Value of altered methylation patterns of genes RANBP3, LCP2 and GRAP2 in cfDNA in breast cancer diagnosis

Hu Qin; Mao Yu; Lan Haomiao; Wei Yi; Chen Yuehua; Ye Qiang; Che Hongying

doi:10.5937/jomb0-47507

Journal of Medical Biochemistry (Jan 2024)

Value of altered methylation patterns of genes RANBP3, LCP2 and GRAP2 in cfDNA in breast cancer diagnosis

Hu Qin,
Mao Yu,
Lan Haomiao,
Wei Yi,
Chen Yuehua,
Ye Qiang,
Che Hongying

Affiliations

Hu Qin: Zigong Maternal and Child Health Hospital, Department of Clinical Laboratory, Zigong, China
Mao Yu: Zigong First People's Hospital, Department of Thyroid and Breast Surgery, Zigong, China
Lan Haomiao: Zigong First People's Hospital, Department of Thyroid and Breast Surgery, Zigong, China
Wei Yi: Zigong Maternal and Child Health Hospital, Department of Clinical Laboratory, Zigong, China
Chen Yuehua: Zigong Maternal and Child Health Hospital, Department of Clinical Laboratory, Zigong, China
Ye Qiang: Zigong Maternal and Child Health Hospital, Department of Clinical Laboratory, Zigong, China
Che Hongying: Zigong First People's Hospital, Department of Thyroid and Breast Surgery, Zigong, China

DOI: https://doi.org/10.5937/jomb0-47507
Journal volume & issue: Vol. 43, no. 3
pp. 387 – 396

Abstract

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Background: The purpose of this study was to investigate the potential of plasma cfDNA methylation patterns in reflecting tumour methylation changes, focusing on three candidate sites, cg02469161, cg11528914, and cg20131654. These sites were selected for verification, with a particular emphasis on their association with breast cancer. Methods: We conducted a comprehensive analysis of 850k whole-methylation sequencing data to identify potential markers for breast cancer detection. Subsequently, we investigated the methylation status of the genes Ran-binding protein 3 (RANBP3), Lymphocyte cytoplasmic protein 2 (LCP2), and GRB2 related adaptor protein 2 (GRAP2), situated at the specified sites, using cancer and canceradjacent tissues from 17 breast cancer patients. We also examined the methylation patterns in different molecular subtypes and pathological grades of breast cancer. Additionally, we compared the methylation levels of these genes in plasma cfDNA to their performance in tissues. Results: Our analysis revealed that RANBP3, LCP2, and GRAP2 genes exhibited significant methylation differences between cancer and cancer-adjacent tissues. In breast cancer, these genes displayed diagnostic efficiencies of 91.0%, 90.6%, and 92.2%, respectively. Notably, RANBP3 showed a tendency towards lower methylation in HR+ breast cancer, and LCP2 methylation was correlated with tumour malignancy. Importantly, the methylation levels of these three genes in plasma cfDNA closely mirrored their tissue counterparts, with diagnostic efficiencies of 83.3%, 83.9%, and 77.6% for RANBP3, LCP2, and GRAP2, respectively. Conclusions: Our findings propose that the genes RANBP3, LCP2, and GRAP2, located at the identified methylation sites, hold significant potential as molecular markers in blood for the supplementary diagnosis of breast cancer. This study lays the groundwork for a more in-depth investigation into the changes in gene methylation patterns in circulating free DNA (cfDNA) for the early detection not only of breast cancer but also for various other types of cancer

Published in Journal of Medical Biochemistry

ISSN: 1452-8258 (Print); 1452-8266 (Online)
Publisher: Society of Medical Biochemists of Serbia, Belgrade
Country of publisher: Serbia
LCC subjects: Science: Chemistry: Organic chemistry: Biochemistry
Website: https://scindeks.ceon.rs/journaldetails.aspx?issn=1452-8258&lang=en

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