Your search keyword '"Jeffrey M. Trent"' showing total 10 results

1. 8q24 risk alleles and prostate cancer in African-Barbadian men

Author

Tae Hwi Schwantes-An, Anselm Hennis, Cheryl D. Cropp, Christiane M. Robbins, Joan E. Bailey-Wilson, Lyndon Waterman, John D. Carpten, Jeffrey M. Trent, Xin Sheng, Christopher A. Haiman, M. Cristina Leske, Barbara Nemesure, Ronald Worrell, and Suh Yuh Wu

Subjects

Genetics, Oncology, medicine.medical_specialty, education.field_of_study, business.industry, Urology, Population, Haplotype, Case-control study, Single-nucleotide polymorphism, medicine.disease, Prostate cancer, Internal medicine, Genotype, medicine, business, education, Genetic association, Founder effect

Abstract

BACKGROUND African American men (AA) exhibit a disproportionate share of prostate cancer (PRCA) incidence, morbidity, and mortality. Several genetic association studies have implicated select 8q24 loci in PRCA risk in AA. The objective of this investigation is to evaluate the association between previously reported 8q24 risk alleles and PRCA in African-Barbadian (AB) men known to have high rates of PRCA. METHODS Ten previously reported candidate tag SNPs were genotyped and/or imputed in the 8q24 region in 532 AB men with PRCA and 513 AB controls from the Prostate Cancer in a Black Population (PCBP) study. RESULTS Rs2124036 was significant in AB men, (OR = 2.7, 95% CI (1.3–5.3), P = 0.005, Empirical (max (T), corrected for multiple testing) P = 0.03) for the homozygous C/C genotype. Only a single SNP from this region remained statistically significant in our analysis of our AB population. These results may indicate the presence of a founder effect or due to the chosen SNPs not tagging an ancestral haplotype bearing the 8q24 risk allele(s) in this population or could reflect inadequate power to detect an association. We conducted a meta-analysis including our AB population along with two additional African Caribbean populations from Tobago and Jamaica for SNPs rs16901979 and rs1447295. Meta-analysis results were most significant for rs16901979 A allele (Z score 2.73; P = 0.006) with a summary OR = 1.31 (95% CI: 1.09–1.58). CONCLUSIONS Additional studies are needed to provide deeper genotype coverage to further interrogate the 8q24 region to understand its contribution to PRCA in this population. Prostate 74: 1579–1588, 2014. © 2014 Wiley Periodicals, Inc.

Published

2014

2. Contribution of HPC1 (RNASEL ) and HPCX variants to prostate cancer in a founder population

Author

Suzanne Leanza, Robert D. Burk, John D. Carpten, Jeffrey M. Trent, Joan E. Bailey-Wilson, Lorrie Smith, and Ilir Agalliu

Subjects

Genetics, education.field_of_study, Urology, Population, RNASEL Gene, Cancer, Locus (genetics), Biology, medicine.disease, Malignancy, Prostate cancer, Oncology, Genetic predisposition, medicine, education, Founder effect

Abstract

Background Prostate cancer is a genetically complex disease with locus and disease heterogeneity. The RNASEL gene and HPCX locus have been implicated in hereditary prostate cancer; however, their contributions to sporadic forms of this malignancy remain uncertain.

Published

2010

3. Genome-wide screen for prostate cancer susceptibility genes in men with clinically significant disease

Author

Jeffrey M. Trent, Elizabeth M. Gillanders, Sarah D. Isaacs, William B. Isaacs, Patrick C. Walsh, Bao Li Chang, S. Lilly Zheng, Jianfeng Xu, Deborah A. Meyers, and Kathy E. Wiley

Subjects

Male, PCA3, Oncology, medicine.medical_specialty, Pathology, Genetic Linkage, Urology, Disease, Severity of Illness Index, Metastasis, Prostate cancer, Risk Factors, Internal medicine, Biopsy, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Family history, Family Health, medicine.diagnostic_test, Genome, Human, business.industry, Prostatic Neoplasms, Cancer, medicine.disease, Etiology, business

Abstract

BACKGROUND One of the difficulties confronting genetic studies of prostate cancer is the complex and heterogeneous etiology. Given the high population frequency of lesions meeting the histological definition of prostate cancer, a significant portion of men with a positive family history may be diagnosed due to increased surveillance and associated higher likelihood of biopsy. Over diagnosis decreases power to detect genes that increase susceptibility to a clinically significant prostate cancer. METHODS We re-evaluated all 623 men with prostate cancer in our 188 hereditary prostate cancer families and identified a subset of 244 men with more aggressive disease based upon meeting at least one of the following clinical and/or pathologic criteria: tumor grade Gleason score ≥7, tumor stage T2c or higher, pretreatment PSA ≥20 ng/ml, rising PSA after treatment, evidence of metastasis, or death from prostate cancer. RESULTS Genome-wide screens were re-performed by defining men as affected only if they met the criteria for clinically significant disease. The new analyses identified stronger evidence for linkage in Xq27-28 and 22q, as well as several novel loci, including 3p and 9p. CONCLUSIONS Although, these results need to be confirmed in independent studies, our approach represents an important step to overcome the impact of over diagnosis in genetic studies of prostate cancer. Larger studies that incorporate this approach are needed. © 2005 Wiley-Liss, Inc.

Published

2005

4. Genome-wide scan for linkage in finnish hereditary prostate cancer (HPC) families identifies novel susceptibility loci at 11q14 and 3p25-26

Author

Diana Freas-Lutz, Jeffrey M. Trent, Mary Pat Jones, Tommi Kainu, Carol Markey, Mika P. Matikainen, Pasi A. Koivisto, Johanna Schleutker, Teuvo L.J. Tammela, Kenneth D. Gibbs, Derek Gildea, Olli Kallioniemi, Agnes Baffoe-Bonnie, Julie Albertus, Elizabeth M. Gillanders, Erica Riedesel, and Joan E. Bailey-Wilson

Subjects

Male, Genetic Linkage, Urology, Population, cancer predisposition, homogeneous population, Polymerase Chain Reaction, Statistics, Nonparametric, familiar cancer, Genetic determinism, Prostate cancer, SDG 3 - Good Health and Well-being, Stomach Neoplasms, Genetic linkage, Prostate, medicine, Genetic predisposition, Humans, Family, Genetic Predisposition to Disease, education, Finland, Aged, Aged, 80 and over, Linkage (software), Genetics, education.field_of_study, Autosome, Genome, Human, business.industry, Chromosomes, Human, Pair 11, Prostatic Neoplasms, DNA, Neoplasm, Sequence Analysis, DNA, Middle Aged, medicine.disease, medicine.anatomical_structure, Oncology, Female, Chromosomes, Human, Pair 3, business, Microsatellite Repeats, genetic susceptibility

Abstract

BACKGROUND In order to identify predisposition loci to hereditary prostate cancer (HPC), we performed a genome-wide linkage analysis using samples from a genetically homogeneous population, with 13 Finnish multiplex prostate cancer families. METHODS Altogether 87 DNA samples were genotyped from 13 families. Logarithm-of-odds (LOD) scores were calculated for all autosomes using FASTLINK and GENEHUNTER designating all unaffected men and all women as unknown. RESULTS The highest LOD scores in the affected-only analyses were found at 11q14, where the two-point LOD score was 2.97 (θ = 0.0 at D11S901), GENEHUNTER heterogeneity LOD (HLOD) of 3.36, and a non-parametric-linkage (NPL) score of 2.67 (P = 0.008). A second positive site was at 3p25-26, with a two-point LOD score of 2.57 (θ = 0.01 at D3S1297), HLOD of 2.15, and NPL score of 2.27 (P = 0.02). CONCLUSIONS The results suggest two HPC regions in the Finnish population, which have not been reported previously and warrant further study. Prostate 57: 280–289, 2003. © 2003 Wiley-Liss, Inc.

Published

2003

5. Genome-wide scan for prostate cancer susceptibility genes using families from the University of Michigan prostate cancer genetics project finds evidence for linkage on chromosome 17 nearBRCA1

Author

Erica Riedesel, Cralen Davis, W. Mark Brown, Jennifer Beebe Dimmer, Jeffrey M. Trent, Elizabeth M. Gillanders, Diana Freas-Lutz, James E. Montie, Carol Markey, Mary Pat Jones, Derek Gildea, Joel K. Campbell, Ethan M. Lange, Veda N. Giri, Julie Albertus, and Kathleen A. Cooney

Subjects

Male, Candidate gene, Genetic Linkage, Urology, Genes, BRCA1, Black People, Polymerase Chain Reaction, Genome, White People, Prostate cancer, Genetic linkage, medicine, Humans, Family, Genetic Predisposition to Disease, Age of Onset, Aged, Linkage (software), Genetics, Genome, Human, business.industry, Prostatic Neoplasms, DNA, Neoplasm, Sequence Analysis, DNA, Middle Aged, medicine.disease, Chromosome 17 (human), ELAC2, Oncology, Genetic marker, business, Chromosomes, Human, Pair 17, Microsatellite Repeats

Abstract

BACKGROUND Previous linkage studies have suggested prostate cancer susceptibility genes located on chromosomes 1, 20, and X. Several putative prostate cancer candidate genes have also been identified including RNASEL, MSR1, and ELAC2. Presently, these linkage regions and candidate genes appear to explain only a small proportion of hereditary prostate cancer cases suggesting the need for additional whole genome analyses. METHODS A genome-wide mode-of-inheritance-free linkage scan, using 405 genetic markers, was conducted on 175 pedigrees, the majority containing three or more affected individuals diagnosed with prostate cancer. Stratified linkage analyses were performed based on previously established criteria. RESULTS Results based on the entire set of 175 pedigrees showed strong suggestive evidence for linkage on chromosome 17q (LOD = 2.36), with strongest evidence coming from the subset of pedigrees with four or more affected individuals (LOD = 3.27). Race specific analyses revealed strong suggestive evidence for linkage in our African-American pedigrees on chromosome 22q (LOD = 2.35). CONCLUSIONS Genome-wide analysis of a large set of prostate cancer families indicates new areas of the genome that may harbor prostate cancer susceptibility genes. Specifically, our linkage results suggest that there is a prostate cancer susceptibility gene on chromosome 17 that is independent of ELAC2. Further research including combined analyses of independent genome-wide scan data may clarify the most important regions for future investigation. Prostate 57: 326–334, 2003. Published 2003 Wiley-Liss, Inc.

Published

2003

6. Genome-wide scan for prostate cancer susceptibility genes in the Johns Hopkins hereditary prostate cancer families

Author

Mary Pat Jones, Jeffrey M. Trent, Kathy E. Wiley, Sarah D. Isaacs, Erica Riedesel, S. Lilly Zheng, Bao Li Chang, Elizabeth M. Gillanders, Diana Freas-Lutz, Jianfeng Xu, Carol Markey, Julie Albertus, Patrick C. Walsh, Derek Gildea, Deborah A. Meyers, and William B. Isaacs

Subjects

Genetic Markers, Male, Genetic Linkage, Urology, Chromosome 9, Disease, Biology, Polymerase Chain Reaction, Statistics, Nonparametric, Genetic determinism, Prostate cancer, Prostate, Genetic linkage, Genotype, medicine, Humans, Family, Genetic Predisposition to Disease, Aged, Genetics, Genome, Human, Prostatic Neoplasms, DNA, Neoplasm, Sequence Analysis, DNA, Middle Aged, medicine.disease, medicine.anatomical_structure, Oncology, Genetic marker

Abstract

BACKGROUND Although the subject of intensive study, the genetic influences responsible for familial clustering of prostate cancer remain largely unidentified. Genome-wide scans for linkage in prostate cancer families can be used to systematically search for genes capable of affecting risk for the disease. METHODS All available family members from 188 families, each having at least three first-degree relatives affected with prostate cancer, were genotyped at 406 markers distributed across the genome at average intervals of less than 10 cM. Genotype data was analyzed using primarily a non-parametric, multipoint approach, although parametric analyses were performed as well. RESULTS The strongest evidence for linkage was observed at D4S1615, at 4q21 (LOD of 2.8, P = 0.0002). Two other regions had LOD scores over 2.0: at 9q34 (marker D9S1826, LOD = 2.17, P = 0.0008) and at 2q23 (marker D2S151, LOD = 2.03, P = 0.001). An additional 12 regions had LOD scores over 1.0, including markers at 1q24-25 and 7q22 having scores >1.6. Stratifying the linkage results by age of diagnosis indicated that the linkages to chromosomes 2 and 4 were strongest in families with early and late ages of diagnosis, respectively. CONCLUSIONS Our data implicate several new loci as harboring prostate cancer susceptibility genes, and provide confirmatory evidence of linkage at several loci identified previously in other genome-wide scans, including the three regions (4q21, 9q34, and 2q23) with strongest evidence for prostate cancer linkage. These data also emphasize the need to combine linkage data from large numbers of prostate cancer families in efforts to effectively address the extensive heterogeneity that characterizes genetic aspects of this disease. Prostate 57: 320–325, 2003. © 2003 Wiley-Liss, Inc.

Published

2003

7. Gene expression signature of benign prostatic hyperplasia revealed by cDNA microarray analysis

Author

Thomas A. Dunn, Jeffrey M. Trent, Jun Luo, Jurga Sauvageot, Charles M. Ewing, Yi Chen, and William B. Isaacs

Subjects

Adult, Male, PCA3, Pathology, medicine.medical_specialty, Candidate gene, Urology, Prostatic Hyperplasia, Biology, Kruppel-Like Factor 4, Prostate, Thrombospondin 4, Gene expression, medicine, Humans, education, Aged, Oligonucleotide Array Sequence Analysis, Aged, 80 and over, education.field_of_study, Microarray analysis techniques, Gene Expression Profiling, Middle Aged, Molecular biology, Gene expression profiling, medicine.anatomical_structure, Oncology, Gene chip analysis

Abstract

BACKGROUND Despite the high prevalence of benign prostatic hyperplasia (BPH) in the aging male, little is known regarding the etiology of this disease. A better understanding of the molecular etiology of BPH would be facilitated by a comprehensive analysis of gene expression patterns that are characteristic of benign growth in the prostate gland. Since genes differentially expressed between BPH and normal prostate tissues are likely to reflect underlying pathogenic mechanisms involved in the development of BPH, we performed comparative gene expression analysis using cDNA microarray technology to identify candidate genes associated with BPH. METHODS Total RNA was extracted from a set of 9 BPH specimens from men with extensive hyperplasia and a set of 12 histologically normal prostate tissues excised from radical prostatectomy specimens. Each of these 21 RNA samples was labeled with Cy3 in a reverse transcription reaction and cohybridized with a Cy5 labeled common reference sample to a cDNA microarray containing 6,500 human genes. Normalized fluorescent intensity ratios from each hybridization experiment were extracted to represent the relative mRNA abundance for each gene in each sample. Weighted gene and random permutation analyses were performed to generate a subset of genes with statistically significant differences in expression between BPH and normal prostate tissues. Semi-quantitative PCR analysis was performed to validate differential expression. RESULTS A subset of 76 genes involved in a wide range of cellular functions was identified to be differentially expressed between BPH and normal prostate tissues. Semi-quantitative PCR was performed on 10 genes and 8 were validated. Genes consistently upregulated in BPH when compared to normal prostate tissues included: a restricted set of growth factors and their binding proteins (e.g. IGF-1 and -2, TGF-β3, BMP5, latent TGF-β binding protein 1 and -2); hydrolases, proteases, and protease inhibitors (e.g. neuropathy target esterase, MMP2, alpha-2-macroglobulin); stress response enzymes (e.g. COX2, GSTM5); and extracellular matrix molecules (e.g. laminin alpha 4 and beta 1, chondroitin sulfate proteoglycan 2, lumican). Genes consistently expressing less mRNA in BPH than in normal prostate tissues were less commonly observed and included the transcription factor KLF4, thrombospondin 4, nitric oxide synthase 2A, transglutaminase 3, and gastrin releasing peptide. CONCLUSIONS We identified a diverse set of genes that are potentially related to benign prostatic hyperplasia, including genes both previously implicated in BPH pathogenesis as well as others not previously linked to this disease. Further targeted validation and investigations of these genes at the DNA, mRNA, and protein levels are warranted to determine the clinical relevance and possible therapeutic utility of these genes. Prostate 51: 189–200, 2002. © 2002 Wiley-Liss, Inc.

Published

2002

8. 8q24 risk alleles and prostate cancer in African-Barbadian men

Author

Cheryl D, Cropp, Christiane M, Robbins, Xin, Sheng, Anselm J M, Hennis, John D, Carpten, Lyndon, Waterman, Ronald, Worrell, Tae-Hwi, Schwantes-An, Jeffrey M, Trent, Christopher A, Haiman, M Cristina, Leske, Suh-Yuh, Wu, Joan E, Bailey-Wilson, and Barbara, Nemesure

Subjects

Male, Genotype, Incidence, Prostatic Neoplasms, Barbados, Polymorphism, Single Nucleotide, Article, Caribbean Region, Haplotypes, Risk Factors, Case-Control Studies, Africa, Humans, Genetic Predisposition to Disease, Alleles, Chromosomes, Human, Pair 8

Abstract

African American men (AA) exhibit a disproportionate share of prostate cancer (PRCA) incidence, morbidity, and mortality. Several genetic association studies have implicated select 8q24 loci in PRCA risk in AA. The objective of this investigation is to evaluate the association between previously reported 8q24 risk alleles and PRCA in African-Barbadian (AB) men known to have high rates of PRCA.Ten previously reported candidate tag SNPs were genotyped and/or imputed in the 8q24 region in 532 AB men with PRCA and 513 AB controls from the Prostate Cancer in a Black Population (PCBP) study.Rs2124036 was significant in AB men, (OR = 2.7, 95% CI (1.3-5.3), P = 0.005, Empirical (max (T), corrected for multiple testing) P = 0.03) for the homozygous C/C genotype. Only a single SNP from this region remained statistically significant in our analysis of our AB population. These results may indicate the presence of a founder effect or due to the chosen SNPs not tagging an ancestral haplotype bearing the 8q24 risk allele(s) in this population or could reflect inadequate power to detect an association. We conducted a meta-analysis including our AB population along with two additional African Caribbean populations from Tobago and Jamaica for SNPs rs16901979 and rs1447295. Meta-analysis results were most significant for rs16901979 A allele (Z score 2.73; P = 0.006) with a summary OR = 1.31 (95% CI: 1.09-1.58).Additional studies are needed to provide deeper genotype coverage to further interrogate the 8q24 region to understand its contribution to PRCA in this population.

Published

2013

9. Association of prostate cancer risk with SNPs in regions containing androgen receptor binding sites captured by ChIP-On-chip analyses

Author

Edward Suh, Yi Zhu, James Lowey, S. Lilly Zheng, John D. Carpten, Jishan Sun, Kevin Campbell, Jeffrey M. Trent, Jin Woo Kim, Yizhen Lu, Junjie Feng, Henrik Grönberg, Daru Lu, David Duggan, Tao Jin, Latchezar Dimitrov, Wennuan Liu, Seong Tae Kim, Jielin Sun, Andrew Karim Kader, William B. Isaacs, Zheng Zhang, and Jianfeng Xu

Subjects

Male, Urology, Molecular Sequence Data, Single-nucleotide polymorphism, Genome-wide association study, Biology, Genome, Polymorphism, Single Nucleotide, Article, Androgen receptor binding, Cohort Studies, Prostate cancer, Risk Factors, medicine, Humans, Genetic Predisposition to Disease, Genetic association, Oligonucleotide Array Sequence Analysis, Genetics, Binding Sites, Base Sequence, Prostatic Neoplasms, DNA, Neoplasm, ChIP-on-chip, medicine.disease, Androgen receptor, Oncology, Receptors, Androgen, Case-Control Studies, Genome-Wide Association Study

Abstract

BACKGROUND Genome-wide association studies (GWAS) have identified approximately three dozen single nucleotide polymorphisms (SNPs) consistently associated with prostate cancer (PCa) risk. Despite the reproducibility of these associations, the molecular mechanism for most of these SNPs has not been well elaborated as most lie within non-coding regions of the genome. Androgens play a key role in prostate carcinogenesis. Recently, using ChIP-on-chip technology, 22,447 androgen receptor (AR) binding sites have been mapped throughout the genome, greatly expanding the genomic regions potentially involved in androgen-mediated activity. METHODOLOGY/PRINCIPAL FINDINGS To test the hypothesis that sequence variants in AR binding sites are associated with PCa risk, we performed a systematic evaluation among two existing PCa GWAS cohorts; the Johns Hopkins Hospital and the Cancer Genetic Markers of Susceptibility (CGEMS) study population. We demonstrate that regions containing AR binding sites are significantly enriched for PCa risk-associated SNPs, that is, more than expected by chance alone. In addition, compared with the entire genome, these newly observed risk-associated SNPs in these regions are significantly more likely to overlap with established PCa risk-associated SNPs from previous GWAS. These results are consistent with our previous finding from a bioinformatics analysis that one-third of the 33 known PCa risk-associated SNPs discovered by GWAS are located in regions of the genome containing AR binding sites. CONCLUSIONS/SIGNIFICANCE The results to date provide novel statistical evidence suggesting an androgen-mediated mechanism by which some PCa associated SNPs act to influence PCa risk. However, these results are hypothesis generating and ultimately warrant testing through in-depth molecular analyses. Prostate 72:376–385, 2012. © 2011 Wiley Periodicals, Inc.

Published

2011

10. Genome-wide linkage of 77 families from the African American Hereditary Prostate Cancer study (AAHPC)

Author

Terry Mason, Rick A. Kittles, Kate Berg, John D. Carpten, Jeffrey M. Trent, Francis S. Collins, Curtis A. Pettaway, Paulette Furbert-Harris, James T. Bennett, Christiane M. Robbins, Meghan Klaric, Gerald Hoke, Derek Gildea, William Boykin, Erica Riedesel, Chiledum Ahaghotu, Mary Pat Jones, Elizabeth M. Gillanders, Agnes Baffoe-Bonnie, Julie Albertus, Mezbah U. Faruque, Tracy Moses, Asha George, Charmaine D.M. Royal, Sally P. Weinrich, Liang Ou, Srinivasan Vijayakumar, Isaac Powell, Erica Lockwood, Georgia M. Dunston, and Joan E. Bailey-Wilson

Subjects

Genetic Markers, Male, Genetic Linkage, Urology, Locus (genetics), Disease, Genome, Genetic determinism, Prostate cancer, Genetic linkage, Genetic predisposition, Medicine, Humans, Gene, Aged, Genetics, business.industry, Genome, Human, Prostatic Neoplasms, Middle Aged, medicine.disease, United States, Pedigree, Black or African American, Oncology, Lod Score, business

Abstract

BACKGROUND The African American Hereditary Prostate Cancer (AAHPC) Study was designed to recruit families with early-onset disease fulfilling criteria of ≥4 affected. METHODS We present a ∼10 cM genome-wide linkage (GWL) analysis on 77 families including 254 affected and 274 unaffected genotyped. RESULTS Linkage analysis revealed three chromosomal regions with GENEHUNTER multipoint HLOD scores ≥1.3 for all 77 families at 11q22, 17p11, and Xq21. One family yielded genome-wide significant evidence of linkage (LOD = 3.5) to the 17p11 region with seven other families ≥2.3 in this region. Twenty-nine families with no-male-to-male (MM) transmission gave a peak HLOD of 1.62 (α = 0.33) at the Xq21 locus. Two novel peaks ≥0.91 for the 16 families with ‘>6 affected’ occurred at 2p21 and 22q12. CONCLUSIONS These chromosomal regions in the genome warrant further follow-up based on the hypothesis of multiple susceptibility genes with modest effects, or several major genes segregating in small subsets of families. Prostate 67:22–31, 2007. © 2006 Wiley-Liss, Inc.

Published

2006