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Carcinoembryonic Antigen (CEA)
Post your experienceCarcinoembryonic Antigen (CEA) is a glycoprotein which is produced in significant amounts by the large intestine during fetal development. It was first identified by Freedman and Gold in 1965 and acquired its name because it was found in the fetal colon and in colon adenocarcinoma, but not in healthy bowel. It has since been discovered that small amounts are present in the healthy colon intestine and in the blood. It may also be produced in significant amounts by other types of tumours (see below). Because raised levels may signify the presence of a tumour, it is known as a cancer marker.1
- Colorectal cancer
- Colorectal liver metastases
- Breast cancer2
- Lung cancer3
- Skeletal metastases
- Nonmalignant liver disease4
- Pancreatic disease5
- Smoking
- Ageing6
- Atherosclerosis6
Studies of patients with colorectal tumours suggest that the CEA level deemed to be normal is 2.5 mcg/L or less.1 This level can double in smokers.
Colorectal cancer
Diagnosis - The CEA test has a specificity of between 30-80%7 and it is not recommended by NICE for the diagnosis of early colorectal cancer. NICE guidance advises that such a diagnosis should be based on a history of red flag symptoms and the finding of an abdominal or rectal mass. The only laboratory result of note is a finding of iron deficiency anaemia. In fact, NICE do not recommend delaying referral for the results of any tests, if there is sufficient clinical concern about the diagnosis.8
Staging - CEA in combination with other tumour markers (e.g. mucin tumour markers CA19-9, CA242) it can be used in pre-operative staging and thereby assist in the planning of the type of surgery required and future management options.9
Prognosis - The CEA test is of much more useful in determining prognosis than it is as an early diagnostic test for colon cancer. CEA levels tend to be higher in advanced disease. One study found that using a cut off point of 5 μg/L the proportions of patients with increased values were 3%, 25%, 45%, and 65% for patients with Dukes' A, B, C, and D disease respectively.1 Well-differentiated carcinomas tend to produce more CEA than poorly-differentiated ones. Tumours on the right side of the colon tend to produce more CEA than tumours on the left side.
By comparing the levels before and after surgery, the test can be used to detect recurrence of tumour and monitor for the development of liver metastases. The CEA level can also be used to assess the response to chemotherapy. There is little evidence that monitoring CEA levels in all patients with colorectal cancer contributes to improved survival or enhanced quality of life and further work needs to be done on the quantitative significance of abnormal tests in specific clinical situations. However, it is likely that post-treatment CEA levels will eventually become a useful prognostic tool in selected cases in secondary care.5 One study suggests that post-treatment levels are helpful in identifying recurrence, but normal levels do not necessarily indicate that recurrence has not occurred.10
Breast cancer
Similar considerations apply to the diagnosis of breast cancer. The sensitivity of CEA is too low for it to be used as a primary diagnostic test.11 In conjunction with other tumour markers (CA27.29, tissue polypeptide antigen and especially CA 15-3), it may however be helpful in disease surveillance,12 in identifying patients with skeletal metastases2 and in response to chemotherapy.13 One study suggested that it may be helpful in determining prognosis.14
Document references
- Duffy MJ; Carcinoembryonic antigen as a marker for colorectal cancer: is it clinically useful? Clin Chem. 2001 Apr;47(4):624-30. [abstract]
- Duffy MJ; Serum tumor markers in breast cancer: are they of clinical value? Clin Chem. 2006 Mar;52(3):345-51. Epub 2006 Jan 12. [abstract]
- Molina R, Auge JM, Escudero JM, et al; Mucins CA 125, CA 19.9, CA 15.3 and TAG-72.3 as Tumor Markers in Patients with Lung Cancer: Comparison with CYFRA 21-1, CEA, SCC and NSE. Tumour Biol. 2008 Dec 8;29(6):371-380. [abstract]
- Tsukushi S, Katagiri H, Kataoka T, et al; Serum tumor markers in skeletal metastasis. Jpn J Clin Oncol. 2006 Jul;36(7):439-44. Epub 2006 Jun 30. [abstract]
- El-Deiry W; Colon Cancer, Adenocarcinoma eMedicine, 2006.
- Ishizaka N, Ishizaka Y, Toda E, et al; Are serum carcinoembryonic antigen levels associated with carotid atherosclerosis in Japanese men? Arterioscler Thromb Vasc Biol. 2008 Jan;28(1):160-5. Epub 2007 Oct 19. [abstract]
- Fletcher RH; Carcinoembryonic antigen. Ann Intern Med. 1986 Jan;104(1):66-73. [abstract]
- Service guidance for the NHS in England and Wales Improving Outcomes for Colorectal Cancer (update), NICE (2004)
- Levy M, Visokai V, Lipska L, et al; Tumor markers in staging and prognosis of colorectal carcinoma. Neoplasma. 2008;55(2):138-42. [abstract]
- Hara M, Kanemitsu Y, Hirai T, et al; Negative serum carcinoembryonic antigen has insufficient accuracy for excluding recurrence from patients with Dukes C colorectal cancer: analysis with likelihood ratio and posttest probability in a follow-up study. Dis Colon Rectum. 2008 Nov;51(11):1675-80. [abstract]
- Arslan N, Serdar M, Deveci S, et al; Use of CA15-3, CEA and prolactin for the primary diagnosis of breast cancer and correlation with the prognostic factors at the time of initial diagnosis. Ann Nucl Med. 2000 Oct;14(5):395-9. [abstract]
- Brooks M; Breast cancer screening and biomarkers. Methods Mol Biol. 2009;472:307-21. [abstract]
- Yonemori K, Katsumata N, Noda A, et al; Development and verification of a prediction model using serum tumor markers to predict the response to chemotherapy of patients with metastatic or recurrent breast cancer. J Cancer Res Clin Oncol. 2008 Nov;134(11):1199-206. Epub 2008 Jun 5. [abstract]
- Uehara M, Kinoshita T, Hojo T, et al; Long-term prognostic study of carcinoembryonic antigen (CEA) and carbohydrate antigen 15-3 (CA 15-3) in breast cancer. Int J Clin Oncol. 2008 Oct;13(5):447-51. Epub 2008 Oct 23. [abstract]
DocID: 3181
Document Version: 21
DocRef: bgp25955
Last Updated: 14 Jan 2009
Review Date: 14 Jan 2011
The authors and editors of this article are employed to create accurate and up to date content reflecting reliable research evidence, guidance and best clinical practice. They are free from any commercial conflicts of interest. Find out more about updating.
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