Your search keyword '"Bismar, Tarek A."' showing total 74 results

1. Elevated LAMTOR4 Expression Is Associated with Lethal Prostate Cancer and Its Knockdown Decreases Cell Proliferation, Invasion, and Migration In Vitro.

Author

Gamallat, Yaser, Alwazan, Huseen, Turko, Rasoul, Dang, Vincent, Seyedi, Sima, Ghosh, Sunita, and Bismar, Tarek A.

Subjects

TRANSURETHRAL prostatectomy, GENE expression, SCAFFOLD proteins, METASTASIS, CANCER invasiveness

Abstract

Late endosomal/lysosomal adaptor, MAPK and mTOR, or LAMTOR, is a scaffold protein complex that senses nutrients and integrates growth factor signaling. The role of LAMTOR4 in tumorigenesis is still unknown. However, there is a considerable possibility that LAMTOR4 is directly involved in tumor cell proliferation and metastasis. In the current study, we investigated the protein expression of LAMTOR4 in a cohort of 314 men who were undergoing transurethral resection of prostate (TURP) consisting of incidental, advanced and castration-resistant cases. We also correlated the data with ERG and PTEN genomic status and clinicopathological features including Gleason score and patients' outcome. Additionally, we performed in vitro experiments utilizing knockdown of LAMTOR4 in prostate cell lines, and we performed mRNA expression assessment using TCGA prostate adenocarcinoma (TCGA-PRAD) to explore the potential differentially expressed genes and pathways associated with LAMTOR4 overexpression in PCa patients. Our data indicate that high LAMTOR4 protein expression was significantly associated with poor overall survival (OS) (HR: 1.44, CI: 1.01–2.05, p = 0.047) and unfavorable cause-specific survival (CSS) (HR: 1.71, CI: 1.06–2.77, p = 0.028). Additionally, when high LAMTOR4 expression was combined with PTEN-negative cases (score 0), we found significantly poorer OS (HR: 2.22, CI: 1.37–3.59, p = 0.001) and CSS (HR: 3.46, CI: 1.86–6.46, p < 0.0001). Furthermore, ERG-positive cases with high LAMTOR4 exhibited lower OS (HR: 1.98, CI: 1.18–3.31, p = 0.01) and CSS (HR: 2.54, CI: 1.32–4.87, p = 0.005). In vitro assessment showed that knockdown of LAMTOR4 decreases PCa cell proliferation, migration, and invasion. Our data further showed that knockdown of LAMTOR4 in the LNCaP cell line significantly dysregulated the β catenin/mTOR pathway and tumorigenesis associated pathways. Inhibiting components of the mTOR pathway, including LAMTOR4, might offer a strategy to inhibit tumor progression and metastasis in prostate cancer. [ABSTRACT FROM AUTHOR]

Published

2024

2. Fluorine-18 Prostate-Specific Membrane Antigen–1007 PET/CT vs Multiparametric MRI for Locoregional Staging of Prostate Cancer.

Author

Mookerji, Nikhile, Pfanner, Tyler, Hui, Amaris, Huang, Guocheng, Albers, Patrick, Mittal, Rohan, Broomfield, Stacey, Dean, Lucas, St. Martin, Blair, Jacobsen, Niels-Erik, Evans, Howard, Gao, Yuan, Hung, Ryan, Abele, Jonathan, Dromparis, Peter, Lima, Joema Felipe, Bismar, Tarek, Michelakis, Evangelos, Sutendra, Gopinath, and Wuest, Frank

Published

2024

3. Exploring The Prognostic Significance of SET-Domain Containing 2 (SETD2) Expression in Advanced and Castrate-Resistant Prostate Cancer.

Author

Gamallat, Yaser, Felipe Lima, Joema, Seyedi, Sima, Li, Qiaowang, Rokne, Jon George, Alhajj, Reda, Ghosh, Sunita, and Bismar, Tarek A.

Subjects

CASTRATION-resistant prostate cancer, RESEARCH funding, TUMOR markers, DESCRIPTIVE statistics, CELLULAR signal transduction, GENE expression, TRANSFERASES, CONFIDENCE intervals, OVERALL survival, DISEASE progression

Abstract

Simple Summary: SETD2, a histone methyltransferase and epigenetic modifier, and SETD2 protein expression were explored in a prostate cancer non-surgical cohort of 202 cases. Notably, SETD2 showed higher intensity in advanced and castrate-resistant disease compared to incidental cases. Moreover, elevated SETD2 expression is significantly associated with poorer prognosis, lower overall survival (OS), and decreased cancer-specific survival (CSS). High-risk SETD2 combined with PTEN loss or ERG positivity improved the prognostication for these outcomes. Additionally, the TCPA protein database and TCGA PRAD GSEA implicated SETD2 in pathways linked to tumor progression, chemoresistance, and adverse prognosis, including the AMPK, cAMP, and PI3K-Akt signaling pathways. SET-domain containing 2 (SETD2) is a histone methyltransferase and an epigenetic modifier with oncogenic functionality. In the current study, we investigated the potential prognostic role of SETD2 in prostate cancer. A cohort of 202 patients' samples was assembled on tissue microarrays (TMAs) containing incidental, advanced, and castrate-resistant CRPCa cases. Our data showed significant elevated SETD2 expression in advanced and castrate-resistant disease (CRPCa) compared to incidental cases (2.53 ± 0.58 and 2.21 ± 0.63 vs. 1.9 ± 0.68; p < 0.001, respectively). Interestingly, the mean intensity of SETD2 expression in deceased vs. alive patients was also significantly different (2.31 ± 0.66 vs. 2 ± 0.68; p = 0.003, respectively). Overall, high SETD2 expression was found to be considered high risk and was significantly associated with poor prognosis and worse overall survival (OS) (HR 1.80; 95% CI: 1.28–2.53, p = 0.001) and lower cause specific survival (CSS) (HR 3.14; 95% CI: 1.94–5.08, p < 0.0001). Moreover, combining high-intensity SETD2 with PTEN loss resulted in lower OS (HR 2.12; 95% CI: 1.22–3.69, p = 0.008) and unfavorable CSS (HR 3.74; 95% CI: 1.67–8.34, p = 0.001). Additionally, high SETD2 intensity with ERG positive expression showed worse prognosis for both OS (HR 1.99, 95% CI 0.87–4.59; p = 0.015) and CSS (HR 2.14, 95% CI 0.98–4.68, p = 0.058). We also investigated the protein expression database TCPA, and our results showed that high SETD2 expression is associated with a poor prognosis. Finally, we performed TCGA PRAD gene set enrichment analysis (GSEA) data for SETD2 overexpression, and our data revealed a potential association with pathways involved in tumor progression such as the AMPK signaling pathway, the cAMP signaling pathway, and the PI3K-Akt signaling pathway, which are potentially associated with tumor progression, chemoresistance, and a poor prognosis. [ABSTRACT FROM AUTHOR]

Published

2024

4. Genomic Biomarker Discovery in Disease Progression and Therapy Response in Bladder Cancer Utilizing Machine Learning.

Author

Liosis, Konstantinos Christos, Marouf, Ahmed Al, Rokne, Jon G., Ghosh, Sunita, Bismar, Tarek A., and Alhajj, Reda

Subjects

BLADDER tumors, SEQUENCE analysis, MACHINE learning, TREATMENT effectiveness, CANCER patients, GENE expression, SURVIVAL rate, GENOMICS, KAPLAN-Meier estimator, TUMOR markers, RNA probes, EVALUATION

Abstract

Simple Summary: Cancer in all its forms of expression is a major cause of death. The bladder cancer is also causes the same. finding the biomarkers responsible for the cancer is a challenging task and in certain cases, such as disease progression and therapy response, it become more challenging. The advancements in technology provides latest machine learning methods that help to identify the genomic biomarkers computationally. In this paper, the genomic biomarkers are tracked for bladder cancer from Univeristy of Calgary cohort and different bioinformatics methods, such as differential gene expression, survival rate estimation, consensus gene selection approaches were optimally used. The elastic-net based regression method has been utilized as a machine learning method which shows satisfactory results. Cancer in all its forms of expression is a major cause of death. To identify the genomic reason behind cancer, discovery of biomarkers is needed. In this paper, genomic data of bladder cancer are examined for the purpose of biomarker discovery. Genomic biomarkers are indicators stemming from the study of the genome, either at a very low level based on the genome sequence itself, or more abstractly such as measuring the level of gene expression for different disease groups. The latter method is pivotal for this work, since the available datasets consist of RNA sequencing data, transformed to gene expression levels, as well as data on a multitude of clinical indicators. Based on this, various methods are utilized such as statistical modeling via logistic regression and regularization techniques (elastic-net), clustering, survival analysis through Kaplan–Meier curves, and heatmaps for the experiments leading to biomarker discovery. The experiments have led to the discovery of two gene signatures capable of predicting therapy response and disease progression with considerable accuracy for bladder cancer patients which correlates well with clinical indicators such as Therapy Response and T-Stage at surgery with Disease Progression in a time-to-event manner. [ABSTRACT FROM AUTHOR]

Published

2023

5. Disparities in prostate cancer screening, diagnoses, management, and outcomes between Indigenous and non‐Indigenous men in a universal health care system.

Author

Kiciak, Alex, Clark, Wayne, Uhlich, Maxwell, Letendre, Angeline, Littlechild, Randy, Lightning, Patrick, Vasquez, Catalina, Singh, Raja, Broomfield, Stacey, Martin, Anais Medina, Huang, Guocheng, Fairey, Adrian, Kolinsky, Michael, Wallis, Christopher J. D., Fung, Christopher, Hyndman, Eric, Yip, Steven, Bismar, Tarek A., Lewis, John, and Ghosh, Sunita

Subjects

UNIVERSAL healthcare, PROSTATE cancer, EARLY detection of cancer, MEN'S health, PROSTATE cancer patients, DIAGNOSIS

Abstract

Background: Indigenous Peoples have higher morbidity rates and lower life expectancies than non‐Indigenous Canadians. Identification of disparities between Indigenous and non‐Indigenous men regarding prostate cancer (PCa) screening, diagnoses, management, and outcomes was sought. Methods: An observational cohort of men diagnosed with PCa between June 2014 and October 2022 was studied. Men were prospectively enrolled in the province‐wide Alberta Prostate Cancer Research Initiative. The primary outcomes were tumor characteristics (stage, grade, and prostate‐specific antigen [PSA]) at diagnosis. Secondary outcomes were PSA testing rates, time from diagnosis to treatment, treatment modality, and metastasis‐free, cancer‐specific, and overall survivals. Results: Examination of 1,444,974 men for whom aggregate PSA testing data were available was performed. Men in Indigenous communities were less likely to have PSA testing performed than men outside of Indigenous communities (32 vs. 46 PSA tests per 100 men [aged 50–70 years] within 1 year; p <.001). Among 6049 men diagnosed with PCa, Indigenous men had higher risk disease characteristics: a higher proportion of Indigenous men had PSA ≥ 10 ng/mL (48% vs. 30%; p <.01), TNM stage ≥ T2 (65% vs. 47%; p <.01), and Gleason grade group ≥ 2 (79% vs. 64%; p <.01) compared to non‐Indigenous men. With a median follow‐up of 40 months (interquartile range, 25–65 months), Indigenous men were at higher risk of developing PCa metastases (hazard ratio, 2.3; 95% CI, 1.2–4.2; p <.01) than non‐Indigenous men. Conclusions: Despite receiving care in a universal health care system, Indigenous men were less likely to receive PSA testing and more likely to be diagnosed with aggressive tumors and develop PCa metastases than non‐Indigenous men. Disparities between Indigenous and non‐Indigenous men regarding prostate cancer screening, diagnoses, management, and outcomes were identified. Despite receiving care in a universal health care system, Indigenous men were less likely to receive prostate‐specific antigen testing and more likely to be diagnosed with aggressive tumors and develop prostate cancer metastases than non‐Indigenous men. [ABSTRACT FROM AUTHOR]

Published

2023

6. Cleavage and Polyadenylation-Specific Factor 4 (CPSF4) Expression Is Associated with Enhanced Prostate Cancer Cell Migration and Cell Cycle Dysregulation, In Vitro.

Author

Choudhry, Muhammad, Gamallat, Yaser, Ghosh, Sunita, and Bismar, Tarek A.

Subjects

CANCER cell migration, CELL migration, CELL cycle, PROSTATE cancer, ONCOGENES, CELL proliferation

Abstract

Potential oncogene cleavage and polyadenylation specific factor 4 (CPSF4) has been linked to several cancer types. However, little research has been conducted on its function in prostate cancer (PCa). In benign, incidental, advanced, and castrate resistant PCa (CRPCa) patient samples, protein expression of CPSF4 was examined on tissue microarray (TMAs) of 353 PCa patients using immunohistochemistry. Using the 'The Cancer Genome Atlas' Prostate Adenocarcinoma (TCGA PRAD) database, significant correlations were found between high CPSF4 expression and high-risk genomic abnormalities such as ERG-fusion, ETV1-fusion, and SPOP mutations. Gene Set Enrichment Analysis (GSEA) of CPSF4 revealed evidence for the increase in biological processes such as cellular proliferation and metastasis. We further examined the function of CPSF4 in vitro and confirmed CPSF4 clinical outcomes and its underlying mechanism. Our findings showed a substantial correlation between Gleason groups and CPSF4 protein expression. In vitro, CPSF4 knockdown reduced cell invasion and migration while also causing G1 and G2 arrest in PC3 cell lines. Our findings demonstrate that CPSF4 may be used as a possible biomarker in PCa and support its oncogenic function in cellular proliferation and metastasis. [ABSTRACT FROM AUTHOR]

Published

2023

7. Editorial: The Application of Proteogenomics to Urine Analysis for the Identification of Novel Biomarkers of Prostate Cancer: An Exploratory Study.

Author

Gamallat, Yaser and Bismar, Tarek A.

Subjects

BIOMARKERS, GENETIC mutation, PROTEOMICS, GENOMICS, URINALYSIS, PROSTATE-specific antigen, PROSTATE tumors

Abstract

Short Summary: In this editorial context, we aim to leverage the potential of proteogenomics, which integrates genomic and proteomic data, to discover novel biomarkers that can aid in the diagnosis and management of prostate cancer. We highlight the importance of proteogenomics for understanding the functional consequences of somatic mutations in cancer and demonstrating how proteogenomic analysis can provide insights into the effects of genetic alterations on the proteomic landscape and identify potential therapeutic targets. This article also emphasizes the potential of urine analysis for the detection of prostate cancer. Overall, our editorial paper provides general insights on the application of proteogenomics to urine analysis for the identification of novel biomarkers of prostate cancer. [ABSTRACT FROM AUTHOR]

Published

2023

8. Loss of KLK4::KLKP1 pseudogene expression by RNA chromogenic in-situ hybridization is associated with PTEN loss and increased risk of biochemical recurrence in a cohort of middle eastern men with prostate cancer.

Author

Bakker, Andrea, Slack, Jonathan C., Palanisamy, Nalla, Carskadon, Shannon, Ghosh, Sunita, Khalifeh, Ibrahim, and Bismar, Tarek A.

Subjects

PROSTATE cancer, IN situ hybridization, GENE expression, ANDROGEN drugs, PROSTATE cancer patients, SURGICAL margin, RADICAL prostatectomy

Abstract

Background: KLK4::KLKP1 fusion is a recently described pseudogene that is enriched in prostate cancer (PCa). This new biomarker has not been characterized in the Middle Eastern population. Objective: To establish the incidence and prognostic value of KLK4::KLKP1 fusion in a cohort of Middle Eastern men with PCa and explore the relationship of this marker to other relevant biomarkers (PTEN, ERG, SPINK1). Design, setting, and participants: We interrogated a cohort of 340 Middle Eastern men with localized PCa treated by radical prostatectomy between 2005 and 2015. KLK4::KLKP1 fusion status was assessed by RNA Chromogenic in situ hybridization (CISH) and correlated to pathological and clinical parameters. Outcome measurements and statistical analysis: RNA-CISH expression of KLK4::KLKP1 was correlated with prognostic factors, ERG, PTEN, and SPINK1 expression, and biochemical recurrence (BCR) following prostatectomy. Results and limitations: 51.7% of patient samples showed positive KLK4::KLKP1 expression; more commonly in cores of PCa (38%) versus non-cancer (20.6%) (p < 0.0001) and in lower Gleason Grade Group tumors (1–3) vs (4–5). KLK4::KLKP1 expression positively correlated with ERG positivity and inversely associated with PTEN loss. No significant association was found with SPINK1 expression, seminal vesicle invasion, positive surgical margin, pathological stage, or patient age (< 50 or ≥ 50). The association between PTEN loss and BCR increased when combined with KLK4::KLKP1 negativity (HR 2.31, CI 1.03–5.20, p = 0.042). Conclusions: KLK4::KLKP1 expression is more common in this cohort of Middle Eastern men than has been reported in North American men. It is associated with ERG positivity and inversely correlated with PTEN loss. In isolation, KLK4::KLKP1 expression was not significantly associated with clinical outcome or pathological parameters. However, its expression is associated with certain molecular subtypes (ERG-positive, PTEN-intact) and as we demonstrate may help further stratify the risk of recurrence within these groups. [ABSTRACT FROM AUTHOR]

Published

2023

9. Large, Nested Variant of Urothelial Carcinoma Is Enriched with Activating Mutations in Fibroblast Growth Factor Receptor-3 among Other Targetable Mutations.

Author

Gamallat, Yaser, Afsharpad, Mitra, El Hallani, Soufiane, Maher, Christopher A., Alimohamed, Nimira, Hyndman, Eric, and Bismar, Tarek A.

Subjects

BLADDER tumors, FIBROBLAST growth factors, GENETIC mutation, SEQUENCE analysis, CANCER invasiveness, GENETIC testing, METASTASIS, TREATMENT effectiveness, COMPARATIVE studies, GENOMES, RESEARCH funding, EVALUATION

Abstract

Simple Summary: Urothelial carcinoma of the large, nested variant is a specific histological morphology subtype of urothelial carcinoma. Although it is a rare variant, it requires specific attention due to its bland histology and the fact that it may potentially be missed in routine biopsies. In this study, we identify Fibroblast Growth Factor Receptor-3 (FGFR-3) as the most common mutation present in this subtype among other potential targetable mutations. All our cases of this variant also harbored other potentially actionable mutations in other genes, which could also be amenable to novel targeted therapy. Patients with this variant may benefit from additional molecular screening to identify potential therapeutic targets that could improve the clinical outcome of such patients. The large, nested variant of urothelial carcinoma (LNVUC) is characterized by bland histomorphology mimicking that of benign von Brunn nests. In the current study, we aimed to investigate the Fibroblast Growth Factor Receptor-3 (FGFR-3) activation and missense mutation in 38 cases, including 6 cases diagnosed with LNVUC and 32 with metastatic invasive urothelial carcinoma (UC). Initially, six formalin-fixed paraffin-embedded (FFPE) tissue samples of the LNVUC were subjected to whole-exome sequencing (WES), and then we performed targeted sequencing on 32 cases of metastatic invasive UC of various morphological subtypes, which were interrogated for the FGFR3. Our results revealed 3/6 (50%) LNVUC cases evaluated by WES in our study showed an activating mutation in FGFR-3, 33% showed an activating mutation in PIK3CA, and 17% showed activating mutation in GNAS or MRE11. Additionally, 33% of cases showed a truncating mutation in CDKN1B. All LNVUC in our study that harbored the FGFR-3 mutation showed additional activating or truncating mutations in other genes. Overall, 6/32 (18.75%) cases of random metastatic invasive UC showed missense mutations of the FGFR-3 gene. The LNVUC variant showed the higher incidence of FGFR-3 mutations compared to other types of mutations. Additionally, all LNVUC cases show additional activating or truncating mutations in other genes, thus being amenable to novel targeted therapy. [ABSTRACT FROM AUTHOR]

Published

2023

10. Serrate RNA Effector Molecule (SRRT) Is Associated with Prostate Cancer Progression and Is a Predictor of Poor Prognosis in Lethal Prostate Cancer.

Author

Gamallat, Yaser, Choudhry, Muhammad, Li, Qiaowang, Rokne, Jon George, Alhajj, Reda, Abdelsalam, Ramy, Ghosh, Sunita, Arbet, Jaron, Boutros, Paul C., and Bismar, Tarek A.

Subjects

THERAPEUTIC use of antineoplastic agents, DISEASE progression, ANTIANDROGENS, IMMUNOHISTOCHEMISTRY, RNA, GENE expression, CASTRATION-resistant prostate cancer, GENETIC markers, GENOMICS, CELL proliferation, CHROMOSOME abnormalities, MESSENGER RNA, MEMBRANE proteins, PROSTATE tumors, TUMOR grading, OVERALL survival

Abstract

Simple Summary: This is the first study that has investigate the potential role of the SRRT gene in prostate cancer using clinical samples. We found that high expression of SRRT was significantly associated with poor overall and cause-specific survival. High SRRT expression was also significantly associated with high Gleason score, PSA abundance, pathological T category, and common genomic aberrations in PCa such as PTEN loss, ERG gain, mutant TP53, or ATM. Gene set enrichment analysis suggested that SRRT may play a role in regulating the expression of genes contributing to prostate cancer aggressiveness. Our findings suggest that SRRT could be a prognostic and diagnostic biomarker for lethal PCa, as well as a potential therapeutic target. Arsenite-resistance protein 2, also known as serrate RNA effector molecule (ARS2/SRRT), is known to be involved in cellular proliferation and tumorigenicity. However, its role in prostate cancer (PCa) has not yet been established. We investigated the potential role of SRRT in 496 prostate samples including benign, incidental, advanced, and castrate-resistant patients treated by androgen deprivation therapy (ADT). We also explored the association of SRRT with common genetic aberrations in lethal PCa using immunohistochemistry (IHC) and performed a detailed analysis of SRRT expression using The Cancer Genome Atlas (TCGA PRAD) by utilizing RNA-seq, clinical information (pathological T category and pathological Gleason score). Our findings indicated that high SRRT expression was significantly associated with poor overall survival (OS) and cause-specific survival (CSS). SRRT expression was also significantly associated with common genomic aberrations in lethal PCa such as PTEN loss, ERG gain, mutant TP53, or ATM. Furthermore, TCGA PRAD data revealed that high SRRT mRNA expression was significantly associated with higher Gleason scores, PSA levels, and T pathological categories. Gene set enrichment analysis (GSEA) of RNAseq data from the TCGA PRAD cohort indicated that SRRT may play a potential role in regulating the expression of genes involved in prostate cancer aggressiveness. Conclusion: The current data identify the SRRT's potential role as a prognostic for lethal PCa, and further research is required to investigate its potential as a therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2023

11. Investigation of androgen receptor-dependent alternative splicing has identified a unique subtype of lethal prostate cancer.

Author

Seltzer, Sean, Giannopoulos, Paresa N., Bismar, Tarek A., Trifiro, Mark, and Paliouras, Miltiadis

Abstract

A complete proteomics study characterizing active androgen receptor (AR) complexes in prostate cancer (PCa) cells identified a diversity of protein interactors with tumorigenic annotations, including known RNA splicing factors. Thus, we chose to further investigate the functional role of AR-mediated alternative RNA splicing in PCa disease progression. We selected two AR-interacting RNA splicing factors, Src associated in mitosis of 68 kDa (SAM68) and DEAD (Asp-Glu-Ala-Asp) box helicase 5 (DDX5) to examine their associative roles in AR-dependent alternative RNA splicing. To assess the true physiological role of AR in alternative RNA splicing, we assessed splicing profiles of LNCaP PCa cells using exon microarrays and correlated the results to PCa clinical datasets. As a result, we were able to highlight alternative splicing events of clinical significance. Initial use of exon-mini gene cassettes illustrated hormone-dependent AR-mediated exon-inclusion splicing events with SAM68 or exon-exclusion splicing events with DDX5 overexpression. The physiological significance in PCa was investigated through the application of clinical exon array analysis, where we identified exon-gene sets that were able to delineate aggressive disease progression profiles and predict patient disease-free outcomes independently of pathological clinical criteria. Using a clinical dataset with patients categorized as prostate cancer-specific death (PCSD), these exon gene sets further identified a select group of patients with extremely poor disease-free outcomes. Overall, these results strongly suggest a nonclassical role of AR in mediating robust alternative RNA splicing in PCa. Moreover, AR-mediated alternative spicing contributes to aggressive PCa progression, where we identified a new subtype of lethal PCa defined by AR-dependent alternative splicing. [ABSTRACT FROM AUTHOR]

Published

2023

12. Downregulation of BUD31 Promotes Prostate Cancer Cell Proliferation and Migration via Activation of p-AKT and Vimentin In Vitro.

Author

Choudhry, Muhammad, Gamallat, Yaser, Khosh Kish, Ealia, Seyedi, Sima, Gotto, Geoffrey, Ghosh, Sunita, and Bismar, Tarek A.

Subjects

RNA splicing, CANCER cell proliferation, CANCER cell migration, PROSTATE cancer, VIMENTIN, ANDROGEN receptors

Abstract

Among men, prostate cancer (PCa) is the second most frequently diagnosed cancer subtype and has demonstrated a high degree of prevalence globally. BUD31, also known as Functional Spliceosome-Associated Protein 17, is a protein that works at the level of the spliceosome; it is functionally implicated in pre-mRNA splicing as well as processing, while also acting as a transcriptional regulator of androgen receptor (AR) target genes. Clinically, the expression of BUD31 and its functions in the development and progression of PCa is yet to be elucidated. The BUD31 expression was assessed using IHC in a tissue microarray (TMA) constructed from a cohort of 284 patient samples. In addition, we analyzed the prostate adenocarcinoma (TCGAPRAD-) database. Finally, we used PCa cell lines to knockdown BUD31 to study the underlying mechanisms in vitro.Assesment of BUD31 protein expression revealed lower expression in incidental and advanced PCa, and significantly lower expression was observed in patients diagnosed with castrate-resistant prostate cancer. Additionally, bioinformatic analysis and GSEA revealed that BUD31 increased processes related to cancer cell migration and proliferation. In vitro results made evident that BUD31 knockdown in PC3 cells led to an increase in the G2 cell population, indicating a more active and proliferative state. Additionally, an investigation of metastatic processes revealed that knockdown of BUD31 significantly enhanced the ability of PC3 cells to migrate and invade. Our in vitro results showed BUD31 knockdown promotes cell proliferation and migration of prostate cancer cells via activation of p-AKT and vimentin. These results support the clinical data, where low expression of BUD31 was correlated to more advanced stages of PCa. [ABSTRACT FROM AUTHOR]

Published

2023

13. Glycyl-tRNA Synthetase (GARS) Expression Is Associated with Prostate Cancer Progression and Its Inhibition Decreases Migration, and Invasion In Vitro.

Author

Khosh Kish, Ealia, Gamallat, Yaser, Choudhry, Muhammad, Ghosh, Sunita, Seyedi, Sima, and Bismar, Tarek A.

Subjects

GENE expression, PROSTATE cancer, CANCER invasiveness, ONCOGENES, CELL migration, CELL proliferation

Abstract

Glycyl-tRNA synthetase (GARS) is a potential oncogene associated with poor overall survival in various cancers. However, its role in prostate cancer (PCa) has not been investigated. Protein expression of GARS was investigated in benign, incidental, advanced, and castrate-resistant PCa (CRPC) patient samples. We also investigated the role of GARS in vitro and validated GARS clinical outcomes and its underlying mechanism, utilizing The Cancer Genome Atlas Prostate Adenocarcinoma (TCGA PRAD) database. Our data revealed a significant association between GARS protein expression and Gleason groups. Knockdown of GARS in PC3 cell lines attenuated cell migration and invasion and resulted in early apoptosis signs and cellular arrest in S phase. Bioinformatically, higher GARS expression was observed in TCGA PRAD cohort, and there was significant association with higher Gleason groups, pathological stage, and lymph nodes metastasis. High GARS expression was also significantly correlated with high-risk genomic aberrations such as PTEN, TP53, FXA1, IDH1, SPOP mutations, and ERG, ETV1, and ETV4 gene fusions. Gene Set Enrichment Analysis (GSEA) of GARS through the TCGA PRAD database provided evidence for upregulation of biological processes such as cellular proliferation. Our findings support the oncogenic role of GARS involved in cellular proliferation and poor clinical outcome and provide further evidence for its use as a potential biomarker in PCa. [ABSTRACT FROM AUTHOR]

Published

2023

14. SWI/SNF-deficient lung adenocarcinoma: A case report.

Author

Abbott, Marcia, Hamidi, Mahboobsadat, Bismar, Tarek A., and Zargham, Ramin

Subjects

LUNG cancer diagnosis, ADENOCARCINOMA, LUNG cancer, STAINS & staining (Microscopy), IMMUNOHISTOCHEMISTRY, PROTEIN deficiency, CYTOLOGY, NEEDLE biopsy

Abstract

Copyright of Canadian Journal of Pathology is the property of Canadian Association of Pathologists and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2022

15. The Association between Cyclin Dependent Kinase 2 Associated Protein 1 (CDK2AP1) and Molecular Subtypes of Lethal Prostate Cancer.

Author

Gamallat, Yaser, Bakker, Andrea, Khosh Kish, Ealia, Choudhry, Muhammad, Walker, Simon, Aldakheel, Saood, Seyedi, Sima, Huang, Kuo-Cheng, Ghosh, Sunita, Gotto, Geoffrey, and Bismar, Tarek A.

Subjects

PROSTATE cancer, TRANSURETHRAL prostatectomy, CYCLINS, P53 protein, REGULATOR genes, MOLECULAR interactions, CYCLIN-dependent kinases

Abstract

Prostate cancer (PCa) is one of the most commonly diagnosed types of malignancy and is the second leading cause of cancer-related death in men in developed countries. Cyclin dependent kinase 2 associate protein 1(CDK2AP1) is an epigenetic and cell cycle regulator gene which has been downregulated in several malignancies, but its involvement in PCa has not yet been investigated in a clinical setting. We assessed the prognostic value of CDK2AP1 expression in a cohort of men diagnosed with PCa (n = 275) treated non-surgically by transurethral resection of the prostate (TURP) and studied the relationship between CDK2AP1 expression to various PCa molecular subtypes (ERG, PTEN, p53 and AR) and evaluated the association with clinical outcome. Further, we used bioinformatic tools to analyze the available TCGA PRAD transcriptomic data to explore the underlying mechanism. Our data confirmed increased expression of CDK2AP1 with higher Gleason Grade Group (GG) and metastatic PCa (p <0.0001). High CDK2AP1 expression was associated with worse overall survival (OS) (HR: 1.62, CI: 1.19–2.21, p = 0.002) and cause-specific survival (CSS) (HR: 2.012, CI 1.29–3.13, p = 0.002) using univariate analysis. When compared to each sub-molecular type. High CDK2AP1/PTEN-loss, abnormal AR or p53 expression showed even worse association to poorer OS and CCS and remained significant when adjusted for GG. Our data indicates that CDK2AP1 directly binds to p53 using the Co-Immunoprecipitation (Co-IP) technique, which was validated using molecular docking tools. This suggests that these two proteins have a significant association through several binding features and correlates with our observed clinical data. In conclusion, our results indicated that the CDK2AP1 overexpression is associate with worse OS and CSS when combined with certain PCa molecular subtypes; interaction between p53 stands out as the most prominent candidate which directly interacts with CDK2AP1. [ABSTRACT FROM AUTHOR]

Published

2022

16. The Expression of Proto-Oncogene ETS-Related Gene (ERG) Plays a Central Role in the Oncogenic Mechanism Involved in the Development and Progression of Prostate Cancer.

Author

Khosh Kish, Ealia, Choudhry, Muhammad, Gamallat, Yaser, Buharideen, Sabrina Marsha, D, Dhananjaya, and Bismar, Tarek A.

Subjects

PROSTATE cancer, CANCER invasiveness, GENE fusion, CELL polarity, EPITHELIAL-mesenchymal transition, ANDROGEN receptors, PROSTATE-specific antigen

Abstract

The ETS-related gene (ERG) is proto-oncogene that is classified as a member of the ETS transcription factor family, which has been found to be consistently overexpressed in about half of the patients with clinically significant prostate cancer (PCa). The overexpression of ERG can mostly be attributed to the fusion of the ERG and transmembrane serine protease 2 (TMPRSS2) genes, and this fusion is estimated to represent about 85% of all gene fusions observed in prostate cancer. Clinically, individuals with ERG gene fusion are mostly documented to have advanced tumor stages, increased mortality, and higher rates of metastasis in non-surgical cohorts. In the current review, we elucidate ERG's molecular interaction with downstream genes and the pathways associated with PCa. Studies have documented that ERG plays a central role in PCa progression due to its ability to enhance tumor growth by promoting inflammatory and angiogenic responses. ERG has also been implicated in the epithelial–mesenchymal transition (EMT) in PCa cells, which increases the ability of cancer cells to metastasize. In vivo, research has demonstrated that higher levels of ERG expression are involved with nuclear pleomorphism that prompts hyperplasia and the loss of cell polarity. [ABSTRACT FROM AUTHOR]

Published

2022

17. Patients with Muscle-Invasive Bladder Cancer with Nonluminal Subtype Derive Greatest Benefit from Platinum Based Neoadjuvant Chemotherapy.

Author

Yair Lotan, de Jong, Joep J., Liu, Vinnie Y. T., Bismar, Tarek A., Boorjian, Stephen A., Huei-Chung Huang, Davicioni, Elai, Mian, Omar Y., Wright, Jonathan L., Necchi, Andrea, Dall'Era, Marc A., Kaimakliotis, Hristos Z., Black, Peter C., Gibb, Ewan A., and Boormans, Joost L.

Published

2022

18. Expression of ISL1 and its partners in prostate cancer progression and neuroendocrine differentiation.

Author

Alshalalfa, Mohammed, Abou-Ouf, Hatem, Davicioni, Elai, Karnes, R. Jeffrey, Alhajj, Reda, and Bismar, Tarek A.

Subjects

CANCER invasiveness, PROGNOSIS, CANCER patients, MULTIPLE tumors, PROSTATE cancer, PROSTATE tumors, BIOMARKERS, CANCER cell differentiation

Abstract

Introduction and objectives: ISL1 serves as a biomarker of metastasis and neuroendocrine neoplasia in multiple tumors. However, the expression and relation of ISL1 to other biomarkers in prostate cancer have not been fully elucidated. Here, we characterize the expression of ISL1 and its partners in PCa and document its association to disease progression and post castration resistance neuroendocrine differentiation. Methods: The expression of ISL1 was interrogated in > 6000 primary samples from the Decipher GRID registry and 250 mCRPC samples to assess its prognostic value and relation to neuroendocrine differentiation. Results: ISL1 was highly correlated to MEIS genes and other genes related to cell motility. ISL1 down-regulation in PCa was associated with cancer progression, aggressive primary tumors, and metastatic outcome. We found that ISL1 is highly correlated to MEIS genes across multiple primary PCa and mCRPC cohorts. The expression of ISL1 and MEIS genes were significantly and inversely related to metastasis-free survival and lethal disease, and were downregulated in CRPC and hormone naïve metastatic tumors but showed upregulation in neuroendocrine tumors. Co-immunoprecipitation showed MEIS2 and ISL1 interacting with each supporting their role in modulating transcriptional regulation and nominating this complex for potential targeted therapy. Conclusions: ISL1 complex with MEIS2 serves a critical role in prostate tumor progression and its upregulation in mCRPC/NE provides a rationale for assessing the role of ISL1 and its associated protein in treatment resistance. [ABSTRACT FROM AUTHOR]

Published

2021

19. Molekularpathologie bei urologischen Tumoren: Empfehlungen der Konsenskonferenz der Internationalen Gesellschaft für Uropathologie (ISUP) 2019.

Author

Hommerding, Oliver, Allory, Yves, Argani, Pedram, Bismar, Tarek A., Bubendorf, Lukas, Canete-Portillo, Sofía, Chaux, Alcides, Chen, Ying-Bei, Cheng, Liang, Cubilla, Antonio L., Egevad, Lars, Gill, Anthony J., Grignon, David J., Hartmann, Arndt, Hes, Ondrej, Idrees, Muhammad T., Kao, Chia-Sui, Knowles, Margaret A., Looijenga, Leendert H. J., and Lotan, Tamara L.

Abstract

Copyright of Der Pathologe is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2021

20. Development and Validation of a Genomic Tool to Predict Seminal Vesicle Invasion in Adenocarcinoma of the Prostate.

Author

Hall, William A., Fishbane, Nick, Liu, Yang, Xu, Melody J., Davicioni, Elai, Mahal, Brandon A., Den, Robert B., Dess, Robert T., Jackson, William C., Wong, Anthony C., Schaeffer, Edward M., Karnes, R. Jeffrey, Carroll, Peter R., Cooperberg, Matthew R., Bismar, Tarek A., Kim, Hyung L., Klein, Eric A., Davis, John W., Ross, Ashley E., and Tosoian, Jeffrey J.

Subjects

SEMINAL vesicles, PROSTATE, ADENOCARCINOMA, NOMOGRAPHY (Mathematics), LOGISTIC regression analysis

Abstract

PURPOSE: Pretreatment estimates of seminal vesicle invasion (SVI) are challenging and significantly influence the management of prostate cancer. We sought to improve current models to predict SVI through the development of an SVI prediction genomic signature. PATIENTS AND METHODS: A total of 15,889 patients who underwent radical prostatectomy (RP) with available baseline clinical, pathology, and transcriptome data were retrieved from the GRID registry (ClinicalTrials.gov identifier: NCT02609269) and other retrospective cohorts. These data were divided into a training (n = 6,766), test (n = 3,363), and two validation (n = 5,062 and 698) cohorts. Multivariable logistic regression was performed to assess the predictive effect of the genomic SVI (gSVI) classifier in the presence of established nomograms (Partin Tables and Memorial Sloan Kettering Cancer Center [MSKCC]). RESULTS: In the training cohort, univariable filtering identified 2,132 genes that were differentially expressed between RP tumors with and without SVI. Model parameters were tuned to maximize the area under the curve (AUC) in the testing cohort, resulting in a logistic generalized linear model with 581 genes. The gSVI model scores range from 0 to 1. In the first validation set, gSVI showed superior discrimination of patients with and without SVI at RP compared with other prognostic signatures trained to predict distant metastasis or clinical recurrence. Of the 698 patients in the second validation set, gSVI combined with the MSKCC nomogram had a superior AUC (0.86) compared with either nomogram individually (0.81). CONCLUSION: The gSVI represents a novel and validated expression signature to predict the presence of SVI before treatment with surgery. This genomic tool adds discriminatory power to existing clinical predictive nomograms and may help with pretreatment counseling and decision making. [ABSTRACT FROM AUTHOR]

Published

2020

21. Clonal evaluation of prostate cancer molecular heterogeneity in biopsy samples by dual immunohistochemistry and dual RNA in situ hybridization.

Author

Dedigama-Arachchige, Pavithra, Carskadon, Shannon, Li, Jia, Loveless, Ian, Alhamar, Mohamed, Peabody, James O., Stricker, Hans, Chitale, Dhananjay A., Rogers, Craig G., Menon, Mani, Gupta, Nilesh S., Bismar, Tarek A., Williamson, Sean R., and Palanisamy, Nallasivam

Published

2020

22. Molecular characterization of prostate cancer in Middle Eastern population highlights differences with Western populations with prognostic implication.

Author

Abdelsalam, Ramy A., Khalifeh, Ibrahim, Box, Alan, Kalantarian, Maria, Ghosh, Sunita, Abou-Ouf, Hatem, Lotfi, Tamara, Shahait, Mohammed, Palanisamy, Nallasivam, and Bismar, Tarek A.

Subjects

PTEN protein, SURGICAL site, PROTEIN expression, MULTIVARIATE analysis, GLEASON grading system

Abstract

Background: To investigate the incidence and prognostication of ERG, PTEN and SPINK1 protein expressions in prostate cancer cohort of Middle Eastern descent in comparison to published data from Western population. Methods: Immunohistochemistry for ERG, PTEN and SPINK1 was performed in a cohort of localized PCA (n = 340). The data were correlated to pathological and clinical outcomes and compared to Western populations. Results: ERG expression and PTEN loss were noted in 123/288 (42.7%) and 91/297 (30.6%) of patients, respectively. SPINK1 expression was assessed in a subset of cases, noted in 6/150 (4%) of patients. Only ERG expression was associated with grade groups, being more common in the lower grade groups (1–3 vs 4–5; p = 0.04). In contrast to the Western population, PTEN loss foci were more likely to be ERG negative, observed in 81% of tumor foci and patients with PTEN neg/ERG pos were more likely to exhibit biochemical recurrence (OR 2.831; 95% CI 1.10–726, p = 0.03). This association remained significant in multivariate analysis (OR 2.68; 95% CI 0.98–7.33, p = 0.05), after adjusting for GG, path stage and surgical margin. Conclusion: This study documents significant differences in key molecular events in PCA in Middle Eastern population compared to Western populations that could explain differences in PCA incidence, progression and prognostication. ERG, PTEN and SPINK1 genomic alteration occur less frequently and the enrichment of ERG for PTEN loss is not observed. Additionally, patients with combined PTEN loss/ERG positive are at highest risk for BCR vs North American Caucasian population where PTEN loss alone seems to be associated with the worst clinical outcome. The data presented here further support differences in clonal evolution between Middle Eastern and Western population in relation to PCA and add further insight to understanding PCA molecular pathways. [ABSTRACT FROM AUTHOR]

Published

2020

23. Report From the International Society of Urological Pathology (ISUP) Consultation Conference on Molecular Pathology of Urogenital Cancers. I. Molecular Biomarkers in Prostate Cancer.

Author

Lotan, Tamara L., Tomlins, Scott A., Bismar, Tarek A., Van der Kwast, Theodorus H., Grignon, David, Egevad, Lars, Kristiansen, Glen, Pritchard, Colin C., Rubin, Mark A., and Bubendorf, Lukas

Published

2020

24. DNA methylation signatures of Prostate Cancer in peripheral T-cells.

Author

Mehdi, Ali, Cheishvili, David, Arakelian, Ani, Bismar, Tarek A., Szyf, Moshe, and Rabbani, Shafaat A.

Subjects

DNA methylation, PREMENSTRUAL syndrome, PROSTATE cancer, T cells, GLEASON grading system, BLOOD cells, CIRCULATING tumor DNA

Abstract

Background: Prostate Cancer (PCa) is the second most common cancer in men where advancements have been made for early detection using imaging techniques, however these are limited by lesion size. Immune surveillance has emerged as an effective approach for early detection and to monitor disease progression. In recent studies, we have shown that host peripheral blood immune cells undergo changes in DNA methylation in liver and breast cancer.Methods: In the current study, we examined the DNA methylation status of peripheral blood T cells of men with positive biopsy for PCa versus men with negative biopsy having benign prostate tissue, defined as controls. T cells DNA was isolated and subjected to Illumina Infinium methylation EPIC array and validated using Illumina amplicon sequencing and pyrosequencing platforms.Results: Differential methylation of 449 CG sites between control and PCa T cell DNA showed a correlation with Gleason score (p < 0.05). Two hundred twenty-three differentially methylated CGs between control and PCa (∆ß +/- 10%, p < 0.05), were enriched in pathways involved in immune surveillance system. Three CGs which were found differentially methylated following DMP (Differentially methylated probes) analysis of ChAMP remained significant after BH (Benjamini-Hochberg) correction, of which, 2 CGs were validated. Predictive ability of combination of these 3 CGs (polygenic methylation score, PMS) to detect PCa had high sensitivity, specificity and overall accuracy. PMS also showed strong positive correlation with Gleason score and tumor volume of PCa patients.Conclusions: Results from the current study provide for the first-time a potential role of DNA methylation changes in peripheral T cells in PCa. This non-invasive methodology may allow for early intervention and stratification of patients into different prognostic groups to reduce PCa associated morbidity from repeat invasive prostate biopsies and design therapeutic strategy to reduce PCa associated mortality. [ABSTRACT FROM AUTHOR]

Published

2020

25. Clonal evaluation of early onset prostate cancer by expression profiling of ERG, SPINK1, ETV1, and ETV4 on whole‐mount radical prostatectomy tissue.

Author

Lu, Zhichun, Williamson, Sean R., Carskadon, Shannon, Arachchige, Pavithra D., Dhamdhere, Gaury, Schultz, Daniel S., Stricker, Hans, Peabody, James O., Jeong, Wooju, Chitale, Dhananjay A., Bismar, Tarek A., Rogers, Craig G., Menon, Mani, Gupta, Nilesh S., and Palanisamy, Nallasivam

Published

2020

26. Characterization of transcriptomic signature of primary prostate cancer analogous to prostatic small cell neuroendocrine carcinoma.

Author

Alshalalfa, Mohammed, Liu, Yang, Wyatt, Alexander W., Gibb, Ewan A., Tsai, Harrison K., Erho, Nicholas, Lehrer, Jonathan, Takhar, Mandeep, Ramnarine, Varune R., Collins, Colin C., Den, Robert B., Schaeffer, Edward M., Davicioni, Elai, Lotan, Tamara L., and Bismar, Tarek A.

Subjects

CASTRATION-resistant prostate cancer, SMALL cell carcinoma, PROSTATE cancer, POLY ADP ribose, LUNG cancer, PROSTATE tumors

Abstract

Prostatic small cell neuroendocrine carcinoma (SC/NE) is well studied in metastatic castration‐resistant prostate cancer; however, it is not well characterized in the primary setting. Herein, we used gene expression profiling of SC/NE prostate cancer (PCa) to develop a 212 gene signature to identify treatment‐naïve primary prostatic tumors that are molecularly analogous to SC/NE (SC/NE‐like PCa). The 212 gene signature was tested in several cohorts confirming similar molecular profile between prostatic SC/NE and small cell lung carcinoma. The signature was then translated into a genomic score (SCGScore) using modularized logistic regression modeling and validated in four independent cohorts achieving an average AUC >0.95. The signature was evaluated in more than 25,000 primary adenocarcinomas to characterize the biology, prognosis and potential therapeutic response of predicted SC/NE‐like tumors. Assessing SCGScore in a prospective cohort of 17,967 RP and 6,697 biopsy treatment‐naïve primary tumors from the Decipher Genomic Resource Information Database registry, approximately 1% of the patients were found to have a SC/NE‐like transcriptional profile, whereas 0.5 and 3% of GG1 and GG5 patients respectively showed to be SC/NE‐like. More than 80% of these patients are genomically high‐risk based on Decipher score. Interrogating in vitro drug sensitivity analyses, SC/NE‐like prostatic tumors showed higher response to PARP and HDAC inhibitors. What's new? While genomic/transcriptomic data analysis has revolutionized cancer biology, this analysis is frequently only available late in the cancer history, often after years of therapy. Here the authors built a single sample genomic classifier to predict primary prostate cancer tumors with early small cell neuroendocrine differentiation. They show in three independent cohorts that small cell neuroendocrine tumors of the prostate are similar to small cell tumors of the lung and predict the specific prostate tumors to be responsive to inhibitors of poly ADP ribose polymerase and histone deacetylases, underscoring the use of these drugs in this subtype of prostate cancer. [ABSTRACT FROM AUTHOR]

Published

2019

27. Development of a predictive model for stromal content in prostate cancer samples to improve signature performance.

Author

Boufaied, Nadia, Takhar, Mandeep, Nash, Claire, Erho, Nicholas, Bismar, Tarek A, Davicioni, Elai, and Thomson, Axel A

Subjects

PROSTATE cancer, PREDICTION models, CANCER invasiveness, CELL lines, DECONVOLUTION (Mathematics), DISEASE progression

Abstract

Prostate cancer is heterogeneous in both cellular composition and patient outcome, and development of biomarker signatures to distinguish indolent from aggressive tumours is a high priority. Stroma plays an important role during prostate cancer progression and undergoes histological and transcriptional changes associated with disease. However, identification and validation of stromal markers is limited by a lack of datasets with defined stromal/tumour ratio. We have developed a prostate‐selective signature to estimate the stromal content in cancer samples of mixed cellular composition. We identified stromal‐specific markers from transcriptomic datasets of developmental prostate mesenchyme and prostate cancer stroma. These were experimentally validated in cell lines, datasets of known stromal content, and by immunohistochemistry in tissue samples to verify stromal‐specific expression. Linear models based upon six transcripts were able to infer the stromal content and estimate stromal composition in mixed tissues. The best model had a coefficient of determination R2 of 0.67. Application of our stromal content estimation model in various prostate cancer datasets led to improved performance of stromal predictive signatures for disease progression and metastasis. The stromal content of prostate tumours varies considerably; consequently, deconvolution of stromal proportion may yield better results than tumour cell deconvolution. We suggest that adjusting expression data for cell composition will improve stromal signature performance and lead to better prognosis and stratification of men with prostate cancer. © 2019 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland. [ABSTRACT FROM AUTHOR]

Published

2019

28. Combined loss of TFF3 and PTEN is associated with lethal outcome and overall survival in men with prostate cancer.

Author

Abou-Ouf, Hatem, Ghosh, Sunita, Box, Adrian, Palanisamy, Nallasivam, and Bismar, Tarek A.

Subjects

FLUORESCENCE in situ hybridization, PROSTATE cancer, CANCER in men, GLEASON grading system, TRANSURETHRAL prostatectomy, TREFOIL factors

Abstract

Background: Trefoil Factor 3 (TFF3) has been implicated in Prostate Cancer (PCa) progression. However, its prognostic value and association with other biomarkers have not been fully explored. We assessed the combined value of TFF3 and PTEN in two cohorts: one is managed surgically for localized PCa and the second is managed non-surgically by androgen deprivation therapy for advanced disease. Design: 228 radical prostatectomies (RP) and 318 transurethral resection of prostate (TURP) samples were assessed by immunohistochemistry (IHC) for TFF3 and by IHC and fluorescent in situ hybridization (FISH) for PTEN. Results of biomarkers expression were correlated with various pathological and clinical outcome parameters including biochemical recurrence (BCR) in the RP cohort and cancer-specific mortality (PCSM) and overall survival (OS) in the TURP cohort. Results: TFF3 expression was detected in 131/226 (57.9%) RP samples and 148/318 (46.5%) of TURP cases. In general, TFF3 positivity was less frequently observed with advanced Gleason Groups. TFF3 expression was also assessed in relation to PTEN expression. Only 15–16% of TFF3-expressed cases were present in association with complete loss of PTEN expression in the TURP and localized cohorts, respectively. Loss of TFF3 expression was not related to BCR after RP, but was prognostic in the non-surgical cohort and associated with decrease OS and PCSM (HR 2.31, CI: 1.67–3.18, p < 0.0001) and (HR 3.99, CI: 2.43–6.56; p < 0.0001), respectively. Adjusting for Gleason score, combined loss of TFF3/PTEN was most associated with OS (HR 2.33, CI: 1.49–3.62; p < 0.0001) and PCSM (HR = 3.44, CI: 1.75–6.78, p < 0.0001). Conclusion: The study documents for the first time significant association for combined status of TFF3 expression and PTEN loss in OS and PCSM in patients not managed by surgical intervention. Prospective assessment of PTEN and TFF3 may provide further insight into molecularly subtyping PCa and aid in stratifying patients at risk for lethal disease. [ABSTRACT FROM AUTHOR]

Published

2019

29. Genomic Characterization of Prostatic Ductal Adenocarcinoma Identifies a High Prevalence of DNA Repair Gene Mutations.

Author

Schweizer, Michael T., Antonarakis, Emmanuel S., Bismar, Tarek A., Guedes, Liana B., Cheng, Heather H., Tretiakova, Maria S., Vakar-Lopez, Funda, Klemfuss, Nola, Konnick, Eric Q., Mostaghel, Elahe A., Hsieh, Andrew C., Nelson, Peter S., Yu, Evan Y., Montgomery, R. Bruce, True, Lawrence D., Epstein, Jonathan I., Lotan, Tamara L., and Pritchard, Colin C.

Subjects

DNA repair, DNA damage, ADENOCARCINOMA, GENES, PROSTATE cancer

Abstract

PURPOSE: Ductal prostate cancer (dPC) is a rare variant of prostatic adenocarcinoma associated with poor outcomes. Although its histopathologic features are well characterized, the underlying molecular hallmarks of this aggressive subtype are not well described. We sought to provide a comprehensive overview of the spectrum of mutations associated with dPC. METHODS: Three case series across multiple institutions were assembled. All patients had a diagnosis of dPC, and histopathologic classification was confirmed by an expert genitourinary pathologist. Case series 1 included men who were prospectively enrolled in a tumor sequencing study at the University of Washington (n = 22). Case series 2 and 3 included archival samples from men treated at Johns Hopkins Hospital (n = 21) and University of Calgary (n = 8), respectively. Tumor tissue was sequenced on a targeted next-generation sequencing assay, UW-OncoPlex, according to previously published methods. The frequency of pathogenic/likely pathogenic mutations are reported. RESULTS: Overall, 25 patients (49%) had at least one DNA damage repair gene alteration, including seven (14%) with a mismatch repair gene mutation and 16 (31%) with a homologous repair mutation. Germline autosomal dominant mutations were confirmed or suspected in 10 patients (20%). Activating mutations in the PI3K pathway (n = 19; 37%), WNT pathway (n = 16; 31%), and MAPK pathway (n = 8; 16%) were common. CONCLUSION: This study strongly suggests that dPCs are enriched for actionable mutations, with approximately 50% of patients demonstrating DNA damage repair pathway alteration(s). Patients with dPC should be offered next-generation sequencing to guide standard-of-care treatment (eg, immune checkpoint inhibitors) or triaged toward an appropriate clinical trial (eg, poly [ADP-ribose] polymerase inhibitors). [ABSTRACT FROM AUTHOR]

Published

2019

30. Expression of IGF/insulin receptor in prostate cancer tissue and progression to lethal disease.

Author

Ahearn, Thomas U, Peisch, Sam, Pettersson, Andreas, Ebot, Ericka M, Zhou, Cindy Ke, Graff, Rebecca E, Sinnott, Jennifer A, Fazli, Ladan, Judson, Gregory L, Bismar, Tarek A, Rider, Jennifer R, Gerke, Travis, Chan, June M, Fiorentino, Michelangelo, Flavin, Richard, Sesso, Howard D, Finn, Stephen, Giovannucci, Edward L, Gleave, Martin, and Loda, Massimo

Subjects

PROSTATE cancer, INSULIN receptors, PROSTATE, CANCER invasiveness

Abstract

Circulating insulin-like growth factor-1 (IGF-1) is consistently associated with prostate cancer risk. IGF-1 binds to IGF-1 receptor (IGF1R) and insulin receptor (IR), activating cancer hallmark pathways. Experimental evidence suggests that TMPRSS2:ERG may interact with IGF/insulin signaling to influence progression. We investigated IGF1R and IR expression and its association with lethal prostate cancer among 769 men. Protein expression of IGF1R, IR and ERG (i.e. a surrogate of ERG fusion genes) were assayed by immunohistochemistry. Cox models estimated hazard ratios (HR) and 95% confidence intervals (CI) adjusted for clinical characteristics. Among patients, 29% had strong tumor IGF1R expression and 10% had strong IR expression. During a mean follow-up of 13.2 years through 2012, 80 men (11%) developed lethal disease. Tumors with strong IGF1R or IR expression showed increased cell proliferation, decreased apoptosis and a higher prevalence of ERG. In multivariable models, strong IGF1R was associated with a borderline increased risk of lethal prostate cancer (HR 1.7; 95% CI 0.9–3.1). The association appeared greater in ERG-positive tumors (HR 2.8; 95% CI 0.9–8.4) than in ERG-negative tumors (HR 1.3; 95% CI 0.6–3.0, p-heterogeneity 0.08). There was no association between IR and lethal prostate cancer (HR 0.8; 95% CI 0.4–1.9). These results suggest that tumor IGF1R expression may play a role in prostate cancer progression to a lethal phenotype and that ERG-positive tumors may be more sensitive to IGF signaling. These data may improve our understanding of IGF signaling in prostate cancer and suggest therapeutic options for disease subtypes. [ABSTRACT FROM AUTHOR]

Published

2018

31. Clinical utility of assessing PTEN and ERG protein expression in prostate cancer patients: a proposed method for risk stratification.

Author

Bismar, Tarek A., Hegazy, Samar, Feng, Zhaoyong, Yu, Darryl, Donnelly, Bryan, Palanisamy, Nallasivam, and Trock, Bruce J.

Subjects

PTEN protein, PROTEIN expression, IMMUNOHISTOCHEMISTRY, GLEASON grading system, CANCER-related mortality

Abstract

Objectives: To assess the prognostic value of ERG and PTEN protein expression as two of the most common genetic aberration in men with prostate cancer managed non-surgically by androgen deprivation therapy (ADT).Materials and methods: 463 tumor samples were assessed by double immunohistochemistry stains for ERG and PTEN and data correlated with clinical pathological features including, Gleason score, patients’ outcome and ADT.Results: ERG expression and PTEN protein loss were present in 28.2% and 38% of total patients respectively. There was a significant interplay between ERG and PTEN expression with 21.8% PTEN negative tumors being ERG positive (p < 0.001). Both ERG and PTEN showed significant association with lethal disease in all patients and those treated with prior ADT representing castrate-resistant disease. However, only PTEN remained significant in multivariable proportional hazards regression analysis, when including Gleason score and patients’ age. Depending on patient’s subgroup, intact positive PTEN intensity showed better cancer-specific survival with HR ranging from 0.25 to 0.4 compared to tumors with loss of PTEN expression. Assessing combined marker status, patients with decreased PTEN intensity without ERG positivity showed the worst clinical outcome compared to those with no PTEN loss and no ERG expression, where they had best clinical outcome. Patients with ERG expression with or without PTEN loss showed intermediate risk in relation to lethal disease.Conclusion: This study confirms a significant prognostic role for assessing ERG and PTEN in men with prostate cancer. It supports a role for utilizing combined ERG/PTEN status clinically and prospectively for stratifying PCa patients into different prognostic groups. [ABSTRACT FROM AUTHOR]

Published

2018

32. Quantitative in vivo whole genome motility screen reveals novel therapeutic targets to block cancer metastasis.

Author

Stoletov, Konstantin, Willetts, Lian, Paproski, Robert J., Bond, David J., Raha, Srijan, Jovel, Juan, Adam, Benjamin, Robertson, Amy E., Wong, Francis, Woolner, Emma, Sosnowski, Deborah L., Bismar, Tarek A., Wong, Gane Ka-Shu, Zijlstra, Andries, and Lewis, John D.

Subjects

CANCER cell motility, METASTASIS, CELL motility, GENE targeting, CANCER cells, CHICKEN embryos

Abstract

Metastasis is the most lethal aspect of cancer, yet current therapeutic strategies do not target its key rate-limiting steps. We have previously shown that the entry of cancer cells into the blood stream, or intravasation, is highly dependent upon in vivo cancer cell motility, making it an attractive therapeutic target. To systemically identify genes required for tumor cell motility in an in vivo tumor microenvironment, we established a novel quantitative in vivo screening platform based on intravital imaging of human cancer metastasis in ex ovo avian embryos. Utilizing this platform to screen a genome-wide shRNA library, we identified a panel of novel genes whose function is required for productive cancer cell motility in vivo, and whose expression is closely associated with metastatic risk in human cancers. The RNAi-mediated inhibition of these gene targets resulted in a nearly total (>99.5%) block of spontaneous cancer metastasis in vivo. [ABSTRACT FROM AUTHOR]

Published

2018

33. Validation of a 10-gene molecular signature for predicting biochemical recurrence and clinical metastasis in localized prostate cancer.

Author

Abou-Ouf, Hatem, Alshalalfa, Mohammed, Takhar, Mandeep, Erho, Nicholas, Donnelly, Bryan, Davicioni, Elai, Karnes, R. Jeffrey, and Bismar, Tarek A.

Subjects

PROSTATE cancer & genetics, CANCER relapse, PROSTATECTOMY, GLEASON grading system, HEALTH outcome assessment, CANCER risk factors

Abstract

Purpose: To validate a previously characterized 10-gene signature in prostate cancer with implication to distinguish aggressive and indolent disease within low and intermediate patients’ risk groups.Methods: A case-control study design used to select 545 patients from the Mayo clinic tumor registry who underwent radical prostatectomy. A training set from this cohort (n = 359) was used to build a 10-gene model, based on high-dimensional discriminant analysis (HDDA10) to predict several endpoints of clinical patients’ outcome. An independent set (n = 219) from the same institution was used as validation set.Results: HDDA10 showed significant performance for predicting metastasis (Mets) (AUC 0.68, p = 6.4E - 6) and biochemical recurrence (BCR) (AUC = 0.65, p = 0.003) in the validation set outperforming Gleason grade grouping (GG) for BCR (AUC 0.57, p = 0.03) and with comparable performance for Mets endpoint (GG AUC 0.66, p = 8.1E - 5). HDDA10 prognostic significance was superior to any clinical-pathological parameter within GG2 + 3 (GS7) patients achieving an AUC of 0.74 (p = 0.0037) for BCR compared to Gleason pattern 4 (AUC 0.64) (p = 0.015) and AUC for Mets of 0.68 versus AUC of 0.65 for Gleason pattern 4 (p = 0.01). HDDA10 remained significant for both BCR and Mets in multivariate analysis, suggesting that it can be used to increase accuracy in stratifying patients eligible for active surveillance.Conclusion: HDDA10 is of added value to GG and other clinical-pathological parameters in predicting BCR and Mets endpoint, especially in the low to intermediate patients’ risk groups. HDDA10 prognostic value should be further validated prospectively in stratifying patients specifically in low to intermediate GS (GG1-2), such as active surveillance programs. [ABSTRACT FROM AUTHOR]

Published

2018

34. ING3 promotes prostate cancer growth by activating the androgen receptor.

Author

Nabbi, Arash, McClurg, Urszula L., Thalappilly, Subhash, Almami, Amal, Mobahat, Mahsa, Bismar, Tarek A., Binda, Olivier, and Riabowol, Karl T.

Subjects

ANDROGEN receptors, PROSTATE cancer, PROGNOSIS, ONCOGENES, LYSINE

Abstract

Background: The androgen receptor (AR) is a major driver of prostate cancer, and increased AR levels and co-activators of the receptor promote the development of prostate cancer. INhibitor of Growth (ING) proteins target lysine acetyltransferase or lysine deacetylase complexes to the histone H3K4Me3 mark of active transcription, to affect chromatin structure and gene expression. ING3 is a stoichiometric member of the TIP60 lysine acetyltransferase complex implicated in prostate cancer development.Methods: Biopsies of 265 patients with prostate cancer were stained for ING3, pan-cytokeratin, and DNA. LNCaP and C4-2 androgen-responsive cells were used for in vitro assays including immunoprecipitation, western blotting, Luciferase reporter assay and quantitative polymerase chain reaction. Cell viability and migration assays were performed in prostate cancer cell lines using scrambled siRNA or siRNA targeting ING3.Results: We find that ING3 levels and AR activity positively correlate in prostate cancer. ING3 potentiates androgen effects, increasing expression of androgen-regulated genes and androgen response element-driven reporters to promote growth and anchorage-independent growth. Conversely, ING3 knockdown inhibits prostate cancer cell growth and invasion. ING3 activates the AR by serving as a scaffold to increase interaction between TIP60 and the AR in the cytoplasm, enhancing receptor acetylation and translocation to the nucleus. Activation is independent of ING3's ability to target the TIP60 complex to H3K4Me3, identifying a previously unknown chromatin-independent cytoplasmic activity for ING3. In agreement with in vitro observations, analysis of The Cancer Genome Atlas (TCGA) data (n = 498) and a prostate cancer tissue microarray (n = 256) show that ING3 levels are higher in aggressive prostate cancers, with high levels of ING3 predicting shorter patient survival in a low AR subgroup. Including ING3 levels with currently used indicators such as the Gleason score provides more accurate prognosis in primary prostate cancer.Conclusions: In contrast to the majority of previous reports suggesting tumor suppressive functions in other cancers, our observations identify a clear oncogenic role for ING3, which acts as a co-activator of AR in prostate cancer. Data from TCGA and our previous and current tissue microarrays suggest that ING3 levels correlate with AR levels and that in patients with low levels of the receptor, ING3 level could serve as a useful prognostic biomarker. [ABSTRACT FROM AUTHOR]

Published

2017

35. Ankyrin G expression is associated with androgen receptor stability, invasiveness, and lethal outcome in prostate cancer patients.

Author

Wang, Tingting, Abou-Ouf, Hatem, Hegazy, Samar, Alshalalfa, Mohammed, Stoletov, Konstantin, Lewis, John, Donnelly, Bryan, and Bismar, Tarek

Subjects

PROSTATE cancer patients, CANCER invasiveness, ANKYRINS, PROTEIN expression, ANDROGEN receptors, CANCER cell physiology

Abstract

Ankyrin G (ANK3) is a member of the Ankyrin family, which functions to provide cellular stability by anchoring the cytoskeleton to the plasma membrane. Deregulation of ANK3 expression has been observed in multiple human cancers but its mechanism remains unknown. ANK3 expression in relation to disease progression and patients' outcome was investigated in two cohorts of prostate cancer (PCA). Mechanistic studies were carried out in vitro and in vivo using several PCA cell lines and the avian embryo model. Silencing ANK3 resulted in significant reduction of cell proliferation through an AR-independent mechanism. Decreased ANK3 expression delayed S phase to G2/M cell cycle transition and reduced the expression of cyclins A and B. However, cells with knocked-down ANK3 exhibited significant increase in cell invasion through an AR-dependent mechanism. Furthermore, we found that ANK3 is a regulator of AR protein stability. ANK3 knockdown also promoted cancer cell invasion and extravasations in vivo using the avian embryo model ( p < 0.01). In human samples, ANK3 expression was dramatically upregulated in high grade intraepithelial neoplasia (HGPIN) and localized PCA ( p < 0.0001). However, it was downregulated castration resistant stage ( p < 0.0001) and showed inverse relation to Gleason score ( p < 0.0001). In addition, increased expression of ANK3 in cancer tissues was correlated with better cancer-specific survival of PCA patients ( p = 0.012). Key message: [ABSTRACT FROM AUTHOR]

Published

2016

36. High alpha-methylacyl-CoA racemase (AMACR) is associated with ERG expression and with adverse clinical outcome in patients with localized prostate cancer.

Author

Box, Adrian, Alshalalfa, Mohammed, Hegazy, Samar, Donnelly, Bryan, and Bismar, Tarek

Abstract

Alpha-methylacyl-CoA racemase (AMACR) is a well-characterized marker extensively utilized in prostate cancer (PCA) diagnosis. However, the prognostic value of AMACR expression and its relation to TMPRSS2-ERG gene rearrangement as one of the most common molecular alterations in PCA is not fully explored. AMACR expression was investigated in a cohort of 218 men with localized PCA treated by radical prostatectomy and correlated with ERG and various clinical and pathological parameters. In vitro studies assessed AMACR changes to ERG knockdown and other related genes. In addition, bioinformatics validated the significance of AMACR/ERG expression and assessed relevant genetic signatures in relation to AMACR/ERG expression. AMACR expression was significantly associated with disease progression and with ERG ( p ∼0). Seventeen percent of cancer foci showed negative/weak AMACR expression while being ERG positive. High AMACR expression was significantly associated with positive surgical margins ( p = 0.01), specifically in tumors with lower Gleason score <7, with ∼95 % exhibiting positive surgical margin ( p = 0.008). High AMACR showed marginal association with PSA biochemical recurrence (BCR) ( p = 0.06) which was slightly more pronounced in ERG-positive tumors ( p = 0.04). This was validated in other public cohorts. However, in this cohort, the association with BCR was not statistically significant in multivariate analysis ( p = 0.09). Using in vitro cellular models, AMACR messenger RNA (mRNA) expression, but not protein levels, showed an association with ERG expression. We report for the first time a significant association between AMACR and ERG with prognostic implication. Patients with high AMACR/ERG-positive PCA may be at higher risk for disease progression, and additional studies in larger cohorts are needed to confirm the above findings. Functional studies investigating the molecular pathways connecting AMACR and ERG may provide an additional insight into PCA progression pathways. [ABSTRACT FROM AUTHOR]

Published

2016

37. ERG expression in prostate cancer: biological relevance and clinical implication.

Author

Abou-Ouf, Hatem, Zhao, Liena, and Bismar, Tarek

Subjects

PROSTATE cancer patients, PROSTATE cancer, DIAGNOSIS, PROSTATE cancer treatment, PROSTATE-specific antigen, PROSTATE cancer prognosis

Abstract

Introduction: Screening for increased levels of prostate-specific antigen (PSA) has allowed early detection of a large majority of prostate cancer (PCa) cases. However, the relative lack of specificity of PSA has resulted in significant over-diagnosis and unnecessary treatment for indolent tumors. The fusion of the transmembrane protease serine 2 with E26 transformation-specific family genes, particularly ERG, is the most widespread genetic alteration in prostate cancer, and data suggest that it is more specific for neoplastic prostate disease and may be of added prognostic value and point toward molecular subtype of PCa. Methods: In this review, retrospective studies and clinical trials were analyzed to highlight the recent advances in our understanding of the cellular consequence of ERG rearrangement, describe its interactions with other genetic and molecular pathways, and discuss its potential diagnostic and prognostic value. Conclusion: ERG over-expression has an emerging role in the diagnosis of PCa pathology, although there is still debate about its prognostic value. Elucidation of the mechanisms of ERG gene rearrangements and expression promises novel therapeutic and diagnostic avenues for prostate cancer. [ABSTRACT FROM AUTHOR]

Published

2016

38. ING3 is associated with increased cell invasion and lethal outcome in ERG-negative prostate cancer patients.

Author

Almami, Amal, Hegazy, Samar, Nabbi, Arash, Alshalalfa, Mohammed, Salman, Asma, Abou-Ouf, Hatem, Riabowol, Karl, and Bismar, Tarek

Abstract

The inhibitor of growth family member 3 (ING3) is a member of the ING tumor suppressor family. Although its expression has been reported in various types of cancers, the role of ING3 and its prognostic value in prostate cancer (PCa) has not been investigated. ING3 expression and prognostic value was assessed in a cohort of PCa patients ( n = 312) treated with transurethral resection of prostate using immumoflourescent automated quantitative analysis (AQUA) system. In vitro studies were carried out in conjunction to investigate its expression in various PCa cell lines. ING3 knockdown was also carried out in DU145 cell lines to assess for any changes in invasion and migration. ING3 expression was highest in benign prostate tissues (mean 3.2 ± 0.54) compared to PCa (mean 2.5 ± 0.26) ( p = 0.437), advanced prostate cancer (AdvPCa) (mean 1.5 ± 0.32) ( p = 0.004), and castration-resistant prostate cancer (CRPC) (mean 2.28 ± 0.32) ( p = 0.285). ING3 expression was inversely correlated to Gleason score ( p = 0.039) and ETS-related gene (ERG) expression ( p = 0.019). Higher ING3 expression was marginally associated with lethal disease ( p = 0.052), and this was more pronounced in patients with ERG-negative status ( p = 0.018). Inhibition of ING3 in DU145 PCa cells using small interfering RNA (siRNA) was associated with decreased cell invasion ( p = 0.0016) and cell migration compared to control cells. ING3 is significantly associated with PCa disease progression and cancer-specific mortality. To our knowledge, this is the first report suggesting an oncogenic function of ING3, previously well known as a tumor suppressor protein. Further studies should investigate potential-related pathways in association to ING3. [ABSTRACT FROM AUTHOR]

Published

2016

39. microRNA 338-3p exhibits tumor suppressor role and its down-regulation is associated with adverse clinical outcome in prostate cancer patients.

Author

Bakkar, Ashraf, Alshalalfa, Mohammed, Petersen, Lars, Abou-Ouf, Hatem, Al-Mami, Amal, Hegazy, Samar, Feng, Felix, Alhajj, Reda, Bijian, Krikor, Alaoui-Jamali, Moulay, and Bismar, Tarek

Abstract

MicroRNAs (miRNAs) are small non-coding RNAs that function in transcriptional and post-transcriptional regulation of gene expression. Several miRNAs have been implicated in regulating prostate cancer (PCa) progression. Deregulations of miRNA regulatory networks have been reported in ERG positive PCa, which accounts for ~50 % of PCa and have been suggested to affect tumor aggressiveness. The function of miR338-3p, its prognostic significance, and its association with ERG positive PCa has not been fully investigated. Using microarray expression profiling, we identified miRNA338-3p as among the top deregulated miRNAs associated with ERG status in PCa. We investigated miR338-3p function using in vitro and in vivo experimental models and its expression was assessed and validated in clinical samples and a public cohort of localized and metastatic prostate cancer. miR338-3p was significantly down-regulated with disease progression from benign prostate tissue to primary and metastatic lesions. In localized disease, patients with lower miR338-3p expression levels showed increased association to biochemical recurrence and several adverse pathological parameters compared to patients with higher miRNA338-3p tissue expression levels. Using in vitro PCa cell models, overexpression of miR338-3p resulted in a decrease in cell invasion and expression of chemokine signalling genes CXCL12, CXCR4, and CXCR7. In vivo, orthotropic implantation of PC3 cells stably expressing miR338-3p was associated with a significant decrease in tumor weights compared to control cells. miR338-3p has anti-proliferative and anti-invasive properties. It affects CXCR4 axis, and its down-regulation is associated with adverse clinical outcomes in PCa patients. [ABSTRACT FROM AUTHOR]

Published

2016

40. Functional characterization of miRNAs in prostate cancer using functional protein networks.

Author

Alshalalfa, Mohammed, Qabaja, Ala, Bismar, Tarek A., and Alhajj, Reda

Abstract

The cell is a highly organized system of interacting molecules including DNA, proteins, mRNAs and miRNAs. Analyzing the cell from a systems perspective by integrating different types of data helps reveal the complexity behind the biological process. Although there is emerging evidence that some microRNAs can function as oncogenes or tumour suppressors, the role of microRNAs in mediating cancer progression and metastasis remains not fully explored. In this work we integrate functional protein networks to characterize the downstream effect of miRNA-mRNA interaction. The proposed method infers a novel miRNA-mRNA regulatory network, not only based on the correlation between miRNA and their targets, but also by taking into account the down stream effects of miRNA-mRNA interaction on interacting proteins. In here we build a model that integrates mRNA and miRNA expression data, a predicted miRNA-mRNA regulatory network (based on sequence complementary) and functional protein interaction data to better characterize the functional role of individual miRNAs. The network is used to predict the effect of miRNA on cancer progression. The model is then applied to two prostate cancer datasets that include normal, primary and metastatic cancer samples to identify prognostic miRNAs that are associated with cancer progression. Network based model demonstrated promising to predict cancer recurrence and death. Furthermore, the model is used to predict miRNA that have similar mode of action to drugs. Results revealed that the proposed method identify miRNA-mRNA modules that play a key role in prostate cancer progression and they are promising targets as prognostic biomarkers. [ABSTRACT FROM PUBLISHER]

Published

2012

41. The prognostic significance of combined ERG and androgen receptor expression in patients with prostate cancer managed by androgen deprivation therapy.

Author

Kuo-Cheng Huang, Alshalalfa, Mohammed, Hegazy, Samar A., Dolph, Michael, Donnelly, Bryan, and Bismar, Tarek A.

Published

2014

42. Cysteine- Rich Secretory Protein 3 (CRISP3), ERG and PTEN define a molecular subtype of prostate cancer with implication to patients' prognosis.

Author

Al Bashir, Samir, Alshalalfa, Mohammed, Hegazy, Samar A., Dolph, Michael, Donnelly, Bryan, and Bismar, Tarek A.

Subjects

CYSTEINE, BIOMOLECULES, PROSTATE cancer, PROTEINS, ORGANIC compounds, IMMUNOHISTOCHEMISTRY, MESSENGER RNA

Abstract

Cysteine- rich secretory protein 3 (CRISP3) prognostic significance in prostate cancer (PCA) has generated mixed result. Herein, we investigated and independently validated CRISP3 expression in relation to ERG and PTEN genomic aberrations and clinical outcome. CRISP3 protein expression was examined by immunohistochemistry using a cohort of patients with localized PCA (n = 215) and castration resistant PCA (CRPC) (n = 46). The Memorial Sloan Kettering (MSKCC) and Swedish cohorts were used for prognostic validation. Results showed, CRISP3 protein intensity to be significantly associated with neoplastic epithelium, being highest in CRPC vs. benign prostate tissue (p < 0.0001), but was not related to Gleason score (GS). CRISP3 mRNA was significantly associated with higher GS (p = 0.022 in MSKCC, p = 1.1e-4 in Swedish). Significant association between CRISP3 expression and clinical outcome was documented at the mRNA but not the protein expression levels. CRISP3 mRNA expression was related to biochemical recurrence in the MSKCC (p = 0.038) and lethal disease in the Swedish cohort (p = 0.0086) and retained its prognostic value in the subgroup of patients with GS 6 & 7. Furthermore, CRISP3 protein and mRNA expression was significantly associated with positive ERG status and with PTEN deletions. Functional biology analysis documented phenylalanine metabolism as the most significant pathway governing high CRISP3 and ERG expression in this subtype of PCA. In conclusion, the combined status of CRISP3, ERG and PTEN define a molecular subtype of PCA with poorest and lethal outcome. Assessing their combined value may be of added value in stratifying patients into different prognostic groups and identify those with poorest clinical outcome. [ABSTRACT FROM AUTHOR]

Published

2014

43. Interrogation of ERG gene rearrangements in prostate cancer identifies a prognostic 10-gene signature with relevant implication to patients' clinical outcome.

Author

Bismar, Tarek A., Alshalalfa, Mohammed, Petersen, Lars F., Teng, Liang Hong, Gerke, Travis, Bakkar, Ashraf, Al‐Mami, Amal, Liu, Shuhong, Dolph, Michael, Mucci, Lorelei A., and Alhajj, Reda

Subjects

PROGNOSTIC tests, PROSTATE cancer patients, SINGULAR value decomposition, CONFIDENCE intervals, BIOINFORMATICS

Abstract

Objectives • ERG-gene rearrangement defines a distinct molecular subtype of PCA with potential biological and clinical implications. • To identify a molecular signature reflective of the downstream effects of ERG-mediated transcriptional regulation with prognostic implication in patients with prostate cancer (PCA). Material and Methods • We used a singular value decomposition (SVD) bioinformatics approach to re-analyse gene expression data previously generated from 46 prostate tumours, and identified an ERG-like gene signature. • The signature was validated on several patient cohorts and individual genes were correlated to ERG expression and PCA progression. Results • An ERG-like 10-gene signature was identified and validated in PCA cohorts of the physician health study (p115) (n = 110) in addition to three independent public datasets, and was significantly associated with disease progression, biochemical recurrence and PCA-specific mortality. • Patients with the ERG-like signature were significantly associated with disease recurrence on univariate (hazard ratio [HR] 2.6; 95% confidence interval [CI]:1.3-5.2; P = 0.004) and multivariate analysis (HR 2.3; 95% CI:1.1-4.6, P = 0.016) compared with patients without this signature. • Within the group of patients with Gleason score (GS) 6 and 7 PCA, the signature added prognostic value beyond GS and identified patients at higher risk of cancer deaths more accurately than GS alone or in combination with ERG status. • Protein expression of the 10 genes were significantly associated with ERG and disease progression regardless of ERG status. Conclusion • The characterized ERG-like signature was reflective of aggressive features of ERG-mediated transcription and was prognostically robust. • The combination of this signature with clinicopathological variables should be validated prospectively to explore its clinical utility in stratifying patients with PCA and in identifying those at higher risk of metastatic and lethal disease. [ABSTRACT FROM AUTHOR]

Published

2014

44. Coordinate MicroRNA-Mediated Regulation of Protein Complexes in Prostate Cancer.

Author

Alshalalfa, Mohammed, D. Bader, Gary, Bismar, Tarek A., and Alhajj, Reda

Subjects

MICRORNA, GENETIC regulation, PROSTATE cancer, PROTEIN analysis, GENE targeting, ENTROPY, GENE expression, RAS oncogenes

Abstract

MicroRNAs are a class of small non-coding regulatory RNA molecules that regulate mRNAs post-transcriptionally. Recent evidence has shown that miRNAs target entire functionally related proteins such as protein complexes and biological pathways. However, characterizing the influence of miRNAs on genes whose encoded proteins are part of protein complexes has not been studied in the context of disease. We propose an entropy-based framework to identify miRNA-mediated dysregulation of functionally related proteins during prostate cancer progression. The proposed framework uses experimentally verified miRNA-target interactions, functionally related proteins and expression data to identify miRNA-influenced protein complexes in prostate cancer, and identify genes that are dysregulated as a result. The framework constructs correlation matrixes between functionally related proteins and miRNAs that have targets in the complex, and assesses the changes in the Shannon entropy of the modules across different stages of prostate cancer. Results reveal that SMAD4 and HDAC containing protein complexes are highly affected and disrupted by miRNAs, particularly miRNA-1 and miRNA-16. Using biological pathways to define functionally related proteins reveals that NF-kB-, RAS-, and Syndecan-mediated pathways are dysregulated due to miRNA-1- and miRNA-16-mediated regulation. These results suggest that miRNA-1 and miRNA-16 are important master regulators of miRNA-mediated regulation in prostate cancer. Moreover, results reveal that miRNAs with high-influence on the disrupted protein complexes are diagnostic and prognostic biomarker candidates for prostate cancer progression. The observation of miRNA-mediated protein complex regulation and miRNA-mediated pathway regulation, with partial experimental verification from previous studies, demonstrates that our framework is a promising approach for the identification of novel miRNAs and protein complexes related to disease progression. [ABSTRACT FROM AUTHOR]

Published

2013

45. ERG Protein Expression Is of Limited Prognostic Value in Men with Localized Prostate Cancer.

Author

Liang Hong Teng, Cheng Wang, Dolph, Michael, Donnelly, Bryan, and Bismar, Tarek A.

Abstract

Background. The prognostic significance of ERG expression in prostate cancer (PCA) has generated mixed results. We sought to investigate the prognostic significance of ERG expression in a localized cohort of men with PCA. Material and Methods. We investigated ERG protein expression in a cohort of 198 men with localized PCA. ERG expression was correlated with patients' clinical outcome and several pathological parameters, including Gleason score (GS), pathological stage, surgical margin, and extracapsular extension. Results. ERG expression was detected in 86/198 (43.4%) patients exclusively in neoplastic epithelium. Overall, ERG mean expression intensity was 1.01 ± 1.27 versus 0.37 ± 0.83 in acinar PCA compared to foamy type PCA (P < 0.001). In HGPIN, ERG intensity levels were comparable to those in foamy type PCA (0.13 ± 0.56) but significantly lower than those in acinar PCA (P < 0.001). ERG expression was significantly associated with extra-prostatic extension and higher pathological stage and showed a trend toward seminal vesicle invasion. Herein, ERG expression was documented in 50/131 (38.1%) patients with pT2 versus 30/55 (54.5%) patients with pT3 (P = 0.04). ERG association with higher pathological stage was more pronounced in patients with GS > 7. Grouping patients into those with GS ≤ 7 versus >7, there was no significant association between ERG expression and GS. Similarly, no association was present in relation to either surgical margins or postsurgical serum PSA levels. Conclusion. We report significant association between ERG protein levels and extra-prostatic extension and higher pathological stage. ERG expression is not associated with adverse clinical outcome and is of limited prognostic value in localized PCA. [ABSTRACT FROM AUTHOR]

Published

2013

46. ERG Protein Expression Is of Limited Prognostic Value in Men with Localized Prostate Cancer.

Author

Liang Hong Teng, Cheng Wang, Dolph, Michael, Donnelly, Bryan, and Bismar, Tarek A.

Subjects

CHI-squared test, PROBABILITY theory, PROGNOSIS, PROSTATE tumors, PROTEINS, RESEARCH funding, TUMOR markers, TISSUE arrays, KAPLAN-Meier estimator

Abstract

Background. The prognostic significance of ERG expression in prostate cancer (PCA) has generated mixed results. We sought to investigate the prognostic significance of ERG expression in a localized cohort of men with PCA. Material and Methods. We investigated ERG protein expression in a cohort of 198 men with localized PCA. ERG expression was correlated with patients' clinical outcome and several pathological parameters, including Gleason score (GS), pathological stage, surgical margin, and extracapsular extension. Results. ERG expression was detected in 86/198 (43.4%) patients exclusively in neoplastic epithelium. Overall, ERG mean expression intensity was 1.01 ± 1.27 versus 0.37 ± 0.83 in acinar PCA compared to foamy type PCA (P < 0.001). In HGPIN, ERG intensity levels were comparable to those in foamy type PCA (0.13 ± 0.56) but significantly lower than those in acinar PCA (P < 0.001). ERG expression was significantly associated with extra-prostatic extension and higher pathological stage and showed a trend toward seminal vesicle invasion. Herein, ERG expression was documented in 50/131 (38.1%) patients with pT2 versus 30/55 (54.5%) patients with pT3 (P = 0.04). ERG association with higher pathological stage was more pronounced in patients with GS > 7. Grouping patients into those with GS ≤ 7 versus >7, there was no significant association between ERG expression and GS. Similarly, no association was present in relation to either surgical margins or postsurgical serum PSA levels. Conclusion. We report significant association between ERG protein levels and extra-prostatic extension and higher pathological stage. ERG expression is not associated with adverse clinical outcome and is of limited prognostic value in localized PCA. [ABSTRACT FROM AUTHOR]

Published

2013

47. Interactions and relationships of PTEN, ERG, SPINK1 and AR in castration-resistant prostate cancer.

Author

Bismar, Tarek A, Yoshimoto, Maisa, Duan, Qiuli, Liu, Shuhong, Sircar, Kanishka, and Squire, Jeremy A

Subjects

CASTRATION, PROSTATE cancer, SERINE proteinases, PHOSPHATASES, ANDROGEN receptors, FLUORESCENCE in situ hybridization

Abstract

Bismar T A, Yoshimoto M, Duan Q, Liu S, Sircar K & Squire J A (2012) Histopathology 60, 645-652 Interactions and relationships of PTEN, ERG, SPINK1 and AR in castration-resistant prostate cancer Aims: Recently, ETS-related gene ( ERG) gene rearrangements, phosphatase tensin homologue ( PTEN) deletions and serine protease inhibitor Kazal type 1 (SPINK1) overexpression were investigated as potential markers for molecularly subtyping prostate cancer (PCA). However, their incidence and co-association in castration-resistant PCA (CRPC) has not been characterized fully. Methods and results: A cohort of 59 CRPC patients was investigated for ERG rearrangements, PTEN deletions and androgen receptor ( AR) amplification by fluorescence in-situ hybridization. SPINK1 overexpression was assessed by immunohistochemistry. ERG rearrangements and PTEN deletions were detected in 22 of 53 (41.5%) and 35 of 55 (63.6%) of cases, with 15 of 22 (68.1%) of ERG rearrangements occurring through deletions. SPINK1 overexpression occurred in three of 51 (5.8%) of cases exclusively in non- ERG rearranged and AR amplification was detected in 12 of 49 (24.4%) of cases. Only PTEN deletions showed intrafocal heterogeneity occurring in nine of 35 (25.7%) of cases. PTEN deletions were significantly associated with each of ERG rearrangements occurring by deletions only ( P = 0.001), AR amplification ( P = 0.002) and SPINK1 overexpression ( P = 0.002). None of the SPINK1 overexpressing tumours showed AR amplification ( P = 0.005) and all occurred in PTEN deleted foci ( P = 0.002). Conclusion: The study supports the heterogeneous nature of CRPC and confirms a significant association between PTEN, ERG, AR and SPINK1. Characterizing combined markers will aid in defining PCA subgroups relevant to prognosis contributing to the design of improved therapeutic approaches for CRPC. [ABSTRACT FROM AUTHOR]

Published

2012

48. Elevated physiological levels of folic acid can increase in vitro growth and invasiveness of prostate cancer cells.

Author

Petersen, Lars F., Brockton, Nigel T., Bakkar, Ashraf, Liu, Shuhong, Wen, Jing, Weljie, Aalim M., and Bismar, Tarek A.

Subjects

PROSTATE cancer, FOLIC acid, CANCER cell growth, VITAMIN B complex, BIOCHEMISTRY

Abstract

What's known on the subject? and What does the study add? Evidence has emerged identifying folic acid supplementation as a potential risk factor for cancer development or progression. Long-term folic acid supplementation has been shown to increase the risk of prostate cancer development by three-fold. Sarcosine is a byproduct of folate metabolism and has been proposed as a biomarker for aggressive prostate cancer phenotypes. We looked at the effects of physiologically relevant levels of folic acid on in vitro prostate cancer cell growth and invasion, and demonstrated that higher levels can have the effect of increasing both of these biological processes. We also show that these changes toward a more aggressive phenotype are not linked to increased sarcosine levels, however other metabolic pathways may be involved. OBJECTIVES [ABSTRACT FROM AUTHOR]

Published

2012

49. PTEN genomic deletions that characterize aggressive prostate cancer originate close to segmental duplications.

Author

Yoshimoto, Maisa, Ludkovski, Olga, DeGrace, Dave, Williams, Julia L., Evans, Andrew, Sircar, Kanishka, Bismar, Tarek A., Nuin, Paulo, and Squire, Jeremy A.

Published

2012

50. Prognostic significance of CD8.

Author

Baker, Kristi, Lachapelle, Jonathan, Zlobec, Inti, Bismar, Tarek A., Terracciano, Luigi, and Foulkes, William D.

Subjects

LYMPHOCYTES, LEUCOCYTES, BREAST cancer, ESTROGEN receptors, HISTOPATHOLOGY

Abstract

Baker K, Lachapelle J, Zlobec I, Bismar T A, Terracciano L & Foulkes W D (2011) Histopathology [ABSTRACT FROM AUTHOR]

Published

2011