This study aims to explore the sensitivity of an innovative marker, HE4, in the diagnosis approach of endometrial cancer in case of postmenopausal bleedings.
Endometrial cancer is the most common pelvic gynecological cancer in France, ranking 5th among cancers in women in terms of incidence. The most frequent symptom is post-menopausal bleeding and is one of the primary reasons for consultation in gynecological emergencies. The diagnosis of endometrial cancer is made by histological analysis of endometrial tissue taken during a surgical intervention. The latter is mostly reassuring. These interventions are often performed in mild situations and there is currently no element to be sufficiently reassuring to avoid surgery. At present, there is no biological marker used in current practice. In the population of patients with post-menopausal bleeding requiring surgical exploration for diagnosis, the pathology results are often reassuring. These procedures could have been avoided, especially as these patients often have numerous co-morbidities and these surgeries are therefore more risky. The appearance of a new tumour marker could be useful in the management of these patients and avoid many unnecessary and risky surgeries This study aims to explore the sensitivity of an innovative marker, HE4, in the diagnosis approach of endometrial cancer in case of postmenopausal bleedings.
Study Type
OBSERVATIONAL
Enrollment
100
Any patient presenting post-menopausal bleeding who is to undergo hysteroscopy or hysterectomy will have an additional blood tube taken during her pre-operative blood work-up for the determination of the serum markers HE4 and CA125, after having obtained her non-opposition to participate in the study. The blood tube collected for the research will be sent to the biochemistry laboratory of the Nantes University Hospital for a centralized analysis. This analysis will be done sequentially and the results will not be transmitted to the investigator. At D0, the day of surgery, the operative report will be retrieved as well as the quality of life questionnaires SF12 and PGI-I and the acceptability questionnaire completed before surgery. At 1 month after surgery, the anatomopathological results will be retrieved as well as the value of the tumour markers CA125 and HE4.
Blood was collected in a standard heparinized vial. Samples were sent to a central laboratory unit (biochemistry laboratory at the Nantes university hospital), centrifuged and plasmas were stored at -20°C until analysis. Plasma CA125 and HE4 concentrations were determined by run in single measurements using an electrochemiluminescence Elecsys immunoassay (ECLIA) on a Roche Diagnostics Cobas 8000® e602 analyser (Roche Diagnostics, Mannheim, Germany).
Saint-Nazaire Hospital
Saint-Nazaire, Loire-Atlantique, France
RECRUITINGVendee Hospital Center
La Roche-sur-Yon, Vendee, France
RECRUITINGTo evaluate the sensitivity of the HE4 marker in patients with postmenopausal bleeding in the diagnosis of endometrial cancer
The HE4 assays will be performed using the electrochemiluminescence (ECL) technique on Cobas Pro module E801, Roche Diagnostics. The HE4 assay is based on a sandwich-type electrochemiluminescence method. The HE4 assay with the Roche Diagnostics Elecsys reagent has been standardized against the Fujirebo Diagnostics HE4 EIA method. Positive/negative HE4 result for the estimation of the sensitivity of HE4 in the diagnosis of endometrial cancer. The commonly accepted threshold for ovarian cancer management of 140pmol/l in postmenopausal patients should be used. The gold standard for endometrial cancer is the pathological result (absence/presence of cancer) of the sample taken.
Time frame: Until the pathological results (About 10-15 days)
Assess other diagnostic parameters (specificity, PPV, NPV) of HE4
ROC curve for the HE4 marker in the diagnosis of endometrial cancer.
Time frame: Until the pathological results (About 10-15 days)
Establish the optimal threshold of HE4 for the diagnosis of endometrial cancer (use of an ROC curve)
Search for the threshold with the best specificity of HE4 in the diagnosis of endometrial cancer
Time frame: Until the pathological results (About 10-15 days)
Evaluate the diagnostic capabilities of CA125 alone and in combination with HE4, as well as the REM and REM-B algorithms for the diagnosis of endometrial cancer
Estimation of sensitivity, specificity, PPV and NPV in the diagnosis of endometrial cancer for the CA125 biomarker and the REM and REM B algorithms
Time frame: Until the pathological results (About 10-15 days)
Establish the existence of thresholds for HE4 and/or CA125 markers predictive of disease severity (FIGO stage)
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Search for HE4 and CA125 marker thresholds to assess disease severity by FIGO stage
Time frame: Until the results of the extension assessment in the event of proven endometrial cancer (1 month)
Reassess the pathological threshold value of endometrial thickness on ultrasound
Search for the pathological threshold of endometrial thickness in the diagnosis of endometrial cancer
Time frame: Until the pathological results (About 10-15 days)
Assess the relationship between endometrial thickness on ultrasound and HE4 and CA125 marker values
Estimation of the relationship between CA125 and HE4 markers and endometrial thickness on ultrasound
Time frame: Until the pathological results (About 10-15 days)
To evaluate the diagnostic capabilities of HE4 and CA125 in subgroups of smoking patients and patients with renal failure
Estimation of sensitivity, specificity, PPV and NPV in the diagnosis of endometrial cancer for HE4 and CA125 in patients with active smoking and/or renal failure
Time frame: Until the pathological results (About 10-15 days)
Identify potential confounding factors associated with the value of the HE4 marker like treatments, comorbidities (renal insufficiency, high BMI) and others criteria that are collected in the medical files
Analyses of variables measured at inclusion that may influence the value of the HE4 marker.
Time frame: Until the pathological results (About 10-15 days)