CA125 Test Research Articles

Risk of Malignancy Index is not accurate as a Triage Tool for Ovarian Cancer

Objective: To evaluate Risk of Malignancy Index (RMI) as a triage tool for ovarian cancer in Dr. Cipto Mangunkusumo Hospital.
 Method: This is a retrospective study conducted from January 2008-December 2012 in patients diagnosed with ovarian mass. Patients admitted for surgery due to ovarian masses were included to this study. RMI 3 score was calculated based on ultrasonography examination in Dr. Cipto Mangunkusumo Hospital, CA-125 test and menopausal status. Patients without final pathological report and incomplete data were excluded from study. Data were analysed using SPSS 20 to evaluate RMI result and final pathlogical report in benign and malignant case.
 Result: From 882 patients identified with ovarian masses from cancer registry, only 99 patients aged 17-70 y.o were included in this study. Most of the patients were nully-parity (28.3%), non-menopausal women (60.6%), normal body mass index (40.4%), and with stage IIIC ovarian cancer (33.3%). Ultrasonography examination showed that most of patients had solid mass and ascites (19.2%). Meanwhile, CA-125 showed that patients with <35 U/ml were 10.1% and ≥ 35 U/ml were 89.9%. Patients with RMI scores <200 (benign cases) were 19 cases (19.2%) and ≥ 200 (malignant cases) were 80 cases (80.8%). Meanwhile, patients with benign final pathological report were 23 cases (23.2%) and malignant cases were 76 cases (76.8%). There was no statistical difference in RMI between benign and malignant cases based on final pathological report.
 Conclusion: Our study showed that RMI was not accurate as triage tool for ovarian cancer in our hospital. Further investigation and more patients are needed to confirm this study.
 Keywords: CA-125, menopausal status, ovarian cancer, risk of malignancy index (RMI), ultrasonography.

Abstract C29: Combination of SP17 with CA125 serologic measurement for detection of ovarian cancer

Abstract Ovarian cancer (OC) is a serious healthy issue for women worldwide, ranking second for mortality rates among gynecological malignancies. CA125 (MUC16) is the only available biomarker to monitor disease and treatment response in OC but it suffers from poor performance for diagnostic purposes. As a consequence, increasing efforts are being made for the identification of novel tumor biomarkers to improve CA125 test specificity and sensitivity. More than 30 serum biomarkers have been studied alone or in combination with CA125. We have previously shown that SP17, a member of the cancer/testis antigen (CTA) family, is a potential biomarker that allows for the discrimination of the normal ovary from OC cells and for the tracking of OC disease in a xenograft mouse model. Here we hypothesized that SP17 serum levels could be exploited as a diagnostic test to detect early lesions of OC and to discriminate between malignant and benign lesions. We analyzed SP17 expression in primary ovarian tissues from ovarian cancer patients, benign ovarian lesions and healthy subjects through RT-PCR and immunohistochemistry. SP17 and CA125 levels were measured in the sera of the same subjects by ELISA. We found that SP17 expression was restricted to OC cells at the transcriptional and translational levels, and that the measurement of SP17 concentration in the serum afforded accurate discrimination between subjects with different prognoses allowing for predicting overall survival time. SP17 assay alone was superior to CA125 in discriminating between ovarian cancer and benign ovarian tumors: combining SP17 and CA125 assays, we obtained 96% sensitivity, 89% specificity and 97% PPV. SP17 is a novel serum biomarker for ovarian cancer. SP17 serum measurement in combination with CA125 affords improved positive predictive value for diagnostic purposes. Citation Format: Maurizio Chiriva-Internati, Leonardo Mirandola, Yuefei Yu, Marjorie R. Jenkins, Everardo Cobos, Jose A. Figueroa, Hans W. Nijman, W. Martin Kast. Combination of SP17 with CA125 serologic measurement for detection of ovarian cancer. [abstract]. In: Proceedings of the Twelfth Annual AACR International Conference on Frontiers in Cancer Prevention Research; 2013 Oct 27-30; National Harbor, MD. Philadelphia (PA): AACR; Can Prev Res 2013;6(11 Suppl): Abstract nr C29.

Computed tomography adnexal mass score to estimate risk for ovarian cancer

We wish to develop a CT scan-based scoring system which estimates the probability of adnexal mass malignancy. Patients (324) undergoing adnexal mass surgery were recruited into the study from June 1, 2002, to January 1, 2009. All study patients had a preoperative CT scan and serum CA-125 test. CT scan abnormalities included any solid tumor components, ascites, and pelvic or abdominal lymphadenopathy and omental caking. There were 225 (70%) benign and 99 (30%) malignant ovarian masses. Using logistic regression with the area under the curve of the receiver operating curve of 82%, the cancer probability was determined by the equation. e(-3.6372+0.0306*(A)+0.001*(C)+1.551*(D)+1.7377*(E)+2.76*(F)) / 1+e(-3.6372+0.0306*(A)+0.001*(B)+0.876*(C)+1.551*(D)+1.7377*(E)+2.76*(F)) where A = age, B = CA-125, C = solid adnexal mass is 1 and cystic is 0, D = ascites is 1, E = omental caking is 1 and absence is 0, F = node size ≥1 cm is 1 and <1 cm is 0 value. The natural logarithm e is a constant [2.718281828]. For example, for a woman of age 60, CA-125 = 50 U/mL, with solid adnexal mass, ascites, omental caking, and lymphadenopathy, the probability is 0.994. Hence, this woman has a 99.4% probability of having cancer. The computed tomography adnexal mass score combines CT scan findings, CA-125, and patient age into an equation to predict the malignant probability of an adnexal mass.

Quantitative Analysis of Serum IgG Galactosylation Assists Differential Diagnosis of Ovarian Cancer

CA-125, the most frequently used biomarker for ovarian cancer detection, cannot provide accurate diagnosis due to its poor specificity as it may also increase in many benign gynecological conditions. Thus, reducing the false-positive outcomes is urgently needed. Decrease in terminal galactosylated N-glycans of serum IgG has been found in various malignancies compared to healthy controls. Here, this alteration of IgG galactosylation was extended to be investigated between ovarian cancer and benign conditions with similar elevated CA-125 levels, in an attempt to effectively distinguish between false-positive subjects and ovarian cancer patients. In the study of 58 patients with elevated CA-125 levels (>35 U/mL), the degree of IgG galactosylation was measured from the relative intensities of IgG digalactosyl (G2), monogalactosyl (G1), and agalactosylated (G0) N-glycans according to the formula G0/(G1+G2·2). This ratio was found significantly higher in the malignant group than in the benign group (0.74 vs 0.34; p<0.0001). ROC analysis demonstrated an improved specificity from 65.2% (by CA-125 test alone) to 84.6%, while maintaining sensitivity at 90% by incorporating quantitative analysis of IgG galactosylation in the current assay. The results suggest that combining quantitative alteration of IgG galactosylation with CA-125 may generate an overall more robust approach for differential diagnosis of ovarian cancer.

CA-125 and risk of malignancy index for screening for malignancy in fertile aged females with ovarian cyst, which is more cost effectiveness?

Background:Ovarian tumor is a cause of infertility in the fertile-aged women. Also, it can also turns into malignancy and causes deadly outcome. Screening for malignancy is an important management.Aims:The available screening methods that are widely used at present include CA-125 determination and the risk of malignancy index (RMX), which is a combined CA-125 with ultrasonography, determination.Materials and Methods:Here, the author tries to assess cost-effectiveness of both alternative in screening by basic medical economics technique.Statistics:Classical descriptive analysis was used for cost effectiveness calculation.Results:In this work, from the cost-effectiveness analysis, the CA-125 test is more cost-effectiveness than RMX.Conclusion:This reflects that the usage of additional ultrasonography test for increasing the diagnostic activity in screening for ovarian cyst in the fertile aged females in Thailand is still not appropriate.

Psychological outcomes of familial ovarian cancer screening: No evidence of long-term harm

ObjectivesOvarian cancer screening for women at increased genetic risk in the UK involves 4-monthly CA125 tests and annual ultrasound, with further tests prompted by an abnormal result. The study evaluated the longer-term psychological and behavioural effects of frequent ovarian screening. MethodsWomen completed T1 questionnaires before their first routine 4-monthly CA125 test, and T2 follow-up questionnaires one week after their result. Women with abnormal results completed a further questionnaire one week after return to routine screening (T3 primary end-point). T4 questionnaires were sent at nine months. Measures included cancer distress, general anxiety/depression, reassurance, and withdrawal from screening. ResultsA total 1999 (62%) of 3224 women completed T1 questionnaires. T2 questionnaires were completed by 1384/1609 participants (86%): 1217 (89%) with normal results and 167/242 (69%) with abnormal results. T3 questionnaires were completed by 141/163 (87%) women, with 912/1173 (78%) completing T4 questionnaires. Analysis of covariance indicated that, compared to women with normal results, women with abnormal results reported moderate cancer distress (F=27.47, p≤.001, η2=0.02) one week after their abnormal result and were significantly more likely to withdraw from screening (OR=4.38, p≤.001). These effects were not apparent at T3 or T4. The effect of screening result on general anxiety/depression or overall reassurance was not significant. ConclusionsWomen participating in frequent ovarian screening who are recalled for an abnormal result may experience transient cancer-specific distress, which may prompt reconsideration of risk management options. Health professionals and policy makers may be reassured that frequent familial ovarian screening does not cause sustained psychological harm.

Physician Knowledge and Awareness of CA-125 as a Screen for Ovarian Cancer in the Asymptomatic, Average-Risk Population

Effective early detection strategies for ovarian cancer do not exist. Current screening guidelines recommend against routine screening using CA-125 alone or in combination with transvaginal ultrasonography (TVS). In this study, the authors used the 2008 DocStyles survey to measure clinician beliefs about the effectiveness of CA-125 and TVS in the asymptomatic, average-risk population in the United States. To assess the need for provider education, the authors used the 2008 HealthStyles survey to examine public awareness of CA-125. Of 1,250 physician respondents, 40.4% said both CA-125 and TVS were effective screens, and 28.3% said neither was an effective ovarian cancer screen in the asymptomatic, average-risk population. Obstetrician/gynecologists [OB/GYNs] more often had responses consistent with current guidelines: 56.5% of OB/GYNs, compared with 34.4% and 29.8% of family/general practitioners and internists, respectively, said neither CA-125 nor TVS was an effective screen. Almost one third of women surveyed reported having heard of CA-125, and about one tenth said they had the CA-125 test. These findings support the need for additional provider education. Educational efforts should include lack of evidence for, as well as the potential harms of, screening for ovarian cancer with CA-125.

A New Approach for Identifying Patients With Ovarian Epithelial Neoplasms Based on High-Resolution Mass Spectrometry

We investigated the serum profiles of patients with ovarian neoplasm using high-performance liquid chromatography (HPLC) and high-resolution mass spectrometry (HRMS) to obtain serum "fingerprints" for use in identifying patients with these neoplasms. We used HPLC-HRMS to analyze serum samples from patients with ovarian neoplasms and control subjects. Serum samples from 145 patients were analyzed, including 85 with ovarian epithelial neoplasms. We also compared the results of this serum-fingerprinting approach with the results of the CA-125 test and imaging. Fingerprinting successfully permitted the separation of control patients and patients with ovarian neoplasms. The sensitivity and specificity of the test were between 96% and 100%. When the results of this test were concordant with the results of the CA-125 test, 99% of serum samples were correctly classified as being from a patient with an ovarian neoplasm or with no ovarian neoplasm. We found that a metabolite of molecular weight 472 is the main metabolite in the separation of patients with ovarian neoplasms from control subjects. HPLC-HRMS serum profiling could become a screening test for ovarian neoplasms.

CA 125 serum values in surgically treated endometriosis patients and its relationships with anatomic sites of endometriosis and pregnancy rate

Endometriosis is a benign gynecologic disease defined as the presence of functional endometrial glands and stroma outside the uterine cavity, causing dysmenorrhea, dyspareunia, menstrual irregularities, and infertility. Serum CA-125 measurement is now a consolidated method for diagnosing this condition, and its interpretation has posed a number of problems, particularly regarding utility in diagnosing minimal-mild endometriosis, whereas its value as a diagnostic aid in moderate-severe stages is well recognized. In our cohort, serum CA-125 values were significantly elevated in patients with ovarian and mixed endometriosis lesions (median levels 48 U/mL), compared with those who had exclusively extraovarian foci (median levels 27 U/mL), and so the correlation between this marker and the surgical and pathologic finding of ovarian and deep endometriosis was found to be statistically significant; however, the location did not affect the fertility rate.

Preoperative prediction model of lymph node metastasis in endometrial cancer.

We aimed to develop a preoperative prediction model identifying the low-risk group for lymph node metastasis in endometrial cancer. In 110 patients who underwent preoperative magnetic resonance imaging and serum CA-125 test, logistic analysis was performed to identify predictors. The coefficients obtained from logistic regression were used to construct a scoring system, and a receiver operator characteristic curve was created. Lymph node metastases were found in 14 (12.7%) of 110 patients. After multivariate logistic regression analysis, histologic grade, preoperative CA-125 levels, disease extent, and myometrial invasion assessed by magnetic resonance imaging were selected as viable predictors. The scoring system was internally validated using bootstrapping (P < 0.001), and receiver operator characteristic curve yielded the area under the curve of 0.902. The patients with the score of 0 or 1 (57.3%) were identified as a low-risk group, and no nodal metastasis was observed among them (negative predictive value, 100%: 95% confidence interval, 94.3%-100%). The current study suggests that preoperative prediction system to identify the risk of lymph node metastasis is feasible. This model may be useful in preoperative counseling about cost and benefit of systemic lymph node dissection.

Cancergazing? CA125 and post-treatment surveillance in advanced ovarian cancer

Post-treatment surveillance of advanced ovarian cancer involves regular testing of asymptomatic patients using the CA125 test. This practice is based on a rationale that is not supported by evidence from clinical trials. This paper aims to stimulate critical reflection concerning the effect of investigative tests on clinical decisions and interactions, and the experience of illness, particularly in the context of advanced malignant disease. Drawing on the idea of the "medical gaze", and building on previous health communication research, we present an analysis of in-depth interviews and psychometric tests collected in a prospective study of 20 Australian women with advanced ovarian cancer conducted between 2006 and 2009. We describe the demands placed on patients by the use of the CA125 test, some hazards it creates for decision-making, and some of the test's subjective benefits. It is widely believed that the CA125 test generates anxiety among patients, and the proposed solution is to educate women more about the test. We found no evidence that anxiety was a problem requiring a response over and above existing services. We conclude that the current debate is simplistic and limited. Focussing on patient anxiety does not account for other important effects of post-treatment surveillance, and educating patients about the test is unlikely to mitigate anxiety because testing is part of a wider process by which patients become aware of a disease that--once it has relapsed--will certainly kill them in the near future.

Abstract A25: Public and provider awareness and use of a CA-125 test for ovarian cancer

Abstract Introduction: CA-125 is a serum marker approved for detecting recurrent ovarian cancer in women with a personal history of ovarian cancer. Several large trials have investigated the use of CA-125 (alone or in combination with transvaginal ultrasound [TVU]) as a screening test for ovarian cancer. However, this test has generally been associated with a low positive predictive value and trials have concluded that screening asymptomatic women in the average risk population with CA-125 is not beneficial. Still, there remains widespread discussion and marketing of ovarian cancer screening tests that include CA-125. Since little is known about public and provider awareness of CA-125, the objective of this study was to measure women's familiarity with the CA-125 test, and clinician beliefs about the effectiveness of screening for ovarian cancer with CA-125 in the United States. Methods: In 2008, CDC funded the collection of data as part of its national awareness campaign, Inside Knowledge: Get the Facts About Gynecologic Cancer. Several questions related to CA-125 were included as part of a standardized, survey administered annually in the contiguous United States by Porter Novelli. The HealthStyles survey included 2,991 female respondents age ≥ 18 years, and the DocStyles survey included 1,250 physician respondents of family/general practitioners (n=510), internists (n=490), and obstetrician/gynecologists (n=250). Participant responses to CA-125-related questions for the HealthStyles survey were weighted to match the demographic distribution of the general population. Chi-square tests were used to assess differences with the p-value set to 0.05. Results: Overall, most women (56%) had not heard of the CA-125 test, 29% had heard of it, and 15% were unsure. Demographic characteristics generally were similar for women who had not heard of the CA-125 test, except that women who had heard of the test more often were over age 45 (58% vs 37%) (p&amp;lt;0.0001) and were peri- or post-menopausal (54% vs 35%) (p&amp;lt;0.0001), compared to women who had not heard of CA-125. Few women (12%) had ever had a CA-125 test. About 15% of women who reported being “very concerned” about getting ovarian cancer also reported having had a CA-125 test. In the DocStyles results, the majority (53%) of physicians said that both CA-125 and TVU are effective screening tests for ovarian cancer. A greater proportion of OB/GYNs (57%) reported neither CA125 nor TVU were effective as screening tests for asymptomatic women in the average risk population than family/general practitioners (34%) or internists (30%) (p&amp;lt;0.0001). Conclusions: The large percentage of physicians who believe CA-125 is an effective screen for ovarian cancer signals the need for improved education. Educational efforts geared toward the public and providers that include both lack of evidence for screening with CA-125, as well as the potential harms of false-positive CA-125 tests should be a priority for public health programs and awareness campaigns. Citation Information: Cancer Prev Res 2010;3(1 Suppl):A25.

Use of a Symptom Index, CA125, and HE4 to predict ovarian cancer

Background. Prior studies suggest that combining the Symptom Index (SI) with a serum HE4 test or a CA125 test may improve prediction of ovarian cancer. However, these three tests have not been evaluated in combination. Methods. A prospective case–control study design including 74 women with ovarian cancer and 137 healthy women was used with logistic regression analysis to evaluate the independent contributions of HE4 and CA125, and the SI to predict ovarian cancer status in a multivariate model. The diagnostic performance of various decision rules for combinations of these tests was assessed to evaluate potential use in predicting ovarian cancer. Results. The SI, HE4, and CA125 all made significant independent contributions to ovarian cancer prediction. A decision rule based on any one of the three tests being positive had a sensitivity of 95% with specificity of 80%. A rule based on any two of the three tests being positive had a sensitivity of 84% with a specificity of 98.5%. The SI alone had sensitivity of 64% with specificity of 88%. If the SI index is used to select women for CA125 and HE4 testing, specificity is 98.5% and sensitivity is 58% using the 2-of-3-positive decision rule. Conclusions. A 2-of-3-positive decision rule yields acceptable specificity, and higher sensitivity when all 3 tests are performed than when the SI is used to select women for screening by CA125 and HE4. If positive predictive value is a high priority, testing by CA125 and HE4 prior to imaging may be warranted for women with ovarian cancer symptoms.

Clinical Significance of the detection of CA153,CA125,CEA and SF Serum Test in Breast Cancer

Objective To study the clinical significance of sernm CA153,CA125 and CEA test in breast cancer.Methods The levels of CA153,CA125,carcinoembryonic antigen(CEA)and ferritin were measured in 60 patients with breast cancer(breast cancer group),36 patients with benign breast diseases(benign breast diseases group)and 40 healthy people(control group)by chemiluminometry.The four indices were compared and analyzed for their complementary diagnostic value to breast cancer.Results The levels of CA153,CA125,CEA,SF[(52.8±21.3)u/ml,(44.2±20.1)ng/ml,(8.9±5.2)ng/ml,(350.5±113.8)ng/ml]in breast cancer group were significantly higher than that of benign breast disease group[(17.3±8.8)u/ml,(15.6±8.5)u/ml,(2.0±0.8)u/ml,(1220.7±46.91)ng/ml](t=2.671,t=2.684,t=2.898,t=2.844,P＜0.01);The levels of CA153,CA125,CEA and SF pretreatment in breast cancer group were significantly higher than that after treatment[(25.5±3.7)u/ml,(15.0±8.4)u/ml,(4.6±3.3)ng/ml,(98.5±58.6)ng/ml](t=2.210,t=2.165,t=2.224,t=2.234,P＜0.05);The positive rate of 53.3%in breast cancer group for CA153+CA125+CEA+SF were lower than that CA153(56.7%),CA125(58.3%),CEA(63.3%),SF(68.3%)(χ~2=2.52,χ~2=2.652,P＞0.05;χ~2=3.85,χ~2=3.90,χ~2=3.98,P＜0.05);joint determination of CA153+CEA+SF experimental efficient 89.0%higher than the other four groups of the joint determination,but had no signiflcanle(χ~2=2.78,χ~2=3.10,χ~2=2.99,χ~2=3.01,P＞0.05).Conclusion The positive rate may be increased by combining test of serum CA153,CA125,CEA and ferritin in breast cancer.Thus the combined test might be of high value for the early diagnosis,improving the therapeutic effect and prognosis of breast cancer. Key words: Tumor markers; Breast Neoplasms; Diagnosis

A Gynecologic Oncology Group Study of serum CA-125 levels in patients with stage III optimally debulked ovarian cancer treated with intraperitoneal compared to intravenous chemotherapy: An analysis of patients enrolled in GOG 172

ObjectiveSerum CA-125 values have been advocated in the monitoring of ovarian cancer patients receiving intravenous (IV) chemotherapy. This evaluation sought to determine if the CA-125 test can be used to monitor treatment effect among patients receiving intraperitoneal chemotherapy (IP). MethodsPatient charts from a phase III clinical trial (GOG 172) were retrospectively reviewed. Serum CA-125 levels prior to each cycle of therapy were collected and compared between the IV and IP chemotherapy delivery. The association between CA-125 and progression-free survival (PFS) or overall survival (OS) was estimated and the homogeneity of the results between IP and IV chemotherapy was assessed. ResultsA total of 177 patients were treated with IV chemotherapy and 165 patients with IP chemotherapy with CA-125 data available were included in this analysis. The observed difference was not statistically significant in median CA-125 levels between the IV and IP arms at any time point (P > 0.05 for all). Following surgery and adjuvant chemotherapy, patients with an abnormal CA-125 > 35 U/ml were 2.45 times more likely to have disease progression (95% CI: 1.52–3.95, P < 0.001) and 2.78 times more likely to die of disease (95% CI: 1.66–4.65, P < 0.001), compared to those with a CA-125 < 35 U/ml. These results were consistent with IP and IV chemotherapy. ConclusionSerum CA-125 levels decrease in a similar manner during IP chemotherapy when compared to IV chemotherapy. Serum CA-125 algorithms for monitoring treatment effect that have been established for IV chemotherapy may also be applied for patients receiving IP chemotherapy.

A randomized study of screening for ovarian cancer: a multicenter study in Japan

Ovarian cancer is common in women from developed countries. We designed a prospective randomized controlled trial of ovarian cancer screening to establish an improved strategy for the early detection of cancers. Asymptomatic postmenopausal women were randomly assigned between 1985 and 1999 to either an intervention group (n = 41,688) or a control group (n = 40,799) in a ratio of 1:1, with follow-up of mean 9.2 years, in Shizuoka district, Japan. The original intention was to offer women in the intervention group annual screens by gynecological examination (sequential pelvic ultrasound [US] and serum CA125 test). Women with abnormal US findings and/or raised CA125 values were referred for surgical investigation by a gynecological oncologist. In December 2002, the code was broken and the Shizuoka Cohort Study of Ovarian Cancer Screening and Shizuoka Cancer Registry were searched to determine both malignant and nonmalignant diagnoses. Twenty-seven cancers were detected in the 41,688-screened women. Eight more cancers were diagnosed outside the screening program. Detection rates of ovarian cancer were 0.31 per 1000 at the prevalent screen and 0.38-0.74 per 1000 at subsequent screens; they increased with successive screening rounds. Among the 40,779 control women, 32 women developed ovarian cancer. The proportion of stage I ovarian cancer was higher in the screened group (63%) than in the control group (38%), which did not reach statistical significance (P = 0.2285). This is to our knowledge the first prospective randomized report of the ovarian cancer screening. The rise in the detection of early-stage ovarian cancer in asymptomatic postmenopausal women is not significant, but future decisions on screening policy should be informed by further follow-up from this trial.

Feasibility of screening for ovarian cancer using symptoms as selection criteria*

Retrospective studies have reported that 95% of women with ovarian cancer have symptoms prior to diagnosis and that women with these symptoms are at an increased risk of ovarian cancer. Failure to recognise these symptoms may result in a delay in referral and diagnosis. We assess the feasibility of screening for ovarian cancer using symptoms as selection criteria. A randomised controlled trial. General practices in East London. Three hundred and ninety GPs. GPs were randomised by practice, and those in the study group were given rapid access to ultrasound and CA125 test for women, >45 years, suffering from symptoms that may be caused by ovarian cancer. Symptoms leading to referral, ultrasound and CA125 results and ovarian cancer diagnosis. Seventy nine practices containing 197 GPs were randomised to the study arm. Three hundred and seventeen women were referred, of which 315 were eligible. Women reported the following symptoms: abdominal 87%, gastrointestinal 41% and constitutional 29%. Twenty-three women had abnormal findings on ultrasound: 20 were managed conservatively and 3 surgically. Histology revealed a mucinous cystadenoma, a Brenner tumour and a serous cystadenoma. Incidental findings included endometrial pathology in 13 women and bladder pathology in 2. Ninety five percent of CA125 results were <35 units/ml. This pilot study confirms the feasibility of screening for ovarian cancer using symptoms as selection criteria. Specificity was high and patient compliance good. Initial concerns about referral volumes and additional investigations and referrals generated were not confirmed. No ovarian cancers were detected in this pilot study, and this may be due to the size of the cohort.

Environmental Medicine : Blood Test to Detect Lung Cancer

Vol. 114, No. 12 EnvironewsOpen AccessEnvironmental Medicine : Blood Test to Detect Lung Cancer Victoria McGoverns Victoria McGoverns Search for more papers by this author Published:1 December 2006https://doi.org/10.1289/ehp.114-a693aAboutSectionsPDF ToolsDownload CitationsTrack Citations ShareShare onFacebookTwitterLinked InReddit Lung cancer kills more Americans each year than all leukemias and cancers of the breast, prostate, and ovary combined. But a new diagnostic that may allow early detection of the dominant form of the disease could change that grim picture. A team of researchers at the University of Kentucky Chandler Medical Center in Lexington led by Li Zhong, an assistant professor in the Division of Pulmonary, Critical Care, and Sleep Medicine, has developed a blood test for detecting non–small cell lung cancer (NSCLC), the disease associated with 80% of diagnosed lung cancers.An estimated 175,000 new cases of lung cancer will be diagnosed in 2006, according to the American Cancer Society, and about 162,000 people will die of the disease. Fewer people are dying of NSCLC than in the past, which may reflect fewer people smoking. Still, those diagnosed tend to be diagnosed late, and those diagnosed late tend to die of the disease.Spiral computed tomography (CT) imaging is today’s gold standard for lung cancer detection, able to identify tumors less than 1 cm in diameter. But at more than $400 a test, spiral CT imaging is far too costly for population-level screening. Further, there is growing concern that spiral CT imaging is overdetecting lung cancers that, left alone, would not progress, and might even regress. A better test would be one specific for cancers that are actively progressing.Zhong’s test, described in the July 2006 issue of the Journal of Thoracic Oncology, uses a panel of five cancer-associated protein markers identified by their reactivity to antibodies in cancer patients’ blood. The markers were identified by generating a panel of proteins corresponding to genes expressed in NSCLC cells, then probing them with antibodies from NSCLC patients’ blood. The five proteins that were the most discriminating—reacting to antibodies from patients much more than they reacted to antibodies found in the blood of nonpatients—were tested together for their ability to discern between blood samples drawn from diagnosed NSCLC patients and those from nonpatient controls.Used together, the five markers form a “fingerprint” for cancerous samples, with a readout that is highly specific, able to separate cancer and noncancer samples in 87.5% of cases tested. By comparison, the widely hailed prostate-specific antigen test for diagnosing prostate cancer is just 36% accurate, and the CA125 test for ovarian cancer is 57% accurate. The new test can also recognize cancerous samples in earlier stages.The cost of the new test will depend on the diagnostic platform ultimately developed, but is expected to be significantly less than the current standard. “We can lower the risk of people [progressing] to advanced-stage lung cancer,” Zhong says. “If you can screen less expensively first, then you can suggest some people for follow-up—come back in six months and redo the test, or for some, go ahead and take the CT test now.”Jonathan Cohen, whose Rockville, Maryland, company 20/20 GeneSystems is developing the new test toward clinical application, is confident that the test could change outcomes. “A lot of diagnostic products stumble because they won’t make a clear clinical impact,” he says. “This is one where there’s a significant unmet need and a clear and very compelling clinical utility.”Ruth Etzioni, a cancer statistician at the Fred Hutchinson Cancer Research Center in Seattle, recommends caution, though. Of this and the other new fingerprint diagnostics coming into use, she says, “The sensitivity and the ability to identify tumors is only the first step. Then whether it actually carries with it a significant benefit and a low harm profile is the key.”Pinpointing lung cancerA new blood test may help doctors detect non–small cell lung cancers earlier.FiguresReferencesRelatedDetails Vol. 114, No. 12 December 2006Metrics About Article Metrics Publication History Originally published1 December 2006Published in print1 December 2006 Financial disclosuresPDF download License information EHP is an open-access journal published with support from the National Institute of Environmental Health Sciences, National Institutes of Health. All content is public domain unless otherwise noted. Note to readers with disabilities EHP strives to ensure that all journal content is accessible to all readers. However, some figures and Supplemental Material published in EHP articles may not conform to 508 standards due to the complexity of the information being presented. If you need assistance accessing journal content, please contact [email protected]. Our staff will work with you to assess and meet your accessibility needs within 3 working days.

Emerging role of inhibin as a biomarker for ovarian cancer

Ovarian cancer is the most lethal gynecological malignancy as it is diagnosed at a late clinical stage in more than 80% of patients. The development of diagnostic tests that can detect all types of ovarian cancers with high specificity and sensitivity, and at an early stage would improve survival rates. Serum inhibin is an ovarian hormone involved in the regulation of fertility, decreasing to undetectable levels after menopause. Certain ovarian malignancies, such as mucinous carcinomas and granulosa cell tumors, continue to produce inhibin, which is detectable in serum. A test for serum inhibin has been developed which is able to diagnose granulosa cell tumors and mucinous carcinomas with high accuracy. When the inhibin assay is used in conjunction with the CA125 test, which detects epithelial ovarian carcinomas, the two tests detect the majority of ovarian cancers with high sensitivity (95%) and specificity (95%). This article discusses the application of the inhibin test in ovarian cancer.

Emerging Role of Inhibin as a Biomarker for Ovarian Cancer

Ovarian cancer is the most lethal gynecological malignancy as it is diagnosed at a late clinical stage in more than 80% of patients. The development of diagnostic tests that can detect all types of ovarian cancers with high specificity and sensitivity, and at an early stage would improve survival rates. Serum inhibin is an ovarian hormone involved in the regulation of fertility, decreasing to undetectable levels after menopause. Certain ovarian malignancies, such as mucinous carcinomas and granulosa cell tumors, continue to produce inhibin, which is detectable in serum. A test for serum inhibin has been developed which is able to diagnose granulosa cell tumors and mucinous carcinomas with high accuracy. When the inhibin assay is used in conjunction with the CA125 test, which detects epithelial ovarian carcinomas, the two tests detect the majority of ovarian cancers with high sensitivity (95%) and specificity (95%). This article discusses the application of the inhibin test in ovarian cancer.