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BY-NC-ND 3.0 license Open Access Published by De Gruyter Open Access May 7, 2017

Serum CA125, CA199 and CEA combined detection for epithelial ovarian cancer diagnosis: A meta-analysis

  • Junhong Guo , Jiangtao Yu , Xiaojie Song and Haixia Mi EMAIL logo
From the journal Open Medicine

Abstract

Objective

To evaluate the diagnostic value of combination detection of serum cancer antigen 125 (CA125), carbohydrate antigen 19-9 (CA199) and carci noembryonic antigen(CEA) in patients with epithelial ovarian cancer by pooling the open published studies according to meta-analysis method.

Methods

Diagnostic studies related to combination detection of serum CA125, CA199 and CEA in patients with epithelial ovarian cancer were electronic searched in the databases of PubMed, Cochrane, Google scholar, EMBASE, ISI Web of Knowledge and CNKI by two independent reviewers. The combined diagnostic sensitivity, specificity, positive likely hood ratio (+LR), negative likely hood ratio (-LR), diagnostic odds ratio (DOR), and area under the receiver operating characteristic curve (AUC) were pooled by Med DiSc1.4 software.

Results

Twelve prospective diagnostic publications were finally fulfilled the inclusion criteria and were included in this meta-analysis. The pooled diagnostic sensitivity specificity, positive likely hood ratio, negative likely hood ratio, diagnostic odds ratio, and AUC were 0.90 (95%CI: 0.80 to 0.92), 0.83 (95%CI: 0.80 to 0.86), 5.35(95%CI:3.90 to 7.33), 0.13 (95%CI: 0.10 to 0.16), 48.53 (95%CI: 29.91 to 78.72) and 0.92 (95%C: 0.89 to 0.94) respectively by fixed or random effect model. No publication bias was found according to the funnel plot and line regression test (t=-1.34, P=0.21).

Conclusion

Combination detection serum CA125, CA199 and CEA was a promising biomarker forepithelial ovarian cancer diagnosis with relative high sensitivity and specificity.

1 Introduction

In the past two decades, several serum biomarkers for epithelial ovarian cancer diagnosis have been studied, such as Ca125, Ca199, CEA, HE4 and et al [1]. Ca125 is also known as mucin 16 or MUC16, a protein that in humans is encoded by the MUC16 gene. It was found serum Ca125 had been elevated in patients with specific types of cancers, which could be a potential biomarker [2]. Several studies have discussed the serum Ca125 level in ovarian cancer patients and found about 80% of advanced patients had elevated levels of Ca125 in their blood [3,4]. However, studies also found that serum Ca125 can also elevated in individuals without ovarian cancer which made the diagnostic specificity relative low. Previously studies [5,6] indicated Ca199 can be elevated in gastrointestinal cancer, such as colorectal cancer, esophageal cancer and pancreatic cancer. Published study [7] showed elevated Ca199 also can be detected in ovarian cancer patients in their bloods. CEA was one of the most used serum biomarker for solid malignant carcinoma diagnosis such as lung cancer, esophageal cancer colorectal cancer and epithelial ovarian cancer. However, the diagnostic sensitivity or specificity was not high enough of a single serum biomarker of Ca125, Ca199 or CEA for diagnosis of epithelial ovarian cancer. Then, combination detection several serum biomarkers may increase the diagnostic value [8-10]. Several diagnostic studies had discussed the combination detection serum CA125, CA199 and CEA in epithelial ovarian cancer patients with relative high sensitivity and specificity [11-13]. However, because of the small sample size of each individual study, the conclusion was not consistent. In this meta-analysis, we searched the related databases and included open published studies related to combination detection serum CA125, CA199 and CEA in diagnostic epithelial ovarian cancer in order to provide more evidence for its clinical use.

2 Material and methods

2.1 Publication searching

Diagnostic studies related to combination detection serum CA125, CA199 and CEA in patients with epithelial ovarian cancer were electronic searched in the databases of PubMed, Cochrane, Google scholar, EMBASE, ISI Web of Knowledge and CNKI by two independent reviewers (Guo Junhong&Yu Jiangtao). The searching words were “ epithelial ovarian cancer”, “malignant ovary tumor”, “ca 125 antigen”, “ca 125”, “cancer antigen 125”, “CA199”, “carbohydrate antigen 19-9”, “CEA”, “carcino-embryonic antigen”. All potential relevant studies were assessed in detail and additional and all citations of the included articles were further evaluated in order to identify additional suitable studies.

2.2 Data extraction

The data of each included study was extracted by two reviewers Guo JH & Mi HX independently. The general character such as year of publication, first and corresponding author and control type were extracted from each of the included studies. The case number of the true positive (tp), false positive (fp), false negative (fn) and true negative(tn) of the each study were also recorded and cross checked by two reviewers.

2.3 Statistical analysis

Med DiSc1.4 (http://www.biomedsearch.com/nih/Meta-DiSc-software-meta-analysis.) and Stata11.0 (http://www.stata.com; Stata Corporation, College Station, TX) statistical software were used to do all the statistical analysis. Statistical heterogeneity across the included studies was assessed by chi-square/Cochran-Q test and demonstrated by I2 for the effect size of sensitivity, specificity, positive likely hood ratio, negative likely hood ratio and diagnostic odds ratio. Without statistical heterogeneity, the effect size was pooled by fixed effect model, otherwise it was pooled by random effect model. P<0.05 was considered as statistical significant.

3 Results

3.1 Publication searching results

After searching the related databases, 712 papers were initially identified. And 661 articles were excluded after reading the title and abstract. 39 publications were excluded after reading the whole text paper. Finally 12 prospective diagnostic publications were fulfilled the inclusion criteria and were included in this meta-analysis [11-22]. Six studies used benign ovarian tumor as the control group, 3 publications used healthy subjects as the control group and left 3 articles used mixed subjects as the controls. The general characteristics of included 12 papers were demonstrated in Table 1.

Table 1

General characteristics of included studies

First authorYearTPFPFNTNSenSepControl type
Luo XH200626163360.900.69Benign ovarian tumor
Shao JL200736147240.840.63Benign ovarian tumor
Song XL200740102800.950.89Mixed
Pu ZY20105048460.860.92Healthy subjects
Li L20106936470.920.94Healthy subjects
Huang F201037133820.930.86Mixed
Qian M20104246360.880.90Benign ovarian tumor
Liu L20117778540.910.89Benign ovarian tumor
Zhang FL201128212520.930.71Mixed
Yu B20113784330.900.80Healthy subjects
Jiang J201471169640.890.80Benign ovarian tumor
Zhang T2016592451350.920.85Benign ovarian tumor

3.2 Statistical heterogeneity

Statistical heterogeneity across the included studies was assessed by chi-square/Cochran-Q test and demonstrated by I2 for the effect size of sensitivity, specificity, positive likely hood ratio, negative likely hood ratio and diagnostic odds ratio. Significant heterogeneity was found in the effect size of specificity, positive likely hood ratio and diagnostic odds ratio(P 003<0.05). These effect size were pooled by random effect model, Table 2.

Table 2

Statisticalheterogeneityevaluationby chi-square/ Cochran-Q test

Effect sizeChi-square/Cochran-QI2 (%)P
Sensitivity5.930.00.88
Specificity36.9270.20.0001
Positive likely hood ratio43.5274.70.0000
Negative likely hood ratio8.840.00.63
Diagnostic odds ratio20.6246.60.03

3.3 Pooled sensitivity

Without significant statistical heterogeneity, diagnostic sensitivity was pooled by fixed effect model. The pooled diagnostic sensitivity of combination detection serum CA125, CA199 and CEA for epithelial ovarian cancer was 0.90 (95%CI: 0.80 to 0.92), Figure 1.

Figure 1 Forest plot for diagnostic sensitivity of ovarian cancer by combination detection serum CA125 CA199 and CEA.
Figure 1

Forest plot for diagnostic sensitivity of ovarian cancer by combination detection serum CA125 CA199 and CEA.

3.4 Pooled specificity

With significant statistical heterogeneity, diagnostic specificity was pooled by random effect model. The pooled diagnostic specificity of combination detection serum CA125, CA199 and CEA for epithelial ovarian cancer was 0.83 (95%CI: 0.80 to 0.86), Figure 2.

Figure 2 Forest plot for diagnostic specificity of ovarian cancer by combination detection serum CA125 CA199 and CEA.
Figure 2

Forest plot for diagnostic specificity of ovarian cancer by combination detection serum CA125 CA199 and CEA.

3.5 Pooled positive likely hood ratio

Significant heterogeneity was found in the effect size of positive likely hood ratio. The pooled positive likely hood ratio was 5.35(95%CI:3.90 to 7.33) by random effect model, Figure 3.

Figure 3 Forest plot for positive likely hood ratio by combination detection serum CA125 CA199 and CEA.
Figure 3

Forest plot for positive likely hood ratio by combination detection serum CA125 CA199 and CEA.

3.6 Pooled negative likely hood ratio

The negative likely hood ratio was pooled by fixed effect model without statistical heterogeneity. It was 0.13 with its 95%CI of 0.10 to 0.16, Figure 4.

Figure 4 Forest plot for negative likely hood ratio by combination detection serum CA125 CA199 and CEA.
Figure 4

Forest plot for negative likely hood ratio by combination detection serum CA125 CA199 and CEA.

3.7 Pooleddiagnostic odds ratio

The diagnostic odds ratio was pooled by random effect model for significant statistical heterogeneity. The pooled diagnostic odds ratio was 48.53 (95%CI: 29.91 to 78.72), Figure 5.

Figure 5 Forest plot for diagnostic odds ratio by combination detection serum CA125 CA199 and CEA.
Figure 5

Forest plot for diagnostic odds ratio by combination detection serum CA125 CA199 and CEA.

3.8 Pooled SCOR

The pooled area under the receiver operating characteristic curve (ROC) was 0.92 (95%C: 0.89 to 0.94), Figure 6.

Figure 6 The pooled receiver operating characteristic curve of combination detection serum CA125 CA199 and CEA.
Figure 6

The pooled receiver operating characteristic curve of combination detection serum CA125 CA199 and CEA.

3.9 Subgroup analysis

We further performed subgroup analysis for diagnostic sensitivity, specificity, positive likely hood ratio, negative likely hood ratio, diagnostic odds ratio, and AUC according the control type. The subgroup analysis results were showed in Table 3.

Table 3

Subgroup analysis according to control type

Effect sizeBenign ovarian tumorHealthy subjects
Sen0.89 (0.85 to 0.92)0.90 (0.84 to 0.94)
Sep0.81 (0.77 to 0.85)0.89 (0.83 to 0.94)
+LR4.51 (2.94 to 6.90)8.37 (3.73 to 18.77)
-LR0.14 (0.10 to 0.19)0.12 (0.08 to 0.18)
DOR34.37 (17.37 to 67.98)75.45 (32.10 to 177.34)
AUC0.93 (0.89to 0.95)0.91 (0.87 to 0.96)

3.10 Publication bias

No publication bias was found according to the funnel plot (Figure 7) and line regression test (t=-1.34, P=0.21), Figure 7.

Figure 7 Funnel plot for evaluation publication bias.
Figure 7

Funnel plot for evaluation publication bias.

4 Discussion

Epithelial ovarian cancer is one of the most diagnosed malignant carcinoma in females [23]. It has been reported that epithelial ovarian cancer was the 2nd most common malignant gynecological carcinoma with an increasing incidence and prevalence [24,25]. Progress has been made for epithelial ovarian cancer early diagnosis; however, most patients were diagnosed in advanced stage with relative poor prognosis (mean 5-year survival rate of 37.6%) [26,27]. The poor 5-year survival rate for epithelial ovarian cancer patients is the result of aggressive biological behavior and a lack of early detection method. It was reported about 70% of epithelial ovarian cancer patients were diagnosed at advanced stage [25]. So, high sensitivity, specificity and accurate methods are need for detection of epithelial ovarian cancer especially for early stage or high-risk subjects. Serum cancer antigen 125 (CA125) are mostly used tumor serum biomarker for several cancers screening including epithelial ovarian cancer, endometrial cancer, cervical cancer, pancreatic cancer, colon cancer, breast cancer and et al. However, the diagnostic sensitivity were not satisfactory. USPSTF stated that detection serum CA125 had almost no effect on reducing ovarian mortality, while instead increasing the risk of harm including diagnostic procedure and decline in quality of life [26]. CA199 is a glucolipid on the cell membrane and a kind of mucin tumor markers, its molecular weight is more than 1 000 Kd. CA199 was another biomarker used for detection of epithelial ovarian cancer. However, it had limited clinical use for epithelial ovarian cancer screening with not satisfactory diagnostic accuracy. CEA is one of the most used tumor markers in clinical application. It has important diagnostic value for gynecology malignant tumor, breast cancer [28], lung cancer [29] and other digestive system malignant tumors. However, single detection serum CA125, CA199 and CEA had little value for epithelial ovarian cancer detection with low sensitivity or specificity. Several published studies has demonstrated that combination detection serum CA125, CA199 and CEA can provide satisfactory diagnostic value for epithelial ovarian cancer [15,16]. However, because of the small sample size of each individual study, the conclusion was not consistent. So, in our present meta-analysis we included 12 prospective diagnostic trials evaluating the diagnostic value of combination detection CA125, CA199 and CEA for epithelial ovarian cancer diagnosis. The results showed pooled diagnostic sensitivity specificity, positive likely hood ratio, negative likely hood ratio, diagnostic odds ratio, and AUC were 0.90 (95%CI: 0.80 to 0.92), 0.83 (95%CI: 0.80 to 0.86), 5.35(95%CI:3.90 to 7.33), 0.13 (95%CI: 0.10 to 0.16), 48.53 (95%CI: 29.91 to 78.72) and 0.92 (95%C: 0.89 to 0.94) respectively. These results indicated that combination detection serum CA125, CA199 and CEA was promising biomarker for epithelial ovarian cancer with relative high sensitivity and specificity.

However, there were several limitations for this meta-analysis. Firstly, only studies published in Chinese or English were searched in the databases and included in this study. This may result in publication searching bias. Secondly, significant statistical heterogeneity was existed in this meta-analysis, which may decrease the statistical power and weaken the conclusion. Thirdly, the original studies included in this manuscript did not use the same cut-off value to determine the serum protein of CA125,CA199 and CEA negative or positive. This is an important clinical heterogeneity across the original studies. Fourthly, for the included12 references, the patients were of the same source population, which may limited, its clinical use.

  1. Conflict of interest: No authors report any conflict of interest.

References

[1] Komai K, Nishida T. Tumor marker in ovarian cancer. Gan To Kagaku Ryoho 2002;29:481-486Search in Google Scholar

[2] Bast RC, Xu FJ, Yu YH, Barnhill S, Zhang Z, Mills GB. CA 125: the past and the uture. Int J Biol Markers 1998; 13(4): 179-18710.1177/172460089801300402Search in Google Scholar

[3] Bocheva Y, Bochev P, Ivanov S. Ca-125 in diagnosis and monitoring of patients with ovarian cancer. Akush Ginekol (Sofiia) 2015; 54(1): 11-17Search in Google Scholar

[4] Alexandre J, Brown C, Coeffic D. CA-125 can be part of the tumour evaluation criteria in ovarian cancer trials: experience of the GCIG CALYPSO trial. Br J Cancer 2012; 106(4): 633-637 10.1038/bjc.2011.593Search in Google Scholar PubMed PubMed Central

[5] Shiozawa S, Tsuchiya A, Kim DH, Ogawa K. Prognostic significance of CA19-9 levels in patients with pancreatic cancer.Nihon Rinsho 2006; 64 Suppl 1: 297-300Search in Google Scholar

[6] Liang Y, Wang W, Fang C. Clinical significance and diagnostic value of serum CEA, CA19-9 and CA72-4 in patients with gastric cancer. Oncotarget 2016; 7(31): 49565-4957310.18632/oncotarget.10391Search in Google Scholar PubMed PubMed Central

[7] Canney PA, Wilkinson PM, James RD, Moore M. CA19-9 as a marker for ovarian cancer: alone and in comparison with CA125. Br J Cancer 1985; 52(1): 131-13310.1038/bjc.1985.161Search in Google Scholar PubMed PubMed Central

[8] Wang J, Gao J, Yao H, Wu Z, Wang M, Qi J. Diagnostic accuracy of serum HE4, CA125 and ROMA in patients with ovarian cancer: a meta-analysis. Tumour Biol 2014;35:6127-613810.1007/s13277-014-1811-6Search in Google Scholar PubMed

[9] Dayyani F, Uhlig S, Colson B, Simon K, Rolny V, Morgenstern D, Schlumbrecht M. Diagnostic Performance of Risk of Ovarian Malignancy Algorithm Against CA125 and HE4 in Connection With Ovarian Cancer: A Meta-analysis. Int J Gynecol Cancer 2016;26:1586-159310.1097/IGC.0000000000000804Search in Google Scholar PubMed

[10] Lan Z, Fu D, Yu X, Xi M. Diagnostic values of osteopontin combined with CA125 for ovarian cancer: a meta-analysis. Fam Cancer 2016;15:221-23010.1007/s10689-015-9847-3Search in Google Scholar PubMed

[11] Yu B. The dinieal value of the combined detection of CEA, CAl25 and CAl9-9 in ovarian atlrdliOm diagnasis. Jurnal of Binzhou Medical University 2011;34:294-295Search in Google Scholar

[12] Jiang J, Deng XY, Hu XH. Clinical significance of the combined detection of CA125, CA199 and CE in diagnosis of ovarian cancer. Chinese Journal of Laboratory Diagnosis 2014;18:1145-1148Search in Google Scholar

[13] Zhang T, Cheng XJ, Zhang B. CA199, Clinical value of combined detection serum CA125 and CEA for ovarian cancer diagnosis. Guizhou Medical Journal 2016;40:973-975Search in Google Scholar

[14] Luo XH, Ch D, Pan KY, Wang Y, Zeng HY. The value of combined serum CA125, CA199 and CEA test for ovarian cancer diagnosis. Journal of Clinical and Experimental Medicine 2006;5:878-879Search in Google Scholar

[15] Shao LJ, Xu RL, Hu T. Combination detection serum CA125,CA199 and CEA for ovarian cancer diagnosis. Journal of Radioimmunology 2007;20:92-93Search in Google Scholar

[16] Song XL, Wang GS, Luo JM, Zhao ZL. Diagnostic value for combined detection serum CA125, CA199 and CEA in patients with ovarian cancer. Journal of Henan University(Medical Science) 2007;26:70-71Search in Google Scholar

[17] Huang F. Serum CA125,CA199 and CEA combined detection for ovarian cancer diagnosis. Guangxi Medical Journal 2010;32:424-425Search in Google Scholar

[18] Li L, Liao JX. The Clinical Diagnostic Value of joint inspection of Serum CEA、CA19-9、CA125 in the Patients with Ovarian Cancer. Journal of Modern Clinical Medicine 2010;36:122-124Search in Google Scholar

[19] Pu ZY, Liu FJ, Liu YY. Clinical evaluation serum CA125, CEA and CA19-9 combined detection for ovarian cancer diagnosis. West China Medical Journal 2010:1879-1880Search in Google Scholar

[20] Qian M, Yuan JJ, Wang XH, Shu XC.Diagnosis and Prognosis Value of the Serum CA125、CA199、CEA Detection in Patients with Epithelinl Ovarian Cancer. China Practical Medical 2010;05:53-54Search in Google Scholar

[21] Liu L, Zhang MK, Chen JL, Huang RQ.The significance of serum CA125,199 and CEA test in the diagnosis of ovarian cancer. Chongqing Medicine 2011;40:2423-2424,2426Search in Google Scholar

[22] Zhang FL. Ovarian cancer diagnosis by combination detection serum CEA, CA125and CA199. Chinese Journal of Misdiagnostics 2011;11:4646-4647Search in Google Scholar

[23] Siegel RL, Miller KD, Jemal A. Cancer statistics, 2016. CA Cancer J Clin 2016;66:7-3010.3322/caac.21332Search in Google Scholar PubMed

[24] Hunn J, Rodriguez GC. Ovarian cancer: etiology, risk factors, and epidemiology. Clin Obstet Gynecol 2012;55:3-2310.1097/GRF.0b013e31824b4611Search in Google Scholar PubMed

[25] Webb PM, Jordan SJ. Epidemiology of epithelial ovarian cancer. Best Pract Res Clin Obstet Gynaecol 201610.1016/j.bpobgyn.2016.08.006Search in Google Scholar PubMed

[26] Pavlik EJ. Ovarian cancer screening effectiveness: A realization from the UK Collaborative Trial of Ovarian Cancer Screening. Womens Health (Lond) 2016;12:475-47910.1177/1745505716666096Search in Google Scholar PubMed PubMed Central

[27] Voelker R. Ovarian Cancer Screening Tests Don’t Pass Muster. JAMA 2016;316:153810.1001/jama.2016.14614Search in Google Scholar PubMed

[28] Tang S, Zhou F, Sun Y, Wei L, Zhu S, Yang R, Huang Y, Yang J. CEA in breast ductal secretions as a promising biomarker for the diagnosis of breast cancer: a systematic review and meta-analysis. Breast Cancer 2016;23:813-81910.1007/s12282-016-0680-9Search in Google Scholar PubMed

[29] Okamura K, Takayama K, Izumi M, Harada T, Furuyama K, Nakanishi Y. Diagnostic value of CEA and CYFRA 21-1 tumor markers in primary lung cancer. Lung Cancer 2013;80:45-4910.1016/j.lungcan.2013.01.002Search in Google Scholar PubMed

Received: 2017-1-26
Accepted: 2017-2-2
Published Online: 2017-5-7

© 2017 Junhong Guo et al.

This work is licensed under the Creative Commons Attribution-NonCommercial-NoDerivatives 3.0 License.

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