RNA Assays for Endometriosis Detection and Diagnosis (RNA-EndoDx)

Endometriosis is a common disease that affects up to 10% of women of reproductive age. Diagnosis, however, is typically delayed (up to 12 years) and is typically made after surgery. A key unmet need therefore is an accurate, non-invasive biomarker that can be used to detect the disease early.

We hypothesize that endometriosis-related circulating gene expression can be identified using transcriptomic and bioinformatics approaches and used to construct an accurate diagnostic tool for this condition.

The primary objective is to develop a gene signature that detects endometriosis. The hypothesis is that this disease is characterized by a set of genes that characterize endometriosis tumor biology.

The aim is to detect over-expressed genes (elevated mRNA expression) in endometriosis tissue. The goal is to identify 10-25 biomarker genes that are highly expressed to form a candidate biomarker panel.

Highly expressed genes will be determined against samples collected from age/menstrual stage matched controls. A bio-informatics approach will be used to identify these over-expressed genes. This form the basis of a potential diagnostic panel.

Per PICOT criteria:

• The target patient population are women aged 20-35 years with a pathological diagnosis of endometriosis.
• The intervention is sample collection at the time of diagnosis (tissue, blood, saliva)
• The comparison group are normo-ovulatory subjects (age 20-25 years) undergoing surgery for benign cervical lesions.
• The outcome is a gene signature that is associated with endometriosis.
• The follow-up time is one year.

The secondary objective is to test the diagnostic utility of the 10-25 gene panel. This will be undertaken using the retrospectively collected samples.

• Each of the highly expressed genes will be measured and quantified using an RT-PCR approach.

• Genes that are statistically over-expressed in the endometriosis samples will be selected for a PCR panel.

• The expression of genes in the PCR panel will be scored.

• Low scores will be related to "control" and higher scores to "endometriosis".

• The scores will be formally evaluated as a diagnostic (area under the curve analysis, accuracy, sensitivity and specificity metrics).

• A specific comparison will be made between the endometriosis cohort and the control cohort.

• The metrics for a successful assay are:

  • Accuracy >80%
  • Sensitivity >90%
  • Specificity >85%
  • AUC >0.8