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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT04089631
Other study ID # TUD-CIRC01-071
Secondary ID 2018-003691-1201
Status Recruiting
Phase Phase 3
First received
Last updated
Start date June 26, 2020
Est. completion date June 2026

Study information

Verified date August 2020
Source Technische Universität Dresden
Contact Gunnar Folprecht, Prof.
Phone +49 351 458 4794
Email Gunnar.Folprecht@uniklinikum-dresden.de
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The CIRCULATE study evaluates the adjuvant therapy in patients with colon cancer UICC stage II. The primary aim of the study is to compare the disease free survival in patients who are positive for postoperative circulating tumour DNA with vs. without capecitabine.


Description:

CIRCULATE is an investigator-initiated, multicentre, prospective, randomised, controlled trial.

Screening phase:

Patients with colon cancer (or rectal cancer, if a radiation is not indicated i.e. due to the tumour localisation) are postoperatively screened for this trial.

For this purpose, they sign an informed consent for screening. The formalin fixed paraffin embedded (FFPE) tumour block is shipped to one of the central pathological laboratories and is analysed for microsatellite instability and by panel analysis for frequent mutations in the colorectal cancer. A plasma sample is sent in parallel to the central laboratory for ctDNA. The screening is preferably performed before the patient is discharged from the surgical department and at the latest 5 weeks after resection to allow sufficient time for the analysis.

The patient- specific tumour mutations known from the panel analysis are measure in the patients plasma by ultra deep sequencing. The results of the analysis - positive for circulating tumour DNA (ctDNApos) or negative for circulating tumour DNA (ctDNAneg) - is not communicated to the patient or the investigator.

Randomised phase:

Four to eight weeks after resection, the patient presents at an investigator that is experienced with chemotherapy (i.e. Medical Oncologist) and consent for the randomised part of the study with a second informed consent form. If this baseline visit confirms that there are not contraindications to chemotherapy and if no other exclusion criteria exist, the patient is randomised:

- ctDNApos patients are randomised (2:1) in "chemotherapy" (with capecitabine) or "follow-up",

- ctDNAneg patients are randomised (1:4) in "follow-up" or "off study" which means that the follow-up will be organised within the routine clinical practice.

The result of the ctDNA will not be communicated to the patients and investigators, so that patients in the arm "follow-up" remain blinded to the ctDNA result. Due to the randomisation ratio, the prognosis of these patients is similar to those in stage II without any ctDNA analysis and differs only slightly from patients not enrolled into a clinical trial.

Patients in the arm "chemotherapy" receive adjuvant therapy with 6 months capecitabine. The investigator can decide to add oxaliplatin and to shorten the adjuvant chemotherapy to 3 months if oxaliplatin is added.

Patients in the arms "chemotherapy" and "follow-up" are followed with the same methods and time point within the study.

Patients in the arm "off study" are recommended to be follow up according to the guidelines for stage II in the routine practice.


Recruitment information / eligibility

Status Recruiting
Enrollment 4812
Est. completion date June 2026
Est. primary completion date June 2023
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion criteria for screening phase:

1. Resected colon cancer stage II, OR Resected rectal cancer stage II, if there was no indication for radiotherapy (i.e. due to the localisation in the upper third of the rectum ), so that the treatment follows the recommendations for colon cancer. Patients, in whom the tumour stage is not yet know, can be enrolled into the screening.

2. Signed informed consent for the screening Phase

Inclusion criteria for the randomised phase:

1. Resected colon cancer stage II, OR resected rectal cancer stage II, if there was no indication for radiotherapy (i.e. due to the localisation in the upper third of the rectum), so that the treatment follows the recommendations for colon cancer.

2. Known microsatellite or mismatch repair status

3. Confirmation, that the ctDNA result is available

4. Signed second informed consent (for the randomised phase)

Exclusion criteria for Screening:

1. Patients with known microsatellite instability (MSI-H) or mismatch repair deficiency (dMMR)

2. Known clinical high risk situation if it is regarded as certain indication for an adjuvant chemotherapy

3. Patients, who have an obvious contra-indication for adjuvant chemotherapy (i.e. due to the performance status, comorbidity, active second cancer or age). It should be considered that patients with an age of more than 75 years frequently not fulfil criteria for adjuvant chemotherapy.

4. R1- or R2-status (patients with [still] unknown R-status can be screened)

5. Patients, in whom the randomisation or chemotherapy is unfeasible due to logistic reasons (travel distance, compliance)

6. Age < 18 years

7. Pregnant or breast feeding patients

Exclusion criteria for randomised phase:

1. Patients with microsatellite instability (MSI-H) or mismatch repair deficiency (dMMR)

2. Known clinical high risk situation if it is regarded as certain indication for an adjuvant chemotherapy

3. R1- or R2- status, or unknown R- status (Rx)

4. Number of investigated lymph nodes < 10

5. WHO performance status = 2

6. Colon or rectal cancer with UICC stage III or IV

7. Second cancer, except

1. simultaneous or metachronous colon or rectal cancer with UICC stage = I,

2. curatively treated basal cell carcinoma or squamous cell carcinoma of the skin and in-situ cervical carcinoma

3. tumours with a disease free survival of more than five years

8. Contra indications for chemotherapy, especially:

1. Leukocytes < 3,0 Gpt/l

2. Neutrophil granulocytes < 1,5 Gpt/l

3. Thrombocytes < 100 Gpt/l

4. alanine aminotransferase (ALAT) or (aspartate aminotransferase) ASAT > 3x ULN

5. Creatinine clearance (calculated according Cockcroft-Gault) < 30 ml/min

9. Comorbidities relevantly interfering with the prognosis of the patients, i.e.:

1. heart insufficiency NYHA III/IV

2. relevant coronary heart disease,

3. Diabetes mellitus with late sequelae

10. Organ, stem cell or bone marrow transplantation

11. Known hypersensitivity to capecitabine In case of known hypersensitivity to oxaliplatin, the patients can participate, but not receive oxaliplatin

12. Medication with brivudine, sorivudine or analogues in the last four weeks before planned treatment start

13. Known dihydropyrimidine dehydrogenase (DPD)-deficiency

14. Acute infections

15. Known HIV- infections, known active hepatitis B or C-infection

16. Participation at another interventional study for medical treatment during the last four weeks before randomisation

17. Neoadjuvant therapy before resection

18. Patients, in whom the randomisation or chemotherapy is unfeasible due to logistic reasons (travel distance, compliance)

19. Age < 18 years

20. Pregnant or breast feeding patients

21. Women of childbearing potential and men with partner with childbearing potential who are not willing to take appropriate precautions to avoid pregnancy with a highly effective method in case they are randomised to "chemotherapy"

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Capecitabine
6 months capecitabine, in combination with oxaliplatin 3 to 6 months capecitabine

Locations

Country Name City State
Germany Universitaetsklinikum Carl Gustav Carus, Medizinische Klinik Dresden Sachsen

Sponsors (1)

Lead Sponsor Collaborator
Technische Universität Dresden

Country where clinical trial is conducted

Germany, 

Outcome

Type Measure Description Time frame Safety issue
Primary Disease free Survival (DFS) Disease free survival of ctDNA positive patients randomised to "chemotherapy" vs. "follow-up", measured from randomisation to any recurrence, metastasis, second colorectal or non colorectal cancer and death from any cause. The primary endpoint will be tested in all randomised ctDNA positive patients and be evaluated by a stratified log rank test.
Interims analysis after 93 events (approx. 38 months after study start), final analysis for the primary endpoint after 154 events (approx. 60 months after study start).
for the primary endpoint after 154 events (approx. 60 months after study start)
Secondary Overall survival in ctDNApos patients with adjuvant therapy vs follow-up Overall survival in ctDNApos patients with adjuvant therapy vs follow-up, measured from randomisation to death from any cause, in all randomised ctDNA positive patients and be evaluated by a stratified log rank test. 5 years
Secondary Disease free survival in ctDNAneg patients randomised to follow up Disease free survival in ctDNAneg patients randomised to follow up (rate of patients disease free and alive 3 years after randomisation according to Kaplan-Meier estimation with 95% CI, intention-to-treat analysis). Any recurrence, metastasis, second colorectal or non-colorectal cancer and death from any cause is regarded as event (rate of patients disease free and alive 3 years after randomisation according to Kaplan-Meier estimation with 95% CI, intention-to-treat analysis). Any recurrence, metastasis, second colorectal or non- colorectal cancer and death from any cause is regarded as event 3 years
Secondary Overall survival in ctDNAneg patients randomised to "follow up" Overall survival in ctDNAneg patients randomised to "follow up" (rate of patients alive after 5 years after randomisation according to Kaplan-Meier estimation with 95% CI) 5 years
Secondary Disease free and overall survival of ctDNApos vs. ctDNAneg patients randomized to "follow-up" Disease free and overall survival of ctDNApos vs. ctDNAneg patients randomized to "follow-up" (measured from randomisation to the event in an intention-to-treat analysis by stratified log rank test). Any recurrence, metastasis, second colorectal or non-colorectal cancer and death from any cause are regarded as event for DFS. Death of any cause will be regarded as event for overall survival. 3 years and 5 years
Secondary Site of metastases Site of metastases (lymph node vs. peritoneal/local recurrence vs other) in ctDNApos vs. ctDNAneg patients who have a recurrence / metastases 5 years
Secondary Frequency of adverse events from start of chemotherapy until 30 days after chemotherapy Frequency of adverse events from start of chemotherapy until 30 days after chemotherapy (descriptive analysis for patients randomised to "chemotherapy" who have received at least one dose of chemotherapy). 5 years
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