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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT03787056
Other study ID # 69HCL18_0369
Secondary ID
Status Recruiting
Phase N/A
First received
Last updated
Start date December 4, 2018
Est. completion date January 4, 2028

Study information

Verified date July 2021
Source Hospices Civils de Lyon
Contact Benoit YOU, MD
Phone 04 78 86 43 53
Email benoit.you@hu-lyon.fr
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Progastrin is a pro-hormone that, in physiological conditions, is maturated in gastrin in G cells of the stomach. The role of the gastrin is to stimulate the secretion of gastric acids during digestion. It is also important for the regulation of cell growth of the gastric mucosal. In a healthy person, progastrin is not detectable in the peripheral blood. However, progastrin is abnormally released in the blood of patients with different cancers (colorectal, gastric, ovarian, breast, cervix uterus, melanoma…) The gene GAST coding for progastrin is a direct target gene of the WNT/ß-catenin oncogenic pathway. The activation of this oncogenic pathway is an early event in cancer development. Chronic activation of the WNT/ß-catenin oncogenic pathway occurs in almost all human solid tumors and is a central mechanism in cancer biology that induces cellular proliferation, blocking of differentiation leading to primary tumor growth and metastasis formation. Progastrin measured in the peripheral blood of patients on treatments, could be a new powerful marker for diagnosis and prognosis at different stages.


Recruitment information / eligibility

Status Recruiting
Enrollment 410
Est. completion date January 4, 2028
Est. primary completion date January 4, 2028
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility - Histologically and/or cytologically documented (documentation obtained before or after diagnostic surgical procedure when clinical suspicion is strong), cancers for the following cohorts: o Breast carcinomas o Gastric carcinomas o Renal carcinomas o Prostate carcinomas o Lung carcinomas: NSCLC and SCLC o Hepatocellular carcinomas o Colorectal carcinomas - Head and neck carcinomas - Thyroid cancer - Pancreatic carcinomas - Ovarian adenocarcinomas - Glioblastoma - Endometrial adenocarcinomas - Bladder carcinoma - Superficial Oesophago-gastric carcinomas - Diffuse Large B-cell Lymphomas - Patient older than 18 years. - Patients who gave its written informed consent to participate to the study - Patients affiliated to a social insurance regime Specific inclusion criteria for curative treatment strategy cancer patients: - Indication of a treatment strategy with curative intent (surgery; radiotherapy; chemotherapy; hormonotherapy; targeted agents…) - Patient naïve of anticancer treatments for the considered cancer - A prior anti-cancer treatment is allowed if this treatment was performed with curative intent, and if it did not include systemic chemotherapy, and if a complete remission = 6 months was observed in between the end of treatment and relapse. Previous local treatments for superficial lesions are allowed without any time restriction (for example among others, intravesical treatment for superficial bladder cancer lesions). Specific inclusion criteria for non-curative treatment strategy cancer patients: - Indication of a treatment strategy with no curative intent (radiotherapy; chemotherapy; hormonotherapy; immunotherapy; targeted agents, non-curative surgery, …) - Patient naïve of anticancer treatments in non-curative setting (except for metastatic hormone-sensitive prostate cancer, see specific inclusion criteria). The following tumor type specific inclusion criteria must be met in addition to the inclusion criteria listed above: Breast carcinomas • All cohorts: - Invasive breast ductal carcinoma, or - Invasive breast lobular carcinoma - Curative intent treatment patient cohort: - Planned to be treated with surgery, with/without neo-adjuvant and/or adjuvant chemotherapy and/or anti-hormone treatment Gastric carcinomas - All cohorts: o Intestinal-type adenocarcinoma, or o Diffuse cell type adenocarcinoma - Curative intent treatment patient cohort: - Planned to be treated with surgery with/without neo-adjuvant treatment, with/without adjuvant treatment Renal carcinomas • All cohorts: - Any histology of renal cancer is accepted (non-clear cell renal cancer could be included) - A pathology proof of renal cell carcinoma is not necessarily provided if patients present typical radiologic characteristics of renal cancer on imaging • Curative intent treatment patients cohort: - Planned to be treated with partial or total nephrectomy Prostate carcinomas - Curative intent treatment patients cohort: o Localized prostate cancer with high risk features : StageT2b , T2c or T3 and/or Gleason >= 4+3 and/or PSA >= 20 and/or N+ o Planned to be treated with radical prostatectomy or radiotherapy (potentially associated with androgen deprivation therapy). Brachytherapy and/or focused ultrasounds are not allowed. - Non-curative intent treatment patients cohort: - Patients with metastatic castration resistant prostate cancer (mCRPC) defined by validated criteria of EAU, planned to be treated with doceteaxel or cabazitaxel or second generation hormone (i.e. abiraterone or enzalutamide). Patients have to be naïve of treatment for the castration resistant mCRPC. Patients that previously received docetaxel or a 1st or 2nd generation hormonotherapy for their hormone-sensitive prostate cancer in metastatic setting can be included. Lung carcinomas treated by immunotherapy : • Non-curative intent patients cohort: o NSCLC stage IV according to 8th TNM classification planned to be treated with immunotherapy, with/ without chemotherapy Lung carcinomas excluding those treated with immunotherapy: - Curative intent treatment patients cohort: o NSCLC histology only o Stage I-II according to 8th TNM classification o Stage IIIA-B according to 8th TNM classification o Planned to be treated with radical treatment (surgery or radiotherapy with/without concurrent chemotherapy), potentially associated with neo-adjuvant or adjuvant treatment - Non-curative intent patients cohort: - NSCLC or SCLC stage IV according to 8th TNM classification planned to be treated with a first line of chemotherapy, with/without associated treatments except immunotherapy (radiotherapy, targeted therapies…). Immunotherapy can be administrated for the subsequent lines of treatment. Hepatocellular carcinomas A pathology proof of HCC is not necessarily provided if patients present typical radiologic characteristics of hepatocellular carcinoma on imaging - Absence or chronic hepatic encephalopathy, absence of refractory ascites - Curative intent treatment patients cohort: - Indication of a treatment strategy with curative intent, except liver transplantation: surgical resection, monopolar radiofrequency ablation for HCC (1 to 3 nodules =3 cm) or multibipolar radiofrequency if nodule =4 cm). • Non-curative intent patients cohort: - Indication of a treatment strategy with no curative intent: transarterial intra-hepatic chemoembolization, targeted therapies (tyrosine kinase inhibitors or monoclonal antibodies) or immune therapy. Colorectal carcinomas • Curative intent treatment patients cohort: o Lieberkühn adenocarcinoma associated with metastases planned to be treated with peri-operative chemotherapy +/- targeted agent and interval surgery Head and neck carcinomas - All cohorts o Head and neck squamous cell carcinoma from oral cavity, oropharynx, hypopharynx, larynx - Curative intent treatment patients cohort: o Planned to be treated with a radical treatment (surgery and/or radiotherapy potentially associated with concurrent chemotherapy) with/without neo-adjuvant/adjuvant chemotherapy. - Non-curative intent treatment patients cohort: o De novo metastatic or metastatic/loco-regional relapse planned to be treated with chemotherapy and/or immunotherapy Thyroid cancer • Curative intent patient cohort o Thyroid carcinoma differentiated, poorly differentiated, papillary, vesicular, Hurthle Cell o For which a iodine treatment is indicated (Iodine treatment will be discussed after surgery. In the case the histological result does not confirm a high risk thyroid cancer, patient will be withdrawn from the study. In the same way, if a iodine treatment is not recommended after surgery, patient will be withdrawn from the study. In both cases, patient will be replaced). Pancreatic carcinomas • Curative intent patients cohort: o Pancreas exocrine adenocarcinoma planned to be treated with initial surgery with/without neo-adjuvant chemotherapy and with/without adjuvant chemotherapy or radiotherapy Ovarian adenocarcinomas • Non/uncertain curative intent patients cohort: o 1st platinum-sensitive relapse - High or low grade epithelial adenocarcinomas or carcinosarcoma - Planned to be treated with chemotherapy and/or PARP inhibitors based treatment, +/- interval debulking surgery Glioblastoma • Curative intent patients cohort: o Planned to be treated with surgical resection, followed by adjuvant temozolomide and radiotherapy Endometrial adenocarcinomas - Non-curative intent patients cohort: o Type 1 (endometrioid or mucinous) or type 2 endometrial (serous, clear cell, undifferentiated carcinoma and carcinosarcoma) cancers o Planned to be treated with non-curative systemic treatment for metastatic or advanced disease Bladder carcinoma - Transitional cell carcinoma • Curative intent treatment patients: - Patients with localized muscle invasive bladder cancer (>=PT2) - Planned to be treated with neo-adjuvant cisplatin based chemotherapy, or immunotherapy or a combination of chemotherapy and immunotherapy Superficial Oesophago-gastric cancer • Curative intent patients cohort: o Superficial oesophago-gastric carcinomas (adenocarcinomas or epidermoid carcinomas) of Stage T1 planned to be treated by endoscopic surgery Diffuse Large B-Cell Lymphoma (DLBCL) • Curative intent patients cohort: o Patients planned to be treated with R-CHOP (Rituximab-Cyclophosphamide, Hydroxyadriamycine, Oncovin, Prednisone)

Study Design


Related Conditions & MeSH terms

  • B-cell Lymphoma
  • Bladder Cancer
  • Breast Cancer
  • Cancer
  • Carcinoma, Hepatocellular
  • Colorectal Cancer
  • Endometrial Cancer
  • Endometrial Neoplasms
  • Esophageal Cancer
  • Gastric Cancer
  • Glioblastoma
  • Head and Neck Cancer
  • Hepatocellular Cancer
  • Kidney Neoplasms
  • Liver Neoplasms
  • Lung Cancer
  • Melanoma
  • Ovarian Cancer
  • Pancreatic Cancer
  • Prostate Cancer
  • Renal Cancer

Intervention

Other:
Blood draws
Blood draws are realized at each steps of patient disease management. The volume of each blood drawn is 25 mL for progastrin measurements and 5 mL for the dosage of the other tumor markers. The frequency depend to the cancer and treatment administered : Baseline at diagnosis : Local radical treatment : within 24h before surgery, within 24h after surgery and at the post-surgery follow up visit Chemotherapy treatment : every 3 or 4 weeks Radiotherapy : start day and at the end of radiation ("end of treatment" visit) Palliative systemic treatment (only palliative cohorts) : every 3 to 12 weeks. Follow until the third progression or change of treatment line, or alternatively up to 5 years after inclusion In case of PD or TOX Follow up: at each visit scheduled (every 3 months) for the first 2 years, then every 6 months for 3 years Relapse : withdrawn from the study and last progastrin measurement. Patient could be enrolled in the non-curative intent cohort

Locations

Country Name City State
France Service de NEURO-ONCOLOGIE du Groupement Hospitalier EST Bron
France Service d'ONCOLOGIE DIGESTIVE et HEPATOLOGIE de l'hôpital de la Croix-Rousse Lyon
France Service d'ONCOLOGIE DIGESTIVE et HEPATOLOGIE de l'Hôpital E. Herriot Lyon
France Service d'Oto-Rhino-Laryngologie de l'Hôpital de la Croix-Rousse Lyon
France Service d'Urologie de l'Hôpital E. Herriot Lyon
France Service de Gynécologie de l'hôpital de la Croix-Rousse Lyon
France Service de Gynécologie du Groupement Hospitalier Est Lyon
France Service de Pneumologie de l'hôpital de la Croix-Rousse Lyon
France Service de Pneumologie du Groupement Hospitalier Est Lyon
France Service d'Hématologie de l'Hôpital Lyon Sud Pierre-Bénite
France Service d'ONCOLOGIE DIGESTIVE et HEPATOLOGIE du Centre Hospitalier Lyon Sud Pierre-Bénite
France Service d'Oncologie médicale du Centre hospitalier Lyon Sud Pierre-Bénite
France Service d'Urologie de l'hôpital Lyon Sud Pierre-Bénite
France Service de Chirurgie de l'hôpital Lyon Sud Pierre-Bénite
France Service de Dermatologie de l'hôpital Lyon Sud Pierre-Bénite
France Service de Gynécologie de l'hôpital Lyon Sud Pierre-Bénite
France Service de Pneumologie de l'Hôpital Lyon Sud Pierre-Bénite

Sponsors (1)

Lead Sponsor Collaborator
Hospices Civils de Lyon

Country where clinical trial is conducted

France, 

Outcome

Type Measure Description Time frame Safety issue
Primary ROC curve AUC regarding diagnostic accuracy of progastrin levels at baseline in cancer patients compared to non-cancer controls Progastrin concentration in plasma samples will be measured with an ELISA Kit (CancerREAD LAB) provided by ECS Progastrin. At baseline
Secondary Longitudinal kinetic of progastrin values during treatments, assessed by modeled kinetic parameters of interest A nonlinear mixed effect model will be used to model the progastrin measurements done during treatments and follow-up of patients.The effect of each event (chemotherapy, surgery…) on the progastrin value and in the inter-individual variability of production and/or elimination rates of progastrin will be analyzed. Progastrin will be measured by ELISA, and the values will be expressed in pM.
Measures will be done depending on the treatment received. Chemotherapy, every 3 or 4 weeks. Oral treatments: every 3 to 12 weeks. Surgery or radiotherapy: before and after the treatment. Follow up: concomitantly to the visits scheduled for the regular follow up of the patients.
6 years
Secondary Nycthemeral and weekly and post-operative progastrin variations 24 patients will be selected, upon their agreement and serum high levels, to enter in nychtemer (12 patients) or weekly (12 patients) cohorts. For the Nychtemer cohort, progastrin will be assayed at d1 at 8:00 am; 11:00 am; 2:00 pm; 5:00 pm; 8:00 pm and at d2 at 8:00 For the weekly cohort, progastrin will be assayed Day 1; Day 8; Day 15 and +/- Day 22; ideally on the same hour times. Progastrin will be measured by ELISA, and the values will be expressed in pM. every 3 hours within 24 hours for the Nycthemeral cohort, and every week for 2 or 3 weeks for the weekly cohort
Secondary Determinants of progastrin serum values: hepatic function A nonlinear mixed effect model will be used to correlate individual values of progastrin (expressed in pM) with individual characteristic on the patient (hepatic function, as measured by the concentration of AST, ALT and bilirubin).
Measures will be done Chemotherapy, every 3 or 4 weeks. Oral treatments: every 3 to 12 weeks. Surgery or radiotherapy: before and after the treatment. Follow up: concomitantly to the visits scheduled for the regular follow up of the patients
6 years
Secondary Determinants of progastrin serum values: renal function A nonlinear mixed effect model will be used to correlate individual values of progastrin (expressed in pM) with individual characteristic on the patient (renal function, as measured by creatinin concentration and creatinin clearance).
Measures will be done Chemotherapy, every 3 or 4 weeks. Oral treatments: every 3 to 12 weeks. Surgery or radiotherapy: before and after the treatment. Follow up: concomitantly to the visits scheduled for the regular follow up of the patients
6 years
Secondary Determinants of progastrin serum values: age A nonlinear mixed effect model will be used to correlate the individual characteristics of the patient (age and gender) with progastrin concentration at the inclusion. at the inclusion
Secondary Determinants of progastrin serum values: gender A nonlinear mixed effect model will be used to correlate genders with progastrin concentrations at the inclusion. at the inclusion
Secondary Overall survival The relationships between the progastrin kinetics during and after treatment and overall survival will be analyzed. Analyses will be performed separately on patients with curative intent treatment and on patients with palliative intent treatment.
Measures wil be done At the end of the study (6 years for patients enrolled in curative intent and 5 years for patients enrolled in non-curative intent) or alternatively at the occurrence of progression or relapse.
6 years
Secondary recurrence free survival The relationships between the progastrin kinetics during and after treatment and recurrence free survival will be analyzed. Analyses will be performed separately on patients with curative intent treatment and on patients with palliative intent treatment.
Measures wil be done At the end of the study (6 years for patients enrolled in curative intent and 5 years for patients enrolled in non-curative intent) or alternatively at the occurrence of progression or relapse.
6 years
Secondary progression free survival The relationships between the progastrin kinetics during and after treatment and progression free survival will be analyzed. Analyses will be performed separately on patients with curative intent treatment and on patients with palliative intent treatment.
Measures wil be done At the end of the study (6 years for patients enrolled in curative intent and 5 years for patients enrolled in non-curative intent) or alternatively at the occurrence of progression or relapse.
6 years
Secondary The tumor size at cancer diagnosis The size of the tumor will be correlated to progastrin concentration at the time of cancer diagnosis At baseline
Secondary Complete surgery The ability of progastrin kinetics during the neoadjuvant period to predict the outcome of the surgery (complete or not) will be analyzed by a ROC curve. If applicable. 6 years
Secondary time to recurrence (for patients enrolled in curative intent cohorts). The ability of the progastrin kinetics to predict recurrence free survival (curative cohorts), will be based on parameters estimated with a PK/PD model able to characterize the early kinetics of progastrin during and after the end of treatment and during follow up. 6 years
Secondary time to progression (for patients enrolled in non-curative intent cohorts) The ability of the progastrin kinetics to predict progression-free survival (non-curative cohorts) will be based on parameters estimated with a PK/PD model able to characterize the early kinetics of progastrin during and after the end of treatment and during follow up 6 years
Secondary time to death (whenever it occurred) The ability of the progastrin kinetics to predict time to death will be based on parameters estimated with a PK/PD model able to characterize the early kinetics of progastrin during and after the end of treatment and during follow up 6 years
Secondary Comparison of the initial values and of the kinetics of other serum tumor markers (CA15-3, CA 19-9, CA125, CEA, PSA, AFP) with those of progastrin The ROC AUC will be compared between classical markers and the prograstrin. Logistic regression will be used to combine the classical marker(s) and the progastrin in order to estimate the diagnostic value of the marker combination.
progastrin, CA15-3, CA19-9, CA125, CEA, PSA and AFP concentration will be measured on blood sample taken at the inclusion.
at the baseline
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