miR-190和ANXA11对直肠癌新辅助放化疗效用评估价值及相关性分析

doi:10.3969/j.issn.1006-6233.2023.12.03

摘要
图/表
参考文献
相关文章 (15)

全文: PDF (1427 KB) HTML (1 KB)
输出: BibTeX | EndNote (RIS)

摘要 目的: 分析微小核苷酸190(miR-190)及膜联蛋白A11(ANXA11)在直肠癌新辅助放化疗(NAC)评估中的作用及相关性。方法: 选取2019年6月至2022年8月在我院确诊为直肠癌并接受治疗的148例患者作为研究对象,将其纳入直肠癌组,另选取同时期150例健康人作为对照组。实时荧光定量检测(RT-PCR)检测两组受试者血清miR-190、ANXA11 mRNA表达;对所有直肠癌患者术前均采用相同新辅助放化疗(NAC),按照疗效评估标准分为疗效优良组(n=89)与疗效较差组(n=59),对比两组患者血清miR-190、ANXA11 mRNA表达,分析血清miR-190、ANXA11 mRNA表达与临床疗效的关系;绘制Kaplan-meier观察miR-190、ANXA11 mRNA高低表达对NAC临床疗效影响;ROC分析miR-190、ANXA11单一及联合检测对NAC临床效用评估价值。结果: 相比于对照组,直肠癌患者miR-190表达显著降低,而ANXA11 mRNA表达显著升高(0.87±0.18vs1.53±0.30、2.00±0.68vs0.95±0.09,t=-22.719、18.731,P<0.05);相比于疗效较差组,疗效优良组患者miR-190表达显著升高,而ANXA11 mRNA表达显著降低(0.96±0.15vs0.73±0.15、1.81±0.47vs2.28±0.83,t=8.932、-3.958,均P<0.05);Spearman相关系数分析miR-190与NAC疗效呈正相关,而ANXA11 mRNA表达与NAC疗效呈负相关(P<0.05);Kaplan-meier曲线显示,miR-190高表达组患者NAC疗效优良率显著高于miR-190低表达组(χ²=39.120,P<0.001),ANXA11 mRNA低表达组患者NAC疗效优良率显著高于ANXA11 mRNA高表达组(χ²=8.772,P=0.003);ROC显示miR-190、ANXA11联合检测的AUC显著高于单一检测(P<0.05),敏感度为84.75%,特异度为87.64%。结论: miR-190、ANXA11在不同NAC疗效患者中均具有特异性表达特征,并且与NAC疗效之间具有密切联系,通过联合miR-190、ANXA11检测能够有效预测NAC临床效用,为临床评估直肠癌疗效提供新思路。

	服务

	把本文推荐给朋友
	加入我的书架
	加入引用管理器
	E-mail Alert
	RSS
	作者相关文章

关键词 ：直肠癌, miR-190, 膜联蛋白A11

Abstract：Objective: To analyze the roles and relationship of microRNA 190 (miR-190) and membrane-associated protein A11 (ANXA11) in the evaluation of neoadjuvant radiotherapy (NAC) for rectal cancer. Methods: A total of 148 patients who were diagnosed with rectal cancer and received treatment in our hospital from June 2019 through August 2022 were selected as the study subjects and included in the rectal cancer group, and 150 healthy people who underwent general physical examination in our hospital during the same period were selected as the control group, and real-time fluorescence quantitative detection (RT-PCR) detected the expression of serum miR-190 and ANXA11 mRNA in the two groups. All rectal cancer patients were treated with the same neoadjuvant radiotherapy and chemotherapy (NAC) before surgery, and were divided into the excellent efficacy group (n=89) and the poor efficacy group (n=59) according to the efficacy assessment criteria, and the serum miR-190 and ANXA11 mRNA expression of the patients in the two groups were compared. Spearman's correlation coefficient was used to analyze the relationship between serum miR-190, ANXA11 mRNA expression and clinical efficacy; Kaplan-meier was plotted to observe the effect of high and low miR-190, ANXA11 mRNA expression on the clinical efficacy of NAC; Subject operating characteristic curves (ROCs) were plotted to analyze the value of miR-190, ANXA11 single and combined assays for clinical utility assessment of NAC. Results: Compared with the control group, miR-190 expression was significantly lower, while ANXA11 mRNA expression was significantly higher in rectal cancer patients (0.87±0.18 vs 1.53±0.30, 2.00±0.68 vs 0.95±0.09, t=-22.719, 18.731, P<0.05). Compared with the poor-efficacy group, miR-190 expression was significantly higher in patients in the excellent-efficacy group, while ANXA11 mRNA expression was significantly lower (0.96±0.15vs0.73±0.15, 1.81±0.47vs2.28±0.83, t=8.932, -3.958, all P<0.05); Spearman correlation coefficient analysis showed that miR-190 was positively correlated with NAC efficacy, while ANXA11 mRNA expression was negatively correlated with NAC efficacy (P＜0.05); Kaplan-meier curves showed that the NAC efficacy excellence rate of the patients in the miR-190 high-expression group was significantly higher than that of the patients in the miR-190 low-expression group (χ²=39.120, P＜0.001), and the excellent rate of NAC efficacy in patients in the ANXA11 mRNA low expression group was significantly higher than that in the ANXA11 mRNA high expression group (χ²=8.772, P=0.003); the ROC showed that the area under the curve (AUC) of the combined assay of miR-190 and ANXA11 was significantly higher than that of the single assay (P＜0.05), and the sensitivity was 84.75%, the specificity of 87.64%. Conclusion: miR-190 and ANXA11 have specific expression levels in patients with different NAC efficacy, and there is a close association between them and NAC efficacy. miR-190 and ANXA11 detection can effectively predict the clinical utility of NAC by combining miR-190 and ANXA11 assays, which can provide a new idea for the clinical assessment of rectal cancer efficacy.

Key words： Rrectal cancer miR-190 Membrane-bound protein A11

基金资助:江苏省卫生健康委医学科研项目,(编号:2020215)

引用本文:

徐钰, 胡锡池, 赵于天. miR-190和ANXA11对直肠癌新辅助放化疗效用评估价值及相关性分析[J]. 河北医学, 2023, 29(12): 1946-1951.
XU Yu, et al. Evaluation and Correlation Analysis of the Therapeutic Value of miR-190 and ANXA11 in Neoadjuvant Chemoradiotherapy for Rectal Cancer. HeBei Med, 2023, 29(12): 1946-1951.

链接本文:

http://www.hbyxzzs.cn/CN/10.3969/j.issn.1006-6233.2023.12.03 或 http://www.hbyxzzs.cn/CN/Y2023/V29/I12/1946

[1] Wilkinson N.Management of rectal cancer[J].Surg Clin North Am,2020,100(3):615-628.
[2] Lang D,Ciombor KK.Diagnosis and management of rectal cancer in patients younger than 50 years:rising global incidence and unique challenges[J].Natl Compr Canc Netw,2022,20(10):1169-1175.
[3] Keller DS,Berho M,Perez RO,et al.The multidisciplinary management of rectal cancer[J].Nat Rev Gastroenterol Hepatol,2020,17(7):414-429.
[4] Vendrely V,Rivin Del Campo E,Modesto A,et al.Rectal cancer radiotherapy[J].Cancer Radiother,2022,26(1-2):272-278.
[5] Wang Z,Su C.Effects of folic acid deficiency on genetic damage in colorectal cancer cells[J].Am Transl Res,2023,15(5):3162-3171.
[6] Qi J,Wang Z,Zhao Z,et al.EIF3J-AS1 promotes glioma cell growth via up-regulating ANXA11 through sponging miR-1343-3p[J].Cancer Cell Int,2020,20(1):428.
[7] 中华人民共和国国家卫生和计划生育委员会.直肠癌规范化诊疗指南(试行)[J].慢性病学杂志,2013,14(10):721-726.
[8] Liu D,Langer R.Grading der Tumorregression gastrointestinaler karzinome nach neoadjuvanter therapie grading of tumor regression of gastrointestinal carcinomas after neoadjuvant therapy[J].Pathologe,2022,43(1):51-56.
[9] 潘驰,孙晓晖,张增智,等.2014-2020年青岛市居民结直肠癌流行及疾病负担趋势分析[J].中华肿瘤防治杂志,2022,29(20):1439-1445.
[10] Stoffel EM,Murphy CC.Epidemiology and mechanisms of the increasing incidence of colon and rectal cancers in young adults[J].Gastroenterology,2020,158(2):341-353.
[11] Bachet JB,Benoist S,Mas L,et al.Traitement néoadjuvant des cancers du rectum Neoadjuvant treatment for rectal cancer[J].Bull Cancer,2021,108(9):855-867.
[12] Sun G,Liu M,Han H.Overexpression of microRNA-190 inhibits migration,invasion,epithelial-mesenchymal transition,and angiogenesis through suppression of protein kinase B-extracellular signal-regulated kinase signaling pathway via binding to stanniocalicin 2 in breast cancer[J].Cell Physiol,2019,234(10):17824-17838.
[13] Yu Y,Yin W,Yu ZH,et al.miR-190 enhances endocrine therapy sensitivity by regulating SOX9 expression in breast cancer[J].Exp Clin Cancer Res,2019,38(1):22.
[14] Yu Y,Luo W,Yang ZJ,et al.miR-190 suppresses breast cancer metastasis by regulation of TGF-β-induced epithelial-mesenchymal transition[J].Mol Cancer,2018,17(1):70.
[15] Ye R,Lu X,Liu J,et al.CircSOD2 contributes to tumor progression,immune evasion and anti-PD-1 resistance in hepatocellular carcinoma by targeting miR-497-5p/ANXA11 axis[J].Biochem Genet,2023,61(2):597-614.
[16] Liu Z,Wang Y,Wang L,et al.Long non-coding RNA AGAP2-AS1,functioning as a competitive endogenous RNA,upregulates ANXA11 expression by sponging miR-16-5p and promotes proliferation and metastasis in hepatocellular carcinoma retracted in[J].Exp Clin Cancer Res,2022,41(1):317.