<scp>DNA</scp> methylation array analyses identified breast cancer‐associated <scp><i>HYAL2</i></scp> methylation in peripheral blood

Yang, Rongxi; Pfütze, Katrin; Zucknick, Manuela; Sutter, Christian; Wappenschmidt, Barbara; Marmé, Frederik; Qu, Bin; Ćuk, Katarina; Engel, Christoph; Schott, Sarah; Schneeweiß, Andreas; Brenner, Hermann; Claus, Rainer; Plass, Christoph; Bugert, Peter; Hoth, Markus; Sohn, Christof; Schmutzler, Rita K.; Bartram, Claus R.; Burwinkel, Barbara

doi:10.1002/ijc.29205

Cited by 56 publications

(66 citation statements)

References 50 publications

(68 reference statements)

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“…After excluding non-eligible articles (see Fig. 1a and Additional file 1: Supplementary materials), 45 articles could be included in this review, including 26 articles used DNA isolated from whole blood [14–21, 24–41], two articles used DNA isolated from both whole blood and plasma [42, 43], six articles used DNA isolated from plasma [44–49], and 11 articles used DNA isolated from serum [50–60] (Table 1). For the studies that used serum or plasma as DNA source, four of them used two centrifugation steps to get serum or plasma [42, 45, 47, 48] and the rest used one centrifugation step or sample processing procedures are not available (Table 1).…”

Section: Resultsmentioning

confidence: 99%

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Blood-based DNA methylation as biomarker for breast cancer: a systematic review

et al. 2016

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Multiple studies have investigated global DNA methylation profiles and gene-specific DNA methylation in blood-based DNA to develop powerful screening markers for cancer. This systematic review summarizes the current evidence on methylation studies that investigated methylation level of blood-derived DNA of breast cancer (BC) patients in comparison to healthy controls by conducting a systematic literature review in PubMed and Web of Science. Essential results, such as methylation levels of BC cases and healthy controls, p values, and odds ratios, were extracted from these studies by two investigators independently. Overall, 45 publications met the inclusion criteria for this review. DNA from whole blood, as well as cell-free DNA (cfDNA) from serum or plasma, was used in these studies. The most common method used for measuring global DNA methylation was the investigation of repetitive elements as surrogates and the application of array-based genome-wide methylation analysis. For measuring gene-specific methylation level, methylation-specific PCR and pyrosequencing were the most frequently used methods. Epigenome-wide blood DNA hypomethylation in BC patients were reported in several studies; however, the evidence is still not conclusive. The most frequently investigated gene in whole blood was BRCA1, which was found more frequently methylated in patients compared to controls. RASSF1A was the most widely investigated gene in cfDNA of serum or plasma, which was also found more frequently methylated in patients compared to controls. Several of the eligible studies reported the associations of global hypomethylation and increased BC risk. Studies investigated associations between gene-specific methylation and BC risk, while got heterogeneous results. But two studies reported that hypermethylation of ATM gene was associated with increased BC risk, which suggest the potential use of this gene for BC risk stratification. Overall, our review suggests the possibility of using blood-based DNA methylation marker as promising marker for BC risk stratification, as several studies found associations between certain methylation level in blood and BC risk. However, so far, the evidence is still quite limited. Optimal markers are yet to be developed and promising results needed to be validated in prospective study cohorts and tested in large screening populations.Electronic supplementary materialThe online version of this article (doi:10.1186/s13148-016-0282-6) contains supplementary material, which is available to authorized users.

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Section: Resultsmentioning

confidence: 99%

“…Yang et al [21] showed that reduced methylation levels of the HYAL2 gene were significantly associated with increased BC risk. Specifically, women in the highest quartile of HYAL2 methylation were reported to have a 41.47-fold (cohort I) and a 132.98-fold (cohort II) increased BC risk, compared with women in the lowest quartile (Fig.…”

Section: Resultsmentioning

confidence: 99%

Blood-based DNA methylation as biomarker for breast cancer: a systematic review

et al. 2016

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“…Many biomarker genes have been proposed and evaluated; nevertheless, in the absence of a unique biomarker having sufficient specificity and sensitivity, a panel of multiple genes should be used [121][122][123] . Modifications of cancer-related genes could occur at genetic and epigenetic levels, affecting DNA repair.…”

Section: Clinical and Therapeutic Implications Of Intra-tumor Heterogmentioning

confidence: 99%

Breast Cancer Intra-Tumor Heterogeneity: One Tumor, Different Entities

Esparza-López

Escobar-Arriaga

Soto-Germes

et al. 2017

RIC

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In recent years, it has become evident that intra-tumor heterogeneity of breast cancer is a big challenge for the diagnosis, treatment, and clinical course of tumor-bearing patients. The advances in molecular biology and other technologies have led to the knowledge that a breast cancer tumor is comprised of multiple cellular entities. Here we review the two theories that have been described, trying to explain the origin of intra-tumor heterogeneity: clonal evolution and cancer stem cells. The first one considers that a single cell gives rise to many subpopulations through the accumulation of multiple aberrations, while the cancer stem cells theory foresees a hierarchical tumor evolution where only a few cells with self-renewal capacity give rise to different subpopulations. We also analyze the genetic, epigenetic, and microenvironment contributions to breast cancer intra-tumor heterogeneity. Finally, the clinical and therapeutic impact of intra-tumor heterogeneity on the outcome of breast cancer patients is discussed. (REV INVES CLIN. 2017;69:66-76)

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“…To validate genome-wide DNA methylation profiles during multistage hepatocarcinogenesis, Ammerpohl et al [105] revealed that the methylation status have changed gradually from normal to cirrhosis and further to HCC using a methylation array. Nagashiro et al [106] established criteria for carcinogenetic risk estimation based on DNA methylation array profiling to compare samples of noncancerous liver tissue obtained from HCC patients with normal liver tissue samples.…”

Section: Applications Of Microarraysmentioning

confidence: 99%

Genomic-Wide Analysis with Microarrays in Human Oncology

2015

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DNA microarray technologies have advanced rapidly and had a profound impact on examining gene expression on a genomic scale in research. This review discusses the history and development of microarray and DNA chip devices, and specific microarrays are described along with their methods and applications. In particular, microarrays have detected many novel cancer-related genes by comparing cancer tissues and non-cancerous tissues in oncological research. Recently, new methods have been in development, such as the double-combination array and triple-combination array, which allow more effective analysis of gene expression and epigenetic changes. Analysis of gene expression alterations in precancerous regions compared with normal regions and array analysis in drug-resistance cancer tissues are also successfully performed. Compared with next-generation sequencing, a similar method of genome analysis, several important differences distinguish these techniques and their applications. Development of novel microarray technologies is expected to contribute to further cancer research.

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DNA methylation array analyses identified breast cancer‐associated HYAL2 methylation in peripheral blood

Cited by 56 publications

References 50 publications

Blood-based DNA methylation as biomarker for breast cancer: a systematic review

Blood-based DNA methylation as biomarker for breast cancer: a systematic review

Breast Cancer Intra-Tumor Heterogeneity: One Tumor, Different Entities

Genomic-Wide Analysis with Microarrays in Human Oncology

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