Expression and clinical significance of long noncoding RNA CCAT2 in serum of patients with gastric cancer

doi:10.3969/j.issn.1673-8640.2019.09.001

Abstract

Abstract:

Objective To investigate the relative expression of serum long noncoding RNA（lncRNA） colon cancer-associated transcript 2（CCAT2） in patients with gastric cancer（GC） and its role in the early diagnosis and prognosis monitoring of GC. Methods A total of 40 GC patients diagnosed by pathology department were enrolled from the Affiliated Hospital of Nantong University,and their preoperative and postoperative serum samples were collected. Totally,30 patients with gastric benign lesions（gastric ulcers and gastric polyps） and 43 age-matched healthy subjects（healthy control group） were enrolled. The relative expression of CCAT2 was determined by real-time fluorescence quantitation polymerase chain reaction（PCR）,and chemiluminescence immunoassay was used to determine carcinoembryonic antigen（CEA）and carbohydrate antigen 19-9（CA19-9）. Receiver operating characteristic（ROC） curve was used to evaluate the diagnostic efficiency of CCAT2. Results Comparing with gastric benign lesion and healthy control groups,the relative expression of CCAT2 were higher in GC group（P<0.01）,and there was no statistical significance between gastric benign lesion and healthy control groups（P>0.05）. The preoperative relative expression of CCAT2 was higher than postoperative one with statistical significance（P<0.01）. High expression levels of CCAT2 were correlated with tumor size（P=0.028）,TNM stage（P=0.012） and lymph node metastasis（P=0.034）,and there was no correlation with age and sex（P>0.05）. The area under ROC curve（AUC） of CCAT2 was 0.851 [95% confidence interval（CI） 0.772-0.930,P<0.05] for the differential diagnosis of GC patients from healthy subjects. For the differential diagnosis of GC from gastric benign lesions,the AUC was 0.808（95% CI 0.701-0.916,P<0.05） as the cut-off value of 1.125. The combined determination of CCAT2 with CEA and CA19-9 can improve the sensitivity（98%）. There was no correlation between relative expression of CCAT2 and CEA,CA19-9 in GC group. Conclusions As a new biological marker,CCAT2 plays a role in the diagnosis and prognosis monitoring of GC,and it can improve the diagnostic efficiency combined with CEA and CA19-9 in GC patients.

Key words: Gastric cancer, Long noncoding RNA, Colon cancer-associated transcript 2, Early diagnosis

CLC Number:

R446.1

CAO Jijun, WANG Jinhu, SHEN Xianjuan, JU Shaoqing. Expression and clinical significance of long noncoding RNA CCAT2 in serum of patients with gastric cancer[J]. Laboratory Medicine, 2019, 34(9): 775-779.

Figures/Tables 4

References 13

[1]	CHEN W,ZHENG R,BAADE P D,et al.Cancer statistics in China,2015[J]. CA cancer J Clin,2016,66(2):115-132.
[2]	ZHU X,LV M,WANG H,et al.Identification of circulating microRNAs as novel potential biomarkers for gastric cancer detection:a systematic review and meta-analysis[J]. Dig Dis Sci,2014,59(5):911-919.
[3]	WU H H,LIN W C,TSAI K W. Advances in molecular biomarkers for gastric cancer:miRNAs as emerging novel cancer markers[J]. Expert Rev Mol Med,2014,16:el.
[4]	DURÃES C,ALMEIDA G M,SERUCA R,et al. Biomarkers for gastric cancer:prognostic,predictive or targets of therapy?[J]. Virchows Arch,2014,464(3):367-378.
[5]	SOBIN L H,WITTEKIND C H.TNM:classification of malignant tumors[M]. 5th ed. New York:WILEY-LISS,1997:59-62.
[6]	HAMASHIMA C.Current issues and future perspectives of gastric cancer screening[J]. World J Gastroenterol,2014,20(38): 13767-13774.
[7]	魏婷婷, 杨敏, 唐晴琴,等. 长链非编码RNA在免疫炎症反应中的研究进展[J]. 检验医学,2015,30(10):1044-1047.
[8]	SUN W,YANG Y,XU C,et al.Roles of long noncoding RNAs in gastric cancer and their clinical applications[J]. J Cancer Res Clin Oncol, 2016, 142(11): 2231-2237.
[9]	LING H,SPIZZO R,ATLASI Y,et al.CCAT2,a novel noncoding RNA mapping to 8q24,underlies metastatic progression and chromosomal instability in colon cancer[J]. Genome Res,2013,23(9):1446-1461.
[10]	REDIS R S,VELA L E,LU W,et al.Allele-specific reprogramming of cancer metabolism by the long non-coding RNA CCAT2[J]. Mol Cell,2016,61(4):520-534.
[11]	REDIS R S,SIEUWERTS A M,LOOK M P,et al.CCAT2,a novel long non-coding RNA in breast cancer:expression study and clinical correlations[J]. Oncotarget,2013,4(10):1748-1762.
[12]	WANG Y J,LIU J Z,LV P,et al.Long non-coding RNA CCAT2 promotes gastric cancer proliferation and invasion by regulating the E-cadherin and LATS2[J]. Am J Cancer Res,2016,6(11):2651-2660.
[13]	LAM S Y,YU J,WONG S H,et al.The gastrointestinal microbiota and its role in oncogenesis[J]. Best Pract Res Clin Gastroenterol,2017,31(6):607-618.

临床病理特征	例数	CCAT2相对表达 [例（%）]		统计值
临床病理特征	例数	低表达（6例）	高表达（34例）	χ²值	P值
性别				0.60	0.440
男	28	5（21.7）	23（78.3）
女	12	1（8.3）	11（91.7）
年龄（岁）				0.26	0.609
≤60	10	1（10.0）	9（90.0）
>60	30	5（16.7）	25（83.3）
肿瘤大小				4.82	0.028
<5 cm	17	5（29.4）	12（70.6）
≥5 cm	23	1（4.3）	22（95.7）
TNM分期				6.33	0.012
Ⅰ+Ⅱ	15	5（33.3）	10（66.7）
Ⅲ+Ⅳ	25	1（4.0）	24（96.0）
淋巴结转移				4.52	0.034
无	12	4（33.3）	8（66.7）
有	28	2（7.1）	26（92.9）

临床病理特征	例数	CCAT2相对表达 [例（%）]		统计值
临床病理特征	例数	低表达（6例）	高表达（34例）	χ²值	P值
性别				0.60	0.440
男	28	5（21.7）	23（78.3）
女	12	1（8.3）	11（91.7）
年龄（岁）				0.26	0.609
≤60	10	1（10.0）	9（90.0）
>60	30	5（16.7）	25（83.3）
肿瘤大小				4.82	0.028
<5 cm	17	5（29.4）	12（70.6）
≥5 cm	23	1（4.3）	22（95.7）
TNM分期				6.33	0.012
Ⅰ+Ⅱ	15	5（33.3）	10（66.7）
Ⅲ+Ⅳ	25	1（4.0）	24（96.0）
淋巴结转移				4.52	0.034
无	12	4（33.3）	8（66.7）
有	28	2（7.1）	26（92.9）

指标	敏感性	特异性	正确度	阳性预测值	阴性预测值
CCAT2	85.0	67.0	76.0	71.0	83.0
CCAT2+CEA	88.0	42.0	64.0	58.0	78.0
CCAT2+CA19-9	95.0	49.0	71.0	63.0	91.0
CCAT2+CEA+CA19-9	98.0	37.0	66.0	59.0	94.0

指标	敏感性	特异性	正确度	阳性预测值	阴性预测值
CCAT2	85.0	67.0	76.0	71.0	83.0
CCAT2+CEA	88.0	42.0	64.0	58.0	78.0
CCAT2+CA19-9	95.0	49.0	71.0	63.0	91.0
CCAT2+CEA+CA19-9	98.0	37.0	66.0	59.0	94.0

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