Altered cfDNA fragmentation profile in hypomethylated regions as diagnostic markers in breast cancer.

IF 4.2 2区 生物学 Q1 GENETICS & HEREDITY Epigenetics & Chromatin Pub Date : 2023-09-23 DOI:10.1186/s13072-023-00508-4
Jun Wang, Yanqin Niu, Ming Yang, Lirong Shu, Hongxian Wang, Xiaoqian Wu, Yaqin He, Peng Chen, Guocheng Zhong, Zhixiong Tang, Shasha Zhang, Qianwen Guo, Yun Wang, Li Yu, Deming Gou
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Abstract

Background: Breast cancer, the most common malignancy in women worldwide, has been proven to have both altered plasma cell-free DNA (cfDNA) methylation and fragmentation profiles. Nevertheless, simultaneously detecting both of them for breast cancer diagnosis has never been reported. Moreover, although fragmentation pattern of cfDNA is determined by nuclease digestion of chromatin, structure of which may be affected by DNA methylation, whether cfDNA methylation and fragmentation are biologically related or not still remains unclear.

Methods: Improved cfMeDIP-seq were utilized to characterize both cfDNA methylation and fragmentation profiles in 49 plasma samples from both healthy individuals and patients with breast cancer. The feasibility of using cfDNA fragmentation profile in hypo- and hypermethylated regions as diagnostic markers for breast cancer was evaluated.

Results: Mean size of cfDNA fragments (100-220 bp) mapped to hypomethylated regions decreased more in patients with breast cancer (4.60 bp, 172.33 to 167.73 bp) than in healthy individuals (2.87 bp, 174.54 to 171.67 bp). Furthermore, proportion of short cfDNA fragments (100-150 bp) in hypomethylated regions when compared with it in hypermethylated regions was found to increase more in patients with breast cancer in two independent discovery cohort. The feasibility of using abnormality of short cfDNA fragments ratio in hypomethylated genomic regions for breast cancer diagnosis in validation cohort was evaluated. 7 out of 11 patients were detected as having breast cancer (63.6% sensitivity), whereas no healthy individuals were mis-detected (100% specificity).

Conclusion: We identified enriched short cfDNA fragments after 5mC-immunoprecipitation (IP) in patients with breast cancer, and demonstrated the enriched short cfDNA fragments might originated from hypomethylated genomic regions. Furthermore, we proved the feasibility of using differentially methylated regions (DMRs)-dependent cfDNA fragmentation profile for breast cancer diagnosis.

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低甲基化区域cfDNA断裂谱的改变作为乳腺癌症的诊断标志物。
背景:癌症是全球女性最常见的恶性肿瘤,已被证明具有改变的血浆无细胞DNA(cfDNA)甲基化和碎片化特征。尽管如此,同时检测两者用于乳腺癌症诊断的报道从来没有。此外,尽管cfDNA的断裂模式是由染色质的核酸酶消化决定的,染色质的结构可能受到DNA甲基化的影响,但cfDNA甲基化和断裂是否具有生物学相关性仍不清楚。方法:利用改良的cfMeDIP-seq对癌症患者和健康个体的49份血浆样品的cfDNA甲基化和片段化特征进行了表征。评价了在低甲基化和高甲基化区域使用cfDNA片段谱作为癌症诊断标志物的可行性。结果:癌症患者定位于低甲基化区域的cfDNA片段(100-220bp)的平均大小(4.60bp,172.33至167.73bp)比健康人(2.87bp,174.54至171.67bp)减少得更多,在两个独立的发现队列中,发现癌症患者低甲基化区域中短cfDNA片段(100-150bp)的比例与高甲基化区域相比增加更多。评估了在验证队列中使用低甲基化基因组区域短cfDNA片段比率异常用于乳腺癌症诊断的可行性。11名患者中有7名被检测出患有癌症(敏感性63.6%),而没有健康人被检测出有误(特异性100%)。结论:我们在癌症患者中鉴定了经5mC-免疫沉淀(IP)后富集的短cfDNA片段,并证明富集的短cfDNA片段可能来源于低甲基化基因组区域。此外,我们证明了使用差异甲基化区域(DMRs)依赖的cfDNA片段图谱诊断乳腺癌症的可行性。
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来源期刊
Epigenetics & Chromatin
Epigenetics & Chromatin GENETICS & HEREDITY-
CiteScore
7.00
自引率
0.00%
发文量
35
审稿时长
1 months
期刊介绍: Epigenetics & Chromatin is a peer-reviewed, open access, online journal that publishes research, and reviews, providing novel insights into epigenetic inheritance and chromatin-based interactions. The journal aims to understand how gene and chromosomal elements are regulated and their activities maintained during processes such as cell division, differentiation and environmental alteration.
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