Actively Recruiting
Intrinsic Validity of Molecular Marker(s) Detection on Tissular Tumoral DNA to Predict the Efficacy of 177Lutetium-PSMA-617 (Lu-PSMA) Treatment for Castration-resistant Metastatic Prostate Cancer
Led by Centre Jean Perrin · Updated on 2025-12-31
120
Participants Needed
5
Research Sites
507 weeks
Total Duration
On this page
Sponsors
C
Centre Jean Perrin
Lead Sponsor
G
GIRCI Auvergne Rhone-Alpes
Collaborating Sponsor
AI-Summary
What this Trial Is About
Prostate cancer is the most common cancer in men. Its incidence is rising as the population ages. In the localized stage, the 5-year overall survival rate (OS) is 98%. Metastatic progression and resistance to castration have a negative impact on prognosis. Despite recent advances in management, the 5-year OS is around 30%. Therapeutic advances in this indication have been made mainly by the use of taxanes and second-generation hormone therapy. These treatments have improved OS and progression-free survival (PFS). They are now used as standard therapy. More recently, the Phase III VISION trial confirmed the improvement in OS and radiological PFS achieved by treatment with the radioligand 177Lutetium-PSMA-617 (Lu-PSMA) in patients with advanced metastatic castration-resistant prostate cancer (mCRPC). This treatment is currently available in early access in France. Despite encouraging results, 40% of patients will not respond to Lu-PSMA, and there are currently no validated predictive factors. Studies are currently on going, but the identification of biomarkers seems necessary to better stratify risk in these patients. Numerous tissue prognostic tests based on molecular characteristics or cell proliferation are emerging with this in mind. At present, molecular profiling is not a routine technique for prostate cancer, as it is for other solid cancers. At an early stage, the Decipher® Genomic classification tool has shown prognostic utility independently of therapeutic and clinico-pathological data. According to recent studies, methylome analysis would enable the subdivision of mCRPCs and could help identify new therapeutic targets. In the metastatic phase, certain molecular abnormalities involving DNA repair genes are predictive of response to PARP inhibitors. Molecular analysis (mutations, copy number alterations, gene expression, DNA methylation) could therefore be useful in optimizing the management of mCRPC patients treated with Lu-PSMA. If reliable molecular abnormalities are identified on tissue, a diagnostic technique based on circulating tumor DNA (ctDNA) analysis will be useful in decision-making for these patients. A biological collection will therefore be created during the course of this study, with a view to using ctDNA analysis in subsequent research.
CONDITIONS
Official Title
Intrinsic Validity of Molecular Marker(s) Detection on Tissular Tumoral DNA to Predict the Efficacy of 177Lutetium-PSMA-617 (Lu-PSMA) Treatment for Castration-resistant Metastatic Prostate Cancer
Who Can Participate
Eligibility Criteria
You may qualify if you...
- Male over 18 years of age
- ECOG performance status of 2 or less
- Histologically confirmed metastatic castration-resistant prostatic adenocarcinoma with available tumor tissue
- Received at least one taxane chemotherapy line and one second-generation hormone therapy line
- Receiving androgen deprivation therapy with serum testosterone below 50 ng/dL or surgical castration
- Progressive metastatic castration-resistant prostate cancer based on PSA increase, soft-tissue progression, or bone disease progression
- At least one metastasis (bone, soft tissue, or visceral) documented within 43 days prior to inclusion
- Indication for Lu-PSMA treatment confirmed by PET 68Ga-PSMA-11 with positive lesion criteria
- Adequate organ function including bone marrow, liver, and kidney parameters
- Provided free and informed consent
- Covered by social security or beneficiary
You will not qualify if you...
- Continuing second-generation hormone therapy
- Other cancer in the last 3 years affecting life expectancy or disease assessment
- Protected adult status
- Somatic or psychiatric illness interfering with study participation
- Unable to understand or comply with study requirements
- ECOG performance status greater than 2
- Untreated dilation of pyelocalicial cavities
- Bladder obstruction or uncontrollable urinary incontinence
- Symptomatic or imminent spinal cord compression
- Risk of bone fracture
- Active symptomatic brain injury
- Participation in another therapeutic trial or investigational agent within 28 days
- Metastatic tumor tissue only available for diagnosis
- Treatment with certain radiotherapies within 6 months prior
- Previous treatment with PSMA-targeting radioligands
- Known hypersensitivity to study treatments or similar drugs
- Blood transfusion or bone marrow stimulating agents used only to meet study eligibility
AI-Screening
AI-Powered Screening
Complete this quick 3-step screening to check your eligibility
Trial Site Locations
Total: 5 locations
1
Centre Jean PERRIN
Clermont-Ferrand, France, 63011
Actively Recruiting
2
CHU de Grenoble
La Tronche, France, 38700
Not Yet Recruiting
3
Hospices Civiles de Lyon
Pierre-Bénite, France, 69310
Not Yet Recruiting
4
Hôpital privé de la Loire
Saint-Etienne, France, 42100
Not Yet Recruiting
5
Centre Paul STRAUSS
Strasbourg, France, 67091
Not Yet Recruiting
Research Team
J
Judith PASSILDAS JAHANMOHAN, PhD
CONTACT
How is the study designed?
Study Type
INTERVENTIONAL
Masking
NONE
Allocation
NA
Model
SINGLE_GROUP
Primary Purpose
OTHER
Number of Arms
1
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