Evaluation of Treatment PERSOnalization Based on Its Therapeutic Monitoring in Patients With Metastatic Colorectal Cancer Treated With REgorafenib (RePERSO)

• ClinicalTrials.gov Identifier: NCT04874207
• Recruitment Status: Recruiting
• First Posted: May 5, 2021
• Last Update Posted: January 31, 2024
• Sponsor: Rennes University Hospital
• Information provided by (Responsible Party): Rennes University Hospital

Study Description

Brief Summary:

Regorafenib has demonstrated a significant benefit in overall survival in metastatic colorectal cancer (mCRC) patients. However, more than 50% of patients had severe adverse events (grade 3-4), leading to temporary or definitive discontinuation of treatment.

The RePERSO study proposes to adapt the regorafenib dose regimen taking into account firstly the measurement of sum of metabolites M-2 and M-5 and secondly the occurrence of toxicity during treatment. This treatment personalization through therapeutic drug monitoring pharmacological dosing optimization strategy aims at validating the proof of concept of regorafenib therapeutic drug monitoring and at improving the benefit in OS in patients, using the previously defined Csum therapeutic range.

Condition or disease	Intervention/treatment	Phase
Colorectal Cancer Metastatic	Drug: Regorafenib	Phase 4

Detailed Description:

Regorafenib has demonstrated in two multicenter phase III randomized clinical trials a significant benefit in overall survival (OS) in metastatic colorectal cancer (mCRC) patients treated with regorafenib at 160mg/day 3 weeks/4 (3w/4). However, more than 50% of patients had severe adverse events (grade 3-4), leading to temporary or definitive discontinuation of treatment in 2/3 of the patients and a reduction of the dosing in 20% of them. Thus, a part of the therapeutic failures could be explained by an insufficient exposure to regorafenib because of an early toxicity potentially linked to an initial overexposure. The recent randomized phase II ReDOS study has shown that a gradual increase in the dose of regorafenib (from 80 mg to 160 mg/day 3w/4) led to a significantly greater proportion of patients starting a third cycle of regorafenib and showed a trend toward improvement in overall survival of patients when compared to the standard administration schedule (160 mg/day 3 w/4). These results favored the dose-escalation strategy. However, due to the low correlation between dose and concentration, a concentration-controlled study might be of better relevance.

Regorafenib pharmacokinetics is characterized by a hepatic metabolism leading to the production of two main pharmacologically active metabolites (M-2 and M-5) that may induce therapeutic and adverse effects. The production of these metabolites shows a large inter-individual variability. Pharmacokinetic data from phase III studies have suggested the existence of a relationship between exposure to regorafenib and its metabolites and the occurrence of some therapeutic and adverse effects. In an ancillary pharmacokinetic study of the phase II prospective TEXCAN study in which regorafenib was evaluated in its mCRC indication, it was shown a major benefit in OS in patients with an accumulation of M-2 between the first (C1) and the second (C2) cycle of regorafenib (M2 C2/C1). A significant correlation between M-2 C2/C1 ratio and the sum of trough concentrations of regorafenib, M-2 and M-5 measured at D15C1 (C Sum (Rego+M-2+M-5)) was found, which could be a pharmacological marker of efficacy, earlier than the M-2 C2/C1 ratio. The assessment of the relationship between C Sum and in OS according to a Restricted Cubic Spline analysis showed that the benefit is optimal for a concentration between 2.5 mg/L and 5.5 mg/L (median OS of 10.6 months versus 3.3 and 4.0 months in patients with a concentration <2.5 mg/L and ≥5.5 mg/L, respectively). The rate of serious adverse events was also lower in the group in the range [≥2.5; <5.5 mg/L] (0% vs 43% and 20% respectively). This interval seems to allow limiting the severe toxicities that cause treatment discontinuations and/or early progressions that could explain the over-risk of death when the concentrations are outside.

The RePERSO study proposes to adapt the regorafenib dose regimen taking into account firstly the measurement of Csum and secondly the occurrence of toxicity during treatment. This treatment personalization through therapeutic drug monitoring pharmacological dosing optimization strategy aims at validating the proof of concept of regorafenib therapeutic drug monitoring and at improving the benefit in OS in patients, using the previously defined Csum therapeutic range.

Study Design

• Study Type: Interventional (Clinical Trial)
• Estimated Enrollment: 100 participants
• Allocation: N/A
• Intervention Model: Single Group Assignment
• Masking: None (Open Label)
• Primary Purpose: Treatment
• Official Title: Evaluation of Treatment PERSOnalization Based on Its Therapeutic Monitoring in Patients With Metastatic Colorectal Cancer Treated With REgorafenib
• Actual Study Start Date: October 22, 2021
• Estimated Primary Completion Date: October 2024
• Estimated Study Completion Date: May 2025

Arms and Interventions

Arm	Intervention/treatment
Experimental: Patients; Patients	Drug: Regorafenib; Dose adaptation at the beginning of cycle 2 and cycle 3 after regorafenib dosage at day 15

Outcome Measures

Primary Outcome Measures :

1. Time from inclusion to death [ Time Frame: 12 months ]
   Determine whether "optimal exposure" to regorafenib based on plasma concentration of the drug and its metabolites can improve overall survival in mCRC patients

Secondary Outcome Measures :

1. Ten months survival rate [ Time Frame: 10 months ]
   Percentage of patients alive 10 months after inclusion
2. Objective response Rate [ Time Frame: 12 months ]
   Objective response Rate (ORR) defined as the rate of patients with complete or partial response
3. Disease Control Rate [ Time Frame: 12 months ]
   Disease Control Rate (DCR) is defined as the rate of patients with complete response, partial response or stable disease,
4. Progression-free survival [ Time Frame: 12 months ]
   Progression-free survival (PFS) is defined as the time from inclusion to date of first observed disease progression (radiological or clinical) or death due to any cause, if death occurs before progression is documented. The actual date that the tumor scan was performed will be used for this calculation. PFS for patients without disease progression or death at the time of analysis will be censored at the last date of tumor evaluation.
5. Severe toxicities [ Time Frame: 12 months ]
   Percentage of patients with significant toxicities (≥ grade 3). Adverse events will be assessed from inclusion to 28 day after the discontinuation of the study drug and classified according to the National Cancer Institute Common Terminology Criteria for Adverse Events (NCI-CTCAE) version 5.0.
6. Percentage of optimal exposure [ Time Frame: 2 months ]
   Percentage of patients with "optimal exposure" - i.e. with Csum at day 15 within the range [2.5 - 5.5 mg/L]) - at cycle 1 and cycle 2
7. Difference in overall survival between patient with different metabolite 2 plasma ratio [ Time Frame: 2 months ]
   Overall survival for the half of patients with a low ratio of plasma concentration of Metabolite 2 Cycle2/Ccyle1 compared to the overall survival for the half of patients with a high ratio of plasma concentration of Metabolite 2 Cycle2/Cycle1
8. Genetic polymorphism impact [ Time Frame: 12 months ]
   Genetic polymorphisms in gene involved in regorafenib metabolism and plasma concentrations of regorafenib and its metabolites
9. Body composition [ Time Frame: 12 months ]
   Body composition will be determined on Computerized Tomography scan (CT-scan) imaging done at baseline and for tumor response evaluation during treatment.

Eligibility Criteria

• Ages Eligible for Study: 18 Years and older (Adult, Older Adult)
• Sexes Eligible for Study: All
• Accepts Healthy Volunteers: No

Criteria

Inclusion Criteria:

• - Signed and dated informed consent
• Male or female patients ≥ 18 years-old at time of Informed Consent Form (ICF) signature
• Patients must have a histologically proven metastatic colorectal cancer
• Patients who have previously been treated with standard therapy including a fluoropyrimidine, oxaliplatin, irinotecan, an anti-VEGF (bevacizumab or aflibercept) and an anti-EGFR (cetuximab or panitumumab) for patients who had a RAS wild-type tumor
• In mRCC with MSI-H, the patient must have received immunotherapy. For mRCC with BRAF mutation, the patient should have received a BRAF inhibitor if eligible.
• Patients with a BRAF V600E mutation who have previously received treatment with a BRAF inhibitor.
• ECOG PS = 0 or 1
• Imaging target greater than one cm must be visible on CT

• Patients must have adequate bone marrow, renal, and hepatic function, as evidenced by the pre-therapeutic check-up performed within 7 days before regorafenib initiation: Normal organ functions as defined below :

  1. Absolute neutrophil count ≥ 1.3 Giga/L
  2. Platelets > 100 Giga/L
  3. Hemoglobin ≥ 9 g/dL
  4. Serum creatinine ≤ 1.5 x ULN (Upper Limit of Normal) or Glomerular filtration rate (GFR) ≥30 ml/min/1.73m2 according to the modified Diet in Renal Disease (MDRD) or CKD-EPI (Chronic Kidney Disease Epidemiology Collaboration) abbreviated formula
  5. AST and ALT ≤3 x ULN (≤5.0 × ULN for patients with liver involvement of their cancer)
  6. Total Bilirubin ≤2 X ULN
  7. Alkaline phosphatase ≤3 x ULN (≤5 x ULN in patient with liver involvement of their cancer and/or with bone metastases). If Alkaline phosphatase > 3 ULN (or >5 ULN in patient with liver involvement of their cancer and/or with bone metatstases), hepatic isoenzymes 5-nucleotidase or GGT tests must be performed; hepatic isoenzymes 5-nucleotidase must be within the normal range and/or GGT < 3 x ULN
  8. No argument for acute pancreatitis within 3 months before the start of study medication
  9. No proteinuria: ≥ 1+ protein will require a 24-hour urine collection that must show total protein excretion <1000 mg/24 hours
• INR/PTT ≤1.5 x ULN
• Patients who are therapeutically treated with an agent such as warfarin or heparin will be allowed to participate provided that no prior evidence of underlying abnormality in coagulation parameters exists. For patients treated with VKA, Close monitoring of at least weekly evaluations will be performed until INR/PTT is stable based on a measurement that is pre-dose as defined by the local standard of care
• Women of childbearing potential and male patients must agree to use adequate contraception for the duration of study participation and up to 3 months following completion of therapy
• Women of childbearing potential must have a negative serum β-HCG pregnancy test within 7 days prior randomization
• Patients must be willing and able to comply with scheduled visits, treatment plan, laboratory tests and other study procedures
• Patients affiliated to the Social Security System

Exclusion Criteria:

• - Prior treatment with regorafenib, and with any prior antiangiogenic inhibitor except bevacizumab
• Hypersensitivity to the active substance or to any of the excipients
• Systemic cancer therapy with unfinished washout (in general 3 weeks except for example for capecitabin which has a 1 week washout)
• Concomitant treatment with a cytochrome P450 3A4 (CYP3A4) inducer or inhibitor or UGT1A9 inhibitor
• Patients unable to swallow oral medication
• Digestive obstruction, chronic inflammatory bowel disease or any malabsorption condition
• Previous or concurrent cancer that is distinct in primary site or histology from colorectal cancer within 5 years prior to inclusion, except for curatively treated cervical cancer in situ, non-melanoma skin cancer and superficial bladder tumors (Ta [non-invasive tumor], Tis [carcinoma in situ] and T1 [tumor invades lamina propria])
• Ongoing uncontrolled infection (viral, bacterial or fungal)
• Known history of human immunodeficiency virus (HIV) infection, active hepatitis B or C or chronic hepatitis B or C requiring treatment with antiviral therapy
• Breastfeeding
• Uncontrolled hypertension (systolic blood pressure >140 mmHg or diastolic pressure >90 mmHg despite optimal medical management)
• Arterial thrombotic or embolic events such as cerebrovascular accident (including transient ischemic attacks), within 6 months before the start of study medication
• Unstable angina (angina symptoms at rest), new-onset angina (begun within the last 3 months)
• Myocardial infarction less than 6 months before the start of study medication
• Any hemorrhage or bleeding event ≥ Grade 3, NCI-CTCAE v 5.0 within 4 weeks prior to the start of study medication
• Major surgical procedure, open biopsy or significant traumatic injury within 28 days before start of study medication
• Non-healing wound, ulcer or bone fracture
• Unresolved toxicity higher than Grade 1, NCI-CTCAE v 5.0, attributed to any prior therapy/procedure excluding alopecia, anemia, hypothyroidism and oxaliplatin induced neuropathy
• Any psychological, familial, sociological or geographical condition potentially hampering compliance with the study protocol and follow-up schedule
• Adults legally protected (judicial protection, guardianship or supervision), person deprived of their liberty

Contacts and Locations

Contacts

Contact: Astrid Lievre; 2 99 28 43 47 ext +33; astrid.lievre@chu-rennes.fr

Locations

France

CHU Brest; Not yet recruiting

Brest, France

Contact: Jean-Philippe Metges jean-philippe.metges@chu-brest.fr

Contact Jean-Philippe

Principal Investigator: Jean-Philippe Metges, Pr

CHU Caen; Recruiting

Caen, France

Contact: Karine BOUHIER-LEPORRIER bouhierleporrier-k@chu-caen.fr

Principal Investigator: Karine BOUHIER-LEPORRIER

AP-HP Henri Mondor; Recruiting

Créteil, France

Contact: Christophe Tournigand christophe.tournigand@aphp.fr

Principal Investigator: Christophe Tournigand

Institut Daniel Hollard, Groupe Hospitalier Mutualiste de Grenoble; Recruiting

Grenoble, France

Contact: Camille Herve, Md

Principal Investigator: Camille Herve, Md

CHU Nantes; Recruiting

Nantes, France

Contact: Yann Touchefeu yann.touchefeu@chu-nantes.fr

Principal Investigator: Yann Touchefeu

AP-HP La Pitié-Salpétrière; Not yet recruiting

Paris, France

Contact: Jean-Baptiste Bachet

Contact jean-baptiste.bachet@aphp.fr

Principal Investigator: Jean-Baptiste Bachet

AP-HP St Antoine; Recruiting

Paris, France

Contact: Romain Cohen

Principal Investigator: Romain Cohen

CHU Poitiers; Recruiting

Poitiers, France

Contact: David Tougeron david.tougeron@chu-poitiers.fr

Principal Investigator: David Tougeron

Centre Eugène Marquis; Recruiting

Rennes, France

Contact: Samuel Le Sourd s.lesourd@rennes.unicancer.fr

Principal Investigator: Samuel Le Sourd, Md

CHU Rennes; Recruiting

Rennes, France

Contact: Camille Tron, PharmD camille.tron@chu-rennes.fr

Principal Investigator: Astrid Lievre, Pr

CHU Rouen; Recruiting

Rouen, France

Contact: Frédéric Di Fiore frederic.difiore@chu-rouen.fr

Principal Investigator: Frédéric Di Fiore

CHU Tours; Recruiting

Tours, France

Contact: Thierry LECOMTE thierry.lecomte@univ-tours.fr

Principal Investigator: Thierry LECOMTE

Sponsors and Collaborators

Rennes University Hospital

More Information

• Responsible Party: Rennes University Hospital
• ClinicalTrials.gov Identifier: NCT04874207
• Other Study ID Numbers: 35RC20_9803_RePERSO
• First Posted: May 5, 2021
• Last Update Posted: January 31, 2024
• Last Verified: January 2024

Individual Participant Data (IPD) Sharing Statement:

• Plan to Share IPD: No

• Studies a U.S. FDA-regulated Drug Product: No
• Studies a U.S. FDA-regulated Device Product: No

Additional relevant MeSH terms:

Colorectal Neoplasms; Intestinal Neoplasms; Gastrointestinal Neoplasms; Digestive System Neoplasms; Neoplasms by Site; Neoplasms; Digestive System Diseases; Gastrointestinal Diseases; Colonic Diseases; Intestinal Diseases; Rectal Diseases