P90

Q3 Medicine
A. Ponomaryova , E. Rykova , N. Cherdyntseva , E. Morozkin , I. Zaporozhchenko , T. Skvortsova , A. Dobrodeev , A. Zav’yalov , S. Tuzikov , V. Vlassov , P. Laktionov
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引用次数: 3

摘要

血液中循环肿瘤核酸(dna和rna)的分析似乎是发展低侵入性肿瘤检测方法的一种有前途的方法,具有临床应用价值。在血浆/血清中检测到致癌和抑瘤mirna是它们参与发病机制的证据,并提示它们作为肿瘤标志物和治疗靶点的可能性。因此,确定血浆中肿瘤相关mirna的表达水平可以在了解肿瘤的发展和治疗方面取得重大进展。目的评估联合治疗期间肺癌患者血浆中mirna (miR-19b、miR-25、miR-125b、miR-126、miR-205)表达水平的变化,并评估其作为疾病监测标志物的价值。材料和方法取自托木斯克癌症研究所治疗的非小细胞肺癌患者(n = 23)的血液样本。这些样品被稳定并分离成血浆和血细胞。采用单相无酚萃取法从血浆中分离MicroRNA,并在硅基自旋柱上纯化(BioSilica Ltd, Novosibirsk, Russia)。通过定量RT-PCR检测上述5种mirna的浓度,并通过dCt方法归一化为miR-16。结果本研究分析了肺癌患者在联合治疗期间血浆循环DNA的动态表达变化。采用成熟的方法学方法,从非小细胞肺癌患者治疗前、化疗完成后30天内和手术后15天内的血浆样本中分离循环mirna。在对miR-19b和miR-125b进行分析的情况下发现,miRNA的表达水平与化疗和手术的临床反应相关。miR-19b水平升高和miR-125b水平降低与治疗反应相关。通过重复测量方差分析,我们发现在联合治疗期间,miR-19b和miR-125b在三个检查点的表达水平变化具有显著的立方趋势(P = 0.00284和P = 0.029)。治疗后随访期间miRNA-126表达水平变化无明确趋势,与其他mirna表达水平变化无相关性。结果显示miRNA-25和miRNA-205的表达水平有显著的相关性,但没有发现这些mirna水平变化的趋势。结论本研究中循环miR-19b和miR-125b表达分析的临床应用仍有待于在不同肿瘤组织学类型、不同疾病阶段和结局的大队列患者中进行验证。纳入该组的标准之一必须是对治疗的易感性和/或耐药性。这项研究是在俄罗斯科学支持基金会(14-04-01881)的资助下进行的,TPU博士后项目。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
P90

Background

The analysis of circulating tumor nucleic acids (DNAs and RNAs) in the blood seems to be a promising approach for the development of the low-invasive methods of tumor detection, valuable for clinical practice. Detection of oncogenic and tumor suppressor miRNAs in the blood plasma/serum is evidence of their participation in pathogenesis and suggest the possibility of their use as tumor markers and targets for therapy. Thus, the determination of expression level of tumor-associated miRNAs in plasma can lead to significant progress in understanding the tumor development and treatment.

Aim

Estimation the changes in expression level of miRNAs (miR-19b, miR-25, miR-125b, miR-126, miR-205) in blood plasma from lung cancer patients during combined therapy and to estimate their value as disease monitoring markers.

Materials and methods

Blood samples were taken from patients (n = 23) with non-small cell lung cancer treated at the Tomsk Cancer Research Institute. These samples were stabilized and fractionated into plasma and blood cells. MicroRNA was isolated from blood plasma using single-phase phenol-free extraction protocol and purified on silica-based spin columns (BioSilica Ltd, Novosibirsk, Russia). Concentration of five above mentioned miRNAs was measured by quantitative RT-PCR and normalized to miR-16 using dCt method.

Results

In this study we analyzed the dynamic expression changes of circulating DNA in blood plasma from lung cancer patients during the combined therapy. Circulating miRNAs were isolated from plasma samples of non-small cell lung cancer patients before treatment, within 30 days after completing chemotherapy and 15 days after surgery, by using developed methodological approach. In case of miR-19b and miR-125b analysis was found that the miRNA expression level correlates with clinical response to chemotherapy and surgery. Increasing level of miR-19b and decreasing level of miR-125b were associated with therapeutic response. Using Repeated measures ANOVA analysis we demonstrated that the miR-19b and miR-125b expression levels changes throughout three check-up points during the combined treatment are characterized by the significant cubic trend (P = 0.00284 and P = 0.029, respectively). Changes of miRNA-126 expression level during post-treatment follow-up were not characterized by the definite trend and not correlated with changes of other miRNAs expression level. It was shown the significant correlation between miRNA-25 and miRNA-205 expression levels, but was not found the trend of these miRNAs level changes.

Conclusion

The clinical utility of the circulating miR-19b and miR-125b expression analysis from this study remains to be validated in large cohorts of patients with different histological types of tumors, at the different stage of disease and outcomes. One of the criteria for inclusion in the group must be susceptibility and/or resistance to therapy.

The research has been carried out with support of the grant from the Russian Science Support Foundation 14-04-01881, Post-doctorate program in TPU.

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来源期刊
Ejc Supplements
Ejc Supplements 医学-肿瘤学
自引率
0.00%
发文量
0
审稿时长
3.7 months
期刊介绍: EJC Supplements is an open access companion journal to the European Journal of Cancer. As an open access journal, all published articles are subject to an Article Publication Fee. Immediately upon publication, all articles in EJC Supplements are made openly available through the journal''s websites. EJC Supplements will consider for publication the proceedings of scientific symposia, commissioned thematic issues, and collections of invited articles on preclinical and basic cancer research, translational oncology, clinical oncology and cancer epidemiology and prevention. Authors considering the publication of a supplement in EJC Supplements are requested to contact the Editorial Office of the EJC to discuss their proposal with the Editor-in-Chief. EJC Supplements is an official journal of the European Organisation for Research and Treatment of Cancer (EORTC), the European CanCer Organisation (ECCO) and the European Society of Mastology (EUSOMA).
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