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410 results on '"Fazli L"'

1. Prognostic value of Ki67 in localized prostate carcinoma: a multi-institutional study of >1000 prostatectomies.

Author

Tretiakova, MS, Wei, W, Boyer, HD, Newcomb, LF, Hawley, S, Auman, H, Vakar-Lopez, F, McKenney, JK, Fazli, L, Simko, J, Troyer, DA, Hurtado-Coll, A, Thompson, IM, Carroll, PR, Ellis, WJ, Gleave, ME, Nelson, PS, Lin, DW, True, LD, Feng, Z, and Brooks, JD

Subjects
Humans, Prostatic Neoplasms, Recurrence, Prostate-Specific Antigen, Ki-67 Antigen, Neoplasm Staging, Prognosis, Prostatectomy, Tissue Array Analysis, Proportional Hazards Models, Cell Proliferation, Male, Kaplan-Meier Estimate, Neoplasm Grading, Cancer, Urologic Diseases, Prostate Cancer, Patient Safety, Detection, screening and diagnosis, 4.2 Evaluation of markers and technologies, Oncology and Carcinogenesis, Urology & Nephrology
Abstract

BackgroundExpanding interest in and use of active surveillance for early state prostate cancer (PC) has increased need for prognostic biomarkers. Using a multi-institutional tissue microarray resource including over 1000 radical prostatectomy samples, we sought to correlate Ki67 expression captured by an automated image analysis system with clinicopathological features and validate its utility as a clinical grade test in predicting cancer-specific outcomes.MethodsAfter immunostaining, the Ki67 proliferation index (PI) of tumor areas of each core (three cancer cores/case) was analyzed using a nuclear quantification algorithm (Aperio). We assessed whether Ki67 PI was associated with clinicopathological factors and recurrence-free survival (RFS) including biochemical recurrence, metastasis or PC death (7-year median follow-up).ResultsIn 1004 PCs (∼4000 tissue cores) Ki67 PI showed significantly higher inter-tumor (0.68) than intra-tumor variation (0.39). Ki67 PI was associated with stage (P

Published
2016

2. Outcomes of Active Surveillance for Clinically Localized Prostate Cancer in the Prospective, Multi-Institutional Canary PASS Cohort

Author

Newcomb, LF, Thompson, IM, Boyer, HD, Brooks, JD, Carroll, PR, Cooperberg, MR, Dash, A, Ellis, WJ, Fazli, L, Feng, Z, Gleave, ME, Kunju, P, Lance, RS, McKenney, JK, Meng, MV, Nicolas, MM, Sanda, MG, Simko, J, So, A, Tretiakova, MS, Troyer, DA, True, LD, Vakar-Lopez, F, Virgin, J, Wagner, AA, Wei, JT, Zheng, Y, Nelson, PS, and Lin, DW

Subjects
Urology & Nephrology, Clinical Sciences
Abstract

Purpose Active surveillance represents a strategy to address the overtreatment of prostate cancer, yet uncertainty regarding individual patient outcomes remains a concern. We evaluated outcomes in a prospective multicenter study of active surveillance. Materials and Methods We studied 905 men in the prospective Canary PASS enrolled between 2008 and 2013. We collected clinical data at study entry and at prespecified intervals, and determined associations with adverse reclassification, defined as increased Gleason grade or greater cancer volume on followup biopsy. We also evaluated the relationships of clinical parameters with pathology findings in participants who underwent surgery after a period of active surveillance. Results At a median followup of 28 months 24% of participants experienced adverse reclassification, of whom 53% underwent treatment while 31% continued on active surveillance. Overall 19% of participants received treatment, 68% with adverse reclassification, while 32% opted for treatment without disease reclassification. In multivariate Cox proportional hazards modeling the percent of biopsy cores with cancer, body mass index and prostate specific antigen density were associated with adverse reclassification (p=0.01, 0.04, 0.04, respectively). Of 103 participants subsequently treated with radical prostatectomy 34% had adverse pathology, defined as primary pattern 4-5 or nonorgan confined disease, including 2 with positive lymph nodes, with no significant relationship between risk category at diagnosis and findings at surgery (p=0.76). Conclusions Most men remain on active surveillance at 5 years without adverse reclassification or adverse pathology at surgery. However, clinical factors had only a modest association with disease reclassification, supporting the need for approaches that improve the prediction of this outcome.

Published
2016

3. Evaluation of ERG and SPINK1 by immunohistochemical staining and clinicopathological outcomes in a multi-institutional radical prostatectomy cohort of 1067 patients

Author

Carroll, Peter, Brooks, JD, Wei, W, Hawley, S, Auman, H, Newcomb, L, Boyer, H, Fazli, L, Simko, J, Hurtado-Coll, A, and Troyer, DA

Abstract

© 2015 Brooks et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Published
2015

4. A multicenter study shows PTEN deletion is strongly associated with seminal vesicle involvement and extracapsular extension in localized prostate cancer

Author

Carroll, Peter, Troyer, DA, Jamaspishvili, T, Wei, W, Feng, Z, Good, J, Hawley, S, Fazli, L, McKenney, JK, Simko, J, and Hurtado-Coll, A

Abstract

© 2015 The Authors.BACKGROUND. Loss of the phosphatase and tensin homolog (PTEN) tumor suppressor gene is a promising marker of aggressive prostate cancer. Active surveillance and watchful waiting are increasingly recommended to patients with small tumors

Published
2015

9. EVALUATING THE PERFORMANCE OF HIGHER EDUCATION CENTERS BASED ON FUZZY IMPROVED INPUT EFFICIENCY PROFILE MODEL.

Author

Mansouri, E. and Fazli, L.

Subjects
*HIGHER education, *TEST validity
Abstract

Evaluating the quality of the performances of higher education centers is very important due to their important and effective role. Evaluating the quality of the performance of higher education centers leads to identifying strengths and weaknesses, as well as opportunities and factors hindering development, and the possibility of an appropriate planning for improving the situation are also provided. In order to continuously modify and improve the university system, it seems necessary to establish an appropriate performance evaluation mechanism through which the improvement of the entire university system can be considered in addition to improving and enhancing the scientific quality, and at the same time, which has arisen from the text of the university system and conforms to the characteristics of this system. In this research, considering the uncertain decision-making environment, a new evaluation model called Fuzzy Improved Input Efficiency Profiling - Common Weights Based on the Optimal Solution (FIIEP - CWBOS) has been proposed, which improves the performance of the classic input efficiency profile model. The results of this study showed that the proposed model has the necessary validity and optimal performance compared to other models presented so far. [ABSTRACT FROM AUTHOR]

Published
2022
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15. A molecular portrait of epithelial-mesenchymal plasticity in prostate cancer associated with clinical outcome.

Author

Stylianou, N, Lehman, ML, Wang, C, Fard, AT, Rockstroh, A, Fazli, L, Jovanovic, L, Ward, M, Sadowski, MC, Kashyap, AS, Buttyan, R, Gleave, ME, Westbrook, TF, Williams, ED, Gunter, JH, Nelson, CC, Hollier, BG, Stylianou, N, Lehman, ML, Wang, C, Fard, AT, Rockstroh, A, Fazli, L, Jovanovic, L, Ward, M, Sadowski, MC, Kashyap, AS, Buttyan, R, Gleave, ME, Westbrook, TF, Williams, ED, Gunter, JH, Nelson, CC, and Hollier, BG

Abstract

The propensity of cancer cells to transition between epithelial and mesenchymal phenotypic states via the epithelial-mesenchymal transition (EMT) program can regulate metastatic processes, cancer progression, and treatment resistance. Transcriptional investigations using reversible models of EMT, revealed the mesenchymal-to-epithelial reverting transition (MErT) to be enriched in clinical samples of metastatic castrate resistant prostate cancer (mCRPC). From this enrichment, a metastasis-derived gene signature was identified that predicted more rapid cancer relapse and reduced survival across multiple human carcinoma types. Additionally, the transcriptional profile of MErT is not a simple mirror image of EMT as tumour cells retain a transcriptional "memory" following a reversible EMT. This memory was also enriched in mCRPC samples. Cumulatively, our studies reveal the transcriptional profile of epithelial-mesenchymal plasticity and highlight the unique transcriptional properties of MErT. Furthermore, our findings provide evidence to support the association of epithelial plasticity with poor clinical outcomes in multiple human carcinoma types.

Published
2019

17. A molecular portrait of epithelial-mesenchymal plasticity in prostate cancer progression

Author

Stylianou, N, primary, Lehman, ML, additional, Wang, C, additional, Fard, AT, additional, Rockstroh, A, additional, Fazli, L, additional, Jovanovic, L, additional, Ward, M, additional, Sadowski, MC, additional, Kashyap, AS, additional, Buttyan, R, additional, Gleave, ME, additional, Westbrook, TF, additional, Williams, ED, additional, Gunter, JH, additional, Nelson, CC, additional, and Hollier, BG, additional

Published
2019
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18. Trop-2 is up-regulated in invasive prostate cancer and displaces FAK from focal contacts

Author

Trerotola, M., Ganguly, K. K., Fazli, L., Fedele, C., Lu, H., Dutta, A., Liu, Q., Angelis, T., Riddell, L. W., Riobo, N. A., Gleave, M. E., Zoubeidi, A., Pestell, R. G., Altieri, D. C., and Lucia Languino

Subjects
gleason grade, pT2/pT3/pT4 prostate cancer, metastasis, exosome, TRAMP, urologic and male genital diseases, Research Paper
Abstract

In this study, we show that the transmembrane glycoprotein Trop-2 is up-regulated in human prostate cancer (PCa) with extracapsular extension (stages pT3/pT4) as compared to organ-confined (stage pT2) PCa. Consistent with this evidence, Trop-2 expression is found to be increased in metastatic prostate tumors of Transgenic Adenocarcinoma of Mouse Prostate mice and to strongly correlate with α5β1 integrin levels. Using PCa cells, we show that Trop-2 specifically associates with the α5 integrin subunit, as binding to α3 is not observed, and that Trop-2 displaces focal adhesion kinase from focal contacts. In support of the role of Trop-2 as a promoter of PCa metastatic phenotype, we observe high expression of this molecule in exosomes purified from Trop-2-positive PCa cells. These vesicles are then found to promote migration of Trop-2-negative PCa cells on fibronectin, an α5β1 integrin/focal adhesion kinase substrate, thus suggesting that the biological function of Trop-2 may be propagated to recipient cells. In summary, our findings show that Trop-2 promotes an α5β1 integrin-dependent pro-metastatic signaling pathway in PCa cells and that the altered expression of Trop-2 may be utilized for early identification of capsule-invading PCa.

Published
2015

20. Neuropilin-1 is upregulated in the adaptive response of prostate tumors to androgen-targeted therapies and is prognostic of metastatic progression and patient mortality

Author

Tse, BWC, Volpert, M, Ratther, E, Stylianou, N, Nouri, M, McGowan, K, Lehman, ML, McPherson, SJ, Roshan-Moniri, M, Butler, MS, Caradec, J, Gregory-Evans, CY, McGovern, J, Das, R, Takhar, M, Erho, N, Alshalafa, M, Davicioni, E, Schaeffer, EM, Jenkins, RB, Ross, AE, Karnes, RJ, Den, RB, Fazli, L, Gregory, PA, Gleave, ME, Williams, ED, Rennie, PS, Buttyan, R, Gunter, JH, Selth, LA, Russell, PJ, Nelson, CC, Hollier, BG, Tse, BWC, Volpert, M, Ratther, E, Stylianou, N, Nouri, M, McGowan, K, Lehman, ML, McPherson, SJ, Roshan-Moniri, M, Butler, MS, Caradec, J, Gregory-Evans, CY, McGovern, J, Das, R, Takhar, M, Erho, N, Alshalafa, M, Davicioni, E, Schaeffer, EM, Jenkins, RB, Ross, AE, Karnes, RJ, Den, RB, Fazli, L, Gregory, PA, Gleave, ME, Williams, ED, Rennie, PS, Buttyan, R, Gunter, JH, Selth, LA, Russell, PJ, Nelson, CC, and Hollier, BG

Abstract

Recent evidence has implicated the transmembrane co-receptor neuropilin-1 (NRP1) in cancer progression. Primarily known as a regulator of neuronal guidance and angiogenesis, NRP1 is also expressed in multiple human malignancies, where it promotes tumor angiogenesis. However, non-angiogenic roles of NRP1 in tumor progression remain poorly characterized. In this study, we define NRP1 as an androgen-repressed gene whose expression is elevated during the adaptation of prostate tumors to androgen-targeted therapies (ATTs), and subsequent progression to metastatic castration-resistant prostate cancer (mCRPC). Using short hairpin RNA (shRNA)-mediated suppression of NRP1, we demonstrate that NRP1 regulates the mesenchymal phenotype of mCRPC cell models and the invasive and metastatic dissemination of tumor cells in vivo. In patients, immunohistochemical staining of tissue microarrays and mRNA expression analyses revealed a positive association between NRP1 expression and increasing Gleason grade, pathological T score, positive lymph node status and primary therapy failure. Furthermore, multivariate analysis of several large clinical prostate cancer (PCa) cohorts identified NRP1 expression at radical prostatectomy as an independent prognostic biomarker of biochemical recurrence after radiation therapy, metastasis and cancer-specific mortality. This study identifies NRP1 for the first time as a novel androgen-suppressed gene upregulated during the adaptive response of prostate tumors to ATTs and a prognostic biomarker of clinical metastasis and lethal PCa.

Published
2017

26. Neuropilin-1 is upregulated in the adaptive response of prostate tumors to androgen-targeted therapies and is prognostic of metastatic progression and patient mortality

Author

Tse, B W C, primary, Volpert, M, additional, Ratther, E, additional, Stylianou, N, additional, Nouri, M, additional, McGowan, K, additional, Lehman, M L, additional, McPherson, S J, additional, Roshan-Moniri, M, additional, Butler, M S, additional, Caradec, J, additional, Gregory-Evans, C Y, additional, McGovern, J, additional, Das, R, additional, Takhar, M, additional, Erho, N, additional, Alshalafa, M, additional, Davicioni, E, additional, Schaeffer, E M, additional, Jenkins, R B, additional, Ross, A E, additional, Karnes, R J, additional, Den, R B, additional, Fazli, L, additional, Gregory, P A, additional, Gleave, M E, additional, Williams, E D, additional, Rennie, P S, additional, Buttyan, R, additional, Gunter, J H, additional, Selth, L A, additional, Russell, P J, additional, Nelson, C C, additional, and Hollier, B G, additional

Published
2017
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28. The role of homeostatic regulation between tumor suppressor DAB2IP and oncogenic Skp2 in prostate cancer growth

Author

Tsai Y.-S., Lai C.-L., Lai C.-H., Chang K.-H., Wu K., Tseng S.-F., Fazli L., Gleave M., Xiao G., Gandee L., Sharifi N., Moro L., Tzai T.-S., and Hsieh J.-T.

Subjects
Ubiquitin, Prostate neoplasm, Skp2, DAB2IP
Abstract

Altered DAB2IP gene expression often detected in prostate cancer (PCa) is due to epigenetic silencing. In this study, we unveil a new mechanism leading to the loss of DAB2IP protein; an oncogenic S-phase kinase-associated protein-2 (Skp2) as E3 ubiquitin ligase plays a key regulator in DAB2IP degradation. In order to unveil the role of Skp2 in the turnover of DAB2IP protein, both prostate cell lines and prostate cancer specimens with a variety of molecular and cell biologic techniques were employed. We demonstrated that DAB2IP is regulated by Skp2-mediated proteasome degradation in the prostate cell lines. Further analyses identified the N-terminal DAB2IP containing the ubiquitination site. Immunohistochemical study exhibited an inverse correlation between DAB2IP and Skp2 protein expression in the prostate cancer tissue microarray. In contrast, DAB2IP can suppress Skp2 protein expression is mediated through Akt signaling. The reciprocal regulation between DAB2IP and Skp2 can impact on the growth of PCa cells. This reciprocal regulation between DAB2IP and Skp2 protein represents a unique homeostatic balance between tumor suppressor and oncoprotein in normal prostate epithelia, which is apparently altered in cancer cells. The outcome of this study has identified new potential targets for developing new therapeutic strategy for PCa.

Published
2014

30. 929 Targeting lactate transporters for the treatment of urothelial carcinoma

Author

Todenhöfer, T., primary, Seiler, R., additional, Stewart, C., additional, Moskalev, I., additional, Gao, J., additional, Ladar, S., additional, Kamyabi, A., additional, Al Nakouzi, N., additional, Hayashi, T., additional, Choi, S., additional, Wang, Y., additional, Frees, S., additional, Daugaard, M., additional, Zarni Ooh, H., additional, Hennenlotter, J., additional, Bedke, J., additional, Fazli, L., additional, Stenzl, A., additional, and Black, P., additional

Published
2016
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31. 138 Exploring a novel therapeutic target for neuroendocrine prostate cancer using a xenograft model of trans-differentiation

Author

Akamatsu, S., primary, Wyatt, A., additional, Lin, D., additional, Lysakowski, S., additional, Zhang, F., additional, Kawai, Y., additional, Fazli, L., additional, Ogawa, O., additional, Lotan, T., additional, Rubin, M., additional, Beltran, H., additional, Zoubeidi, A., additional, Wang, Y., additional, Gleave, M., additional, and Collins, C., additional

Published
2016
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36. DAB2IP loss confers the resistance of prostate cancer to androgen deprivation therapy through activating STAT3 and inhibiting apoptosis

Author

Zhou, J, primary, Ning, Z, additional, Wang, B, additional, Yun, E-J, additional, Zhang, T, additional, Pong, R-C, additional, Fazli, L, additional, Gleave, M, additional, Zeng, J, additional, Fan, J, additional, Wang, X, additional, Li, L, additional, Hsieh, J-T, additional, He, D, additional, and Wu, K, additional

Published
2015
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44. 495 Divergent androgen regulation of UPR pathways drives prostate cancer

Author

Arnoldussen, Y.J., primary, Storm, M., additional, Sheng, X., additional, Tesikova, M., additional, Jin, Y., additional, Nenseth, H.Z., additional, Zhao, S., additional, Mills, I.G., additional, Fazli, L., additional, Rennie, P., additional, Risberg, B., additional, Wæhre, H., additional, Danielsen, H.E., additional, Hotamisligil, G.S., additional, and Saatcioglu, F., additional

Published
2014
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