476 results on '"Wang-Rodriguez, Jessica"'
Search Results
2. The intratumor microbiome varies by geographical location and anatomical site in head and neck squamous cell carcinoma
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Yalamarty, Rishabh, Magesh, Shruti, John, Daniel, Chakladar, Jaideep, Li, Wei Tse, Brumund, Kevin T., Wang-Rodriguez, Jessica, and Ongkeko, Weg M.
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- 2024
- Full Text
- View/download PDF
3. The renal clear cell carcinoma immune landscape
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Saad, Omar A, Li, Wei Tse, Krishnan, Aswini R, Nguyen, Griffith C, Lopez, Jay P, McKay, Rana R, Wang-Rodriguez, Jessica, and Ongkeko, Weg M
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Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Immunology ,Cancer ,Genetics ,Biotechnology ,Kidney Disease ,Human Genome ,Good Health and Well Being ,Biomarkers ,Carcinoma ,Renal Cell ,Disease Susceptibility ,Gene Expression Regulation ,Neoplastic ,Humans ,Immunity ,Kidney Neoplasms ,Signal Transduction ,Renal clear cell carcinoma ,TCGA ,Clinical Sciences ,Oncology & Carcinogenesis ,Clinical sciences ,Oncology and carcinogenesis - Abstract
A comprehensive evaluation of the clear cell renal cell carcinoma (ccRCC) immune landscape was found using 584 RNA-sequencing datasets from The Cancer Genome Atlas (TCGA), we identified 17 key dysregulated immune-associated genes in ccRCC based on association with clinical variables and important immune pathways. Of the numerous findings from our analyses, we found that several of the 17 key dysregulated genes are heavily involved in interleukin and NF-kB signaling and that somatic copy number alteration (SCNA) hotspots may be causally associated with gene dysregulation. More importantly, we also found that key immune-associated genes and pathways are strongly upregulated in ccRCC. Our study may lend novel insights into the clinical implications of immune dysregulation in ccRCC and suggests potential immunotherapeutic targets for further evaluation.
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- 2022
4. The Landscape of Long Non-Coding RNA Dysregulation and Clinical Relevance in Muscle Invasive Bladder Urothelial Carcinoma.
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Shen, Haotian, Wong, Lindsay, Li, Wei, Chu, Megan, High, Rachel, Chang, Eric, Ongkeko, Weg, and Wang-Rodriguez, Jessica
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TCGA ,bladder carcinoma ,lncRNA-protein interaction ,lncRNAs - Abstract
Bladder cancer is one of the most common cancers in the United States, but few advancements in treatment options have occurred in the past few decades. This study aims to identify the most clinically relevant long non-coding RNAs (lncRNAs) to serve as potential biomarkers and treatment targets for muscle invasive bladder cancer (MIBC). Using RNA-sequencing data from 406 patients in The Cancer Genome Atlas (TCGA) database, we identified differentially expressed lncRNAs in MIBC vs. normal tissues. We then associated lncRNA expression with patient survival, clinical variables, oncogenic signatures, cancer- and immune-associated pathways, and genomic alterations. We identified a panel of 20 key lncRNAs that were most implicated in MIBC prognosis after differential expression analysis and prognostic correlations. Almost all lncRNAs we identified are correlated significantly with oncogenic processes. In conclusion, we discovered previously undescribed lncRNAs strongly implicated in the MIBC disease course that may be leveraged for diagnostic and treatment purposes in the future. Functional analysis of these lncRNAs may also reveal distinct mechanisms of bladder cancer carcinogenesis.
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- 2019
5. Papillary Thyroid Carcinoma Variants are Characterized by Co-dysregulation of Immune and Cancer Associated Genes.
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Ongkeko, Weg, Chakladar, Jaideep, Li, Wei, Bouvet, Michael, Chang, Eric, and Wang-Rodriguez, Jessica
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cancer immunology ,microRNA ,papillary thyroid carcinoma - Abstract
Papillary thyroid carcinoma (PTC) variants exhibit different prognosis, but critical characteristics of PTC variants that contribute to differences in pathogenesis are not well-known. This study aims to characterize dysregulated immune-associated and cancer-associated genes in three PTC subtypes to explore how the interplay between cancer and immune processes causes differential prognosis. RNA-sequencing data from The Cancer Genome Atlas (TCGA) were used to identify dysregulated genes in each variant. The dysregulation profiles of the subtypes were compared using functional pathways clustering and correlations to relevant clinical variables, genomic alterations, and microRNA regulation. We discovered that the dysregulation profiles of classical PTC (CPTC) and the tall cell variant (TCPTC) are similar and are distinct from that of the follicular variant (FVPTC). However, unique cancer or immune-associated genes are associated with clinical variables for each subtype. Cancer-related genes MUC1, FN1, and S100-family members were the most clinically relevant in CPTC, while APLN and IL16, both immune-related, were clinically relevant in FVPTC. RAET-family members, also immune-related, were clinically relevant in TCPTC. Collectively, our data suggest that dysregulation of both cancer and immune associated genes defines the gene expression landscapes of PTC variants, but different cancer or immune related genes may drive the phenotype of each variant.
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- 2019
6. Papillary Thyroid Carcinoma Variants are Characterized by Co-dysregulation of Immune and Cancer Associated Genes.
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Chakladar, Jaideep, Li, Wei Tse, Bouvet, Michael, Chang, Eric Y, Wang-Rodriguez, Jessica, and Ongkeko, Weg M
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cancer immunology ,microRNA ,papillary thyroid carcinoma ,Oncology and Carcinogenesis - Abstract
Papillary thyroid carcinoma (PTC) variants exhibit different prognosis, but critical characteristics of PTC variants that contribute to differences in pathogenesis are not well-known. This study aims to characterize dysregulated immune-associated and cancer-associated genes in three PTC subtypes to explore how the interplay between cancer and immune processes causes differential prognosis. RNA-sequencing data from The Cancer Genome Atlas (TCGA) were used to identify dysregulated genes in each variant. The dysregulation profiles of the subtypes were compared using functional pathways clustering and correlations to relevant clinical variables, genomic alterations, and microRNA regulation. We discovered that the dysregulation profiles of classical PTC (CPTC) and the tall cell variant (TCPTC) are similar and are distinct from that of the follicular variant (FVPTC). However, unique cancer or immune-associated genes are associated with clinical variables for each subtype. Cancer-related genes MUC1, FN1, and S100-family members were the most clinically relevant in CPTC, while APLN and IL16, both immune-related, were clinically relevant in FVPTC. RAET-family members, also immune-related, were clinically relevant in TCPTC. Collectively, our data suggest that dysregulation of both cancer and immune associated genes defines the gene expression landscapes of PTC variants, but different cancer or immune related genes may drive the phenotype of each variant.
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- 2019
7. Identification and characterization of dysregulated P-element induced wimpy testis-interacting RNAs in head and neck squamous cell carcinoma
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Saad, Maarouf A, Ku, Jonjei, Kuo, Selena Z, Li, Pin Xue, Zheng, Hao, Yu, Michael Andrew, Wang-Rodriguez, Jessica, and Ongkeko, Weg M
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Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Dental/Oral and Craniofacial Disease ,Biotechnology ,Genetics ,Substance Misuse ,Alcoholism ,Alcohol Use and Health ,Cancer ,Aetiology ,2.1 Biological and endogenous factors ,Good Health and Well Being ,head and neck squamous cell carcinoma ,piwi-interacting RNA ,alcohol ,epigenetics ,Oncology and carcinogenesis - Abstract
It is clear that alcohol consumption is a major risk factor in the pathogenesis of head and neck squamous cell carcinoma (HNSCC); however, the molecular mechanism underlying the pathogenesis of alcohol-associated HNSCC remains poorly understood. The aim of the present study was to identify and characterize P-element-induced wimpy testis (PIWI)-interacting RNAs (piRNAs) and PIWI proteins dysregulated in alcohol-associated HNSCC to elucidate their function in the development of this cancer. Using next generation RNA-sequencing (RNA-seq) data obtained from 40 HNSCC patients, the piRNA and PIWI protein expression of HNSCC samples was compared between alcohol drinkers and non-drinkers. A separate piRNA expression RNA-seq analysis of 18 non-smoker HNSCC patients was also conducted. To verify piRNA expression, reverse transcription-quantitative polymerase chain reaction (RT-qPCR) was performed on the most differentially expressed alcohol-associated piRNAs in ethanol and acetaldehyde-treated normal oral keratinocytes. The correlation between piRNA expression and patient survival was analyzed using Kaplan-Meier estimators and multivariate Cox proportional hazard models. A comparison between alcohol drinking and non-drinking HNSCC patients demonstrated that a panel of 3,223 piRNA transcripts were consistently detected and differentially expressed. RNA-seq analysis and in vitro RT-qPCR verification revealed that 4 of these piRNAs, piR-35373, piR-266308, piR-58510 and piR-38034, were significantly dysregulated between drinking and non-drinking cohorts. Of these four piRNAs, low expression of piR-58510 and piR-35373 significantly correlated with improved patient survival. Furthermore, human PIWI-like protein 4 was consistently upregulated in ethanol and acetaldehyde-treated normal oral keratinocytes. These results demonstrate that alcohol consumption may cause dysregulation of piRNA expression in HNSCC and in vitro verifications identified 4 piRNAs that may be involved in the pathogenesis of alcohol-associated HNSCC.
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- 2019
8. Pharmacogenetic testing in the Veterans Health Administration (VHA): policy recommendations from the VHA Clinical Pharmacogenetics Subcommittee
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Vassy, Jason L, Stone, Annjanette, Callaghan, John T, Mendes, Margaret, Meyer, Laurence J, Pratt, Victoria M, Przygodzki, Ronald M, Scheuner, Maren T, Wang-Rodriguez, Jessica, and Schichman, Steven A
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Biological Sciences ,Genetics ,Clinical Research ,Patient Safety ,Good Health and Well Being ,Clopidogrel ,Cytochrome P-450 CYP2C19 ,Cytochrome P-450 CYP2D6 ,Genotype ,Glucosephosphate Dehydrogenase ,HLA-B15 Antigen ,Humans ,Pharmacogenetics ,Pharmacogenomic Testing ,Stevens-Johnson Syndrome ,United States ,United States Department of Veterans Affairs ,Veterans ,Veterans Health ,Genetic testing ,Evidence-based practice ,Policymaking ,VHA Clinical Pharmacogenetics Subcommittee ,Clinical Sciences ,Genetics & Heredity - Abstract
PurposeThe Veterans Health Administration (VHA) Clinical Pharmacogenetics Subcommittee is charged with making recommendations about whether specific pharmacogenetic tests should be used in healthcare at VHA facilities. We describe a process to inform VHA pharmacogenetic testing policy.MethodsAfter developing consensus definitions of clinical validity and utility, the Subcommittee identified salient drug-gene pairs with potential clinical application in VHA. Members met monthly to discuss each drug-gene pair, the evidence of clinical utility for the associated pharmacogenetic test, and any VHA-specific testing considerations. The Subcommittee classified each test as strongly recommended, recommended, or not routinely recommended before drug initiation.ResultsOf 30 drug-gene pair tests reviewed, the Subcommittee classified 4 (13%) as strongly recommended, including HLA-B*15:02 for carbamazepine-associated Stevens-Johnston syndrome and G6PD for rasburicase-associated hemolytic anemia; 12 (40%) as recommended, including CYP2D6 for codeine toxicity; and 14 (47%) as not routinely recommended, such as CYP2C19 for clopidogrel dosing.ConclusionOnly half of drug-gene pairs with high clinical validity received Subcommittee support for policy promoting their widespread use across VHA. The Subcommittee generally found insufficient evidence of clinical utility or available, effective alternative strategies for the remainders. Continual evidence review and rigorous outcomes research will help promote the translation of pharmacogenetic discovery to healthcare.
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- 2019
9. Computational Analysis Suggests That AsnGTT 3′-tRNA-Derived Fragments Are Potential Biomarkers in Papillary Thyroid Carcinoma.
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Do, Annie N., Magesh, Shruti, Uzelac, Matthew, Chen, Tianyi, Li, Wei Tse, Bouvet, Michael, Brumund, Kevin T., Wang-Rodriguez, Jessica, and Ongkeko, Weg M.
- Abstract
Transfer-RNA-derived fragments (tRFs) are a novel class of small non-coding RNAs that have been implicated in oncogenesis. tRFs may act as post-transcriptional regulators by recruiting AGO proteins and binding to highly complementary regions of mRNA at seed regions, resulting in the knockdown of the transcript. Therefore, tRFs may be critical to tumorigenesis and warrant investigation as potential biomarkers. Meanwhile, the incidence of papillary thyroid carcinoma (PTC) has increased in recent decades and current diagnostic technology stands to benefit from new detection methods. Although small non-coding RNAs have been studied for their role in oncogenesis, there is currently no standard for their use as PTC biomarkers, and tRFs are especially underexplored. Accordingly, we aim to identify dysregulated tRFs in PTC that may serve as biomarker candidates. We identified dysregulated tRFs and driver genes between PTC primary tumor samples (n = 511) and adjacent normal tissue samples (n = 59). Expression data were obtained from MINTbase v2.0 and The Cancer Genome Atlas. Dysregulated tRFs and genes were analyzed in tandem to find pairs with anticorrelated expression. Significantly anticorrelated tRF-gene pairs were then tested for potential binding affinity using RNA22—if a heteroduplex can form via complementary binding, this would support the hypothesized RNA silencing mechanism. Four tRFs were significantly dysregulated in PTC tissue (p < 0.05), with only AsnGTT 3′-tRF being upregulated. Binding affinity analysis revealed that tRF-30-RY73W0K5KKOV (AsnGTT 3′-tRF) exhibits sufficient complementarity to potentially bind to and regulate transcripts of SLC26A4, SLC5A8, DIO2, and TPO, which were all found to be downregulated in PTC tissue. In the present study, we identified dysregulated tRFs in PTC and found that AsnGTT 3′-tRF is a potential post-transcriptional regulator and biomarker. [ABSTRACT FROM AUTHOR]
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- 2024
- Full Text
- View/download PDF
10. Functional Genomics Profiling of Bladder Urothelial Carcinoma MicroRNAome as a Potential Biomarker
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Li, Wei Tse, Zheng, Hao, Nguyen, Vincent, Wang-Rodriguez, Jessica, and Ongkeko, Weg M
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Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Prevention ,Tobacco ,Cancer ,Human Genome ,Clinical Research ,Tobacco Smoke and Health ,Urologic Diseases ,Biotechnology ,Genetics ,2.1 Biological and endogenous factors ,Aetiology ,Detection ,screening and diagnosis ,4.1 Discovery and preclinical testing of markers and technologies ,Good Health and Well Being ,Biomarkers ,Tumor ,Carcinoma ,Female ,Gene Expression Profiling ,Gene Expression Regulation ,Neoplastic ,Genomics ,Humans ,Male ,MicroRNAs ,Urinary Bladder ,Urinary Bladder Neoplasms ,Clinical Sciences ,Oncology & Carcinogenesis ,Clinical sciences ,Oncology and carcinogenesis - Abstract
Though bladder urothelial carcinoma is the most common form of bladder cancer, advances in its diagnosis and treatment have been modest in the past few decades. To evaluate miRNAs as putative disease markers for bladder urothelial carcinoma, this study develops a process to identify dysregulated miRNAs in cancer patients and potentially stratify patients based on the association of their microRNAome phenotype to genomic alterations. Using RNA sequencing data for 409 patients from the Cancer Genome Atlas, we examined miRNA differential expression between cancer and normal tissues and associated differentially expressed miRNAs with patient survival and clinical variables. We then correlated miRNA expressions with genomic alterations using the Wilcoxon test and REVEALER. We found a panel of six miRNAs dysregulated in bladder cancer and exhibited correlations to patient survival. We also performed differential expression analysis and clinical variable correlations to identify miRNAs associated with tobacco smoking, the most important risk factor for bladder cancer. Two miRNAs, miR-323a and miR-431, were differentially expressed in smoking patients compared to nonsmoking patients and were associated with primary tumor size. Functional studies of these miRNAs and the genomic features we identified for potential stratification may reveal underlying mechanisms of bladder cancer carcinogenesis and further diagnosis and treatment methods for urothelial bladder carcinoma.
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- 2018
11. Computational methods reveal novel functionalities of PIWI-interacting RNAs in human papillomavirus-induced head and neck squamous cell carcinoma.
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Ongkeko, Weg, Krishnan, Aswini, Qu, Yuanhao, Li, Pin, Wang-Rodriguez, Jessica, Califano, Joseph, and Zou, Angela
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HNSCC ,HPV ,ncRNA ,piRNA - Abstract
Human papillomavirus (HPV) infection is the fastest growing cause of head and neck squamous cell carcinoma (HNSCC) today, but its role in malignant transformation remains unclear. This study aimed to conduct a comprehensive investigation of PIWI-interacting RNA (piRNA) alterations and functionalities in HPV-induced HNSCC. Using 77 RNA-sequencing datasets from TCGA, we examined differential expression of piRNAs between HPV16(+) HNSCC and HPV(-) Normal samples, identifying a panel of 30 HPV-dysregulated piRNAs. We then computationally investigated the potential mechanistic significances of these transcripts in HPV-induced HNSCC, identifying our panel of piRNAs to associate with the protein PIWIL4 as well as the RTL family of retrotransposon-like genes, possibly through direct binding interactions. We also recognized several HPV-dysregulated transcripts for their correlations with well-documented mutations and copy number variations in HNSCC as well as HNSCC clinical variables, demonstrating the potential ability of our piRNAs to play important roles in large-scale modulation of HNSCC in addition to their direct, smaller-scale interactions in this malignancy. The differential expression of key piRNAs, including NONHSAT077364, NONHSAT102574, and NONHSAT128479, was verified in vitro by evaluating endogenous expression in HPV(+) cancer vs. HPV(-) normal cell lines. Overall, our novel study provides a rigorous investigation of piRNA dysregulation in HPV-related HNSCC, and lends critical insight into the idea that these small regulatory transcripts may play crucial and previously unidentified roles in tumor pathogenesis and progression.
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- 2018
12. Computational methods reveal novel functionalities of PIWI-interacting RNAs in human papillomavirus-induced head and neck squamous cell carcinoma
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Krishnan, Aswini R, Qu, Yuanhao, Li, Pin Xue, Zou, Angela E, Califano, Joseph A, Wang-Rodriguez, Jessica, and Ongkeko, Weg M
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Cervical Cancer ,Sexually Transmitted Infections ,Cancer ,Infectious Diseases ,Dental/Oral and Craniofacial Disease ,Rare Diseases ,Genetics ,Underpinning research ,2.1 Biological and endogenous factors ,Aetiology ,1.1 Normal biological development and functioning ,piRNA ,HNSCC ,ncRNA ,HPV ,Oncology and Carcinogenesis - Abstract
Human papillomavirus (HPV) infection is the fastest growing cause of head and neck squamous cell carcinoma (HNSCC) today, but its role in malignant transformation remains unclear. This study aimed to conduct a comprehensive investigation of PIWI-interacting RNA (piRNA) alterations and functionalities in HPV-induced HNSCC. Using 77 RNA-sequencing datasets from TCGA, we examined differential expression of piRNAs between HPV16(+) HNSCC and HPV(-) Normal samples, identifying a panel of 30 HPV-dysregulated piRNAs. We then computationally investigated the potential mechanistic significances of these transcripts in HPV-induced HNSCC, identifying our panel of piRNAs to associate with the protein PIWIL4 as well as the RTL family of retrotransposon-like genes, possibly through direct binding interactions. We also recognized several HPV-dysregulated transcripts for their correlations with well-documented mutations and copy number variations in HNSCC as well as HNSCC clinical variables, demonstrating the potential ability of our piRNAs to play important roles in large-scale modulation of HNSCC in addition to their direct, smaller-scale interactions in this malignancy. The differential expression of key piRNAs, including NONHSAT077364, NONHSAT102574, and NONHSAT128479, was verified in vitro by evaluating endogenous expression in HPV(+) cancer vs. HPV(-) normal cell lines. Overall, our novel study provides a rigorous investigation of piRNA dysregulation in HPV-related HNSCC, and lends critical insight into the idea that these small regulatory transcripts may play crucial and previously unidentified roles in tumor pathogenesis and progression.
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- 2018
13. A comprehensive study of smoking-specific microRNA alterations in head and neck squamous cell carcinoma
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Krishnan, Aswini R, Zheng, Hao, Kwok, James G, Qu, Yuanhao, Zou, Angela E, Korrapati, Avinaash, Li, Pin Xue, Califano, Joseph A, Hovell, Melbourne F, Wang-Rodriguez, Jessica, and Ongkeko, Weg M
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Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Dentistry ,Tobacco Smoke and Health ,Tobacco ,Prevention ,Cancer ,Rare Diseases ,Dental/Oral and Craniofacial Disease ,Biotechnology ,Genetics ,2.1 Biological and endogenous factors ,Aetiology ,Good Health and Well Being ,Carcinoma ,Squamous Cell ,Head and Neck Neoplasms ,Humans ,MicroRNAs ,Sequence Analysis ,RNA ,Smoking ,Squamous Cell Carcinoma of Head and Neck ,Head and neck neoplasms ,RNA ,Untranslated ,Public Health and Health Services ,Oncology & Carcinogenesis ,Oncology and carcinogenesis - Abstract
ObjectiveWhile tobacco smoking is a well-known risk factor for head and neck squamous cell carcinoma (HNSCC), the molecular mechanisms underlying tobacco-induced HNSCC remain unclear. This study sought to comprehensively identify microRNA (miRNA) alterations and evaluate their clinical relevance in smoking-induced HNSCC pathogenesis and progression.Materials and methodsUsing small RNA-sequencing data and clinical data from 145 HNSCC patients, we performed a series of differential expression and correlation analyses to identify a panel of tobacco-dysregulated miRNAs associated with key clinical characteristics in HNSCC. We then examined the expression patterns of these miRNAs in normal epithelial cell lines following exposure to cigarette smoke extract.ResultsOur analyses revealed distinct panels of miRNAs to be dysregulated with smoking status and associated with additional clinical features, including tumor stage, metastasis, anatomic site, and patient survival. The differential expression of key miRNAs, including miR-101, miR-181b, miR-486, and miR-1301, was verified in cigarette-treated epithelial cell lines, suggesting their potential roles in the early development of smoking-related HNSCCs.ConclusionSpecific alterations in miRNA expression may be traced to tobacco use and are associated with important HNSCC clinical characteristics. Future studies of these miRNAs may be valuable for furthering the understanding and targeted treatment of smoking-associated HNSCC.
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- 2017
14. Smoking status regulates a novel panel of PIWI-interacting RNAs in head and neck squamous cell carcinoma.
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Krishnan, Aswini R, Korrapati, Avinaash, Zou, Angela E, Qu, Yuanhao, Wang, Xiao Qi, Califano, Joseph A, Wang-Rodriguez, Jessica, Lippman, Scott M, Hovell, Melbourne F, and Ongkeko, Weg M
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Humans ,Carcinoma ,Squamous Cell ,Head and Neck Neoplasms ,RNA ,Small Interfering ,Smoking ,Female ,Male ,Squamous Cell Carcinoma of Head and Neck ,Head and neck neoplasms ,RNA ,Small interfering ,Cancer ,Biotechnology ,Genetics ,Dental/Oral and Craniofacial Disease ,Human Genome ,Tobacco ,Rare Diseases ,Tobacco Smoke and Health ,Good Health and Well Being ,Dentistry ,Oncology and Carcinogenesis ,Public Health and Health Services ,Oncology & Carcinogenesis - Abstract
ObjectiveSmoking remains a primary etiological factor in head and neck squamous cell carcinoma (HNSCC). Given that non-coding RNAs (ncRNAs), including PIWI-interacting RNAs (piRNAs), have emerged as mediators of initiation and progression in head and neck malignancies, we undertook a global study of piRNA expression patterns in smoking-associated HNSCC.Materials and methodsUsing RNA-sequencing data from 256 current smoker and lifelong nonsmoker samples in The Cancer Genome Atlas (TCGA), we analyzed the differential expression patterns of 27,127 piRNAs across patient cohorts stratified by tobacco use, with HPV16 status and tumor status taken into account. We correlated their expression to clinical characteristics and to smoking-induced alterations of PIWI proteins, the functional counterparts of piRNAs. Finally, we correlated our identified piRNAs and PIWI proteins to known chromosomal aberrations in HNSCC to understand their wider-ranging genomic effects.Results and conclusionOur analyses implicated a 13-member piRNA panel in smoking-related HNSCC, among which NONHSAT123636 and NONHSAT113708 associated with tumor stage, NONHSAT067200 with patient survival, and NONHSAT081250 with smoking-altered PIWIL1 protein expression. 6 piRNAs as well as PIWIL1 correlated with genomic alterations common to HNSCC, including TP53 mutation, TP53-3p co-occurrence, and 3q26, 8q24, and 11q13 amplification. Collectively, our findings provide novel insights into the etiology-specific piRNA landscape of smoking-induced HNSCC.
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- 2017
15. Alcohol-dysregulated microRNAs in hepatitis B virus-related hepatocellular carcinoma.
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Zheng, Hao, Zou, Angela E, Saad, Maarouf A, Wang, Xiao Qi, Kwok, James G, Korrapati, Avinaash, Li, Pinxue, Kisseleva, Tatiana, Wang-Rodriguez, Jessica, and Ongkeko, Weg M
- Subjects
Humans ,Hepatitis B virus ,Carcinoma ,Hepatocellular ,Liver Neoplasms ,MicroRNAs ,Polymerase Chain Reaction ,Alcohol Drinking ,Carcinoma ,Hepatocellular ,General Science & Technology - Abstract
Alcohol consumption and chronic hepatitis B virus (HBV) infection are two well-established risk factors for Hepatocellular carcinoma (HCC); however, there remains a limited understanding of the molecular pathway behind the pathogenesis and progression behind HCC, and how alcohol promotes carcinogenesis in the context of HBV+ HCC. Using next-generation sequencing data from 130 HCC patients and 50 normal liver tissues, we identified a panel of microRNAs that are significantly dysregulated by alcohol consumption in HBV+ patients. In particular, two microRNAs, miR-944 and miR-223-3p, showed remarkable correlation with clinical indication and genomic alterations. We confirmed the dysregulation of these two microRNAs in liver cell lines treated by alcohol and acetaldehyde, and showed that manipulation of miR-223-3p and miR-944 expression induces significant changes in cellular proliferation, sensitivity to doxorubicin, and the expression of both direct-binding and downstream mRNA targets. Together, the results of this study suggest that alcohol consumption in HBV+ HCCs regulates microRNAs that likely play previously uncharacterized roles in the alcohol-associated carcinogenesis of HCC, and future studies of these microRNAs may be valuable for furthering the understanding and treatment of alcohol and HBV-associated HCC.
- Published
- 2017
16. Utilization of iron (III)-doped nanoshells for in vivo marking of nonpalpable tumors using a VX2 rabbit model.
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Ward, Erin P, Wang, James, Mendez, Natalie, Yang, Jian, Barback, Chris, Wang-Rodriguez, Jessica, Trogler, William, Kummel, Andrew C, and Blair, Sarah
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Animals ,Rabbits ,Breast Neoplasms ,Disease Models ,Animal ,Ferric Compounds ,Ultrasonography ,Interventional ,Surgery ,Computer-Assisted ,Female ,Nanoshells ,Breast cancer ,Nonpalpable ,Silica nanoparticles ,Tumor localization ,Cancer ,Clinical Sciences ,Surgery - Abstract
BackgroundWe aimed to evaluate the potential for ultrasound (US) visible biodegradable nanoshells (NS) as an alternative to wire-guided localization for nonpalpable tumors in vivo.MethodsVX2 tumor was injected in bilateral thighs of 22 New Zealand rabbits and after 5 to 10 days, 1 tumor was marked with a wire as a control and the contralateral tumor was injected with 1 mL of 500 nm gas-filled silica NS under Doppler US. Tumors were excised after 24 hours. Chi-square was used for significance, P = .05.ResultsOne rabbit was excluded on postoperative day 1 due to equipment failure, no ill effects were observed from the NS. The NS were used to localize and resect 100% of marked tissue, 4/21 wires were displaced (P < .05).ConclusionsWe have shown that preoperatively injected US visible silica NS can be successfully used to mark nonpalpable tumors in vivo more consistently than WL.
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- 2016
17. Analysis of the immune landscape in virus-induced cancers using a novel integrative mechanism discovery approach
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Wong, Lindsay M., Li, Wei Tse, Shende, Neil, Tsai, Joseph C., Ma, Jiayan, Chakladar, Jaideep, Gnanasekar, Aditi, Qu, Yuanhao, Dereschuk, Kypros, Wang-Rodriguez, Jessica, and Ongkeko, Weg M.
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- 2021
- Full Text
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18. The non-coding landscape of head and neck squamous cell carcinoma
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Zou, Angela E, Zheng, Hao, Saad, Maarouf A, Rahimy, Mehran, Ku, Jonjei, Kuo, Selena Z, Honda, Thomas K, Wang-Rodriguez, Jessica, Xuan, Yinan, Korrapati, Avinaash, Yu, Vicky, Singh, Pranav, Grandis, Jennifer R, King, Charles C, Lippman, Scott M, Wang, Xiao Qi, Hinton, Andrew, and Ongkeko, Weg M
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Dental/Oral and Craniofacial Disease ,Cancer ,Human Genome ,Rare Diseases ,Genetics ,Biotechnology ,Good Health and Well Being ,Adult ,Aged ,Aged ,80 and over ,Carcinoma ,Squamous Cell ,Cell Line ,Tumor ,Female ,Gene Expression Profiling ,Gene Expression Regulation ,Neoplastic ,Head and Neck Neoplasms ,Humans ,Male ,MicroRNAs ,Middle Aged ,RNA ,Long Noncoding ,RNA ,Untranslated ,Sequence Analysis ,RNA ,Squamous Cell Carcinoma of Head and Neck ,Transcriptome ,head and neck cancer ,non-coding RNA ,RNA-sequencing ,cancer transcriptomics ,Oncology and Carcinogenesis - Abstract
Head and neck squamous cell carcinoma (HNSCC) is an aggressive disease marked by frequent recurrence and metastasis and stagnant survival rates. To enhance molecular knowledge of HNSCC and define a non-coding RNA (ncRNA) landscape of the disease, we profiled the transcriptome-wide dysregulation of long non-coding RNA (lncRNA), microRNA (miRNA), and PIWI-interacting RNA (piRNA) using RNA-sequencing data from 422 HNSCC patients in The Cancer Genome Atlas (TCGA). 307 non-coding transcripts differentially expressed in HNSCC were significantly correlated with patient survival, and associated with mutations in TP53, CDKN2A, CASP8, PRDM9, and FBXW7 and copy number variations in chromosomes 3, 5, 7, and 18. We also observed widespread ncRNA correlation to concurrent TP53 and chromosome 3p loss, a compelling predictor of poor prognosis in HNSCCs. Three selected ncRNAs were additionally associated with tumor stage, HPV status, and other clinical characteristics, and modulation of their expression in vitro reveals differential regulation of genes involved in epithelial-mesenchymal transition and apoptotic response. This comprehensive characterization of the HNSCC non-coding transcriptome introduces new layers of understanding for the disease, and nominates a novel panel of transcripts with potential utility as prognostic markers or therapeutic targets.
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- 2016
19. Electronic cigarettes induce DNA strand breaks and cell death independently of nicotine in cell lines
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Yu, Vicky, Rahimy, Mehran, Korrapati, Avinaash, Xuan, Yinan, Zou, Angela E, Krishnan, Aswini R, Tsui, Tzuhan, Aguilera, Joseph A, Advani, Sunil, Crotty Alexander, Laura E, Brumund, Kevin T, Wang-Rodriguez, Jessica, and Ongkeko, Weg M
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Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Cancer ,Tobacco ,Genetics ,Rare Diseases ,Dental/Oral and Craniofacial Disease ,2.2 Factors relating to the physical environment ,Carcinoma ,Squamous Cell ,Cell Death ,Cell Line ,Tumor ,DNA Damage ,Electronic Nicotine Delivery Systems ,Epithelial Cells ,Head and Neck Neoplasms ,Humans ,Nicotine ,Nicotinic Agonists ,Volatilization ,Oral cancer ,Head and neck squamous cell carcinoma ,Electronic cigarettes ,Smoking ,DNA damage ,Strand breaks ,Dentistry ,Public Health and Health Services ,Oncology & Carcinogenesis ,Oncology and carcinogenesis - Abstract
ObjectivesEvaluate the cytotoxicity and genotoxicity of short- and long-term e-cigarette vapor exposure on a panel of normal epithelial and head and neck squamous cell carcinoma (HNSCC) cell lines.Materials and methodsHaCaT, UMSCC10B, and HN30 were treated with nicotine-containing and nicotine-free vapor extract from two popular e-cigarette brands for periods ranging from 48 h to 8 weeks. Cytotoxicity was assessed using Annexin V flow cytometric analysis, trypan blue exclusion, and clonogenic assays. Genotoxicity in the form of DNA strand breaks was quantified using the neutral comet assay and γ-H2AX immunostaining.ResultsE-cigarette-exposed cells showed significantly reduced cell viability and clonogenic survival, along with increased rates of apoptosis and necrosis, regardless of e-cigarette vapor nicotine content. They also exhibited significantly increased comet tail length and accumulation of γ-H2AX foci, demonstrating increased DNA strand breaks.ConclusionE-cigarette vapor, both with and without nicotine, is cytotoxic to epithelial cell lines and is a DNA strand break-inducing agent. Further assessment of the potential carcinogenic effects of e-cigarette vapor is urgently needed.
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- 2016
20. 2353. SARS-CoV-2 Variants among US Veterans after COVID-19 Bivalent Vaccine Administration
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Holodniy, Mark, primary, Pei, Ying, additional, Stack, Gary, additional, Wade, Christopher L, additional, Agrawal, Yashpal, additional, Barasch, Nicholas, additional, Baddoura, Fady, additional, Carmen Frias-Kletecka, M, additional, Stacey Klutts, J, additional, and Wang-rodriguez, Jessica, additional
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- 2023
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21. Alcohol-dysregulated miR-30a and miR-934 in head and neck squamous cell carcinoma.
- Author
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Saad, Maarouf, Kuo, Selena, Rahimy, Elham, Korrapati, Avinaash, Rahimy, Mehran, Kim, Elizabeth, Zheng, Hao, Yu, Michael, Ongkeko, Weg, Wang-Rodriguez, Jessica, and Zou, Angela
- Subjects
Acetaldehyde ,Adult ,Alcohols ,Apoptosis ,Carcinoma ,Squamous Cell ,Cell Line ,Tumor ,Cell Proliferation ,Ethanol ,Female ,Gene Expression Regulation ,Neoplastic ,Head and Neck Neoplasms ,Humans ,Male ,MicroRNAs ,Middle Aged ,Reverse Transcriptase Polymerase Chain Reaction ,Squamous Cell Carcinoma of Head and Neck - Abstract
BACKGROUND: Alcohol consumption is a well-established risk factor for head and neck squamous cell carcinoma (HNSCC); however, the molecular mechanisms by which alcohol promotes HNSCC pathogenesis and progression remain poorly understood. Our study sought to identify microRNAs that are dysregulated in alcohol-associated HNSCC and investigate their contribution to the malignant phenotype. METHOD: Using RNA-sequencing data from 136 HNSCC patients, we compared the expression levels of 1,046 microRNAs between drinking and non-drinking cohorts. Dysregulated microRNAs were verified by qRT-PCR in normal oral keratinocytes treated with biologically relevant doses of ethanol and acetaldehyde. The most promising microRNA candidates were investigated for their effects on cellular proliferation and invasion, sensitivity to cisplatin, and expression of cancer stem cell genes. Finally, putative target genes were identified and evaluated in vitro to further establish roles for these miRNAs in alcohol-associated HNSCC. RESULTS: From RNA-sequencing analysis we identified 8 miRNAs to be significantly upregulated in alcohol-associated HNSCCs. qRT-PCR experiments determined that among these candidates, miR-30a and miR-934 were the most highly upregulated in vitro by alcohol and acetaldehyde. Overexpression of miR-30a and miR-934 in normal and HNSCC cell lines produced up to a 2-fold increase in cellular proliferation, as well as induction of the anti-apoptotic gene BCL-2. Upon inhibition of these miRNAs, HNSCC cell lines exhibited increased sensitivity to cisplatin and reduced matrigel invasion. miRNA knockdown also indicated direct targeting of several tumor suppressor genes by miR-30a and miR-934. CONCLUSIONS: Alcohol induces the dysregulation of miR-30a and miR-934, which may play crucial roles in HNSCC pathogenesis and progression. Future investigation of the alcohol-mediated pathways effecting these transformations will prove valuable for furthering the understanding and treatment of alcohol-associated HNSCC.
- Published
- 2015
22. Alcohol-dysregulated miR-30a and miR-934 in head and neck squamous cell carcinoma.
- Author
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Saad, Maarouf A, Kuo, Selena Z, Rahimy, Elham, Zou, Angela E, Korrapati, Avinaash, Rahimy, Mehran, Kim, Elizabeth, Zheng, Hao, Yu, Michael Andrew, Wang-Rodriguez, Jessica, and Ongkeko, Weg M
- Subjects
Cell Line ,Tumor ,Humans ,Carcinoma ,Squamous Cell ,Head and Neck Neoplasms ,Alcohols ,Ethanol ,Acetaldehyde ,MicroRNAs ,Reverse Transcriptase Polymerase Chain Reaction ,Apoptosis ,Cell Proliferation ,Gene Expression Regulation ,Neoplastic ,Adult ,Middle Aged ,Female ,Male ,Squamous Cell Carcinoma of Head and Neck ,Head and neck squamous cell carcinoma ,microRNA ,RNA-sequencing ,Alcohol ,Cell Line ,Tumor ,Carcinoma ,Squamous Cell ,Gene Expression Regulation ,Neoplastic ,Oncology & Carcinogenesis ,Oncology and Carcinogenesis - Abstract
BackgroundAlcohol consumption is a well-established risk factor for head and neck squamous cell carcinoma (HNSCC); however, the molecular mechanisms by which alcohol promotes HNSCC pathogenesis and progression remain poorly understood. Our study sought to identify microRNAs that are dysregulated in alcohol-associated HNSCC and investigate their contribution to the malignant phenotype.MethodUsing RNA-sequencing data from 136 HNSCC patients, we compared the expression levels of 1,046 microRNAs between drinking and non-drinking cohorts. Dysregulated microRNAs were verified by qRT-PCR in normal oral keratinocytes treated with biologically relevant doses of ethanol and acetaldehyde. The most promising microRNA candidates were investigated for their effects on cellular proliferation and invasion, sensitivity to cisplatin, and expression of cancer stem cell genes. Finally, putative target genes were identified and evaluated in vitro to further establish roles for these miRNAs in alcohol-associated HNSCC.ResultsFrom RNA-sequencing analysis we identified 8 miRNAs to be significantly upregulated in alcohol-associated HNSCCs. qRT-PCR experiments determined that among these candidates, miR-30a and miR-934 were the most highly upregulated in vitro by alcohol and acetaldehyde. Overexpression of miR-30a and miR-934 in normal and HNSCC cell lines produced up to a 2-fold increase in cellular proliferation, as well as induction of the anti-apoptotic gene BCL-2. Upon inhibition of these miRNAs, HNSCC cell lines exhibited increased sensitivity to cisplatin and reduced matrigel invasion. miRNA knockdown also indicated direct targeting of several tumor suppressor genes by miR-30a and miR-934.ConclusionsAlcohol induces the dysregulation of miR-30a and miR-934, which may play crucial roles in HNSCC pathogenesis and progression. Future investigation of the alcohol-mediated pathways effecting these transformations will prove valuable for furthering the understanding and treatment of alcohol-associated HNSCC.
- Published
- 2015
23. Transcriptome sequencing uncovers novel long noncoding and small nucleolar RNAs dysregulated in head and neck squamous cell carcinoma
- Author
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Zou, Angela E, Ku, Jonjei, Honda, Thomas K, Yu, Vicky, Kuo, Selena Z, Zheng, Hao, Xuan, Yinan, Saad, Maarouf A, Hinton, Andrew, Brumund, Kevin T, Lin, Jonathan H, Wang-Rodriguez, Jessica, and Ongkeko, Weg M
- Subjects
Biological Sciences ,Bioinformatics and Computational Biology ,Rare Diseases ,Genetics ,Stem Cell Research ,Cancer ,Biotechnology ,Dental/Oral and Craniofacial Disease ,Stem Cell Research - Nonembryonic - Human ,Aetiology ,2.1 Biological and endogenous factors ,Adult ,Aged ,Aged ,80 and over ,Carcinoma ,Squamous Cell ,Cell Line ,Tumor ,Cell Movement ,Cell Proliferation ,Epithelial-Mesenchymal Transition ,Female ,Gene Expression Profiling ,Gene Expression Regulation ,Neoplastic ,Head and Neck Neoplasms ,High-Throughput Nucleotide Sequencing ,Humans ,Male ,Middle Aged ,RNA ,Long Noncoding ,RNA ,Small Nucleolar ,Sequence Analysis ,RNA ,Survival Analysis ,HNSCC ,long noncoding RNAs ,RNA-sequencing ,small nucleolar RNAs ,Biochemistry and Cell Biology ,Developmental Biology ,Biochemistry and cell biology - Abstract
Head and neck squamous cell carcinoma persists as one of the most common and deadly malignancies, with early detection and effective treatment still posing formidable challenges. To expand our currently sparse knowledge of the noncoding alterations involved in the disease and identify potential biomarkers and therapeutic targets, we globally profiled the dysregulation of small nucleolar and long noncoding RNAs in head and neck tumors. Using next-generation RNA-sequencing data from 40 pairs of tumor and matched normal tissues, we found 2808 long noncoding RNA (lncRNA) transcripts significantly differentially expressed by a fold change magnitude ≥2. Meanwhile, RNA-sequencing analysis of 31 tumor-normal pairs yielded 33 significantly dysregulated small nucleolar RNAs (snoRNA). In particular, we identified two dramatically down-regulated lncRNAs and one down-regulated snoRNA whose expression levels correlated significantly with overall patient survival, suggesting their functional significance and clinical relevance in head and neck cancer pathogenesis. We confirmed the dysregulation of these noncoding RNAs in head and neck cancer cell lines derived from different anatomic sites, and determined that ectopic expression of the two lncRNAs inhibited key EMT and stem cell genes and reduced cellular proliferation and migration. As a whole, noncoding RNAs are pervasively dysregulated in head and squamous cell carcinoma. The precise molecular roles of the three transcripts identified warrants further characterization, but our data suggest that they are likely to play substantial roles in head and neck cancer pathogenesis and are significantly associated with patient survival.
- Published
- 2015
24. Richter transformation with c-MYC overexpression: report of three cases.
- Author
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Wang, Ling, Aghel, Azadeh, Peterson, Brandon, Wang-Rodriguez, Jessica, Wang, Huan-You, and Zhao, Xianfeng Frank
- Subjects
Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Lymphoma ,Cancer ,Hematology ,Rare Diseases ,Aetiology ,2.1 Biological and endogenous factors ,Aged ,Aged ,80 and over ,Biomarkers ,Tumor ,Cell Transformation ,Neoplastic ,Fatal Outcome ,Female ,Gene Rearrangement ,Humans ,Immunohistochemistry ,In Situ Hybridization ,Fluorescence ,Leukemia ,Lymphocytic ,Chronic ,B-Cell ,Lymphoma ,Large B-Cell ,Diffuse ,Male ,Middle Aged ,Proto-Oncogene Proteins c-myc ,Time Factors ,Treatment Outcome ,Up-Regulation ,Chronic lymphocytic leukemia/small lymphocytic lymphoma ,Richter syndrome ,MYC ,diffuse large B-cell lymphoma ,Biochemistry and Cell Biology ,Microbiology ,Oncology & Carcinogenesis ,Oncology and carcinogenesis - Abstract
Pathogenesis of Richter transformation (RT) or Richter syndrome (RS) of chronic lymphocytic leukemia (CLL) is still largely unknown. Increasing evidences show that c-MYC may play a role in the development of RS. Here we report three cases of RS with overexpression of c-MYC. The first case was a 78-year-old male who initially presented with CLL and then developed diffuse lymphadenopathy and ascites shortly after. Ascites cytology showed a population of large lymphoid cells positive for MYC (8q24) rearrangement by fluorescence in situ hybridization (FISH) and overexpression of c-MYC by immunohistochemistry (IHC). The second case was a 66-year-old male presented with rapidly enlarging lymph nodes and pleural effusion after a long history of CLL. Biopsy showed large B-cells positive for c-MYC overexpression and high Ki-67 proliferation index (80-90%). The third case was a 62-year-old female with CLL who presented for lobectomy for lung adenocarcinoma. Interestingly, along with the carcinoma, large B-cell lymphoma was incidentally found which had the same immunophenotype as the CLL. FISH analysis revealed gain of c-MYC at 8q and IHC showed increased c-MYC expression. This study supports that c-MYC plays a critical role in RS.
- Published
- 2015
25. Primary mucin-producing urothelial-type adenocarcinoma of the prostatic urethra diagnosed on TURP: a case report and review of literature.
- Author
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Sebesta, Elisabeth M, Mirheydar, Hossein S, Parsons, J Kellogg, Wang-Rodriguez, Jessica, and Kader, A Karim
- Subjects
Humans ,Adenocarcinoma ,Urethral Neoplasms ,Mucins ,Diagnosis ,Differential ,Transurethral Resection of Prostate ,Aged ,80 and over ,Male ,Mucin-producing adenocarcinoma ,Prostatic urethra ,Trans-urethral resection of prostate ,Urothelial-type adenocarcinoma ,Urologic Diseases ,Rare Diseases ,Cancer ,Urology & Nephrology ,Clinical Sciences - Abstract
BackgroundMucin-producing urothelial-type adenocarcinoma of the prostatic urethra is extremely rare. These lesions must be differentiated from other mucinous tumors including mucin-producing prostatic adenocarcinoma and metastases from either colonic or bladder primaries.Case presentationWe report here a case of urothelial-type adenocarcinoma arising from the prostatic urethra. The patient is an 81 year-old man with a history of pT1 urothelial cell carcinoma of the bladder status post trans-urethral resection of bladder tumor (TURBT) who initially presented with irritative lower urinary tract symptoms and mucosuria refractory to Flomax and finasteride. A shared decision was made for the patient to undergo trans-urethral resection of prostate (TURP). At the time of surgery, a papillary tumor emanating from the prostatic urethra was found and no urothelial lesions were noted in the bladder. Pathology of the resected prostatic chips revealed an invasive adenocarcinoma with intestinal-type differentiation that stained positive for CK7, CK20, and villin, but negative for PSA, PSAP, uroplakin, and CDX-2. Colonoscopy was normal and CT scan did not show any evidence of colonic lesions nor visceral or lymph node metastases. Thus, the patient was diagnosed with a primary urothelial-type adenocarcinoma of the prostatic urethra.ConclusionHerein we review the literature regarding this unusual entity, and discuss the differential diagnosis, immunohistochemistry, and the importance of correctly identifying this rare tumor.
- Published
- 2014
26. Parathyroid hormone related-protein promotes epithelial-to-mesenchymal transition in prostate cancer.
- Author
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Ongkeko, Weg M, Burton, Doug, Kiang, Alan, Abhold, Eric, Kuo, Selena Z, Rahimy, Elham, Yang, Meng, Hoffman, Robert M, Wang-Rodriguez, Jessica, and Deftos, Leonard J
- Subjects
Bone and Bones ,Cell Line ,Tumor ,Animals ,Humans ,Mice ,Mice ,Nude ,Mice ,SCID ,Prostatic Neoplasms ,Vimentin ,Parathyroid Hormone-Related Protein ,Cadherins ,Protein Isoforms ,Transcription Factors ,Microscopy ,Fluorescence ,Transplantation ,Heterologous ,Reverse Transcriptase Polymerase Chain Reaction ,Gene Expression Regulation ,Neoplastic ,RNA Interference ,Male ,Matrix Metalloproteinase 9 ,Epithelial-Mesenchymal Transition ,Snail Family Transcription Factors ,Cell Line ,Tumor ,Gene Expression Regulation ,Neoplastic ,Nude ,SCID ,Microscopy ,Fluorescence ,Transplantation ,Heterologous ,General Science & Technology - Abstract
Parathyroid hormone-related protein (PTHrP) possesses a variety of physiological and developmental functions and is also known to facilitate the progression of many common cancers, notably their skeletal invasion, primarily by increasing bone resorption. The purpose of this study was to determine whether PTHrP could promote epithelial-to-mesenchymal transition (EMT), a process implicated in cancer stem cells that is critically involved in cancer invasion and metastasis. EMT was observed in DU 145 prostate cancer cells stably overexpressing either the 1-141 or 1-173 isoform of PTHrP, where there was upregulation of Snail and vimentin and downregulation of E-cadherin relative to parental DU 145. By contrast, the opposite effect was observed in PC-3 prostate cancer cells where high levels of PTHrP were knocked-down via lentiviral siRNA transduction. Increased tumor progression was observed in PTHrP-overexpressing DU 145 cells while decreased progression was observed in PTHrP-knockdown PC-3 cells. PTHrP-overexpressing DU 145 formed larger tumors when implanted orthoptopically into nude mice and in one case resulted in spinal metastasis, an effect not observed among mice injected with parental DU 145 cells. PTHrP-overexpressing DU 145 cells also caused significant bone destruction when injected into the tibiae of nude mice, while parental DU 145 cells caused little to no destruction of bone. Together, these results suggest that PTHrP may work through EMT to promote an aggressive and metastatic phenotype in prostate cancer, a pathway of importance in cancer stem cells. Thus, continued efforts to elucidate the pathways involved in PTHrP-induced EMT as well as to develop ways to specifically target PTHrP signaling may lead to more effective therapies for prostate cancer.
- Published
- 2014
27. Generation of "Virtual"� Control Groups for Single Arm Prostate Cancer Adjuvant Trials
- Author
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Jia, Zhenyu, Lilly, Michael B, Koziol, James A, Chen, Xin, Xia, Xiao-Qin, Wang, Yipeng, Skarecky, Douglas, Sutton, Manuel, Sawyers, Anne, Ruckle, Herbert, Carpenter, Philip M, Wang-Rodriguez, Jessica, Jiang, Jun, Deng, Mingsen, Pan, Cong, Zhu, Jian-guo, McLaren, Christine E, Gurley, Michael J, Lee, Chung, McClelland, Michael, Ahlering, Thomas, Kattan, Michael W, Mercola, Dan, and Filleur, Stephanie
- Subjects
radical prostatectomy ,postoperative nomograms ,preoperative nomogram ,10-year probability ,disease recurrence ,clinical-trial ,follow-up ,high-risk ,docetaxel ,efficacy - Published
- 2014
28. Expression differences between African American and Caucasian prostate cancer tissue reveals that stroma is the site of aggressive changes
- Author
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Kinseth, Matthew A, Jia, Zhenyu, Rahmatpanah, Farahnaz, Sawyers, Anne, Sutton, Manuel, Wang‐Rodriguez, Jessica, Mercola, Dan, and McGuire, Kathleen L
- Subjects
Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Aging ,Genetics ,Urologic Diseases ,Cancer ,Prostate Cancer ,2.1 Biological and endogenous factors ,Aetiology ,Black or African American ,Epithelial-Mesenchymal Transition ,Humans ,Male ,Middle Aged ,Neoplasm Grading ,Prostatic Neoplasms ,Tissue Array Analysis ,Transcriptome ,Tumor Microenvironment ,White People ,prostate cancer ,racial disparity ,stroma expression ,EMT ,immune response ,Oncology & Carcinogenesis ,Oncology and carcinogenesis - Abstract
In prostate cancer, race/ethnicity is the highest risk factor after adjusting for age. African Americans have more aggressive tumors at every clinical stage of the disease, resulting in poorer prognosis and increased mortality. A major barrier to identifying crucial gene activity differences is heterogeneity, including tissue composition variation intrinsic to the histology of prostate cancer. We hypothesized that differences in gene expression in specific tissue types would reveal mechanisms involved in the racial disparities of prostate cancer. We examined 17 pairs of arrays for AAs and Caucasians that were formed by closely matching the samples based on the known tissue type composition of the tumors. Using pair-wise t-test we found significantly altered gene expression between AAs and CAs. Independently, we performed multiple linear regression analyses to associate gene expression with race considering variation in percent tumor and stroma tissue. The majority of differentially expressed genes were associated with tumor-adjacent stroma rather than tumor tissue. Extracellular matrix, integrin family and signaling mediators of the epithelial-to-mesenchymal transition (EMT) pathways were all downregulated in stroma of AAs. Using MetaCore (GeneGo) analysis, we observed that 35% of significant (p < 10(-3)) pathways identified EMT and 25% identified immune response pathways especially for interleukins-2, -4, -5, -6, -7, -10, -13, -15 and -22 as the major changes. Our studies reveal that altered immune and EMT processes in tumor-adjacent stroma may be responsible for the aggressive nature of prostate cancer in AAs.
- Published
- 2014
29. Early Human Prostate Adenocarcinomas Harbor Androgen-Independent Cancer Cells
- Author
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Fiñones, Rita R, Yeargin, Jo, Lee, Melissa, Kaur, Aman Preet, Cheng, Clari, Sun, Paulina, Wu, Christopher, Nguyen, Catherine, Wang-Rodriguez, Jessica, Meyer, April N, Baird, Stephen M, Donoghue, Daniel J, and Haas, Martin
- Subjects
Biological Sciences ,Biomedical and Clinical Sciences ,Clinical Sciences ,Oncology and Carcinogenesis ,Aging ,Stem Cell Research - Nonembryonic - Non-Human ,Biotechnology ,Prostate Cancer ,Urologic Diseases ,Stem Cell Research ,Cancer ,Clinical Research ,Aetiology ,2.1 Biological and endogenous factors ,Adenocarcinoma ,Aldehyde Dehydrogenase ,Androgens ,Animals ,Biomarkers ,Tumor ,Castration ,Cell Count ,Cell Proliferation ,Cell Shape ,Collagen ,Drug Combinations ,Epithelial Cells ,Gene Expression Regulation ,Neoplastic ,Humans ,Laminin ,Male ,Mice ,Neoplasm Staging ,Neoplastic Stem Cells ,Oncogene Proteins ,Fusion ,Prostatic Neoplasms ,Proteoglycans ,Spheroids ,Cellular ,Tumor Cells ,Cultured ,Xenograft Model Antitumor Assays ,General Science & Technology - Abstract
Although blockade of androgen receptor (AR) signaling represents the main treatment for advanced prostate cancer (PrCa), many patients progress to a lethal phenotype of "Castration-Resistant" prostate cancer (CR-PrCa). With the hypothesis that early PrCa may harbor a population of androgen-unresponsive cancer cells as precursors to CR-recurrent disease, we undertook the propagation of androgen-independent cells from PrCa-prostatectomy samples of early, localized (Stage-I) cases. A collection of 120 surgical specimens from prostatectomy cases was established, among which 54 were adenocarcinomas. Hormone-free cell culture conditions were developed allowing routine propagation of cells expressing prostate basal cell markers and stem/progenitor cell markers, and which proliferated as spheres/spheroids in suspension cultures. Colonies of androgen-independent epithelial cells grew out from 30/43 (70%) of the adenocarcinoma cases studied in detail. Fluorescence microscopy and flow cytometry showed that CR-PrCa cells were positive for CD44, CD133, CK5/14, c-kit, integrin α2β1, SSEA4, E-Cadherin and Aldehyde Dehydrogenase (ALDH). All 30 CR-PrCa cell cultures were also TERT-positive, but negative for TMPRSS2-ERG. Additionally, a subset of 22 of these CR-PrCa cell cultures was examined by orthotopic xenografting in intact and castrated SCID mice, generating histologically typical locally-invasive human PrCa or undifferentiated cancers, respectively, in 6-8 weeks. Cultured PrCa cells and orthotopically-induced in vivo cancers lacked PSA expression. We report here the propagation of Cancer Initiating Cells (CIC) directly from Stage I human PrCa tissue without selection or genetic manipulation. The propagation of stem/progenitor-like CR-PrCa cells derived from early human prostate carcinomas suggests the existence of a subpopulation of cells resistant to androgen-deprivation therapy and which may drive the subsequent emergence of disseminated CR-PrCa.
- Published
- 2013
30. Salinomycin induces cell death and differentiation in head and neck squamous cell carcinoma stem cells despite activation of epithelial-mesenchymal transition and Akt
- Author
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Kuo, Selena Z, Blair, Katherine J, Rahimy, Elham, Kiang, Alan, Abhold, Eric, Fan, Jian-Bing, Wang-Rodriguez, Jessica, Altuna, Xabier, and Ongkeko, Weg M
- Abstract
Abstract Background Cancer stem cells (CSC) are believed to play a crucial role in cancer recurrence due to their resistance to conventional chemotherapy and capacity for self-renewal. Recent studies have reported that salinomycin, a livestock antibiotic, selectively targets breast cancer stem cells 100-fold more effectively than paclitaxel. In our study we sought to determine the effects of salinomycin on head and neck squamous cell carcinoma (HNSCC) stem cells. Methods MTS and TUNEL assays were used to study cell proliferation and apoptosis as a function of salinomycin exposure in JLO-1, a putative HNSCC stem cell culture. MTS and trypan blue dye exclusion assays were performed to investigate potential drug interactions between salinomycin and cisplatin or paclitaxel. Stem cell-like phenotype was measured by mRNA expression of stem cell markers, sphere-forming capacity, and matrigel invasion assays. Immunoblotting was also used to determine expression of epithelial-mesenchymal transition (EMT) markers and Akt phosphorylation. Arrays by Illumina, Inc. were used to profile microRNA expression as a function of salinomycin dose. Results In putative HNSCC stem cells, salinomycin was found to significantly inhibit cell viability, induce a 71.5% increase in levels of apoptosis, elevate the Bax/Bcl-2 ratio, and work synergistically with cisplatin and paclitaxel in inducing cell death. It was observed that salinomycin significantly inhibited sphere forming-capability and repressed the expression of CD44 and BMI-1 by 3.2-fold and 6.2-fold, respectively. Furthermore, salinomycin reduced invasion of HNSCC stem cells by 2.1 fold. Contrary to expectations, salinomycin induced the expression of EMT markers Snail, vimentin, and Zeb-1, decreased expression of E-cadherin, and also induced phosphorylation of Akt and its downstream targets GSK3-β and mTOR. Conclusions These results demonstrate that in HNSCC cancer stem cells, salinomycin can cause cell death and decrease stem cell properties despite activation of both EMT and Akt.
- Published
- 2012
31. Computerized Decision Support System for Intraoperative Analysis of Margin Status in Breast Conservation Therapy
- Author
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Ruidíaz, Manuel E, Blair, Sarah L, Kummel, Andrew C, and Wang-Rodriguez, Jessica
- Subjects
Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Cancer ,Clinical Research ,Breast Cancer - Abstract
Background. Breast conservation therapy (BCT) is the standard treatment for breast cancer; however, 32-63% of procedures have a positive margin leading to secondary procedures. The standard of care to evaluate surgical margins is based on permanent section. Imprint cytology (IC) has been used to evaluate surgical samples but is limited by excessive cauterization thus requiring experienced cytopathologist for interpretation. An automated image screening process has been developed to detect cancerous cells from IC on cauterized margins. Methods. IC was prospectively performed on margins during lumpectomy operations for breast cancer in addition to permanent section on 127 patients. An 8-slide training subset and 8-slide testing subset were culled. H&E IC automated analysis, based on linear discriminant analysis, was compared to manual pathologist interpretation. Results. The most important descriptors, from highest to lowest performance, are nucleus color (23%), cytoplasm color (15%), shape (12%), grey intensity (9%), and local area (5%). There was 100% agreement between automated and manual interpretation of IC slides. Conclusion. Although limited by IC sampling variability, an automated system for accurate IC cancer cell identification system is demonstrated, with high correlation to manual analysis, even in the face of cauterization effects which supplement permanent section analysis.
- Published
- 2012
32. ROR1 Is Expressed in Human Breast Cancer and Associated with Enhanced Tumor-Cell Growth
- Author
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Zhang, Suping, Chen, Liguang, Cui, Bing, Chuang, Han-Yu, Yu, Jianqiang, Wang-Rodriguez, Jessica, Tang, Li, Chen, George, Basak, Grzegorz W, and Kipps, Thomas J
- Subjects
Biochemistry and Cell Biology ,Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,Biological Sciences ,Cancer ,Breast Cancer ,Development of treatments and therapeutic interventions ,5.2 Cellular and gene therapies ,Aetiology ,2.1 Biological and endogenous factors ,Animals ,Antibodies ,Monoclonal ,Antibody Specificity ,Breast Neoplasms ,CHO Cells ,Cell Proliferation ,Cell Survival ,Cricetinae ,Cricetulus ,Cyclic AMP Response Element-Binding Protein ,Enzyme Activation ,Female ,Gene Expression Regulation ,Neoplastic ,Humans ,Mice ,Middle Aged ,Phosphatidylinositol 3-Kinases ,Proto-Oncogene Proteins ,Proto-Oncogene Proteins c-akt ,Receptor Tyrosine Kinase-like Orphan Receptors ,Signal Transduction ,Wnt Proteins ,Wnt-5a Protein ,General Science & Technology - Abstract
Receptor-tyrosine-kinase-like orphan receptor 1 (ROR1) is expressed during embryogenesis and by certain leukemias, but not by normal adult tissues. Here we show that the neoplastic cells of many human breast cancers express the ROR1 protein and high-level expression of ROR1 in breast adenocarcinoma was associated with aggressive disease. Silencing expression of ROR1 in human breast cancer cell lines found to express this protein impaired their growth in vitro and also in immune-deficient mice. We found that ROR1 could interact with casein kinase 1 epsilon (CK1ε) to activate phosphoinositide 3-kinase-mediated AKT phosphorylation and cAMP-response-element-binding protein (CREB), which was associated with enhanced tumor-cell growth. Wnt5a, a ligand of ROR1, could induce ROR1-dependent signaling and enhance cell growth. This study demonstrates that ROR1 is expressed in human breast cancers and has biological and clinical significance, indicating that it may be a potential target for breast cancer therapy.
- Published
- 2012
33. Recombinant human erythropoietin promotes the acquisition of a malignant phenotype in head and neck squamous cell carcinoma cell lines in vitro
- Author
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Abhold, Eric, Rahimy, Elham, Wang-Rodriguez, Jessica, Blair, Katherine J, Yu, Michael A, Brumund, Kevin T, Weisman, Robert A, and Ongkeko, Weg M
- Abstract
Abstract Background Recent studies indicate an increase in tumor progression and recurrence in head and neck squamous cell carcinomas (HNSCC) of cancer patients taking recombinant human erythropoietin (rhEpo) for anemia. This study was undertaken to investigate the potential role of rhEpo in invasion, proliferation, and cisplatin-induced cell death in HNSCC cell lines. Methods The following experiments were performed with two HNSCC cell lines, UMSCC-10B and UMSCC-22B. Presence of EpoR in both cell lines was determined by western blot and quantitative PCR. Colorimetric MTS assays and clonogenic assays were used to study the effect of rhEpo at pharmacologically relevant doses on cell proliferation. Matrigel invasion assays were performed in order to determine effects of exogenous rhEpo on invasive abilities. Clonogenic assays were also used to study potential cytoprotective effects of rhEpo against cisplatin. Immunoblotting was done to analyze the effect of rhEpo on Akt phosphorylation. Finally, MTS and TUNEL assays were performed to test our hypothesis that Akt activation by PI3K was involved in rhEpo-mediated cisplatin resistance. Results HNSCC cell lines were shown to express Epo receptor (EpoR). RhEpo increased invasion 1.8-fold in UMSCC-10B and 2.6-fold in UMSCC-22B compared to control. RhEpo at 10 U/ml increased cell proliferation by 41% and 53% in UMSCC-10B and UMSCC-22B, respectively, and colony formation by 1.5-fold and 1.8-fold. UMSCC-10B treated with cisplatin and exposed to rhEpo at 1 and 10 U/ml resulted in a 1.7-fold and 3.0-fold increase in colony number compared to control, respectively. UMSCC-22B treated with cisplatin and rhEpo at 1 or 10 U/ml resulted in ~2.5-fold increase in colony number. A TUNEL assay demonstrated a 30.5% and 76.5% increase in survival in UMSCC-10B and UMSCC-22B cells, respectively, in cisplatin and rhEpo-treated cells compared to cisplatin alone. MTS assay showed similar cytoprotective effects. Western blot revealed increased phosphorylation of Akt upon exposure of HNSCC cell lines to rhEpo. MTS assay and TUNEL analyses implicate Akt as a likely contributor to regulation of rhEpo-mediated cytoprotection. Conclusions The results demonstrate that, in HNSCC cells expressing functional EpoR, rhEpo promotes invasion, cell proliferation, and induces resistance to cisplatin, which may contribute to tumor progression.
- Published
- 2011
34. Diagnosis of prostate cancer using differentially expressed genes in stroma.
- Author
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Jia, Zhenyu, Wang, Yipeng, Sawyers, Anne, Yao, Huazhen, Rahmatpanah, Farahnaz, Xia, Xiao-Qin, Xu, Qiang, Pio, Rebecca, Turan, Tolga, Koziol, James A, Goodison, Steve, Carpenter, Philip, Wang-Rodriguez, Jessica, Simoneau, Anne, Meyskens, Frank, Sutton, Manuel, Lernhardt, Waldemar, Beach, Thomas, Monforte, Joseph, McClelland, Michael, and Mercola, Dan
- Subjects
Aged ,Aged ,80 and over ,Biopsy ,Gene Expression Profiling ,Gene Expression Regulation ,Neoplastic ,Humans ,Male ,Middle Aged ,Prostatic Neoplasms: diagnosis ,genetics ,metabolism ,pathology ,RNA ,Neoplasm: biosynthesis ,genetics ,Reproducibility of Results ,Stromal Cells: pathology ,physiology ,age ,article ,classifier ,controlled study ,diagnostic value ,gene ,gene expression ,gene expression profiling ,human ,human tissue ,male ,priority journal ,prostate biopsy ,prostate cancer ,reproducibility ,sensitivity and specificity ,stroma ,tumor microenvironment ,Aged ,Aged ,80 and over ,Biopsy ,Gene Expression Profiling ,Gene Expression Regulation ,Neoplastic ,Humans ,Male ,Middle Aged ,Prostatic Neoplasms ,Reproducibility of Results ,RNA ,Neoplasm ,Stromal Cells - Abstract
More than one million prostate biopsies are performed in the United States every year. A failure to find cancer is not definitive in a significant percentage of patients due to the presence of equivocal structures or continuing clinical suspicion. We have identified gene expression changes in stroma that can detect tumor nearby. We compared gene expression profiles of 13 biopsies containing stroma near tumor and 15 biopsies from volunteers without prostate cancer. About 3,800 significant expression changes were found and thereafter filtered using independent expression profiles to eliminate possible age-related genes and genes expressed at detectable levels in tumor cells. A stroma-specific classifier for nearby tumor was constructed on the basis of 114 candidate genes and tested on 364 independent samples including 243 tumor-bearing samples and 121 nontumor samples (normal biopsies, normal autopsies, remote stroma, as well as stroma within a few millimeters of tumor). The classifier predicted the tumor status of patients using tumor-free samples with an average accuracy of 97% (sensitivity = 98% and specificity = 88%) whereas classifiers trained with sets of 100 randomly generated genes had no diagnostic value. These results indicate that the prostate cancer microenvironment exhibits reproducible changes useful for categorizing the presence of tumor in patients when a prostate sample is derived from near the tumor but does not contain any recognizable tumor.
- Published
- 2011
35. In silico Dissection of Cell-Type-Associated Patterns of Gene Expression in Prostate Cancer
- Author
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Stuart, Robert O., Wachsman, William, Berry, Charles C., Wang-Rodriguez, Jessica, Wasserman, Linda, Klacansky, Igor, Masys, Dan, Arden, Karen, Goodison, Steven, McClelland, Michael, Wang, Yipeng, Sawyers, Anne, Kalcheva, Iveta, Tarin, David, and Mercola, Dan
- Published
- 2004
36. Circulating T-regulatory cells, exercise and the elite adolescent swimmer.
- Author
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Wilson, Lori D, Zaldivar, Frank P, Schwindt, Christina D, Wang-Rodriguez, Jessica, and Cooper, Dan M
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Health Sciences ,Sports Science and Exercise ,Lung ,Asthma ,2.1 Biological and endogenous factors ,Aetiology ,Inflammatory and immune system ,Adolescent ,Case-Control Studies ,Exercise ,Female ,Forkhead Transcription Factors ,Humans ,Lymphocyte Count ,Male ,Physical Exertion ,Rhinitis ,Swimming ,T-Lymphocyte Subsets ,T-Lymphocytes ,Regulatory ,Human Movement and Sports Sciences ,Paediatrics and Reproductive Medicine ,Curriculum and Pedagogy ,Sport Sciences ,Paediatrics ,Sports science and exercise - Abstract
Brief high intensity exercise induces peripheral leukocytosis possibly leading to a higher incidence of allergic symptoms in athletes undergoing excessive training. We studied the exercise-induced alternation of circulating Tregs and FoxP3+ Tregs due to acute intense swim exercise in elite swimmers (n = 22, 12 males, age = 15.4 yrs). Twelve had prior or current rhinitis or asthma and 10 had no current or prior allergy or asthma. Circulating Tregs increased significantly (p < .001) following exercise (pre = 133 +/- 11.2, post = 196 +/- 17.6) as did FoxP3+ cells (pre = 44, post = 64 cells/microl). Increases in Tregs and FoxP3+ Tregs occurred to the same extent in both groups of adolescent swimmers.
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- 2009
37. A comprehensive study of smoking-specific microRNA alterations in head and neck squamous cell carcinoma
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Krishnan, Aswini R., Zheng, Hao, Kwok, James G., Qu, Yuanhao, Zou, Angela E., Korrapati, Avinaash, Li, Pin Xue, Califano, Joseph A., Hovell, Melbourne F., Wang-Rodriguez, Jessica, and Ongkeko, Weg M.
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- 2017
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38. Replacing the Guaiac Fecal Occult Blood Test With the Fecal Immunochemical Test Increases Proportion of Individuals Screened in a Large Healthcare Setting
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Akram, Ali, Juang, Derek, Bustamante, Ranier, Liu, Lin, Earles, Ashley, Ho, Samuel B., Wang-Rodriguez, Jessica, Allison, James E., and Gupta, Samir
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- 2017
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39. Assessment of in vivo systemic toxicity and biodistribution of iron-doped silica nanoshells
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Mendez, Natalie, Liberman, Alexander, Corbeil, Jacqueline, Barback, Christopher, Viveros, Robert, Wang, James, Wang-Rodriguez, Jessica, Blair, Sarah L., Mattrey, Robert, Vera, David, Trogler, William, and Kummel, Andrew C.
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- 2017
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40. Smoking status regulates a novel panel of PIWI-interacting RNAs in head and neck squamous cell carcinoma
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Krishnan, Aswini R., Korrapati, Avinaash, Zou, Angela E., Qu, Yuanhao, Wang, Xiao Qi, Califano, Joseph A., Wang-Rodriguez, Jessica, Lippman, Scott M., Hovell, Melbourne F., and Ongkeko, Weg M.
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- 2017
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41. Nationwide Genomic Surveillance and Response to COVID-19: The VA SEQFORCE and SEQCURE Consortiums.
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Krishnan, Jay, Woods, Christopher W., Holodniy, Mark, Nicholson, Bradly P., Marconi, Vincent C., Ammons, Mary Cloud B., Jinadatha, Chetan, Pyarajan, Saiju, Wang-Rodriguez, Jessica, Garcia, Amanda P., and Battles, Jane K.
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- 2023
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42. Constitutive pro- and anti-inflammatory cytokine and growth factor response to exercise in leukocytes
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Zaldivar, Frank, Wang-Rodriguez, Jessica, Nemet, Dan, Schwindt, Christina, Galassetti, Pietro, Mills, Paul J, Wilson, Lori D, and Cooper, Dan M
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Biomedical and Clinical Sciences ,Clinical Sciences ,Mind and Body ,Clinical Research ,Aetiology ,2.1 Biological and endogenous factors ,Inflammatory and immune system ,Adolescent ,Adult ,Anti-Inflammatory Agents ,Cytokines ,Exercise ,Granulocytes ,Human Growth Hormone ,Humans ,Inflammation Mediators ,Insulin-Like Growth Factor I ,Intercellular Signaling Peptides and Proteins ,Interleukins ,Leukocytes ,Lymphocyte Count ,Lymphocytes ,Male ,Monocytes ,Tumor Necrosis Factor-alpha ,immunology ,interleukin-6 ,growth hormone ,intracellular ,Biological Sciences ,Medical and Health Sciences ,Physiology ,Biological sciences ,Biomedical and clinical sciences ,Health sciences - Abstract
Leukocytosis following exercise is a well-described phenomenon of stress/inflammatory activation in healthy humans. We hypothesized that, despite this increase in circulating inflammatory cells, exercise would paradoxically induce expression of both pro- and anti-inflammatory cytokines and growth factors within these cells. To test this hypothesis, 11 healthy adult men, 18-30 yr old, performed a 30-min bout of heavy cycling exercise; blood sampling was at baseline, end-exercise, and 60 min into recovery. The percentage of leukocytes positive for intracellular cytokines and growth factors and mean fluorescence intensity was obtained by flow cytometry. Proinflammatory cytokines (IL-1alpha, IL-2, IFN-gamma, and TNF-alpha), a pleiotropic cytokine (IL-6), and anti-inflammatory cytokines and growth factors [IL-4, IL-10, growth hormone (GH), and IGF-I] were examined. Median fluorescence intensity was not affected by exercise; however, we found a number of significant changes (P < 0.05 by mixed linear model and modified t-test) in the numbers of circulating cells positive for particular mediators. The pattern of expression reflected both pro- and anti-inflammatory functions. In T-helper lymphocytes, TNF-alpha, but also IL-6, and IL-4 were significantly increased. In monocytes, both IFN-gamma and IL-4 increased. B-lymphocytes positive for GH and IGF-I increased significantly. GH-positive granulocytes also significantly increased. Collectively, these observations indicate that exercise primes an array of pro- and anti-inflammatory and growth factor expression within circulating leukocytes, perhaps preparing the organism to effectively respond to a variety of stressors imposed by exercise.
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- 2006
43. Supplementary Figure 1 from Two-Dimensional Transcriptome Profiling: Identification of Messenger RNA Isoform Signatures in Prostate Cancer from Archived Paraffin-Embedded Cancer Specimens
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Li, Hai-Ri, primary, Wang-Rodriguez, Jessica, primary, Nair, T. Murlidharan, primary, Yeakley, Joanne M., primary, Kwon, Young-Soo, primary, Bibikova, Marina, primary, Zheng, Christina, primary, Zhou, Lixin, primary, Zhang, Kui, primary, Downs, Tracy, primary, Fu, Xiang-Dong, primary, and Fan, Jian-Bing, primary
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- 2023
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44. Supplementary Figure Legend from Two-Dimensional Transcriptome Profiling: Identification of Messenger RNA Isoform Signatures in Prostate Cancer from Archived Paraffin-Embedded Cancer Specimens
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Li, Hai-Ri, primary, Wang-Rodriguez, Jessica, primary, Nair, T. Murlidharan, primary, Yeakley, Joanne M., primary, Kwon, Young-Soo, primary, Bibikova, Marina, primary, Zheng, Christina, primary, Zhou, Lixin, primary, Zhang, Kui, primary, Downs, Tracy, primary, Fu, Xiang-Dong, primary, and Fan, Jian-Bing, primary
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- 2023
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45. Data from Diagnosis of Prostate Cancer Using Differentially Expressed Genes in Stroma
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Jia, Zhenyu, primary, Wang, Yipeng, primary, Sawyers, Anne, primary, Yao, Huazhen, primary, Rahmatpanah, Farahnaz, primary, Xia, Xiao-Qin, primary, Xu, Qiang, primary, Pio, Rebecca, primary, Turan, Tolga, primary, Koziol, James A., primary, Goodison, Steve, primary, Carpenter, Philip, primary, Wang-Rodriguez, Jessica, primary, Simoneau, Anne, primary, Meyskens, Frank, primary, Sutton, Manuel, primary, Lernhardt, Waldemar, primary, Beach, Thomas, primary, Monforte, Joseph, primary, McClelland, Michael, primary, and Mercola, Dan, primary
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- 2023
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46. Supplementary Tables 1-4, Figures 1-4 from Diagnosis of Prostate Cancer Using Differentially Expressed Genes in Stroma
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Jia, Zhenyu, primary, Wang, Yipeng, primary, Sawyers, Anne, primary, Yao, Huazhen, primary, Rahmatpanah, Farahnaz, primary, Xia, Xiao-Qin, primary, Xu, Qiang, primary, Pio, Rebecca, primary, Turan, Tolga, primary, Koziol, James A., primary, Goodison, Steve, primary, Carpenter, Philip, primary, Wang-Rodriguez, Jessica, primary, Simoneau, Anne, primary, Meyskens, Frank, primary, Sutton, Manuel, primary, Lernhardt, Waldemar, primary, Beach, Thomas, primary, Monforte, Joseph, primary, McClelland, Michael, primary, and Mercola, Dan, primary
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- 2023
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47. Supplementary Table 1 from Two-Dimensional Transcriptome Profiling: Identification of Messenger RNA Isoform Signatures in Prostate Cancer from Archived Paraffin-Embedded Cancer Specimens
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Li, Hai-Ri, primary, Wang-Rodriguez, Jessica, primary, Nair, T. Murlidharan, primary, Yeakley, Joanne M., primary, Kwon, Young-Soo, primary, Bibikova, Marina, primary, Zheng, Christina, primary, Zhou, Lixin, primary, Zhang, Kui, primary, Downs, Tracy, primary, Fu, Xiang-Dong, primary, and Fan, Jian-Bing, primary
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- 2023
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48. Supplementary Table 2 from Two-Dimensional Transcriptome Profiling: Identification of Messenger RNA Isoform Signatures in Prostate Cancer from Archived Paraffin-Embedded Cancer Specimens
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Li, Hai-Ri, primary, Wang-Rodriguez, Jessica, primary, Nair, T. Murlidharan, primary, Yeakley, Joanne M., primary, Kwon, Young-Soo, primary, Bibikova, Marina, primary, Zheng, Christina, primary, Zhou, Lixin, primary, Zhang, Kui, primary, Downs, Tracy, primary, Fu, Xiang-Dong, primary, and Fan, Jian-Bing, primary
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- 2023
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49. Development and validation of a standardized blood culture contamination definition and metric dashboard for a large health care system.
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Hancock, Jill A, Campbell, Sheldon, Jones, Makoto M, Wang-Rodriguez, Jessica, Workgroup, VHA Microbiology SME, and Klutts, J Stacey
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MEDICAL care ,VETERANS' health ,DEFINITIONS ,DATA recorders & recording ,PATIENT safety - Abstract
Objectives Blood culture contamination is a major problem in health care, with significant impacts on both patient safety and cost. Initiatives to reduce blood culture contamination require a reliable, consistent metric to track the success of interventions. The objective of our project was to establish a standardized definition of blood culture contamination suitable for use in a Veterans Health Administration (VHA) national data query, then to validate this definition and query. A secondary objective was to construct a national VHA data dashboard to display the data from this query that could be used in VHA quality improvement projects aimed at reducing blood culture contamination. Methods A VHA microbiology expert work group was formed to generate a standardized definition and oversee the validation studies. The standardized definition was used to generate data for calendar year 2021 using a Structured Query Language data query. Twelve VHA hospital microbiology laboratories compared the data from the query against their own locally derived contamination data and recorded those data in a data collection worksheet that all sites used. Data were collated and presented to the work group. Results More than 50,000 blood culture accessions were in the validation data set, with more than 1,200 contamination events. The overall blood culture contamination rate for the 12 facilities participating was 2.56% with local definitions and data and 2.43% with the standardized definitions and data query. The main differences noted between the 2 data sets were deemed to be issues in local definitions. The query and definition were then converted into a national data dashboard that all VHA facilities can now access. Conclusions A standardized definition for blood culture contamination and a national data query were validated for enterprise-wide VHA use. To our knowledge, this represents the first reported standardized, validated, and automated approach for calculating and tracking blood culture contamination. This tool will be key in quality initiatives aimed at reducing contamination events in VHA. [ABSTRACT FROM AUTHOR]
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- 2023
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50. Response to Gammal et al.
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Vassy, Jason L., Stone, Annjanette, Callaghan, John T., Mendes, Margaret, Meyer, Laurence J., Pratt, Victoria M., Przygodzki, Ronald M., Scheuner, Maren T., Wang-Rodriguez, Jessica, Schichman, Steven A., and for the VHA Clinical Pharmacogenetics Subcommittee
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- 2019
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