EXPRESSION PROFILE OF miR-145, -182, -21, -27a, -29b, and -34a IN BREAST CANCER PATIENTS OF YOUNG AGE.

V Chekhun, T Borikun, O Mushii, T Zadvornyi, О Martyniuk, E Kashuba, V Bazas, S Hrybach, M Krotevych, S Lyalkin, N Lukianova
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Abstract

Background: Breast cancer (BC) in young women remains a significant public health concern. While progress has been made in understanding the etiology, diagnosis, and treatment of BC in this population, challenges persist. The identification and utilization of prognostic biomarkers offer valuable tools for tailoring treatment strategies and improving outcomes for BC patients.

Aim: To evaluate the relationship between the expression of tumor-associated microRNAs and the clinical and pathological features of BC in young patients.

Materials and methods: The work is based on the results of the examination and treatment of 50 women younger than 45 years with stage I-II BC. miR-145, -182, -21, -27a, -29b, and -34a expression in tumor samples was analyzed by the real-time reverse transcription polymerase chain reaction.

Results: Higher expression of miR-182, -21, and -29b and lower levels of miR-27a were associated with tumor stage in young BC patients. Patients without lymph node metastases (N0) had significantly higher levels of miR-182, -27a, and -34a and lower levels of miR-29b compared to N1 cases (p < 0.05). Expression of miR-145, -182, -21, -27a, and -29b was associated with molecular BC subtypes.

Conclusion: Obtained results show that a high malignancy degree of BC in young women is associated with an increase in the miR-182, -21, -29b, and -34a expressions and a decrease in the miR-27a level in the tumor tissue, which indicates the prospects of the use of them for predicting the aggressiveness of the disease.

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年轻乳腺癌患者中 miR-145、-182、-21、-27a、-29b 和 -34a 的表达谱。
背景:年轻女性患乳腺癌(BC)仍然是一个重大的公共卫生问题。虽然在了解年轻女性乳腺癌的病因、诊断和治疗方面取得了进展,但挑战依然存在。预后生物标志物的鉴定和利用为调整治疗策略和改善BC患者的预后提供了宝贵的工具。目的:评估肿瘤相关microRNAs的表达与年轻患者BC的临床和病理特征之间的关系:通过实时逆转录聚合酶链反应分析肿瘤样本中miR-145、-182、-21、-27a、-29b和-34a的表达情况:结果:在年轻的 BC 患者中,miR-182、-21 和 -29b 的表达量较高,而 miR-27a 的表达量较低,这与肿瘤分期有关。与 N1 病例相比,无淋巴结转移(N0)患者的 miR-182、-27a 和 -34a 水平明显较高,而 miR-29b 水平较低(p < 0.05)。miR-145、-182、-21、-27a和-29b的表达与BC分子亚型有关:结论:研究结果表明,年轻女性BC恶性程度高与肿瘤组织中miR-182、-21、-29b和-34a表达量的增加以及miR-27a水平的降低有关,这预示着利用它们预测疾病侵袭性的前景。
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