Prospective study of serum CA-125 levels as markers of ovarian cancer
- PMID: 8433467
Prospective study of serum CA-125 levels as markers of ovarian cancer
Abstract
Objective: To evaluate prospectively the sensitivity and specificity of serum CA-125 levels for the detection of ovarian cancer.
Design: Case-control study nested within a cohort of women who donated blood to a community-based serum bank established in 1974.
Setting: Washington County, Maryland.
Population: Cases consisted of 37 women who developed ovarian cancer from 1975 through 1989. Controls consisted of 73 women, matched on age and time since last menstrual period, and free of cancer until the cases' diagnoses. STUDY VARIABLE: Serum CA-125 levels.
Outcome measure: Histologically confirmed ovarian cancer.
Results: Levels of serum CA-125 among cases were higher than among controls for each 3-year interval up to 12 years prior to the time of the cases' diagnoses. The median level for cases diagnosed within the first 3 years of follow-up was 35.4 U/mL compared with 9.0 U/mL for controls (P = .002). The sensitivity of a serum CA-125 level greater than 35 U/mL within the first 3 years was 57% (95% confidence interval, 20% to 88%) and the specificity was 100% (95% confidence interval lower limit, 73%). Sensitivity and specificity decreased with increasing time to diagnosis.
Conclusions: Measurement of serum CA-125 levels, particularly at a reference value of 35 U/mL, is not sufficiently sensitive to be used alone as a screening test for the detection of ovarian cancer. Lower CA-125 reference values could identify women at higher risk of developing ovarian cancer, but CA-125 measurement cannot be recommended for this purpose because of the high proportion of women who would be falsely classified as being at high risk for developing ovarian cancer.
Comment in
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Ovarian cancer.JAMA. 1993 Mar 3;269(9):1163. JAMA. 1993. PMID: 8433473 No abstract available.
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CA-125 as a screening test for ovarian cancer.JAMA. 1993 Jun 23-30;269(24):3106-7. JAMA. 1993. PMID: 8505808 No abstract available.
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