FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2947644940> ?p ?o ?g. }

• W2947644940 endingPage "11" @default.
• W2947644940 startingPage "1" @default.
• W2947644940 abstract "Pancreatic ductal adenocarcinoma (PDAC) remains a devastating disease with a very poor prognosis. At the same time, its incidence is on the rise, and PDAC is expected to become the second leading cause of cancer-related death by 2030. Despite extensive work on new therapeutic approaches, the median overall survival is only 6-12 months after diagnosis and the 5-year survival is less than 7%. While pancreatic cancer is particularly difficult to treat, patients usually succumb not to the growth of the primary tumor, but to extensive metastasis; therefore, strategies to reduce the migratory and metastatic capacity of pancreatic cancer cells merit close attention. The vast majority of pancreatic cancers harbor RAS mutations. The outstanding relevance of the RAS/MEK/ERK pathway in pancreatic cancer biology has been extensively shown previously. Due to their high dependency on Ras mutations, pancreatic cancers might be particularly sensitive to inhibitors acting downstream of Ras. Herein, we use a genetically engineered mouse model of pancreatic cancer and primary pancreatic cancer cells were derived from this model to demonstrate that small-molecule MEK inhibitors functionally abrogate cancer stem cell populations as demonstrated by reduced sphere and organoid formation capacity. Furthermore, we demonstrate that MEK inhibition suppresses TGF β -induced epithelial-to-mesenchymal transition and migration in vitro and ultimately results in a highly significant reduction in circulating tumor cells in mice." @default.
• W2947644940 created "2019-06-07" @default.
• W2947644940 creator A5018996994 @default.
• W2947644940 creator A5021152840 @default.
• W2947644940 creator A5024777066 @default.
• W2947644940 creator A5031406092 @default.
• W2947644940 creator A5038707544 @default.
• W2947644940 creator A5051602756 @default.
• W2947644940 creator A5056191434 @default.
• W2947644940 creator A5056479445 @default.
• W2947644940 creator A5062990199 @default.
• W2947644940 creator A5063946757 @default.
• W2947644940 creator A5067676567 @default.
• W2947644940 creator A5067988849 @default.
• W2947644940 creator A5071888326 @default.
• W2947644940 creator A5072303851 @default.
• W2947644940 creator A5090760545 @default.
• W2947644940 date "2019-06-02" @default.
• W2947644940 modified "2023-10-14" @default.
• W2947644940 title "MEK Inhibition Targets Cancer Stem Cells and Impedes Migration of Pancreatic Cancer Cells<i>In Vitro</i>and<i>In Vivo</i>" @default.
• W2947644940 cites W1939365747 @default.
• W2947644940 cites W1964081206 @default.
• W2947644940 cites W1965822047 @default.
• W2947644940 cites W1968812902 @default.
• W2947644940 cites W1970140424 @default.
• W2947644940 cites W1970147973 @default.
• W2947644940 cites W1983701937 @default.
• W2947644940 cites W1988783376 @default.
• W2947644940 cites W1992976199 @default.
• W2947644940 cites W1993055783 @default.
• W2947644940 cites W1994772304 @default.
• W2947644940 cites W2010916968 @default.
• W2947644940 cites W2013658947 @default.
• W2947644940 cites W2019264784 @default.
• W2947644940 cites W2022366555 @default.
• W2947644940 cites W2039813669 @default.
• W2947644940 cites W2042834671 @default.
• W2947644940 cites W2047992261 @default.
• W2947644940 cites W2065455574 @default.
• W2947644940 cites W2065941404 @default.
• W2947644940 cites W2068982132 @default.
• W2947644940 cites W2079292309 @default.
• W2947644940 cites W2100559817 @default.
• W2947644940 cites W2107414039 @default.
• W2947644940 cites W2109998353 @default.
• W2947644940 cites W2111976640 @default.
• W2947644940 cites W2114621192 @default.
• W2947644940 cites W2117276705 @default.
• W2947644940 cites W2117692326 @default.
• W2947644940 cites W2119578188 @default.
• W2947644940 cites W2131170195 @default.
• W2947644940 cites W2136280424 @default.
• W2947644940 cites W2138498601 @default.
• W2947644940 cites W2151199834 @default.
• W2947644940 cites W2151253787 @default.
• W2947644940 cites W2159291539 @default.
• W2947644940 cites W2165480504 @default.
• W2947644940 cites W2168887286 @default.
• W2947644940 cites W2179438025 @default.
• W2947644940 cites W2197124664 @default.
• W2947644940 cites W2286447252 @default.
• W2947644940 cites W2293755451 @default.
• W2947644940 cites W2563028222 @default.
• W2947644940 cites W2592811885 @default.
• W2947644940 cites W2756705158 @default.
• W2947644940 cites W2771070570 @default.
• W2947644940 cites W2783114553 @default.
• W2947644940 cites W2787016559 @default.
• W2947644940 cites W2901391118 @default.
• W2947644940 cites W4211177171 @default.
• W2947644940 cites W4231038369 @default.
• W2947644940 doi "https://doi.org/10.1155/2019/8475389" @default.
• W2947644940 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6589314" @default.
• W2947644940 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/31281387" @default.
• W2947644940 hasPublicationYear "2019" @default.
• W2947644940 type Work @default.
• W2947644940 sameAs 2947644940 @default.
• W2947644940 citedByCount "11" @default.
• W2947644940 countsByYear W29476449402019 @default.
• W2947644940 countsByYear W29476449402020 @default.
• W2947644940 countsByYear W29476449402021 @default.
• W2947644940 countsByYear W29476449402022 @default.
• W2947644940 countsByYear W29476449402023 @default.
• W2947644940 crossrefType "journal-article" @default.
• W2947644940 hasAuthorship W2947644940A5018996994 @default.
• W2947644940 hasAuthorship W2947644940A5021152840 @default.
• W2947644940 hasAuthorship W2947644940A5024777066 @default.
• W2947644940 hasAuthorship W2947644940A5031406092 @default.
• W2947644940 hasAuthorship W2947644940A5038707544 @default.
• W2947644940 hasAuthorship W2947644940A5051602756 @default.
• W2947644940 hasAuthorship W2947644940A5056191434 @default.
• W2947644940 hasAuthorship W2947644940A5056479445 @default.
• W2947644940 hasAuthorship W2947644940A5062990199 @default.
• W2947644940 hasAuthorship W2947644940A5063946757 @default.
• W2947644940 hasAuthorship W2947644940A5067676567 @default.
• W2947644940 hasAuthorship W2947644940A5067988849 @default.
• W2947644940 hasAuthorship W2947644940A5071888326 @default.
• W2947644940 hasAuthorship W2947644940A5072303851 @default.

• next