Search

Your search keyword '"S. Lilly Zheng"' showing total 205 results
Start Over Author "S. Lilly Zheng" Language undetermined
205 results on '"S. Lilly Zheng"'

1. Association of rare, recurrent nonsynonymous variants in the germline of prostate cancer patients of African ancestry

Author

Jianfeng Xu, Jun Wei, Jennifer Beebe-Dimmer, Zhuqing Shi, Christopher Sample, Guifang Yan, Andrew Rifkin, Azita Sadeghpour, Marta Gielzak, Sodam Choi, David Moon, S. Lilly Zheng, Brian Helfand, Patrick Walsh, Kathleen Cooney, and William Isaacs

Subjects
Oncology, Urology
Abstract

Background: Although men of African ancestry (AA) have the highest mortality rate from prostate cancer (PCa), relatively little is known about the germline variants that are associated with PCa risk in AA men. The goal of this study is to systematically evaluate rare, recurrent nonsynonymous variants across the exome for their association with PCa in AA men. Methods: Whole exome sequencing (WES) of germline DNA in two AA PCa patient cohorts of Johns Hopkins Hospital (N=960) and Wayne State University (N=747) was performed. All nonsynonymous variants presented in both case cohorts, with a carrier rate between 0.3% and 1%, were identified. Their carrier rates were compared with rates from 8,128 African/African American (AFR) control subjects from The Genome Aggregation Database (gnomAD) using Fisher’s exact test. Significant variants, defined as false discovery rate (FDR) adjusted p-value £0.05, were further evaluated in AA PCa cases (N=132) and controls (N=1,184) from the UK Biobank (UKB). Results: Two variants reached a pre-specified statistical significance level. The first was p.R14Q in GPRC5C (found in 0.47% of PCa cases and 0.01% of population controls); odds ratio (OR) for PCa was 37.46 (95%CI 4.68-299.72), pexact=7.01E-06, FDR adjusted p-value=0.05. The second was p.R511Q in IGF1R (found in 0.53% of PCa cases and 0.01% of population controls); OR for PCa was 21.54 (95%CI 4.65-99.76), pexact=5.51E-06, FDR adjusted p-value=0.05. The mean percentage of African ancestry was similar between variant carriers and non-carriers of each variant, p>0.05. In the UKB AA men, GPRC5C R14Q was 0.76% and 0.08% in cases and controls, respectively, OR for PCa was 9.00 (95%CI 0.56-145.23), pexact =0.19. However, IGF1R R511Q was not found in cases or controls. Conclusions: This WES study identified two rare, recurrent nonsynonymous PCa risk-associated variants in AA. Confirmation in additional large populations of AA PCa cases and controls is required.

Published
2022
Full Text
View/download PDF

2. Data from Identifying Phased Mutations and Complex Rearrangements in Human Prostate Cancer Cell Lines through Linked-Read Whole-Genome Sequencing

Author

Srinivasan Yegnasubramanian, William G. Nelson, Sarah J. Wheelan, William B. Isaacs, Christina DeStefano Shields, Jianfeng Xu, S. Lilly Zheng, Michael C. Haffner, Jonathan B. Coulter, McKinzie A. Garrison, Alyza Skaist, Ajay Vaghasia, Harshath Gupta, Anuj Gupta, and Minh-Tam Pham

Abstract

A limited number of cell lines have fueled the majority of preclinical prostate cancer research, but their genomes remain incompletely characterized. Here, we utilized whole-genome linked-read sequencing for comprehensive characterization of phased mutations and rearrangements in the most commonly used cell lines in prostate cancer research including PC3, LNCaP, DU145, CWR22Rv1, VCaP, LAPC4, MDA-PCa-2b, RWPE-1, and four derivative castrate-resistant (CR) cell lines LNCaP_Abl, LNCaP_C42b, VCaP-CR, and LAPC4-CR. Phasing of mutations allowed determination of “gene-level haplotype” to assess whether genes harbored heterozygous mutations in one or both alleles. Phased structural variant analysis allowed identification of complex rearrangement chains consistent with chromothripsis and chromoplexy. In addition, comparison of parental and derivative CR lines revealed previously known and novel genomic alterations associated with the CR phenotype.Implications:This study therefore comprehensively characterized phased genomic alterations in the commonly used prostate cancer cell lines, providing a useful resource for future prostate cancer research.

Published
2023
Full Text
View/download PDF

3. Supplementary Figure from Identifying Phased Mutations and Complex Rearrangements in Human Prostate Cancer Cell Lines through Linked-Read Whole-Genome Sequencing

Author

Srinivasan Yegnasubramanian, William G. Nelson, Sarah J. Wheelan, William B. Isaacs, Christina DeStefano Shields, Jianfeng Xu, S. Lilly Zheng, Michael C. Haffner, Jonathan B. Coulter, McKinzie A. Garrison, Alyza Skaist, Ajay Vaghasia, Harshath Gupta, Anuj Gupta, and Minh-Tam Pham

Abstract

Supplementary Figure from Identifying Phased Mutations and Complex Rearrangements in Human Prostate Cancer Cell Lines through Linked-Read Whole-Genome Sequencing

Published
2023
Full Text
View/download PDF

4. Supplementary Data from Identifying Phased Mutations and Complex Rearrangements in Human Prostate Cancer Cell Lines through Linked-Read Whole-Genome Sequencing

Author

Srinivasan Yegnasubramanian, William G. Nelson, Sarah J. Wheelan, William B. Isaacs, Christina DeStefano Shields, Jianfeng Xu, S. Lilly Zheng, Michael C. Haffner, Jonathan B. Coulter, McKinzie A. Garrison, Alyza Skaist, Ajay Vaghasia, Harshath Gupta, Anuj Gupta, and Minh-Tam Pham

Abstract

Supplementary Data from Identifying Phased Mutations and Complex Rearrangements in Human Prostate Cancer Cell Lines through Linked-Read Whole-Genome Sequencing

Published
2023
Full Text
View/download PDF

5. Supplementary Figure 1 from Distinct Genomic Alterations in Prostate Tumors Derived from African American Men

Author

Jianfeng Xu, William B. Isaacs, Karen S. Sfanos, Sarah Ernst, W. Kyle Resurreccion, Jun Wei, Johnie Gallagher, Jishan Sun, Lin Wei, Rong Na, S. Lilly Zheng, and Wennuan Liu

Abstract

Somatically acquired exon mutations of PIK3CA identified by targeted deeper NGS in PCa of AA/black are compared with those reported in PCa of EA/white in the GDC (upper panel); and CNAs together with B-allele frequency identified by OncoScan (lower panels) in 2 example tumors harboring missense mutation p.I391M. In upper panel, blue = missense, green = synonymous, purple arrow marking a mutation previously reported in AA PCa.

Published
2023
Full Text
View/download PDF

6. Supplementary Tables 1-6 from Distinct Genomic Alterations in Prostate Tumors Derived from African American Men

Author

Jianfeng Xu, William B. Isaacs, Karen S. Sfanos, Sarah Ernst, W. Kyle Resurreccion, Jun Wei, Johnie Gallagher, Jishan Sun, Lin Wei, Rong Na, S. Lilly Zheng, and Wennuan Liu

Abstract

Supplementary Table 1. Gleason grade and TNM stage of the tumors from 83 African American men. Supplementary Table 2. Somatic exon mutations identified by Mutect2 in tumors of 77 AA men. Supplementary Table 3. Performance of the Agilent SureSelect and NimbleGen SeqCap enrichment. Supplementary Table 4. Frequency of exon somatic mutations in targeted 39 genes among 77 AA tumors. Supplementary Table 5. Number of EA/white and AA/black patients in different cohorts used for analysis of DNA copy number alterations. Supplementary Table 6. Comparing the frequency of 13 most common CNAs in EA/white and AA/black PCa.

Published
2023
Full Text
View/download PDF

7. Data from Distinct Genomic Alterations in Prostate Tumors Derived from African American Men

Author

Jianfeng Xu, William B. Isaacs, Karen S. Sfanos, Sarah Ernst, W. Kyle Resurreccion, Jun Wei, Johnie Gallagher, Jishan Sun, Lin Wei, Rong Na, S. Lilly Zheng, and Wennuan Liu

Abstract

We aim to understand, from acquired genetic alterations in tumors, why African American (AA) men are more likely to develop aggressive prostate cancer. By analyzing somatic mutations in 39 genes using deeper next-generation sequencing with an average depth of 2,522 reads for tumor DNA and genome-wide DNA copy-number alterations (CNA) in prostate cancer in a total of 171 AA/black men and comparing with those in 860 European American (EA)/white men, we here present several novel findings. First, >35% of AA men harbor damaging mutations in APC, ATM, BRCA2, KDM6A, KMT2C, KMT2D, MED12, ZFHX3, and ZMYM3, each with >1% of mutated copies. Second, among genes with >10% of mutated copies in tumor cells, ZMYM3 is the most frequently mutated gene in AA prostate cancer. In a patient's tumor with >96% frameshift mutations of ZMYM3, we find allelic imbalances in 10 chromosomes, including losses of five and gains of another four chromosomes, suggesting its role in maintaining genomic integrity. Third, when compared to prostate cancer in EA/white men, a higher frequency of CNAs of MYC, THADA, NEIL3, LRP1B, BUB1B, MAP3K7, BNIP3L and RB1, and a lower frequency of deletions of RYBP, TP53, and TMPRSS2-ERG are observed in AA/black men. Finally, for the above genes with higher frequency of CNAs in AA than in EA, deletion of MAP3K7, BNIP3L, NEIL3 or RB1, or gain of MYC significantly associates with both higher Gleason grade and advanced pathologic stage in AA/black men. Deletion of THADA associates with advanced pathologic stage only.Implications:A higher frequency of damaging mutation in ZMYM3 causing genomic instability along with higher frequency of altered genomic regions including deletions of MAP3K7, BNIP3L, RB1, and NEIL3, and gain of MYC appear to be distinct somatically acquired genetic alterations that may contribute to more aggressive prostate cancer in AA/black men.

Published
2023
Full Text
View/download PDF

14. Supplementary Figure 2 from Elevation of Stromal-Derived Mediators of Inflammation Promote Prostate Cancer Progression in African-American Men

Author

Omar E. Franco, Donald J. Vander Griend, Brandon L. Pierce, Susan E. Crawford, Charles B. Brendler, Jianfeng Xu, S. Lilly Zheng, Yuan Ji, Rodrigo Javier, and Marc Gillard

Abstract

In vitro proliferation of fibroblasts from AA and EA patients. Proliferation of PCa cell lines exposed to CM from AA and EA prostate fibroblasts

Published
2023
Full Text
View/download PDF

16. Data from A Genome-Wide Survey over the ChIP-On-Chip Identified Androgen Receptor-Binding Genomic Regions Identifies a Novel Prostate Cancer Susceptibility Locus at 12q13.13

Author

Jianfeng Xu, S. Lilly Zheng, William B. Isaacs, Henrik Gronberg, Zheng Zhang, Zhong Wang, Yizhen Lu, Seong-Tae Kim, Jielin Sun, and Junjie Feng

Abstract

Background: The molecular mechanisms for the genome-wide association studies (GWAS)-identified prostate cancer (PCa) risk-associated single-nucleotide polymorphisms (SNP) remain largely unexplained. One recent finding that the PCa risk SNPs are enriched in genomic regions containing androgen receptor (AR)-binding sites has suggested altered AR signaling as a potentially important mechanism.Methods: To explore novel associations by leveraging this knowledge, we utilized a meta-analysis previously done over SNPs harbored in ChIP-on-chip identified AR-binding genomic regions using the GWAS data from the Johns Hopkins Hospital (JHH) and the Cancer Genetic Markers of Susceptibility (CGEMS) study, and subsequently evaluated the top associations in a third population from the CAncer of the Prostate in Sweden (CAPS) study.Results: One SNP (rs4919743: G>A), located at the KRT8 locus at 12q13.13 which encodes a keratin protein (K8) long used as a prostate epithelial malignancy marker and implicated in the tumorigenesis of several cancer types, was identified to be associated with PCa risk. The frequency of its minor “A” allele was consistently higher in PCa cases than in controls in all three study populations, with a combined OR of 1.22 (95% CI: 1.13–1.32) and an overall P value of 4.50 × 10−7 (Bonferroni corrected, P = 0.006).Conclusion: We have identified a novel genetic locus that is associated with PCa risk.Impact: This study illustrated the great potential of prior biological knowledge in facilitating the search for novel disease-associated genetic loci. This finding warrants further replication in other studies. Cancer Epidemiol Biomarkers Prev; 20(11); 2396–403. ©2011 AACR.

Published
2023
Full Text
View/download PDF

17. Data from Elevation of Stromal-Derived Mediators of Inflammation Promote Prostate Cancer Progression in African-American Men

Author

Omar E. Franco, Donald J. Vander Griend, Brandon L. Pierce, Susan E. Crawford, Charles B. Brendler, Jianfeng Xu, S. Lilly Zheng, Yuan Ji, Rodrigo Javier, and Marc Gillard

Abstract

Progress in prostate cancer racial disparity research has been hampered by a lack of appropriate research tools and better understanding of the tumor biology. Recent gene expression studies suggest that the tumor microenvironment (TME) may contribute to racially disparate clinical outcomes in prostate cancer. Analysis of the prostate TME has shown increased reactive stroma associated with chronic inflammatory infiltrates in African-American (AA) compared with European-American (EA) patients with prostate cancer. To better understand stromal drivers of changes in TME, we isolated prostate fibroblasts (PrF) from AA (PrF−AA) and EA (PrF−EA) prostate cancer tissues and studied their functional characteristics. PrF−AA showed increased growth response to androgens FGF2 and platelet-derived growth factor. Compared with PrF−EA, conditioned media from PrF−AA significantly enhanced the proliferation and motility of prostate cancer cell lines. Expression of markers associated with myofibroblast activation (αSMA, vimentin, and tenascin-C) was elevated in PrF−AA. In vivo tumorigenicity of an AA patient–derived prostatic epithelial cell line E006AA was significantly increased in the presence of PrF−AA compared with PrF−EA, and RNA-seq data and cytokine array analysis identified a panel of potential proinflammatory paracrine mediators (BDNF, CHI3L1, DPPIV, FGF7, IL18BP, IL6, and VEGF) to be enriched in PrF−AA. E006AA cell lines showed increased responsiveness to BDNF ligand compared with EA-derived LNCaP and C4-2B cells. Addition of a TrkB-specific antagonist significantly reduced the protumorigenic effects induced by PrF−AA compared with PrF−EA. These findings suggest that fibroblasts in the TME of AA patients may contribute to the health disparity observed in the incidence and progression of prostate cancer tumors.Significance: These findings suggest that stromal cells in the tumor microenvironment of African-American men promote progression of prostate cancer by increasing levels of a specific set of pro-inflammatory molecules compared with European-American men.Graphical Abstract: http://cancerres.aacrjournals.org/content/canres/78/21/6134/F1.large.jpg. Cancer Res; 78(21); 6134–45. ©2018 AACR.

Published
2023
Full Text
View/download PDF

19. Data from Comparison of Two Methods for Estimating Absolute Risk of Prostate Cancer Based on Single Nucleotide Polymorphisms and Family History

Author

Jianfeng Xu, Henrik Grönberg, William Isaacs, S. Lilly Zheng, A. Karim Kader, Fredrik Wiklund, Zheng Zhang, Tao Jin, Seong-Tae Kim, Yi Zhu, Jielin Sun, and Fang-Chi Hsu

Abstract

Disease risk–associated single nucleotide polymorphisms (SNP) identified from genome-wide association studies have the potential to be used for disease risk prediction. An important feature of these risk-associated SNPs is their weak individual effect but stronger cumulative effect on disease risk. Several approaches are commonly used to model the combined effect in risk prediction, but their performance is unclear. We compared two methods to model the combined effect of 14 prostate cancer risk–associated SNPs and family history for the estimation of absolute risk for prostate cancer in a population-based case-control study in Sweden (2,899 cases and 1,722 controls). Method 1 weighs each risk allele equally using a simple method of counting the number of risk alleles, whereas method 2 weighs each risk SNP differently based on its odds ratio. We found considerable differences between the two methods. Absolute risk estimates from method 1 were generally higher than those of method 2, especially among men at higher risk. The difference in the overall discriminative performance, measured by area under the curve of the receiver operating characteristic, was small between method 1 (0.614) and method 2 (0.618), P = 0.20. However, the performance of these two methods in identifying high-risk individuals (2- or 3-fold higher than average risk), measured by positive predictive values, was higher for method 2 than for method 1. These results suggest that method 2 is superior to method 1 in estimating absolute risk if the purpose of risk prediction is to identify high-risk individuals. Cancer Epidemiol Biomarkers Prev; 19(4); 1083–8. ©2010 AACR.

Published
2023
Full Text
View/download PDF

21. Supplementary Figure 1 from Elevation of Stromal-Derived Mediators of Inflammation Promote Prostate Cancer Progression in African-American Men

Author

Omar E. Franco, Donald J. Vander Griend, Brandon L. Pierce, Susan E. Crawford, Charles B. Brendler, Jianfeng Xu, S. Lilly Zheng, Yuan Ji, Rodrigo Javier, and Marc Gillard

Abstract

Assessment of collagen deposition and neoangiogenesis in PCa samples from AA and EA patients. Quantitation of IHC staining of stromal markers

Published
2023
Full Text
View/download PDF

23. Supplementary Table 1 from Comparison of Two Methods for Estimating Absolute Risk of Prostate Cancer Based on Single Nucleotide Polymorphisms and Family History

Author

Jianfeng Xu, Henrik Grönberg, William Isaacs, S. Lilly Zheng, A. Karim Kader, Fredrik Wiklund, Zheng Zhang, Tao Jin, Seong-Tae Kim, Yi Zhu, Jielin Sun, and Fang-Chi Hsu

Abstract

Supplementary Table 1 from Comparison of Two Methods for Estimating Absolute Risk of Prostate Cancer Based on Single Nucleotide Polymorphisms and Family History

Published
2023
Full Text
View/download PDF

25. Supplementary Table 2 from Comparison of Two Methods for Estimating Absolute Risk of Prostate Cancer Based on Single Nucleotide Polymorphisms and Family History

Author

Jianfeng Xu, Henrik Grönberg, William Isaacs, S. Lilly Zheng, A. Karim Kader, Fredrik Wiklund, Zheng Zhang, Tao Jin, Seong-Tae Kim, Yi Zhu, Jielin Sun, and Fang-Chi Hsu

Abstract

Supplementary Table 2 from Comparison of Two Methods for Estimating Absolute Risk of Prostate Cancer Based on Single Nucleotide Polymorphisms and Family History

Published
2023
Full Text
View/download PDF

27. Supplementary Figure 1 from A Novel Prostate Cancer Susceptibility Locus at 19q13

Author

S. Lilly Zheng, Jianfeng Xu, Henrik Grönberg, William B. Isaacs, John D. Carpten, David Duggan, Patrick C. Walsh, Bao-Li Chang, Wennuan Liu, Zheng Zhang, Seong-Tae Kim, Yi Zhu, Pär Stattin, Zhengrong Gao, Lina D. Purcell, Kathleen E. Wiley, Sarah D. Isaacs, Fredrik Wiklund, Jielin Sun, and Fang-Chi Hsu

Abstract

Supplementary Figure 1 from A Novel Prostate Cancer Susceptibility Locus at 19q13

Published
2023
Full Text
View/download PDF

28. Data from Association of a Germ-Line Copy Number Variation at 2p24.3 and Risk for Aggressive Prostate Cancer

Author

Bao-Li Chang, S. Lilly Zheng, Henrik Grönberg, William B. Isaacs, John D. Carpten, David Duggan, Jianfeng Xu, Pär Stattin, Sarah D. Isaacs, Kathleen Wiley, Fredrik Wiklund, Jielin Sun, Seong-Tae Kim, Scott Zhang, Yi Zhu, Ge Li, Jishan Sun, and Wennuan Liu

Abstract

We searched for deletions in the germ-line genome among 498 aggressive prostate cancer cases and 494 controls from a population-based study in Sweden [CAncer of the Prostate in Sweden (CAPS)] using Affymetrix SNP arrays. By comparing allele intensities of ∼500,000 SNP probes across the genome, a germ-line deletion at 2p24.3 was observed to be significantly more common in cases (12.63%) than in controls (8.28%); P = 0.028. To confirm the association, we genotyped this germ-line copy number variation (CNV) in additional subjects from CAPS and from Johns Hopkins Hospital (JHH). Overall, among 4,314 cases and 2,176 controls examined, the CNV was significantly associated with prostate cancer risk [odds ratio (OR), 1.25; 95% confidence interval (95% CI), 1.06–1.48; P = 0.009]. More importantly, the association was stronger for aggressive prostate cancer (OR, 1.31; 95% CI, 1.08–1.58; P = 0.006) than for nonaggressive prostate cancer (OR, 1.19; 95% CI, 0.98–1.45; P = 0.08). The biological effect of this germ-line CNV is unknown because no known gene resides in the deletion. Results from this study represent the first novel germ-line CNV that was identified from a genome-wide search and was significantly, but moderately, associated with prostate cancer risk. Additional confirmation of this association and functional studies are warranted. [Cancer Res 2009;69(6):2176–9]

Published
2023
Full Text
View/download PDF

29. Supplementary Table 1 from A Novel Prostate Cancer Susceptibility Locus at 19q13

Author

S. Lilly Zheng, Jianfeng Xu, Henrik Grönberg, William B. Isaacs, John D. Carpten, David Duggan, Patrick C. Walsh, Bao-Li Chang, Wennuan Liu, Zheng Zhang, Seong-Tae Kim, Yi Zhu, Pär Stattin, Zhengrong Gao, Lina D. Purcell, Kathleen E. Wiley, Sarah D. Isaacs, Fredrik Wiklund, Jielin Sun, and Fang-Chi Hsu

Abstract

Supplementary Table 1 from A Novel Prostate Cancer Susceptibility Locus at 19q13

Published
2023
Full Text
View/download PDF

30. Supplementary Figure 1 from Germ-Line Mutation of NKX3.1 Cosegregates with Hereditary Prostate Cancer and Alters the Homeodomain Structure and Function

Author

Jianfeng Xu, Edward P. Gelmann, William B. Isaacs, James Gruschus, James Ferretti, Patrick C. Walsh, Micheas Zemedkun, Wennuan Liu, Kathy E. Wiley, Jishang Sun, Sarah D. Isaacs, Jielin Sun, Elizabeth Ortner, Bao-li Chang, Jeong-ho Ju, and S. Lilly Zheng

Abstract

Supplementary Figure 1 from Germ-Line Mutation of NKX3.1 Cosegregates with Hereditary Prostate Cancer and Alters the Homeodomain Structure and Function

Published
2023
Full Text
View/download PDF

31. Data from A Novel Prostate Cancer Susceptibility Locus at 19q13

Author

S. Lilly Zheng, Jianfeng Xu, Henrik Grönberg, William B. Isaacs, John D. Carpten, David Duggan, Patrick C. Walsh, Bao-Li Chang, Wennuan Liu, Zheng Zhang, Seong-Tae Kim, Yi Zhu, Pär Stattin, Zhengrong Gao, Lina D. Purcell, Kathleen E. Wiley, Sarah D. Isaacs, Fredrik Wiklund, Jielin Sun, and Fang-Chi Hsu

Abstract

A two-stage genome-wide association study (GWAS) of the Cancer Genetic Markers of Susceptibility (CGEMS) initiative identified single nucleotide polymorphisms (SNP) in 150 regions across the genome that may be associated with prostate cancer (PCa) risk. We filtered these results to identify 43 independent SNPs where the frequency of the risk allele was consistently higher in cases than in controls in each of the five CGEMS study populations. Genotype information for 22 of these 43 SNPs was obtained either directly by genotyping or indirectly by imputation in our PCa GWAS of 500 cases and 500 controls selected from a population-based case-control study in Sweden [Cancer of the Prostate in Sweden (CAPS)]. Two of these 22 SNPs were significantly associated with PCa risk (P < 0.05). We then genotyped these two SNPs in the remaining cases (n = 2,393) and controls (n = 1,222) from CAPS and found that rs887391 at 19q13 was highly associated with PCa risk (P = 9.4 × 10−4). A similar trend of association was found for this SNP in a case-control study from Johns Hopkins Hospital (JHH), albeit the result was not statistically significant. Altogether, the frequency of the risk allele of rs887391 was consistently higher in cases than controls among each of seven study populations examined, with an overall P = 3.2 × 10−7 from a combined allelic test. A fine-mapping study in a 110-kb region at 19q13 among CAPS and JHH study populations revealed that rs887391 was the most strongly associated SNP in the region. Additional confirmation studies of this region are warranted. [Cancer Res 2009;69(7):2720–3]

Published
2023
Full Text
View/download PDF

32. Data from Germ-Line Mutation of NKX3.1 Cosegregates with Hereditary Prostate Cancer and Alters the Homeodomain Structure and Function

Author

Jianfeng Xu, Edward P. Gelmann, William B. Isaacs, James Gruschus, James Ferretti, Patrick C. Walsh, Micheas Zemedkun, Wennuan Liu, Kathy E. Wiley, Jishang Sun, Sarah D. Isaacs, Jielin Sun, Elizabeth Ortner, Bao-li Chang, Jeong-ho Ju, and S. Lilly Zheng

Abstract

NKX3.1, a gene mapped to 8p21, is a member of the NK class of homeodomain proteins and is expressed primarily in the prostate. NKX3.1 exerts a growth-suppressive and differentiating effect on prostate epithelial cells. Because of its known functions and its location within a chromosomal region where evidence for prostate cancer linkage and somatic loss of heterozygosity is found, we hypothesize that sequence variants in the NKX3.1 gene increase prostate cancer risk. To address this, we first resequenced the NKX3.1 gene in 159 probands of hereditary prostate cancer families recruited at Johns Hopkins Hospital; each family has at least three first-degree relatives affected with prostate cancer. Twenty-one germ-line variants were identified in this analysis, including one previously described common nonsynonymous change (R52C), two novel rare nonsynonymous changes (A17T and T164A), and a novel common 18-bp deletion in the promoter. Overall, the germ-line variants were significantly linked to prostate cancer, with a peak heterogeneity logarithm of odds of 2.04 (P = 0.002) at the NKX3.1 gene. The rare nonsynonymous change, T164A, located in the homeobox domain of the gene, segregated with prostate cancer in a family with three affected brothers and one unaffected brother. Importantly, nuclear magnetic resonance solution structure analysis and circular dichroism studies showed this specific mutation to affect the stability of the homeodomain of the NKX3.1 protein and decreased binding to its cognate DNA recognition sequence. These results suggest that germ-line sequence variants in NKX3.1 may play a role in susceptibility to hereditary prostate cancer and underscore a role for NKX3.1 as a prostate cancer gatekeeper. (Cancer Res 2006; 66(1): 69-77)

Published
2023
Full Text
View/download PDF

33. Supplementary Figure 1 from Association of a Germ-Line Copy Number Variation at 2p24.3 and Risk for Aggressive Prostate Cancer

Author

Bao-Li Chang, S. Lilly Zheng, Henrik Grönberg, William B. Isaacs, John D. Carpten, David Duggan, Jianfeng Xu, Pär Stattin, Sarah D. Isaacs, Kathleen Wiley, Fredrik Wiklund, Jielin Sun, Seong-Tae Kim, Scott Zhang, Yi Zhu, Ge Li, Jishan Sun, and Wennuan Liu

Abstract

Supplementary Figure 1 from Association of a Germ-Line Copy Number Variation at 2p24.3 and Risk for Aggressive Prostate Cancer

Published
2023
Full Text
View/download PDF

34. Supplementary Table 3 from A Novel Prostate Cancer Susceptibility Locus at 19q13

Author

S. Lilly Zheng, Jianfeng Xu, Henrik Grönberg, William B. Isaacs, John D. Carpten, David Duggan, Patrick C. Walsh, Bao-Li Chang, Wennuan Liu, Zheng Zhang, Seong-Tae Kim, Yi Zhu, Pär Stattin, Zhengrong Gao, Lina D. Purcell, Kathleen E. Wiley, Sarah D. Isaacs, Fredrik Wiklund, Jielin Sun, and Fang-Chi Hsu

Abstract

Supplementary Table 3 from A Novel Prostate Cancer Susceptibility Locus at 19q13

Published
2023
Full Text
View/download PDF

35. Supplementary Table 2 from A Novel Prostate Cancer Susceptibility Locus at 19q13

Author

S. Lilly Zheng, Jianfeng Xu, Henrik Grönberg, William B. Isaacs, John D. Carpten, David Duggan, Patrick C. Walsh, Bao-Li Chang, Wennuan Liu, Zheng Zhang, Seong-Tae Kim, Yi Zhu, Pär Stattin, Zhengrong Gao, Lina D. Purcell, Kathleen E. Wiley, Sarah D. Isaacs, Fredrik Wiklund, Jielin Sun, and Fang-Chi Hsu

Abstract

Supplementary Table 2 from A Novel Prostate Cancer Susceptibility Locus at 19q13

Published
2023
Full Text
View/download PDF

36. Supplementary Figure 2 from Association of a Germ-Line Copy Number Variation at 2p24.3 and Risk for Aggressive Prostate Cancer

Author

Bao-Li Chang, S. Lilly Zheng, Henrik Grönberg, William B. Isaacs, John D. Carpten, David Duggan, Jianfeng Xu, Pär Stattin, Sarah D. Isaacs, Kathleen Wiley, Fredrik Wiklund, Jielin Sun, Seong-Tae Kim, Scott Zhang, Yi Zhu, Ge Li, Jishan Sun, and Wennuan Liu

Abstract

Supplementary Figure 2 from Association of a Germ-Line Copy Number Variation at 2p24.3 and Risk for Aggressive Prostate Cancer

Published
2023
Full Text
View/download PDF

37. Supplementary Table 4 from A Novel Prostate Cancer Susceptibility Locus at 19q13

Author

S. Lilly Zheng, Jianfeng Xu, Henrik Grönberg, William B. Isaacs, John D. Carpten, David Duggan, Patrick C. Walsh, Bao-Li Chang, Wennuan Liu, Zheng Zhang, Seong-Tae Kim, Yi Zhu, Pär Stattin, Zhengrong Gao, Lina D. Purcell, Kathleen E. Wiley, Sarah D. Isaacs, Fredrik Wiklund, Jielin Sun, and Fang-Chi Hsu

Abstract

Supplementary Table 4 from A Novel Prostate Cancer Susceptibility Locus at 19q13

Published
2023
Full Text
View/download PDF

38. Association of Sickle Cell Trait with Risk and Mortality of COVID-19: Results from the United Kingdom Biobank

Author

W. Kyle Resurreccion, Brian T. Helfand, S. Lilly Zheng, Janardan D. Khandekar, Jun Wei, Joseph Hulsizer, Liana K. Billings, Clay Struve, Rong Na, Chi-Hsiung Wang, Jianfeng Xu, Zhuqing Shi, and Michael S. Caplan

Subjects
Adult, Male, medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), Population, Short Report, Black People, Disease, Sickle Cell Trait, Diabetes Complications, Risk Factors, Virology, Internal medicine, Diabetes mellitus, Odds Ratio, medicine, Humans, Aged, Biological Specimen Banks, Sickle cell trait, Preexisting Condition Coverage, business.industry, Mortality rate, COVID-19, Odds ratio, Middle Aged, medicine.disease, Biobank, United Kingdom, Confidence interval, Infectious Diseases, Female, Parasitology, business
Abstract

Sickle cell trait (SCT) carriers inherit one copy of the Glu6Val mutation in the hemoglobin gene and is particularly common in Black individuals (5–10%). Considering the roles of hemoglobin in immune responses and the higher risk for coronavirus disease (COVID-19) among Black individuals, we tested whether Black SCT carriers were at increased risk for COVID-19 infection and mortality according to the United Kingdom Biobank. Among Black individuals who were tested for COVID-19, we found similar infection rates among SCT carriers (14/72; 19.7%) and noncarriers (167/791; 21.1%), but higher COVID-19 mortality rates among SCT carriers (4/14; 28.6%) than among noncarriers (21/167; 12.6%) (odds ratio [OR], 3.04; 95% confidence interval [CI], 0.69–11.82; P = 0.12). Notably, SCT carriers with preexisting diabetes had significantly higher COVID-19 mortality (4/4; 100%) than those without diabetes (0/10; 0%; (OR, 90.71; 95% CI, 5.66–infinite; P = 0.0005). These findings suggest that Black SCT carriers with preexisting diabetes are at disproportionally higher risk for COVID-19 mortality. Confirmation by larger studies is warranted.

Published
2021
Full Text
View/download PDF

39. Observed evidence for guideline‐recommended genes in predicting prostate cancer risk from a large population‐based cohort

Author

Wancai Yang, Jianfeng Xu, Jim Lu, Qiang Wang, W. Kyle Resurreccion, Brian T. Helfand, William B. Isaacs, Valentina Engelmann, S. Lilly Zheng, Peter J. Hulick, Kathleen A. Cooney, Lucy Lu, Jun Wei, and Zhuqing Shi

Subjects
Adult, Male, Oncology, medicine.medical_specialty, Urology, Genetic counseling, Population, Risk Assessment, Germline mutation, Internal medicine, Biomarkers, Tumor, Humans, Medicine, Genetic Predisposition to Disease, Genetic Testing, education, CHEK2, Germ-Line Mutation, Aged, Aged, 80 and over, education.field_of_study, business.industry, Prostatic Neoplasms, Odds ratio, Middle Aged, Confidence interval, Cohort, business, Risk assessment
Abstract

BACKGROUND Germline testing for prostate cancer (PCa) is now recommended by the National Comprehensive Cancer Network. While multi-gene testing has been proposed, evidence for their association with PCa risk is not well established. METHODS We tested associations of pathogenic/likely pathogenic mutations in 10 guideline-recommended genes (ATM, BRCA1, BRCA2, CHEK2, PALB2, MLH1, MSH2, MSH6, PMS2, and HOXB13) with PCa risk in the UK Biobank, a population-based cohort. Mutations were annotated based on prostate-specific transcripts using the American College of Medical Genetics and Genomics standards. Associations were tested in 4399 PCa cases and 85,403 unaffected male controls using logistic regression adjusting for age and genetic background. p

Published
2021
Full Text
View/download PDF

40. Reliability of Ancestry-specific Prostate Cancer Genetic Risk Score in Four Racial and Ethnic Populations

Author

Zhuqing Shi, Jianan Zhan, Jun Wei, Skylar Ladson-Gary, Chi-Hsiung Wang, Peter J. Hulick, S. Lilly Zheng, Kathleen A. Cooney, William B. Isaacs, Brian T. Helfand, Bertram L. Koelsch, and Jianfeng Xu

Subjects
Urology
Abstract

Reliability of prostate cancer (PCa) genetic risk score (GRS), that is, the concordance between its estimated risk and observed risk, is required for genetic testing at the individual level. Reliability data are lacking for non-European racial/ethnic populations, which hinders its clinical use and exacerbates racial disparity.To calibrate PCa ancestry-specific GRS in four racial/ethnic populations.PCa ancestry-specific GRSs, calculated from published risk-associated single-nucleotide polymorphisms in corresponding racial/ethnic populations, were evaluated in men who participated in 23andMe, Inc. genetic testing and consented for research, including 888 086 of European (EUR), 81 109 of Hispanic (HIS), 30 472 of African (AFR), and 13 985 of East Asian (EAS) ancestry, as classified by 23andMe's ancestry composition algorithm.The concordance between the observed and estimated PCa risks at ten ancestry-specific GRS deciles was measured primarily by using the calibration slope (β), where 1 represents a perfect calibration. Platt scaling was used to correct the systematic bias of GRS.A linear trend of an increased observed PCa prevalence in men with higher ancestry-specific GRS deciles was found in each racial population (allA systematic bias of ancestry-specific GRS in the direction of an overestimated risk for men in the highest decile was found in EUR and non-EUR populations. GRS is well calibrated after correction and is appropriate for genetic testing at the individual level for personalized PCa screening.A corrected genetic risk score is more reliable (supported by the observed prostate cancer [PCa] risk) and appropriate for genetic testing for personalized PCa screening.

Published
2022

41. Germline mutations in high penetrance genes are associated with worse clinical outcomes in patients with non-small cell lung cancer

Author

Seth B. Krantz, Kanwal Zeeshan, Kristine M. Kuchta, Thomas A. Hensing, Kathy A. Mangold, S. Lilly Zheng, and Jianfeng Xu

Subjects
Pulmonary and Respiratory Medicine, Surgery, Cardiology and Cardiovascular Medicine
Abstract

To determine the frequency of pathogenic mutations in high-penetrance genes (HPGs) in patients with non-small cell lung cancer (NSCLC) and identify whether such mutations are associated with clinicopathologic outcomes.Patients with NSCLC who had consented to participate in a linked clinical database and biorepository underwent germline DNA sequencing using a next-generation sequencing panel that included cancer-associated HPGs and cancer risk-associated single nucleotide polymorphisms (SNPs). These data were linked to the clinical database to assess for associations between germline variants and clinical phenotype using Fisher's exact test and multivariable logistic and Cox regression.We analyzed 151 patients, among whom 33% carried any pathogenic HPG mutation and 23% had a genetic risk score (GRS)1.5. Among the patients without any pathogenic mutation, 31% were at cancer stage II or higher, compared with 55% of those with 2 types of HPG mutations (The presence of mutations in HPGs is associated with higher cancer stage, increased risk of recurrence, and worse cancer-specific and overall survival in patients with NSCLC. Further large studies are needed to better delineate the role of HPGs in cancer recurrence and the potential benefit of adjuvant treatment in patients harboring such mutations.

Published
2022

42. Cystic fibrosis F508del carriers and cancer risk: Results from the <scp>UK</scp> Biobank

Author

Rong Na, W. Kyle Resurreccion, Peter J. Hulick, S. Lilly Zheng, Zhuqing Shi, Jun Wei, Mark S. Talamonti, Jianfeng Xu, and Brian T. Helfand

Subjects
Adult, Male, Cancer Research, medicine.medical_specialty, Lung Neoplasms, Cystic Fibrosis, Colorectal cancer, Population, Cystic Fibrosis Transmembrane Conductance Regulator, Bronchi, Cystic fibrosis, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Risk Factors, Neoplasms, Pancreatic cancer, Internal medicine, medicine, Humans, Thyroid Neoplasms, Correlation of Data, education, Thyroid cancer, Aged, Biological Specimen Banks, Sequence Deletion, education.field_of_study, business.industry, Lymphoma, Non-Hodgkin, Gallbladder, Cancer, Middle Aged, medicine.disease, United Kingdom, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Female, Gallbladder Neoplasms, Colorectal Neoplasms, business
Abstract

Cystic fibrosis (CF) carriers carrying one defective copy of a CFTR germline mutation are common in the general population. A recent study reported associations of CF carriers with risk for cancers of digestive organs and pancreatic cancer. In the current study, we assessed associations of CFTR F508del carriers with the risk for 54 types of cancers in the UK Biobank, a large population-based study. In Caucasians, compared to the carrier rate of 3.15% (12 357/392274) in noncancer subjects, the rate was significantly higher in cancer patients overall (2621/79619 = 3.29%), especially in patients with colorectal cancer (247/6667 = 3.70%), cancers of gallbladder and biliary tract (21/351 = 5.98%), thyroid cancer (30/665 = 4.51%) and unspecified non-Hodgkin's lymphoma (74/1805 = 4.10%), all P ≤ .05. In contrast, the carrier rate in patients with cancers of lung and bronchus was significantly lower (89/3463 = 2.57%), P = .05. The association of CFTR F508del carriers with these types of cancer remained significant after adjusting for respective cancer-specific risk factors. For pancreatic cancer, although a higher carrier rate (38/1004 = 3.78%) was found in patients with this cancer, the difference was not statistically significant (P = .26). This null association was unlikely due to lack of statistical power; the large sample size of our study had >80% power, at a significance level of .05, to detect an association of >1.5-fold increased risk. In conclusion, the identified associations of CFTR F508del carriers with multiple types of cancer may have potential biological and clinical implications if confirmed in independent study populations.

Published
2020
Full Text
View/download PDF

43. Distinct Genomic Alterations in Prostate Tumors Derived from African American Men

Author

Karen S. Sfanos, S. Lilly Zheng, William B. Isaacs, Rong Na, Lin Wei, W. Kyle Resurreccion, Johnie Gallagher, Sarah Ernst, Jun Wei, Jishan Sun, Jianfeng Xu, and Wennuan Liu

Subjects
Male, 0301 basic medicine, Genome instability, Cancer Research, DNA Copy Number Variations, Ubiquitin-Protein Ligases, Biology, BUB1B, medicine.disease_cause, Genomic Instability, Frameshift mutation, MED12, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Proto-Oncogene Proteins, Biomarkers, Tumor, medicine, Humans, Allele, Molecular Biology, Gene, Retrospective Studies, Mutation, Tumor Suppressor Proteins, High-Throughput Nucleotide Sequencing, Membrane Proteins, Nuclear Proteins, Prostatic Neoplasms, Sequence Analysis, DNA, MAP Kinase Kinase Kinases, medicine.disease, Black or African American, Retinoblastoma Binding Proteins, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, Neoplasm Grading
Abstract

We aim to understand, from acquired genetic alterations in tumors, why African American (AA) men are more likely to develop aggressive prostate cancer. By analyzing somatic mutations in 39 genes using deeper next-generation sequencing with an average depth of 2,522 reads for tumor DNA and genome-wide DNA copy-number alterations (CNA) in prostate cancer in a total of 171 AA/black men and comparing with those in 860 European American (EA)/white men, we here present several novel findings. First, >35% of AA men harbor damaging mutations in APC, ATM, BRCA2, KDM6A, KMT2C, KMT2D, MED12, ZFHX3, and ZMYM3, each with >1% of mutated copies. Second, among genes with >10% of mutated copies in tumor cells, ZMYM3 is the most frequently mutated gene in AA prostate cancer. In a patient's tumor with >96% frameshift mutations of ZMYM3, we find allelic imbalances in 10 chromosomes, including losses of five and gains of another four chromosomes, suggesting its role in maintaining genomic integrity. Third, when compared to prostate cancer in EA/white men, a higher frequency of CNAs of MYC, THADA, NEIL3, LRP1B, BUB1B, MAP3K7, BNIP3L and RB1, and a lower frequency of deletions of RYBP, TP53, and TMPRSS2-ERG are observed in AA/black men. Finally, for the above genes with higher frequency of CNAs in AA than in EA, deletion of MAP3K7, BNIP3L, NEIL3 or RB1, or gain of MYC significantly associates with both higher Gleason grade and advanced pathologic stage in AA/black men. Deletion of THADA associates with advanced pathologic stage only. Implications: A higher frequency of damaging mutation in ZMYM3 causing genomic instability along with higher frequency of altered genomic regions including deletions of MAP3K7, BNIP3L, RB1, and NEIL3, and gain of MYC appear to be distinct somatically acquired genetic alterations that may contribute to more aggressive prostate cancer in AA/black men.

Published
2020
Full Text
View/download PDF

44. Role of androgen receptor splice variant-7 (AR-V7) in prostate cancer resistance to 2nd-generation androgen receptor signaling inhibitors

Author

Susan L. Dalrymple, Yezi Zhu, Peter S. Nelson, Jun Luo, Jianfeng Xu, Alan K. Meeker, Samuel R. Denmeade, Emmanuel S. Antonarakis, S. Lilly Zheng, William B. Isaacs, Angelo M. De Marzo, Jody E. Hooper, Ilsa Coleman, John T. Isaacs, and W. Nathaniel Brennen

Subjects
Male, 0301 basic medicine, Cancer Research, Biopsy, RNA Splicing, Abiraterone Acetate, medicine.disease_cause, Article, Gene Knockout Techniques, Mice, 03 medical and health sciences, Prostate cancer, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, Nitriles, Phenylthiohydantoin, Genetics, medicine, Animals, Humans, Protein Isoforms, PTEN, Enzalutamide, RNA-Seq, Receptor, Molecular Biology, Aged, Regulation of gene expression, Mutation, biology, Prostate, Abiraterone acetate, Androgen Antagonists, Middle Aged, medicine.disease, Xenograft Model Antitumor Assays, Gene Expression Regulation, Neoplastic, Androgen receptor, Prostatic Neoplasms, Castration-Resistant, 030104 developmental biology, chemistry, Drug Resistance, Neoplasm, Receptors, Androgen, 030220 oncology & carcinogenesis, Benzamides, biology.protein, Cancer research
Abstract

The role of truncated androgen receptor splice variant-7 (AR-V7) in prostate cancer biology is an unresolved question. Is it simply a marker of resistance to 2nd-generation androgen receptor signaling inhibitors (ARSi) like abiraterone acetate (Abi) and enzalutamide (Enza) or a functional driver of lethal resistance via its ligand-independent transcriptional activity? To resolve this question, the correlation between resistance to ARSi and genetic chances and expression of full length AR (AR-FL) vs. AR-V7 were evaluated in a series of independent patient-derived xenografts (PDXs). While all PDXs lack PTEN expression, there is no consistent requirement for mutation in TP53, RB1, BRCA2, PIK3CA, or MSH2, or expression of SOX2 or ERG and ARSi resistance. Elevated expression of AR-FL alone is sufficient for Abi but not Enza resistance, even if AR-FL is gain-of-function (GOF) mutated. Enza resistance is consistently correlated with enhanced AR-V7 expression. In vitro and in vivo growth responses of Abi-/Enza-resistant LNCaP-95 cells in which CRISPR-Cas9 was used to knockout AR-FL or AR-V7 alone or in combination were evaluated. Combining these growth responses with RNAseq analysis demonstrates that both AR-FL- and AR-V7-dependent transcriptional complementation are needed for Abi/Enza resistance.

Published
2020
Full Text
View/download PDF

45. Germline HOXB13 G84E mutation carriers and risk to twenty common types of cancer: results from the UK Biobank

Author

Kathleen A. Cooney, S. Lilly Zheng, Brian T. Helfand, W. Kyle Resurreccion, Jianfeng Xu, William B. Isaacs, Zhuqing Shi, Jun Wei, Chi Hsiung Wang, Peter J. Hulick, and Rong Na

Subjects
Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Genetic testing, Genotype, Genetic counseling, Glycine, Mutation, Missense, Glutamic Acid, Brief Communication, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Germline mutation, Gene Frequency, Risk Factors, Neoplasms, Internal medicine, medicine, Humans, Genetic Predisposition to Disease, Basal cell carcinoma, Cancer genetics, Genetic Association Studies, Germ-Line Mutation, Aged, Biological Specimen Banks, Homeodomain Proteins, business.industry, Case-control study, Cancer, Odds ratio, Middle Aged, medicine.disease, United Kingdom, Amino Acid Substitution, Case-Control Studies, 030220 oncology & carcinogenesis, Mutation, Female, Skin cancer, business
Abstract

Germline HOXB13 G84E mutation has been consistently associated with prostate cancer (PCa) risk, but its association with other cancers is controversial. We systematically tested its association with the 20 most common cancer types in subjects from the UK Biobank. The G84E mutation was found in 1,545 (0.34%) of 460,224 participants of European ancestry. While mutation status did not associate with cancer risk in females, it was significantly associated with increased risk in males; odds ratio (OR) (95% confidence interval) for overall cancer diagnosis was 2.19 (1.89–2.52), P = 2.5E-19. The association remained after excluding PCa; OR = 1.4 (1.16–1.68), P = 0.003, suggesting association with other cancers. Indeed, suggestive novel associations were found for two other cancer types; rectosigmoid cancer, OR = 2.25 (1.05–4.15), P = 0.05 and non-melanoma skin cancer (NMSC), OR = 1.40 (1.12–1.74), P = 0.01. For NMSC, the association was found only in basal cell carcinoma, OR = 1.37 (1.07–1.74), P = 0.03. These findings have potential clinical utility for genetic counselling regarding HOXB13.

Published
2020
Full Text
View/download PDF

46. Feasibility and performance of a novel probe panel to detect somatic DNA copy number alterations in clinical specimens for predicting prostate cancer progression

Author

Rong Na, Chi Hsiung Wang, Jacqueline Petkewicz, S. Lilly Zheng, Charles B. Brendler, Wennuan Liu, W. Kyle Resurreccion, Brian T. Helfand, Yedida Y. Bogachkov, Mary Ann Regner, Jun Hou, William B. Isaacs, Johnie Gallagher, Jianfeng Xu, Jishan Sun, Susan E. Crawford, and Laura Swenson

Subjects
Male, 0301 basic medicine, Oncology, medicine.medical_specialty, Urology, medicine.medical_treatment, Gene Dosage, Disease, Metastasis, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Predictive Value of Tests, Prostate, Internal medicine, medicine, Humans, PTEN, Aged, biology, business.industry, Prostatectomy, Prostatic Neoplasms, Cancer, DNA, Neoplasm, Odds ratio, Middle Aged, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Disease Progression, biology.protein, Feasibility Studies, DNA Probes, business
Abstract

Background To assess the feasibility of a novel DNA-based probe panel to detect copy number alterations (CNAs) in prostate tumor DNA and its performance for predicting clinical progression. Methods A probe panel was developed and optimized to measure CNAs in trace amounts of tumor DNA (2 ng) isolated from formalin-fixed paraffin-embedded tissues. Ten genes previously associated with aggressive disease were targeted. The panel's feasibility and performance were assessed in 175 prostate cancer (PCa) patients who underwent radical prostatectomy with a median 10-year follow-up, including 42 men who developed disease progression (either metastasis and/or PCa-specific death). Association with disease progression was tested using univariable and multivariable analyses. Results The probe panel detected CNAs in all 10 genes in tumor DNA isolated from either diagnostic biopsies or surgical specimens. A four-gene model (PTEN/MYC/BRCA2/CDKN1B) had the strongest association with disease progression; 64.3% of progressors and 22.5% of non-progressors had at least one CNA in these four genes, odds ratio (OR) (95% confidence interval) = 6.21 (2.77-13.87), P = 8.48E-06. The association with disease progression remained significant after adjusting for known clinicopathological variables. Among the seven progressors of the 65 patients with clinically low-risk disease, three (42.9%) had at least one CNA in these four genes. Conclusions The probe panel can detect CNAs in trace amounts of tumor DNA from biopsies or surgical tissues at the time of diagnosis or surgery. CNAs independently predict metastatic/lethal cancer, particularly among men with clinically low-risk disease at diagnosis. If validated, this may improve current abilities to assess tumor aggressiveness.

Published
2020
Full Text
View/download PDF

47. Somatic DNA copy number alterations in non-dysplastic Barrett’s esophagus

Author

Mikhail Attaar, MaryAnn Regner, Jianfeng Xu, S. Lilly Zheng, Craig S. Brown, JoAnn Carbray, Wennuan Liu, Bailey Su, Zachary M. Callahan, Jun Hou, Michael B. Ujiki, Jamaal Rehman, H. Mason Hedberg, and Kristine Kuchta

Subjects
medicine.medical_specialty, medicine.diagnostic_test, business.industry, Hepatology, medicine.disease, Gastroenterology, digestive system diseases, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Dysplasia, 030220 oncology & carcinogenesis, Barrett's esophagus, Internal medicine, Biopsy, medicine, GERD, 030211 gastroenterology & hepatology, Surgery, Medical history, Multiplex ligation-dependent probe amplification, Esophagus, business
Abstract

The purpose of this study was to analyze non-dysplastic Barrett’s esophagus (NDBE) biopsy tissue and compare the rate of somatic DNA copy number alterations (CNAs) in patients who subsequently progressed to high-grade dysplasia (HGD) or esophageal adenocarcinoma (EAC) to those patients who did not. A retrospectively collected database of Barrett’s esophagus (BE) patients spanning a 16-year period was queried. Patients who progressed from NDBE to HGD or EAC were identified and compared to patients who did not. Initial biopsy specimens were microdissected and extracted DNA underwent Multiplex Ligation-dependent Probe Amplification (MLPA) for CNAs. Comparisons between progressors and non-progressors were made with Fisher’s exact and two-sample t tests. Logistic regression assessed factors associated with progression. Of the 2459 patients in the BE database, 36 patients progressed from NDBE to either HGD or EAC. There were eight progressors who had biopsy specimens with adequate DNA for analysis. The progressor and non-progressor cohort had similar demographic information and medical history. The progressor group trended towards being older at diagnosis (72 ± 10 vs. 64 ± 13 years, p = 0.097) and fewer progressors reported reflux symptoms (50 vs. 94.7%, p

Published
2020
Full Text
View/download PDF

48. Correction: Role of androgen receptor splice variant-7 (AR-V7) in prostate cancer resistance to 2nd-generation androgen receptor signaling inhibitors

Author

Jody E. Hooper, Susan L. Dalrymple, Samuel R. Denmeade, Yezi Zhu, Angelo M. De Marzo, W. Nathaniel Brennen, S. Lilly Zheng, Peter S. Nelson, Ilsa Coleman, John T. Isaacs, Jun Luo, Alan K. Meeker, Jianfeng Xu, Emmanuel S. Antonarakis, and William B. Isaacs

Subjects
Androgen receptor, Cancer Research, Prostate cancer, Oncogene, Genetics, Cancer research, medicine, Androgen Receptor Splice Variant 7, Biology, medicine.disease, Molecular Biology
Published
2021
Full Text
View/download PDF

50. PD56-07 STATISTICAL EVIDENCE FOR GUIDELINE-RECOMMENDED GENES FOR PREDICTING PROSTATE CANCER RISK IN A LARGE POPULATION-BASED COHORT

Author

Yasin Bhanji, Brian T. Helfand, Kathleen A. Cooney, Jim Lu, S. Lilly Zheng, W. Kyle Resurreccion, Jun Wei, William B. Isaacs, Christian P. Pavlovich, Zhuqing Shi, Wancai Yang, and Jianfeng Xu

Subjects
Oncology, medicine.medical_specialty, business.industry, Urology, Large population, Guideline, urologic and male genital diseases, medicine.disease, Germline, Prostate cancer, Internal medicine, Cohort, medicine, Risk assessment, business, Gene, Statistical evidence
Abstract

INTRODUCTION AND OBJECTIVE:Germline testing for prostate cancer (PCa) is now recommended by clinical guidelines for PCa risk assessment. Ten genes involved in hereditary cancer syndromes (ATM, BRCA...

Published
2021
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results