FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1853854707> ?p ?o ?g. }

• W1853854707 endingPage "1086" @default.
• W1853854707 startingPage "1074" @default.
• W1853854707 abstract "Colorectal cancer (CRC) remains a major contributor to cancer-related mortality. LIN28A and LIN28B are highly related RNA-binding protein paralogs that regulate biogenesis of let-7 microRNAs and influence development, metabolism, tissue regeneration, and oncogenesis. Here we demonstrate that overexpression of either LIN28 paralog cooperates with the Wnt pathway to promote invasive intestinal adenocarcinoma in murine models. When LIN28 alone is induced genetically, half of the resulting tumors harbor Ctnnb1 (β-catenin) mutation. When overexpressed in Apc Min/+ mice, LIN28 accelerates tumor formation and enhances proliferation and invasiveness. In conditional genetic models, enforced expression of a LIN28-resistant form of the let-7 microRNA reduces LIN28-induced tumor burden, while silencing of LIN28 expression reduces tumor volume and increases tumor differentiation, indicating that LIN28 contributes to tumor maintenance. We detected aberrant expression of LIN28A and/or LIN28B in 38% of a large series of human CRC samples ( n = 595), where LIN28 expression levels were associated with invasive tumor growth. Our late-stage CRC murine models and analysis of primary human tumors demonstrate prominent roles for both LIN28 paralogs in promoting CRC growth and progression and implicate the LIN28/ let-7 pathway as a therapeutic target." @default.
• W1853854707 created "2016-06-24" @default.
• W1853854707 creator A5002413318 @default.
• W1853854707 creator A5004637165 @default.
• W1853854707 creator A5004738203 @default.
• W1853854707 creator A5021093107 @default.
• W1853854707 creator A5022741402 @default.
• W1853854707 creator A5035386197 @default.
• W1853854707 creator A5035573322 @default.
• W1853854707 creator A5037437791 @default.
• W1853854707 creator A5039470925 @default.
• W1853854707 creator A5041701431 @default.
• W1853854707 creator A5043650880 @default.
• W1853854707 creator A5049314303 @default.
• W1853854707 creator A5059348374 @default.
• W1853854707 creator A5066959106 @default.
• W1853854707 creator A5067699583 @default.
• W1853854707 creator A5068560690 @default.
• W1853854707 creator A5076818447 @default.
• W1853854707 creator A5078462698 @default.
• W1853854707 creator A5079504963 @default.
• W1853854707 creator A5085236177 @default.
• W1853854707 date "2015-05-08" @default.
• W1853854707 modified "2023-10-11" @default.
• W1853854707 title "LIN28 cooperates with WNT signaling to drive invasive intestinal and colorectal adenocarcinoma in mice and humans" @default.
• W1853854707 cites W1480960095 @default.
• W1853854707 cites W1544296458 @default.
• W1853854707 cites W1967533656 @default.
• W1853854707 cites W1971204432 @default.
• W1853854707 cites W1975301698 @default.
• W1853854707 cites W1976359234 @default.
• W1853854707 cites W1983031223 @default.
• W1853854707 cites W1983504654 @default.
• W1853854707 cites W1984068087 @default.
• W1853854707 cites W1984935494 @default.
• W1853854707 cites W1985140771 @default.
• W1853854707 cites W1992372073 @default.
• W1853854707 cites W1993748871 @default.
• W1853854707 cites W1999601430 @default.
• W1853854707 cites W2001258296 @default.
• W1853854707 cites W2009229545 @default.
• W1853854707 cites W2010438982 @default.
• W1853854707 cites W2016971867 @default.
• W1853854707 cites W2017044435 @default.
• W1853854707 cites W2019078072 @default.
• W1853854707 cites W2019167811 @default.
• W1853854707 cites W2023372666 @default.
• W1853854707 cites W2023899769 @default.
• W1853854707 cites W2026919212 @default.
• W1853854707 cites W2027266715 @default.
• W1853854707 cites W2030714059 @default.
• W1853854707 cites W2033267718 @default.
• W1853854707 cites W2034806022 @default.
• W1853854707 cites W2040592358 @default.
• W1853854707 cites W2044433401 @default.
• W1853854707 cites W2053352622 @default.
• W1853854707 cites W2062376760 @default.
• W1853854707 cites W2062500929 @default.
• W1853854707 cites W2065597225 @default.
• W1853854707 cites W2065676042 @default.
• W1853854707 cites W2065717887 @default.
• W1853854707 cites W2067158613 @default.
• W1853854707 cites W2068978328 @default.
• W1853854707 cites W2073759231 @default.
• W1853854707 cites W2079957854 @default.
• W1853854707 cites W2093531978 @default.
• W1853854707 cites W2112521802 @default.
• W1853854707 cites W2115005790 @default.
• W1853854707 cites W2115792588 @default.
• W1853854707 cites W2116362436 @default.
• W1853854707 cites W2118807592 @default.
• W1853854707 cites W2130410032 @default.
• W1853854707 cites W2130921932 @default.
• W1853854707 cites W2130978704 @default.
• W1853854707 cites W2134599070 @default.
• W1853854707 cites W2135518377 @default.
• W1853854707 cites W2144038313 @default.
• W1853854707 cites W2146835439 @default.
• W1853854707 cites W2150625137 @default.
• W1853854707 cites W2152785381 @default.
• W1853854707 cites W2152951302 @default.
• W1853854707 cites W2157010562 @default.
• W1853854707 cites W2158733632 @default.
• W1853854707 cites W2159187753 @default.
• W1853854707 cites W2170647698 @default.
• W1853854707 cites W2172157901 @default.
• W1853854707 cites W2262414037 @default.
• W1853854707 cites W3198353739 @default.
• W1853854707 doi "https://doi.org/10.1101/gad.256693.114" @default.
• W1853854707 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4441054" @default.
• W1853854707 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/25956904" @default.
• W1853854707 hasPublicationYear "2015" @default.
• W1853854707 type Work @default.
• W1853854707 sameAs 1853854707 @default.
• W1853854707 citedByCount "85" @default.
• W1853854707 countsByYear W18538547072015 @default.
• W1853854707 countsByYear W18538547072016 @default.
• W1853854707 countsByYear W18538547072017 @default.

• next