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OveRcoming immunosupprEssion aNd rebAlancing the Immune reSponSe in ovAriaN CancEr Study

NCT06611072RecruitingNAINTERVENTIONAL

Summary

Ovarian cancer (OC) is one of the most lethal cancers in the world due to late-stage disease at diagnosis. Standard therapy consists of debulking surgery and chemotherapy. However, despite this aggressive treatment, recurrent disease almost invariably occurs resulting in a five-year survival rate of approximately 30%. Immunotherapy could be a way to increase survival in OC patients. However, a major barrier to a successful deployment of cancer immunotherapy for ovarian cancer patients is the immunosuppressive tumor microenvironment. Envisioned solution/research direction Tumor-related inflammation is one of the hallmarks of cancers in general. Innate immunity specifically is a common denominator that is involved in the pathogenesis of OC. To improve the patient's outcome and identify novel therapeutic targets, one needs a deeper understanding of the tumor-induced changes in the bone marrow myeloid progenitor cells. Furthermore, treatment of these cells by nanoparticles or other agents that induce a program of 'trained immunity' may be a novel way to re- educate myeloid cells and their bone marrow progenitors in OC patients. Hypothesis We hypothesize that by exposing myeloid cells or their progenitors to various agents that induce trained immunity (e.g. trained immunity-inducing agents: BCG, heat-killed Candida,), these immune cells will undergo functional reprogramming to induce a tumor-suppressive phenotype. In the future, this could be explored as a novel immunotherapy for tumors that are refractory to conventional treatment. Objective To characterize and phenotype the immune state of OC patients compared to controls without cancer with a focus on the hematopoietic organs and the immune cells originating from these organs. In addition, the effect of established trained immunity-inducing agents on these cells will be evaluated in vitro, potentially providing new therapies. This will be executed by assessing the transcriptional, epigenetic, and functional reprogramming of circulating monocytes and myeloid progenitor cells in OC and by assessing the in vitro effect of trained immunity inducers on the reprogramming of circulating monocytes and myeloid progenitor cells. Study design: investigator-initiated, multi-center explorative cross-sectional study at the Catharina hospital Eindhoven, Radboud University Medical Center and Eindhoven University of Technology.

Key Facts

Lead Sponsor

Gynaecologisch Oncologisch Centrum Zuid

Enrollment

Start Date

2025-01-01

Completion Date

2027-10-01

Study Type

INTERVENTIONAL

Official Title

OveRcoming immunosupprEssion aNd rebAlancing the Immune reSponSe in ovAriaN CancEr Study

Interventions

Bone marrow aspirationVena puncturePeritoneal fluidSpleen biopsyTumor biopsyOmental biopsy

Conditions

Ovarian NeoplasmsOvarian CancerOvarian CarcinomaImmune SuppressionImmune System Suppression

Eligibility

Age Range

18 Years+

Sex

FEMALE

Inclusion Criteria:

* Subjects should be at least 18 years old and mentally competent;
* Newly diagnosed patients with OC who go for primary debulking surgery or patients with OC who are scheduled for interval debulking;
* Controls: women who undergo surgery for benign gynaecological conditions under general anaesthesia.

Exclusion Criteria:

* Mentally incompetent;
* Pregnant or breastfeeding;
* Known inflammatory of infectious diseases or an immunosuppressive status;
* Using medication interfering with the immune system;
* Severe comorbidities: other active malignancy (except for basal cell carcinoma and other in situ carcinomas);
* Serious psychiatric pathology;
* A self reported alcohol consumption of \>21 units per week.

Outcome Measures

Primary Outcomes

Cell composition of immune organs using flow cytometry

The number and ratios of different types of stem and immune cells will be determined using general cell protein markers in combination with flow cytometry. Analysis will be performed on blood, spleen, bone marrow and the intraperitoneal fluid.

Time frame: 3 years including evaluation phase

Cell composition and epigenetic status of cells of immune organs using ATAC and RNA sequencing

Cell ratios and epigenetic profile of immune cells in the blood, tumor, bone marrow, and spleen will be analyzed using single-cell RNA and single-cell ATAC sequencing.

Time frame: 3 years including evaluation phase

Trained immunity response

We focus on the degree of trained immunity response upon ex vivo stimulation with trained immunity inducers and measured as the concetration of inflammatory cytokines and ROS production.

Time frame: 3 years including evaluation phase

Locations

Catharina Hospital, Eindhoven, Netherlands

Linked Diseases

Ovarian Neoplasms

Ovarian Neoplasms — a type of gynecological cancer.