FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2947099994> ?p ?o ?g. }

• W2947099994 endingPage "1800" @default.
• W2947099994 startingPage "1787" @default.
• W2947099994 abstract "Abstract Alterations in the PI3K/AKT pathway occur in up to 70% of melanomas and are associated with disease progression. The three AKT paralogs are highly conserved but data suggest they have distinct functions. Activating mutations of AKT1 and AKT3 occur in human melanoma but their role in melanoma formation and metastasis remains unclear. Using an established melanoma mouse model, we evaluated E17K, E40K, and Q79K mutations in AKT1, AKT2, and AKT3 and show that mice harboring tumors expressing AKT1E17K had the highest incidence of brain metastasis and lowest mean survival. Tumors expressing AKT1E17K displayed elevated levels of focal adhesion factors and enhanced phosphorylation of focal adhesion kinase (FAK). AKT1E17K expression in melanoma cells increased invasion and this was reduced by pharmacologic inhibition of either AKT or FAK. These data suggest that the different AKT paralogs have distinct roles in melanoma brain metastasis and that AKT and FAK may be promising therapeutic targets. Implications: This study suggests that AKT1E17K promotes melanoma brain metastasis through activation of FAK and provides a rationale for the therapeutic targeting of AKT and/or FAK to reduce melanoma metastasis." @default.
• W2947099994 created "2019-06-07" @default.
• W2947099994 creator A5003652463 @default.
• W2947099994 creator A5015896090 @default.
• W2947099994 creator A5017118097 @default.
• W2947099994 creator A5024135661 @default.
• W2947099994 creator A5029180727 @default.
• W2947099994 creator A5030035753 @default.
• W2947099994 creator A5044257952 @default.
• W2947099994 creator A5048327749 @default.
• W2947099994 creator A5049564276 @default.
• W2947099994 creator A5061736368 @default.
• W2947099994 creator A5075201122 @default.
• W2947099994 creator A5076934461 @default.
• W2947099994 creator A5079211006 @default.
• W2947099994 creator A5081147586 @default.
• W2947099994 creator A5082070319 @default.
• W2947099994 creator A5086797774 @default.
• W2947099994 date "2019-09-01" @default.
• W2947099994 modified "2023-10-14" @default.
• W2947099994 title "AKT1E17K Activates Focal Adhesion Kinase and Promotes Melanoma Brain Metastasis" @default.
• W2947099994 cites W112133451 @default.
• W2947099994 cites W1139788413 @default.
• W2947099994 cites W1796730041 @default.
• W2947099994 cites W1906638461 @default.
• W2947099994 cites W1933401810 @default.
• W2947099994 cites W1950829641 @default.
• W2947099994 cites W1969820174 @default.
• W2947099994 cites W1973767497 @default.
• W2947099994 cites W1982479809 @default.
• W2947099994 cites W1989418405 @default.
• W2947099994 cites W2000749236 @default.
• W2947099994 cites W2018023891 @default.
• W2947099994 cites W2025316386 @default.
• W2947099994 cites W2027988626 @default.
• W2947099994 cites W2028092387 @default.
• W2947099994 cites W2030870003 @default.
• W2947099994 cites W2031196360 @default.
• W2947099994 cites W2038210678 @default.
• W2947099994 cites W2042202721 @default.
• W2947099994 cites W2042302972 @default.
• W2947099994 cites W2045012491 @default.
• W2947099994 cites W2054767091 @default.
• W2947099994 cites W2059549347 @default.
• W2947099994 cites W2090120410 @default.
• W2947099994 cites W2100969832 @default.
• W2947099994 cites W2101297236 @default.
• W2947099994 cites W2105660237 @default.
• W2947099994 cites W2108770100 @default.
• W2947099994 cites W2109610561 @default.
• W2947099994 cites W2116778213 @default.
• W2947099994 cites W2121886536 @default.
• W2947099994 cites W2125882882 @default.
• W2947099994 cites W2129181865 @default.
• W2947099994 cites W2129318139 @default.
• W2947099994 cites W2135238116 @default.
• W2947099994 cites W2136846409 @default.
• W2947099994 cites W2142020978 @default.
• W2947099994 cites W2147690515 @default.
• W2947099994 cites W2152606604 @default.
• W2947099994 cites W2157391644 @default.
• W2947099994 cites W2166545765 @default.
• W2947099994 cites W2177518191 @default.
• W2947099994 cites W2204493619 @default.
• W2947099994 cites W2227972917 @default.
• W2947099994 cites W2265081928 @default.
• W2947099994 cites W2301705957 @default.
• W2947099994 cites W2312892840 @default.
• W2947099994 cites W2417761579 @default.
• W2947099994 cites W2425569687 @default.
• W2947099994 cites W2512745759 @default.
• W2947099994 cites W2557860064 @default.
• W2947099994 cites W2595714719 @default.
• W2947099994 cites W2781878830 @default.
• W2947099994 cites W2888800216 @default.
• W2947099994 cites W2917087462 @default.
• W2947099994 doi "https://doi.org/10.1158/1541-7786.mcr-18-1372" @default.
• W2947099994 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6726552" @default.
• W2947099994 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/31138602" @default.
• W2947099994 hasPublicationYear "2019" @default.
• W2947099994 type Work @default.
• W2947099994 sameAs 2947099994 @default.
• W2947099994 citedByCount "40" @default.
• W2947099994 countsByYear W29470999942019 @default.
• W2947099994 countsByYear W29470999942020 @default.
• W2947099994 countsByYear W29470999942021 @default.
• W2947099994 countsByYear W29470999942022 @default.
• W2947099994 countsByYear W29470999942023 @default.
• W2947099994 crossrefType "journal-article" @default.
• W2947099994 hasAuthorship W2947099994A5003652463 @default.
• W2947099994 hasAuthorship W2947099994A5015896090 @default.
• W2947099994 hasAuthorship W2947099994A5017118097 @default.
• W2947099994 hasAuthorship W2947099994A5024135661 @default.
• W2947099994 hasAuthorship W2947099994A5029180727 @default.
• W2947099994 hasAuthorship W2947099994A5030035753 @default.
• W2947099994 hasAuthorship W2947099994A5044257952 @default.
• W2947099994 hasAuthorship W2947099994A5048327749 @default.
• W2947099994 hasAuthorship W2947099994A5049564276 @default.

• next