FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2334177911> ?p ?o ?g. }

• W2334177911 abstract "The initial growth of most localized prostate cancers (PCa) is slow and dependent on androgens. Thus, early-staged and androgen-dependent cancer is manageable with prostatectomy and primary androgen deprivation therapy by either surgical or medical castration or monotherapy with antiandrogens. However, many prostate cancer patients under primary hormone therapy will relapse and further develop resistance to antiandrogen treatments and progress to a fatal androgen-independent and metastatic stage of which treatment options are limited. Identification of key factors or pathways responsible for the development of androgen-independence and antiandrogen resistance is crucial not only for better understanding of advanced prostate cancer development but also development of novel therapeutic strategies fro this cancer. Based on this background, we have established an antiandrogen-resistant prostate cancer cell line model (LNCaP-BC) by long-term treatment (>6 months) of an androgen-sensitive prostate caner cell line LNCaP with a non-steroidal antiandrogen bicalutamide at various concentrations. Our in vitro growth studies showed that LNCaP-BC cells behaved more malignant and grew aggressively. Compared to LNCaP cells, LNCaP-BC cells grew significantly faster than the untreated LNCaP cells in both normal and androgen-depleted media; were less sensitive to bicalutamide but more sensitive to low level of androgen (R1881); exhibited increased colony formation efficiencies in soft agar assay, enhanced tolerance to hypoxia environment and less sensitive to anticancer drug paclitaxel. Real-time PCR and Western blot results revealed that LNCaP-BC cells exhibited an increased mRNA and protein level of androgen receptor (AR) suggesting that the AR signaling was dysregulated in LNCaP-BC cells. More interestingly, a progressive and persistent up-regulation of an orphan nuclear receptor tailless TLX was observed in LNCaP-BC cells. To determine whether TLX overexpression would be associated with the antiandrogen resistant phenotype in prostate cancer cells, we generated stable-TLX transductants in LNCaP cells, which expressed low endogenous TLX level, by retroviral transduction. The in vitro growth phenotypes of LNCaP-TLX clones were similar to the LNCaP-BC cells, such as less sensitivity to bicalutamide and enhanced growth in charcoal-stripped serum, suggesting that TLX might play a regulatory role in the antiandrogen-resistance in advanced prostate cancer. In summary, we have established a bicalutamide-resistant in vitro model of prostate cancer. Our findings also revealed for the first time that up-regulation of TLX may play a regulatory role in the antiandrogen-resistance development of advanced prostate cancer. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 102nd Annual Meeting of the American Association for Cancer Research; 2011 Apr 2-6; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2011;71(8 Suppl):Abstract nr 4016. doi:10.1158/1538-7445.AM2011-4016" @default.
• W2334177911 created "2016-06-24" @default.
• W2334177911 creator A5004300259 @default.
• W2334177911 creator A5007672814 @default.
• W2334177911 creator A5050688744 @default.
• W2334177911 creator A5051845761 @default.
• W2334177911 creator A5086664284 @default.
• W2334177911 date "2011-04-15" @default.
• W2334177911 modified "2023-09-27" @default.
• W2334177911 title "Abstract 4016: Upregulation of an orphan nuclear receptor TLX may contribute to the development of antiandrogen-resistant prostate cancer" @default.
• W2334177911 doi "https://doi.org/10.1158/1538-7445.am2011-4016" @default.
• W2334177911 hasPublicationYear "2011" @default.
• W2334177911 type Work @default.
• W2334177911 sameAs 2334177911 @default.
• W2334177911 citedByCount "0" @default.
• W2334177911 crossrefType "proceedings-article" @default.
• W2334177911 hasAuthorship W2334177911A5004300259 @default.
• W2334177911 hasAuthorship W2334177911A5007672814 @default.
• W2334177911 hasAuthorship W2334177911A5050688744 @default.
• W2334177911 hasAuthorship W2334177911A5051845761 @default.
• W2334177911 hasAuthorship W2334177911A5086664284 @default.
• W2334177911 hasConcept C121608353 @default.
• W2334177911 hasConcept C126322002 @default.
• W2334177911 hasConcept C134018914 @default.
• W2334177911 hasConcept C2777899217 @default.
• W2334177911 hasConcept C2777911890 @default.
• W2334177911 hasConcept C2779322244 @default.
• W2334177911 hasConcept C2779723316 @default.
• W2334177911 hasConcept C2780192828 @default.
• W2334177911 hasConcept C2780962315 @default.
• W2334177911 hasConcept C502942594 @default.
• W2334177911 hasConcept C61367390 @default.
• W2334177911 hasConcept C71315377 @default.
• W2334177911 hasConcept C71924100 @default.
• W2334177911 hasConceptScore W2334177911C121608353 @default.
• W2334177911 hasConceptScore W2334177911C126322002 @default.
• W2334177911 hasConceptScore W2334177911C134018914 @default.
• W2334177911 hasConceptScore W2334177911C2777899217 @default.
• W2334177911 hasConceptScore W2334177911C2777911890 @default.
• W2334177911 hasConceptScore W2334177911C2779322244 @default.
• W2334177911 hasConceptScore W2334177911C2779723316 @default.
• W2334177911 hasConceptScore W2334177911C2780192828 @default.
• W2334177911 hasConceptScore W2334177911C2780962315 @default.
• W2334177911 hasConceptScore W2334177911C502942594 @default.
• W2334177911 hasConceptScore W2334177911C61367390 @default.
• W2334177911 hasConceptScore W2334177911C71315377 @default.
• W2334177911 hasConceptScore W2334177911C71924100 @default.
• W2334177911 hasLocation W23341779111 @default.
• W2334177911 hasOpenAccess W2334177911 @default.
• W2334177911 hasPrimaryLocation W23341779111 @default.
• W2334177911 hasRelatedWork W1996993772 @default.
• W2334177911 hasRelatedWork W1998786498 @default.
• W2334177911 hasRelatedWork W2000764535 @default.
• W2334177911 hasRelatedWork W2036181871 @default.
• W2334177911 hasRelatedWork W2096851248 @default.
• W2334177911 hasRelatedWork W2097535434 @default.
• W2334177911 hasRelatedWork W2112104987 @default.
• W2334177911 hasRelatedWork W2145777186 @default.
• W2334177911 hasRelatedWork W2172102403 @default.
• W2334177911 hasRelatedWork W2313162381 @default.
• W2334177911 hasRelatedWork W2314955586 @default.
• W2334177911 hasRelatedWork W2369316301 @default.
• W2334177911 hasRelatedWork W2419284765 @default.
• W2334177911 hasRelatedWork W2604442472 @default.
• W2334177911 hasRelatedWork W2739481929 @default.
• W2334177911 hasRelatedWork W2753250048 @default.
• W2334177911 hasRelatedWork W2795783555 @default.
• W2334177911 hasRelatedWork W2801433010 @default.
• W2334177911 hasRelatedWork W2954875053 @default.
• W2334177911 hasRelatedWork W3087584857 @default.
• W2334177911 isParatext "false" @default.
• W2334177911 isRetracted "false" @default.
• W2334177911 magId "2334177911" @default.
• W2334177911 workType "article" @default.