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• W3000183405 endingPage "147" @default.
• W3000183405 startingPage "147" @default.
• W3000183405 abstract "Tropomyosin receptor kinase (Trk) C contributes to the clinicopathology of a variety of human cancers, and new chimeric oncoproteins containing the tyrosine kinase domain of TrkC occur after fusion to the partner genes. Overexpression of TrkC and TrkC fusion proteins was observed in patients with a variety of cancers, including mesenchymal, hematopoietic, and those of epithelial cell lineage. Both microRNAs (miRNAs) and long non-coding RNAs (lncRNAs) were involved in the regulation of TrkC expression through transcriptional and posttranscriptional alteration. Aberrant activation of TrkC and TrkC fusion proteins markedly induces the epithelial-mesenchymal transition (EMT) program, growth rate, tumorigenic capacity via constitutive activation of Ras-MAP kinase (MAPK), PI3K-AKT, and the JAK2-STAT3 pathway. The clinical trial of TrkC or TrkC fusion-positive cancers with newly developed Trk inhibitors demonstrated that Trk inhibitors were highly effective in inducing tumor regression in patients who do not harbor mutations in the kinase domain. Recently, there has been a progressive accumulation of mutations in TrkC or the TrkC fusion protein detected in the clinic and its related cancer cell lines caused by high-throughput DNA sequencing. Despite given the high overall response rate against Trk or Trk fusion proteins-positive solid tumors, acquired drug resistance was observed in patients with various cancers caused by mutations in the Trk kinase domain. To overcome acquired resistance caused by kinase domain mutation, next-generation Trk inhibitors have been developed, and these inhibitors are currently under investigation in clinical trials." @default.
• W3000183405 created "2020-01-23" @default.
• W3000183405 creator A5022279675 @default.
• W3000183405 date "2020-01-08" @default.
• W3000183405 modified "2023-09-26" @default.
• W3000183405 title "Roles of TrkC Signaling in the Regulation of Tumorigenicity and Metastasis of Cancer" @default.
• W3000183405 cites W141636555 @default.
• W3000183405 cites W1494352958 @default.
• W3000183405 cites W1494415215 @default.
• W3000183405 cites W1586151303 @default.
• W3000183405 cites W1591236513 @default.
• W3000183405 cites W1667088041 @default.
• W3000183405 cites W1829677782 @default.
• W3000183405 cites W1848939527 @default.
• W3000183405 cites W1921573595 @default.
• W3000183405 cites W1937853139 @default.
• W3000183405 cites W1970123117 @default.
• W3000183405 cites W1973071934 @default.
• W3000183405 cites W1976059757 @default.
• W3000183405 cites W1976934690 @default.
• W3000183405 cites W1977376661 @default.
• W3000183405 cites W1982687515 @default.
• W3000183405 cites W1995469990 @default.
• W3000183405 cites W1995750237 @default.
• W3000183405 cites W1996987411 @default.
• W3000183405 cites W1998432526 @default.
• W3000183405 cites W1998830584 @default.
• W3000183405 cites W2002547764 @default.
• W3000183405 cites W2011637659 @default.
• W3000183405 cites W2013366650 @default.
• W3000183405 cites W2015049472 @default.
• W3000183405 cites W2015795476 @default.
• W3000183405 cites W2021104084 @default.
• W3000183405 cites W2028415754 @default.
• W3000183405 cites W2030937749 @default.
• W3000183405 cites W2032780125 @default.
• W3000183405 cites W2033406586 @default.
• W3000183405 cites W2035521611 @default.
• W3000183405 cites W2035555871 @default.
• W3000183405 cites W2038329478 @default.
• W3000183405 cites W2041745772 @default.
• W3000183405 cites W2042198997 @default.
• W3000183405 cites W2042337609 @default.
• W3000183405 cites W2043541149 @default.
• W3000183405 cites W2044350615 @default.
• W3000183405 cites W2047024992 @default.
• W3000183405 cites W2047678911 @default.
• W3000183405 cites W2053343049 @default.
• W3000183405 cites W2053349906 @default.
• W3000183405 cites W2053654862 @default.
• W3000183405 cites W2056343475 @default.
• W3000183405 cites W2057441424 @default.
• W3000183405 cites W2059581635 @default.
• W3000183405 cites W2061252595 @default.
• W3000183405 cites W2065903778 @default.
• W3000183405 cites W2071378820 @default.
• W3000183405 cites W2073597876 @default.
• W3000183405 cites W2077340556 @default.
• W3000183405 cites W2086718822 @default.
• W3000183405 cites W2092830359 @default.
• W3000183405 cites W2095296988 @default.
• W3000183405 cites W2095971921 @default.
• W3000183405 cites W2097198003 @default.
• W3000183405 cites W2103117581 @default.
• W3000183405 cites W2103441967 @default.
• W3000183405 cites W2106095322 @default.
• W3000183405 cites W2110465794 @default.
• W3000183405 cites W2114296097 @default.
• W3000183405 cites W2117692326 @default.
• W3000183405 cites W2121695889 @default.
• W3000183405 cites W2127736279 @default.
• W3000183405 cites W2128960139 @default.
• W3000183405 cites W2131545168 @default.
• W3000183405 cites W2133013399 @default.
• W3000183405 cites W2136153756 @default.
• W3000183405 cites W2136272158 @default.
• W3000183405 cites W2138155367 @default.
• W3000183405 cites W2142157691 @default.
• W3000183405 cites W2143824838 @default.
• W3000183405 cites W2144198186 @default.
• W3000183405 cites W2145870089 @default.
• W3000183405 cites W2154727263 @default.
• W3000183405 cites W2157466346 @default.
• W3000183405 cites W2159082261 @default.
• W3000183405 cites W2165200432 @default.
• W3000183405 cites W2166312842 @default.
• W3000183405 cites W2168532311 @default.
• W3000183405 cites W2172151766 @default.
• W3000183405 cites W2174515690 @default.
• W3000183405 cites W2175901504 @default.
• W3000183405 cites W2180425334 @default.
• W3000183405 cites W2194998434 @default.
• W3000183405 cites W2204695746 @default.
• W3000183405 cites W2254163334 @default.
• W3000183405 cites W2263206910 @default.
• W3000183405 cites W2265085667 @default.
• W3000183405 cites W2274032786 @default.
• W3000183405 cites W2279570938 @default.

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