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NCT06329323 Clinical Trial

SerUm and Plasma MicroRNAs in Malignant Ovarian gERm Cell Tumours

Ovarian Cancer Clinical Trial

SUMMER

Official title:
SerUm and Plasma MicroRNAs in Malignant Ovarian gERm Cell Tumours

Clinical Trial Details — Status: Not yet recruiting

Administrative data
NCT number NCT06329323
Other study ID # 23CX8477
Secondary ID
Status Not yet recruiting
Phase
First received
Last updated
Start date April 14, 2024
Est. completion date April 2028

Study information
Verified date March 2024
Source Imperial College London
Contact Nina C Cooper, MBBS BSc
Phone 02033513150
Email nina.cooper3@nhs.net
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

The goal of this observational case-control study is to learn about the circulating and tissue microRNA expression, imaging and radiomic profiles of malignant ovarian germ cell tumours (MOGCT) compared to patients with a benign OGCT and no ovarian pathology. The main question[s] it aims to answer are: 1. To understand the circulating miRNA expression of malignant ovarian germ cell tumours (MOGCTs) compared to those with benign ovarian germ cell tumours (BOGCTs) 2. To understand the imaging profile of MOGCTs compared to that of BOGCTs 3. To establish the relationship between serum and plasma miRNA expression in response to treatment and relapse of disease 4. To discover if miRNA expression correlates with radiomic features of OGCTs on both ultrasound and MRI 5. To see if we can link the micro RNAs in tumour samples to those found in blood samples, and to find a plausible explanation for why these micro RNAs are raised (in terms of the tumour biology itself).aims Participants will have serial blood tests at different time points in their care to assess how circulating miRNA levels are affected by treatment and/or remission and/or relapse. If they have surgery, a pathology sample will be taken from the main tumour specimen. Radiomic analysis will take place on existing ultrasound images of their mass. Researchers will compare the circulating miRNA profile of patients with a benign ovarian germ cell tumour and no ovarian pathology to see where the differences lie. If a patient with a BOGCT requires surgery, a pathology sample will be taken from the main tumour specimen. Radiomic analysis will take place on existing ultrasound images of their benign mass.

Description:

Case population (MOGCTs): 1. Serum aFP (alpha fetoprotein), hCG (human chorionic gonadotrophin), LDH (lactate dehydrogenase) and Ca125 (cancer antigen 125) tumour markers measured at time of diagnosis 2. Additional serum and plasma sample to be obtained at the same time as initial bloods 3. Subsequent serum and plasma samples to be obtained as per study arms 1-3 based on cancer staging 4. Tissue samples will be obtained at the time of surgery Control population: Participants acting as controls will be identified from those attending for TV-USS where either a benign teratoma or no pathology is identified (e.g. from a gynaecology clinic). A total of 26ml of blood will be taken. Serum aFP, hCG, LDH and Ca125 will be measured as per routine clinical practice in patients with a benign OGCT. Patients in the control population (benign germ cell tumours or patients with no known gynaecological pathology) will have a single blood test for miRNA analysis. If participants require an operation for the benign GCT, tissue samples will be obtained at the time of surgery. miRNA analysis will be performed using NanoString for the discovery panel. Further targeted sequencing will be performed in the larger prospective study using specific miRNA panels. This may be done using NanoString or a custom MiRNA assay primer. Endpoint The pilot will be completed after the final patient has completed 12 months of follow up. The pilot data analysis will take place at that point. We anticipate that the study will end 12 months after the final participant has completed 24 months of follow up, which gives 12 months for analysis of the samples. The number of participants to take part will be based on a power calculation performed at the time of analysis of the pilot data. DATA COLLECTION AND MANAGEMENT Patients will enter study arm 1-3 based on cancer staging, or will belong to the control group. Each participant will be followed up for a maximum of 2 years after they receive their definitive treatment (surgery and/or (neo)adjuvant chemotherapy). We anticipate this will be a maximum of 30 months total time in the study. An interim analysis of data will be performed at 12 months, with a view to: 1. Identify key miRNAs for prospective validation 2. Allow for appropriate power calculation of the prospective validation study

Recruitment information / eligibility
Status Not yet recruiting
Enrollment 24
Est. completion date April 2028
Est. primary completion date April 2027
Accepts healthy volunteers No
Gender Female
Age group 16 Years and older
Eligibility Inclusion Criteria: - All patients with a new diagnosis of a malignant ovarian germ cell tumour. - The control population will include all patients with a new diagnosis of a benign ovarian germ cell tumour or no known gynaecological pathology. Exclusion Criteria: - Previous or ongoing chemotherapy for MOGCT - Previous surgery for MOGCT - Pregnancy - this will be verbally communicated for those not having surgery or chemotherapy, for those having surgery or chemotherapy a urine pregnancy test should be negative and documented in the clinical notes. - Fetal circulating DNA is known to be present in maternal blood and therefore pregnant women should not be included in this study - Denial of informed consent - Age <16 years - History of any other cancer

Study Design

Related Conditions & MeSH terms

Intervention

Diagnostic Test:
Blood test
Serum and plasma microRNA quantification
Pathology specimen miRNA expression
Pathology specimen mirNA expression - ALL MOGCT; OPTIONAL for BOGCT

Locations
Country Name City State
n/a

Sponsors (1)
Lead Sponsor Collaborator
Imperial College London

Outcome
Type Measure Description Time frame Safety issue
Primary Difference in microRNA expression (plasma) between benign and malignant masses Comparison of heatmaps based on mean expression of clusters across samples 24 months
Primary Difference in microRNA expression (serum) between benign and malignant masses Comparison of heatmaps based on mean expression of clusters across samples 24 months
Primary microRNA expression (plasma) Differential expression of microRNAs (assessed using a moderated t statistic and P values adjusted for multiple testing) 24 months
Primary microRNA expression (serum) Differential expression of microRNAs (assessed using a moderated t statistic and P values adjusted for multiple testing) 24 months
Secondary Quantitative measure of circulating miRNA before treatment miRNA expression in plasma samples of women with a diagnosis of a MOGCT compared to those of women with BOGCTs using nCounter miRNA Expression panels 24 months
Secondary Quantitative measure of circulating miRNA before treatment miRNA expression in serum samples of women with a diagnosis of a MOGCT compared to those of women with BOGCTs using nCounter miRNA Expression panels 24 months
Secondary Quantitative measure of circulating miRNA after treatment miRNA expression in plasma samples of women with a diagnosis of a MOGCT compared to those of women with BOGCTs using nCounter miRNA Expression panels 24 months
Secondary Quantitative measure of circulating miRNA after treatment miRNA expression in serum samples of women with a diagnosis of a MOGCT compared to those of women with BOGCTs using nCounter miRNA Expression panels 24 months
Secondary Performance of segmentation model on ultrasound images Correlation between identification of region of interest (ROI) to examiner segmentation. Dice surface coefficient (DICE). 24 months
Secondary Performance of segmentation model on MRI images Correlation between identification of region of interest (ROI) to examiner segmentation. Dice surface coefficient (DICE) 24 months
Secondary Performance of classification model on ultrasound images Correlation between benign or malignant diagnosis by model vs ultrasound subjective assessment or histopathological diagnosis (area under the ROC curve (AUC), F1-score) 24 months
Secondary Performance of classification model on MRI images Correlation between benign or malignant diagnosis by model vs ultrasound subjective assessment or histopathological diagnosis (area under the ROC curve (AUC), F1-score) 24 months
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