Hypermethylated PCDHGB7 as a Biomarker for Early Detection of Endometrial Cancer in Endometrial Brush Samples and Cervical Scrapings

Yuan, Jiangzi; Mao, Zhanrui; Lü, Qing; Xu, Peng; Wang, Chengyang; Xu, Xiaona; Zhou, Zhaowei; Zhang, Tongsheng; Yu, Wenqiang; Dong, Shihua; Wang, Yudong; Cheng, Weiwei

doi:10.3389/fmolb.2021.774215

Cited by 8 publications

(10 citation statements)

References 34 publications

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“…Similarly, previous reports documented 3-gene panel (BHLHE22-CDO1-CELF4/BHLHE22-CDO1-TBX5) or single gene-based (PCDHGB7) DNA methylation for EC detection using cervical scrapings, the ROC for these markers ranged from 0.80 to 0.94, or 0.86, respectively. 11 – 13 Also, Wang et al 26 reported a relevant study on methylation marker-based EC screening in endometrial cytological samples using Li Brush. Compared with endometrial sampling, cervical Pap brush sampling is a more acceptable screening tool for the general population.…”

Section: Discussionmentioning

confidence: 99%

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Endometrial Cancer Detection by DNA Methylation Analysis in Cervical Papanicolaou Brush Samples

Wang,

Du,

et al. 2024

Technol Cancer Res Treat

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Background: Endometrial cancer (EC) is the leading gynecological cancer worldwide, yet current EC screening approaches are not satisfying. The purpose of this retrospective study was to evaluate the feasibility and capability of DNA methylation analysis in cervical Papanicolaou (Pap) brush samples for EC detection. Methods: We used quantitative methylation-sensitive PCR (qMS-PCR) to determine the methylation status of candidate genes in EC tissue samples, as well as cervical Pap brushes. The ability of RASSF1A and HIST1H4F to serve as diagnostic markers for EC was then examined in cervical Pap brush samples from women with endometrial lesions of varying degrees of severity. Results: Methylated RASSF1A and HIST1H4F were found in EC tissues. Further, methylation of the two genes was also observed in cervical Pap smear samples from EC patients. Methylation levels of RASSF1A and HIST1H4F increased as endometrial lesions progressed, and cervical Pap brush samples from women affected by EC exhibited significantly higher levels of methylated RASSF1A and HIST1H4F compared to noncancerous controls ( P < .001). Receiver operating characteristic (ROC) curves and area under the curve (AUC) analyses revealed RASSF1A and HIST1H4F methylation with a combined AUC of 0.938 and 0.951 for EC/pre-EC detection in cervical Pap brush samples, respectively. Conclusion: These findings demonstrate that DNA methylation analysis in cervical Pap brush samples may be helpful for EC detection, broadening the scope of the commonly used cytological screening. Our proof-of-concept study provides new insights into the field of clinical EC diagnosis.

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Section: Discussionmentioning

confidence: 99%

“… 11 Similar studies furthermore demonstrated that cervical scrapings, instead of endometrium and blood, are a good source of DNA for molecular testing, and DNA methylated genes as biomarkers for EC detection from cervical scrapings is feasible and appealing. 11 – 13 However, relevant research is relatively uncommon.…”

Section: Introductionmentioning

confidence: 99%

Endometrial Cancer Detection by DNA Methylation Analysis in Cervical Papanicolaou Brush Samples

Wang,

Du,

et al. 2024

Technol Cancer Res Treat

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“…In addition, gene methylation, especially in ADCYAP1 and HAND2 , can be identified prior to the diagnosis of EC [ 42 ]. Hypermethylated PCDHGB7 has been identified as a new cancer marker and is applicable in early screening for EC and CC [ 43 ]. Thus, abnormal DNA methylation could serve as a promising indicator for the detection of EC and CC.…”

Section: Targeting Epigenetic Modifiers In Gynecological Cancersmentioning

confidence: 99%

New insights for gynecological cancer therapies: from molecular mechanisms and clinical evidence to future directions

Zhang

Sheng

Sun

et al. 2023

Cancer Metastasis Rev

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Advanced and recurrent gynecological cancers lack effective treatment and have poor prognosis. Besides, there is urgent need for conservative treatment for fertility protection of young patients. Therefore, continued efforts are needed to further define underlying therapeutic targets and explore novel targeted strategies. Considerable advancements have been made with new insights into molecular mechanisms on cancer progression and breakthroughs in novel treatment strategies. Herein, we review the research that holds unique novelty and potential translational power to alter the current landscape of gynecological cancers and improve effective treatments. We outline the advent of promising therapies with their targeted biomolecules, including hormone receptor-targeted agents, inhibitors targeting epigenetic regulators, antiangiogenic agents, inhibitors of abnormal signaling pathways, poly (ADP-ribose) polymerase (PARP) inhibitors, agents targeting immune-suppressive regulators, and repurposed existing drugs. We particularly highlight clinical evidence and trace the ongoing clinical trials to investigate the translational value. Taken together, we conduct a thorough review on emerging agents for gynecological cancer treatment and further discuss their potential challenges and future opportunities.

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“…Previously, we have proposed the concept of universal cancer–only methylation (UCOM), a collection of cancer-specific epigenetic features shared among most cancer types ( 24 , 25 ). The clinical value of several markers has already been demonstrated in early diagnosis of specific cancer types, including lung cancer, cervical cancer, and endometrial cancer ( 24 , 26 , 27 ). However, the clinical utility of their pan-cancer characteristics remains to be demonstrated in a real-world study with diverse tumor types.…”

Section: Introductionmentioning

confidence: 99%

Diagnosis of malignant body fluids via cancer-universal methylation in cell-free DNA

Mao,

Dong,

Yan

et al. 2024

JCI Insight

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BACKGROUND Differentiating malignant from nonmalignant body fluids remains a clinical challenge because of the unsatisfying performance of conventional cytology. We aimed to improve the sensitivity and ubiquity of cancer cell detection by assaying universal cancer–only methylation (UCOM) markers in supernatant cell-free DNA (cfDNA). METHODS An observational prospective cohort including 1,321 nonmalignant and malignant body fluids of multiple cancers was used to develop and validate a cfDNA UCOM methylation diagnostic assay. All samples were divided into 2 portions for cytology and supernatant cfDNA methylation analysis. RESULTS The significant hypermethylation of a potentially novel UCOM marker, TAGMe, together with the formerly reported PCDHGB7 , was identified in the cfDNA of malignant body fluid samples. The combined model, cell-free cancer-universal methylation (CUE), was developed and validated in a prospective multicancer cohort with markedly elevated sensitivity and specificity, and was further verified in a set containing additional types of malignant body fluids and metastases. In addition, it remained hypersensitive in detecting cancer cells in cytologically negative malignant samples. CONCLUSION cfDNA methylation markers are robust in detecting tumor cells and are applicable to diverse body fluids and tumor types, providing a feasible complement to current cytology-based diagnostic analyses. TRIAL REGISTRATION This study was registered at Chictr.org.cn (ChiCTR2200060532). FUNDING National Natural Science Foundation of China (32270645, 31872814, 32000505, 82170088), the National Key R&D Program of Ningxia Hui Autonomous region (2022BEG01003), Shanghai Municipal Key Clinical Specialty (shslczdzk02201), Science and Technology Commission of Shanghai Municipality (20DZ2261200, 20DZ2254400), and Major Special Projects of Basic Research of Shanghai Science and Technology Commission (18JC1411101).

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Hypermethylated PCDHGB7 as a Biomarker for Early Detection of Endometrial Cancer in Endometrial Brush Samples and Cervical Scrapings

Cited by 8 publications

References 34 publications

Endometrial Cancer Detection by DNA Methylation Analysis in Cervical Papanicolaou Brush Samples

Endometrial Cancer Detection by DNA Methylation Analysis in Cervical Papanicolaou Brush Samples

New insights for gynecological cancer therapies: from molecular mechanisms and clinical evidence to future directions

Diagnosis of malignant body fluids via cancer-universal methylation in cell-free DNA

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