Heterogeneous patterns of DNA methylation-based field effects in histologically normal prostate tissue from cancer patients

Moller, Mia; Strand, Siri H.; Mundbjerg, Kamilla; Liang, Gangning; Gill, Inderbir S.; Haldrup, Christa; Borre, Michael; Høyer, Søren; Ørntoft, Torben F.; Sørensen, Karina Dalsgaard

doi:10.1038/srep40636

Cited by 32 publications

(27 citation statements)

References 53 publications

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“…HOXB4, as a hematopoietic transcription factor, downregulates the expression of Prdm16, which is a proto‐oncogene necessary for self‐renewal and maintenance of murine hematopoietic stem cells . The other eight frequently methylated candidates (CCDC181, DPP4, BEND4, CTNND2, ELMO1, SFMBT2, C1QL3, MIR129–2) confirmed in our study have also shown hypermethylation in other malignancies (Table ) . Among them, SFMBT2 and MIR129–2 have been shown to act as tumor suppressors.…”

Section: Discussionsupporting

confidence: 78%

Discovery and development of differentially methylated regions in human papillomavirus‐related oropharyngeal squamous cell carcinoma

Ren

Gaykalova

Wang

et al. 2018

Intl Journal of Cancer

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Human papillomavirus (HPV)-related oropharyngeal squamous cell carcinoma (OPSCC) exhibits a different composition of epigenetic alterations. In this study, we identified differentially methylated regions (DMRs) with potential utility in screening for HPV-positive OPSCC. Genome wide DNA methylation was measured using methyl-CpG binding domain protein-enriched genome sequencing (MBD-seq) in 50 HPV-positive OPSCC tissues and 25 normal tissues. Fifty-one DMRs were defined with maximal methylation specificity to cancer samples. The Cancer Genome Atlas (TCGA) methylation array data was used to evaluate the performance of the proposed candidates. Supervised hierarchical clustering of 51 DMRs found that HPV-positive OPSCC had significantly higher DNA methylation levels compared to normal samples, and non-HPV-related head and neck squamous cell carcinoma (HNSCC). The methylation levels of all top 20 DNA methylation biomarkers in HPV-positive OPSCC were significantly higher than those in normal samples. Further confirmation using quantitative methylation specific PCR (QMSP) in an independent set of 24 HPV-related OPSCCs and 22 controls showed that 16 of the 20 candidates had significant higher methylation levels in HPV-positive OPSCC samples compared with controls. One candidate, OR6S1, had a sensitivity of 100%, while 17 candidates (KCNA3, EMBP1, CCDC181, DPP4, ITGA4, BEND4, ELMO1, SFMBT2, C1QL3, MIR129-2, NID2, HOXB4, ZNF439, ZNF93, VSTM2B, ZNF137P and ZNF773) had specificities of 100%. The prediction accuracy of the 20 candidates rang from 56.2% to 99.8% by receiver operating characteristic analysis. We have defined 20 highly specific DMRs in HPV-related OPSCC, which can potentially be applied to molecular-based detection tests and improve disease management.

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Section: Discussionsupporting

confidence: 78%

Discovery and development of differentially methylated regions in human papillomavirus‐related oropharyngeal squamous cell carcinoma

Ren

Gaykalova

Wang

et al. 2018

Intl Journal of Cancer

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“…The AUCs of ST6GALNAC3 (0.917–0.995) were generally higher than those of ZNF660 (0.846–0.903) and were similar to those of other published diagnostic candidate methylation markers (Goering et al ., ; Haldrup et al ., , ; Kristensen et al ., ), suggesting that ST6GALNAC3 has promising diagnostic biomarker potential for PC tissue. To further assess this, it would be interesting to evaluate ST6GALNAC3 and ZNF660 promoter methylation also in cancer‐negative diagnostic biopsies, as promoter hypermethylation field effects in cancer‐negative diagnostic biopsies have previously been shown to predict the result of repeat biopsy (Moller et al ., ; Partin et al ., ; Stewart et al ., ; Trock et al ., ; Troyer et al ., ; Van Neste et al ., ). Results of such analyses should, for example, be compared to the commercially available urine‐based PCA3 assay (Progensa) and the tissue‐based methylation test ConfirmMDx (MDxHealth), both designed to determine whether a repeat biopsy is necessary.…”

Section: Discussionmentioning

confidence: 99%

“…Sample set 1 consisted of 20 PC (from RPs) and 21 NM (12 AN from RPs and 9 histologically normal from cystoprostatectomies) macrodissected fresh‐frozen samples (for clinicopathological data, see Table ), as described previously (Haldrup et al ., ; Moller et al ., ; Strand et al ., ). DNA from all samples was analyzed for DNA methylation using the 450K array by The Genome Centre Barts and the London School of Medicine and Dentistry, London, UK, as described previously (Strand et al ., ).…”

Section: Methodsmentioning

confidence: 98%

Biomarker potential of ST6GALNAC3 and ZNF660 promoter hypermethylation in prostate cancer tissue and liquid biopsies

et al. 2018

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Current diagnostic and prognostic tools for prostate cancer (PC) are suboptimal, leading to overdiagnosis and overtreatment. Aberrant promoter hypermethylation of specific genes has been suggested as novel candidate biomarkers for PC that may improve diagnosis and prognosis. We here analyzed ST6GALNAC3 and ZNF660 promoter methylation in prostate tissues, and ST6GALNAC3,ZNF660,CCDC181, and HAPLN3 promoter methylation in liquid biopsies. First, using four independent patient sample sets, including a total of 110 nonmalignant (NM) and 705 PC tissue samples, analyzed by methylation‐specific qPCR or methylation array, we found that hypermethylation of ST6GALNAC3 and ZNF660 was highly cancer‐specific with areas under the curve (AUC) of receiver operating characteristic (ROC) curve analysis of 0.917–0.995 and 0.846–0.903, respectively. Furthermore, ZNF660 hypermethylation was significantly associated with biochemical recurrence in two radical prostatectomy (RP) cohorts of 158 and 392 patients and remained significant also in the subsets of patients with Gleason score ≤7 (univariate Cox regression and log‐rank tests, P < 0.05), suggesting that ZNF660 methylation analysis can potentially help to stratify low‐/intermediate‐grade PCs into indolent vs. more aggressive subtypes. Notably, ZNF660 hypermethylation was also significantly associated with poor overall and PC‐specific survival in the RP cohort (n = 158) with long clinical follow‐up available. Moreover, as proof of principle, we successfully detected highly PC‐specific hypermethylated circulating tumor DNA (ctDNA) for ST6GALNAC3,ZNF660,HAPLN3, and CCDC181 in liquid biopsies (serum) from 27 patients with PC vs. 10 patients with BPH, using droplet digital methylation‐specific PCR analysis. Finally, we generated a three‐gene (ST6GALNAC3/CCDC181/HAPLN3) ctDNA hypermethylation model, which detected PC with 100% specificity and 67% sensitivity. In conclusion, we here for the first time demonstrate diagnostic biomarker potential of ST6GALNAC3 and ZNF660 methylation, as well as prognostic biomarker potential of ZNF660. Furthermore, we show that hypermethylation of four genes can be detected in ctDNA in liquid biopsies (serum) from patients with PC.

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“…In considering richer sources of potential biomarkers for early prostate cancer, DNA hypermethylation is by far the most diverse and prevalent genomic aberration. It is found at higher levels in cancer tissues compared with benign histological samples such as normal/adjacent normal, benign prostate hyperplasia, and prostatic intraepithelial neoplasia . Its stability and ease of detection in archival tissues further enhance the feasibility and appeal of its use in clinical applications.…”

Section: Discussionmentioning

confidence: 99%

“…To date, only one epigenetic assay, ConfirmMDx, is commercially available, which measures methylation at APC , GSTP1 , and RASSF1 loci, and is intended for use on benign prostate biopsies to identify men who are likely to have cancer in a subsequent biopsy. This test, designed to detect molecular features of a field cancerization effect, represents a challenging application since field effects are reportedly variable in time and space . It is, therefore, not surprising that this test shows limited specificity (64%) and sensitivity (66%) with an overall misclassification rate exceeding 35% .…”

Section: Discussionmentioning

confidence: 99%

A three‐gene DNA methylation biomarker accurately classifies early stage prostate cancer

et al. 2019

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Background We identify and validate accurate diagnostic biomarkers for prostate cancer through a systematic evaluation of DNA methylation alterations. Materials and methods We assembled three early prostate cancer cohorts (total patients = 699) from which we collected and processed over 1300 prostatectomy tissue samples for DNA extraction. Using real‐time methylation‐specific PCR, we measured normalized methylation levels at 15 frequently methylated loci. After partitioning sample sets into independent training and validation cohorts, classifiers were developed using logistic regression, analyzed, and validated. Results In the training dataset, DNA methylation levels at 7 of 15 genomic loci (glutathione S‐transferase Pi 1 [GSTP1], CCDC181, hyaluronan, and proteoglycan link protein 3 [HAPLN3], GSTM2, growth arrest‐specific 6 [GAS6], RASSF1, and APC) showed large differences between cancer and benign samples. The best binary classifier was the GAS6/GSTP1/HAPLN3 logistic regression model, with an area under these curves of 0.97, which showed a sensitivity of 94%, and a specificity of 93% after external validation. Conclusion We created and validated a multigene model for the classification of benign and malignant prostate tissue. With false positive and negative rates below 7%, this three‐gene biomarker represents a promising basis for more accurate prostate cancer diagnosis.

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Heterogeneous patterns of DNA methylation-based field effects in histologically normal prostate tissue from cancer patients

Cited by 32 publications

References 53 publications

Discovery and development of differentially methylated regions in human papillomavirus‐related oropharyngeal squamous cell carcinoma

Discovery and development of differentially methylated regions in human papillomavirus‐related oropharyngeal squamous cell carcinoma

Biomarker potential of ST6GALNAC3 and ZNF660 promoter hypermethylation in prostate cancer tissue and liquid biopsies

A three‐gene DNA methylation biomarker accurately classifies early stage prostate cancer

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