation for TRAIL-induced apoptosis needs to be clarified, the role of IL-8 in TRAIL-induced apoptosis of ovarian cancer cells was studied. Results showed that the presence of IL-8 regulates cell-surface expression of TRAIL receptors in ovarian cancer cell lines in vitro. There may be a role for the p38 mitogen-activated protein kinase (MAPK) pathway in TRAIL-induced apoptosis of ovarian cancer cell." @default.
• W1569359062 created "2016-06-24" @default.
• W1569359062 creator A5008002755 @default.
• W1569359062 date "2004-01-01" @default.
• W1569359062 modified "2023-10-16" @default.
• W1569359062 title "Potential for TRAIL as a Therapeutic Agent in Ovarian Cancer" @default.
• W1569359062 cites W1484817497 @default.
• W1569359062 cites W1631361623 @default.
• W1569359062 cites W172276776 @default.
• W1569359062 cites W173852539 @default.
• W1569359062 cites W1964146094 @default.
• W1569359062 cites W1964617786 @default.
• W1569359062 cites W1965391953 @default.
• W1569359062 cites W1967304777 @default.
• W1569359062 cites W1969338183 @default.
• W1569359062 cites W1976586742 @default.
• W1569359062 cites W1978857213 @default.
• W1569359062 cites W1979182118 @default.
• W1569359062 cites W1980831535 @default.
• W1569359062 cites W1981534406 @default.
• W1569359062 cites W1982738210 @default.
• W1569359062 cites W1982786027 @default.
• W1569359062 cites W1984903682 @default.
• W1569359062 cites W1988854695 @default.
• W1569359062 cites W1991865867 @default.
• W1569359062 cites W1992597208 @default.
• W1569359062 cites W1999425834 @default.
• W1569359062 cites W1999764514 @default.
• W1569359062 cites W2002022970 @default.
• W1569359062 cites W2002503549 @default.
• W1569359062 cites W2002507218 @default.
• W1569359062 cites W2007681284 @default.
• W1569359062 cites W2007986629 @default.
• W1569359062 cites W2011027131 @default.
• W1569359062 cites W2011847072 @default.
• W1569359062 cites W2026951979 @default.
• W1569359062 cites W2029790299 @default.
• W1569359062 cites W2031474650 @default.
• W1569359062 cites W2035207372 @default.
• W1569359062 cites W2037647872 @default.
• W1569359062 cites W2039355845 @default.
• W1569359062 cites W2041466047 @default.
• W1569359062 cites W2042409437 @default.
• W1569359062 cites W2043295434 @default.
• W1569359062 cites W2047263793 @default.
• W1569359062 cites W2049474922 @default.
• W1569359062 cites W2050690958 @default.
• W1569359062 cites W2051810280 @default.
• W1569359062 cites W2054116154 @default.
• W1569359062 cites W2056088187 @default.
• W1569359062 cites W2056217426 @default.
• W1569359062 cites W2056397471 @default.
• W1569359062 cites W2059351462 @default.
• W1569359062 cites W2059608477 @default.
• W1569359062 cites W2062720951 @default.
• W1569359062 cites W2064217869 @default.
• W1569359062 cites W2068776651 @default.
• W1569359062 cites W2071309021 @default.
• W1569359062 cites W2072410510 @default.
• W1569359062 cites W2076485183 @default.
• W1569359062 cites W2077880395 @default.
• W1569359062 cites W2078076531 @default.
• W1569359062 cites W2078297328 @default.
• W1569359062 cites W2078303230 @default.
• W1569359062 cites W2083430194 @default.
• W1569359062 cites W2089476060 @default.
• W1569359062 cites W2089521856 @default.
• W1569359062 cites W2092196409 @default.
• W1569359062 cites W2106284224 @default.
• W1569359062 cites W2109165966 @default.
• W1569359062 cites W2113505777 @default.
• W1569359062 cites W2117963070 @default.
• W1569359062 cites W2121921687 @default.
• W1569359062 cites W2123927174 @default.
• W1569359062 cites W2124093732 @default.
• W1569359062 cites W2128667036 @default.
• W1569359062 cites W2130988210 @default.
• W1569359062 cites W2133726754 @default.
• W1569359062 cites W2145921423 @default.
• W1569359062 cites W2156496267 @default.
• W1569359062 cites W2156889170 @default.
• W1569359062 cites W2162063105 @default.
• W1569359062 cites W2162653594 @default.
• W1569359062 cites W2166500526 @default.
• W1569359062 cites W2166527628 @default.
• W1569359062 cites W2167663806 @default.
• W1569359062 cites W2263314269 @default.
• W1569359062 cites W2415834465 @default.
• W1569359062 cites W2734846420 @default.
• W1569359062 doi "https://doi.org/10.1016/s0083-6729(04)67018-x" @default.
• W1569359062 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/15110185" @default.
• W1569359062 hasPublicationYear "2004" @default.
• W1569359062 type Work @default.
• W1569359062 sameAs 1569359062 @default.
• W1569359062 citedByCount "11" @default.
• W1569359062 countsByYear W15693590622012 @default.
• W1569359062 countsByYear W15693590622020 @default.
• W1569359062 countsByYear W15693590622022 @default.

• next