Recurrent copy number alterations in prostate cancer: an in silico meta-analysis of publicly available genomic data (2014)
- Authors:
- Autor USP: SQUIRE, JEREMY ANDREW - FMRP
- Unidade: FMRP
- DOI: 10.1016/j.cancergen.2014.09.003
- Subjects: NEOPLASIAS PROSTÁTICAS (GENÉTICA;PATOLOGIA); MAPEAMENTO CROMOSSÔMICO; BIOINFORMÁTICA; GENÔMICA
- Language: Inglês
- Imprenta:
- Publisher place: Philadelphia
- Date published: 2014
- Source:
- Título: Cancer Genetics
- ISSN: 2210-7762
- Volume/Número/Paginação/Ano: v. 207, n. 10-12, p. 474-488, 2014
- Status:
- Artigo aberto em periódico híbrido (Hybrid Open Access)
- Versão do Documento:
- Versão publicada (Published version)
- Acessar versão aberta:
-
ABNT
WILLIAMS, Julia L e GREER, Peter A e SQUIRE, Jeremy Andrew. Recurrent copy number alterations in prostate cancer: an in silico meta-analysis of publicly available genomic data. Cancer Genetics, v. 207, n. 10-12, p. 474-488, 2014Tradução . . Disponível em: https://doi.org/10.1016/j.cancergen.2014.09.003. Acesso em: 31 mar. 2026. -
APA
Williams, J. L., Greer, P. A., & Squire, J. A. (2014). Recurrent copy number alterations in prostate cancer: an in silico meta-analysis of publicly available genomic data. Cancer Genetics, 207( 10-12), 474-488. doi:10.1016/j.cancergen.2014.09.003 -
NLM
Williams JL, Greer PA, Squire JA. Recurrent copy number alterations in prostate cancer: an in silico meta-analysis of publicly available genomic data [Internet]. Cancer Genetics. 2014 ; 207( 10-12): 474-488.[citado 2026 mar. 31 ] Available from: https://doi.org/10.1016/j.cancergen.2014.09.003 -
Vancouver
Williams JL, Greer PA, Squire JA. Recurrent copy number alterations in prostate cancer: an in silico meta-analysis of publicly available genomic data [Internet]. Cancer Genetics. 2014 ; 207( 10-12): 474-488.[citado 2026 mar. 31 ] Available from: https://doi.org/10.1016/j.cancergen.2014.09.003 - A multicenter study shows PTEN deletion is strongly associated with seminal vesicle involvement and extracapsular extension in localized prostate cancer
- Extracellular vesicles: evolving factors in stem cell biology
- Quantitative assessment of PTEN loss (qPTEN) is strongly associated with biochemical recurrence and may improve treatment decisions after surgery
- In silico shows that PTEN loss and AR overexpression are associated with increased CD8+ T-cell and Treg density and earlier disease recurrence in prostate cancer
- In prostate cancer needle biopsies, detections of PTEN loss by fluorescence in sity hybridization (FISH) and by immunohistochemistry (IHC) are concordant and show consistent association with upgrading
- STAT1-associated intratumoural TH1 immunity predicts chemotherapy resistance in high-grade serous ovarian cancer
- PTEN loss is associated with upgrading of prostate cancer from biopsy to radical prostatectomy
- Digital expression profiling identifies RUNX2, CDC5L, MDM2, RECQL4, and CDK4 as potential predictive biomarkers for neo-adjuvant chemotherapy response in paediatric osteosarcoma
- Application of fluorescence in situ hybridization (FISH) and immunohistochemistry (IHC) for detecting PTEN loss in diagnostic prostate cancer needle biopsies
- Analytic validation of a clinical-grade PTEN immunohistochemistry assay in prostate cancer by comparison with PTEN FISH
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