台湾乳癌患者术后五年无复发的消融部位分析

IF 2.5 4区医学 Q3 ONCOLOGY

Cancer Control Pub Date : 2024-01-01 DOI:10.1177/10732748241300656

Che Lin, Chi-Yen Feng, Gilang P Bahari, Sheng-Min Huang, Cheng-Hao Wei, Qi Xu, Dat Thanh Dinh, Dar-Ren Chen, Po-Hsiung Lin

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引用次数: 0

摘要

目的：这项前瞻性研究旨在通过评估台湾乳腺癌患者术后治疗 5 年未复发（5 年生存者）（n = 70）的消旋位点（嘌呤/近嘧啶位点，AP 位点）背景水平，研究雌激素诱导的癌变。该研究还试图将这些 DNA 病变的程度与健康对照组和治疗前乳腺癌患者的病变程度进行比较：方法：使用醛反应探针测量缺损位点，并以每个核苷酸的缺损位点总数进行量化。使用腐胺或 T7 外切酶（T7 Exo）和/或外切酶 III（Exo III）进行消融位点裂解试验，对本研究招募的受试者的消融位点进行定性：与治疗前的乳腺癌患者（每106个总核苷酸中有50.3 ± 59.2个，P < 0.001）相比，5年存活者中检测到的消减位点数量（每106个总核苷酸中有26.7 ± 10.2个，n = 70）显著减少了46.9%，与健康对照组中观察到的水平（每106个总核苷酸中有23.3 ± 13.5个，P > 0.05）相似。对消融位点具体类型的进一步研究表明，对照组、乳腺癌患者和 5 年存活者中可被腐胺切除的消融位点数量分别为 63.3%、78.6% 和 67.7%。这些研究结果表明，DNA加合物的脱嘌呤/脱嘧啶作用与氧化应激有关，而非与DNA加合物的脱嘌呤/脱嘧啶作用有关。利用外切酶裂解测定法进行了进一步分析，以确定消融位点的具体类型，包括5'裂解位点、3'裂解位点、完整位点和残余消融位点。结果显示，在对照组、乳腺癌患者和 5 年存活者中检测到的残余消减位点比例估计分别为 32.7%、48.8% 和 34.0%：总之，这些研究结果表明，有明确的证据表明，治疗对降低乳腺癌患者的基底层消融点水平以及5年生存者的基底层消融点概况具有相关影响。

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Analysis of the Abasic Sites in Breast Cancer Patients With 5 Year Postoperative Treatment Without Recurrence in Taiwan.

Purpose: This prospective study aimed to investigate estrogen-induced carcinogenesis by assessing the background levels of abasic sites (apurinic/apyrimidinic sites, AP sites) in Taiwanese breast cancer patients following 5 years of postoperative treatment without recurrence (5-year survivors) (n = 70). The study also sought to compare the extent of these DNA lesions with those found in healthy controls and in breast cancer patients prior to treatment.

Methods: Abasic sites were measured using an aldehyde reactive probe and quantified as the total number of abasic sites per total nucleotides. Characterization of the abasic sites in subjects recruited for this study was conducted using the abasic site cleavage assay using putrescine or T7 exonuclease (T7 Exo) and/or exonuclease III (Exo III).

Results: The number of abasic sites detected in 5 year survivors (26.7 ± 10.2 per 10⁶ total nucleotides, n = 70) was significantly reduced by 46.9% compared to those in breast cancer patients before treatment (50.3 ± 59.2 per 10⁶ total nucleotides, P < 0.001), and was similar to the levels observed in healthy controls (23.3 ± 13.5 per 10⁶ total nucleotides, P > 0.05). Further investigation into the specific types of abasic sites indicated that the number of abasic sites excisable by putrescine in controls, breast cancer patients, and 5-year survivors were 63.3%, 78.6%, and 67.7%, respectively. These findings suggest the involvement of oxidative stress rather than depurination/depyrimidination of DNA adducts in the formation of abasic sites. Further analyses were performed using exonuclease cleavage assay to characterize the specific types of abasic sites including 5'-cleaved, 3'-cleaved, intact, and residual abasic sites. Results demonstrated that the proportion of residual abasic sites detected in controls, breast cancer patients, and 5-year survivors were estimated to be 32.7%, 48.8%, and 34.0%, respectively.

Conclusion: Overall, these findings suggest clear evidence of treatment-related effects on the reduction of levels of abasic sites as well as on the profile of abasic sites in 5 year survivors.

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来源期刊

Cancer Control ONCOLOGY-

CiteScore

3.80

自引率

0.00%

发文量

148

审稿时长

>12 weeks

期刊介绍： Cancer Control is a JCR-ranked, peer-reviewed open access journal whose mission is to advance the prevention, detection, diagnosis, treatment, and palliative care of cancer by enabling researchers, doctors, policymakers, and other healthcare professionals to freely share research along the cancer control continuum. Our vision is a world where gold-standard cancer care is the norm, not the exception.