基于血浆 miRNA 表达的子宫内膜异位症无创诊断方法

I. M. Ordiyants, D. S. Novginov, Z. Zyukina, A. M. Khachatryan, S. Titov
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引用次数: 0

摘要

目的根据血浆微RNA浓度开发一种无创诊断外生殖器子宫内膜异位症的方法。回顾性检查在妇科接受常规腹腔镜检查的 80 名育龄妇女,根据腹腔镜检查和组织学检查的结果,将患者分为两组:主组--54 名经腹腔镜检查和组织学检查证实患有外生殖器子宫内膜异位症(EGE)的患者;对照组--26 名未患有外生殖器子宫内膜异位症的患者。腹腔镜检查前,对所有患者抽取血液样本,对 10 种微小核糖核酸的表达进行分子生物学研究:miR-183、miR-125b、miR-126、miR-16、miR-15a、miR-200a、miR-20a、miR-21、miR-222 和 miR-29b。研究和归一化 RNA(U6 RNA 和 103a microRNA)的鉴定是根据 Chen 等人的方法进行的。如果子宫内膜异位症患者组的表达量超过对照组,则以 2-ΔCt(主要)/2-ΔCt(对照)的形式给出表达比;如果反之,则以 2-ΔCt(对照)/2-ΔCt(主要)的形式给出表达比。对两组 10 个 mi-croRNA 的表达进行比较后发现,只有 miR-183 的表达有显著统计学差异:据统计,其在 EGE 患者中的表达是对照组妇女的 1.5 倍(p=0.017)。MIR-16的表达在我们所研究的患者中也没有统计学差异,而一组美国同行的研究表明,在子宫内膜异位症患者和子宫内膜异位症相关卵巢肿瘤患者中,MIR-16的表达有所增加。我们发现 mir-21 的表达没有差异。其他研究人员的研究结果相互矛盾:一些研究人员发现,与异位子宫内膜相比,子宫内膜样囊肿中的mir-21表达增加;与未受影响的子宫内膜相比,患有子宫内膜异位症的输卵管上皮中的mir-21表达增加;其他研究人员没有发现子宫内膜异位症患者的异位子宫内膜与健康妇女的子宫内膜有差异,但发现腹膜病灶和深部浸润性子宫内膜异位症病灶中的mir-21表达比异位子宫内膜低。在我们研究的子宫内膜异位症患者中,mir-222 的表达量减少了,这与现有的关于该 microRNA 促癌作用的观点相悖。在胃癌、膀胱癌、肝癌、肺癌、乳腺癌、子宫内膜癌和卵巢癌中,mir-222 的表达都有所增加。同时,mir-222 在前列腺癌、口腔鳞状细胞癌中的抑制作用也是众所周知的。考虑到通过 ROC 分析发现的 microRNA 表达的显著统计学差异,我们确定了它们在 EGE 诊断中的有效性和特异性。当然,要确认这些生物标志物的诊断价值,还需要对大量患者进行进一步研究。此外,我们的研究还无法确定生育能力受损患者的 microRNA 表达存在统计学差异。在我们的研究中,按 EGE 阶段划分的患者分布并不均衡(根本没有 I 阶段的妇女),因此无法根据疾病的 "服役期 "确定 microRNA 表达的统计学差异。
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Non-invasive diagnostics of endometriosis based on plasma miRNA expression
Aim. To develop a method for noninvasive diagnosis of external genital endometriosis based on plasma microRNA concentrations.Materials and Methods. 80 women of reproductive age who were admitted to the gynecological department for routine laparoscopy were retrospectively examined, according to the results of which and histological examination, the patients were divided into 2 groups: the main group — 54 patients with laparoscopically and histologically confirmed external genital endometriosis (EGE); the control group — 26 patients without EGE. Before laparoscopy, a blood sample was taken from all patients for a molecular-biological study of the expression of 10 microRNAs: miR-183, miR-125b, miR-126, miR-16, miR-15a, miR-200a, miR-20a, miR-21, miR-222 and miR-29b. Identification of the studied and normalizing RNAs (U6 RNA and 103a microRNA) was performed according to the method of Chen et al. The presented values of the expression of the studied microRNAs are given in the form of 2-ΔCt. The expression ratio is given in the form of 2-ΔCt (main)/2-ΔCt (control), if the expression in the group of patients with endometriosis exceeded that in the control group, and in the form of 2-ΔCt (control)/2-ΔCt (main), if vice versa.Results. Comparison of the expression of 10 mi-croRNAs between the two groups revealed statistically significant differences only in miR-183: its expression in patients with EGE was statistically 1.5 times higher than that in women of the control group (p=0.017).We have not detected a difference in the expression of mir-200a, while according to other researchers, representatives of the mir-200 family are among the most frequent whose expression changes with endometriosis. MIR-16 expression also did not differ statistically among the patients we examined, whereas a group of American colleagues revealed its increase in patients with endometriosis and with endometriosis-associated ovarian tumors. We found no difference in mir-21 expression. The results of other researchers are contradictory: some found its increase in endometrioid cysts compared with eutopic endometrium, an increase in the epithelium of the fallopian tubes with their endometriosis compared with unaffected; others did not reveal a difference between the eutopic endometrium of endometriosis patients and healthy women, but showed a decrease in expression in peritoneal foci and foci of deep infiltrative endometriosis compared with eutopic endometrium.The expression of mir-222 was reduced in the patients we examined with endometriosis, which goes against the existing ideas about the pro-oncogenic role of this microRNA. An increase in its expression in cancer of the stomach, bladder, liver, lungs, breast, endometrium, ovaries is described. At the same time, the oncosuppressive effect of mir-222 is also known in prostate cancer, squamous cell carcinoma of the oral cavity.Conclusion. Taking into account the revealed statistically significant difference in microRNA expression by ROC analysis, we determined their effectiveness and specificity in the diagnosis of EGE. Of course, further studies with a large contingent of patients are needed to confirm the diagnostic value of these biomarkers. In addition, our study did not allow us to establish a statistical difference in microRNA expression in patients with impaired fertility. But it is the test that makes it possible to differentiate female infertility — associated with endometriosis and without it, as a rule, tubal-peritoneal genesis — that will become a key tool in the personalized management of patients with infertility.In our work, the distribution of patients by stages of EGE turned out to be uneven (there were no women with stage I at all) and it was not possible to establish a statistical difference in microRNA expression depending on the "length of service" of the disease.
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