Colorectal Neoplasms Malignant Clinical Trial
Official title:
The Effect and Safety on Unresectable CRLM From RFA in Combination With Second-line Chemotherapy and Bevacizumab Compared With the Combination of Second-line Chemotherapy and Bevacizumab: a Randomized and Controlled Clinical Trial
Basing on the strong evidence from former researches, patients with CRLM can benefit from the treatment of bevacizumab combined with sencond-line chemotherapy. Recently, although with the popularization of RFA, the role that RFA plays in the long term survival of patients with metastatic colorectal cancer (CRC) is still confused. In this designed, randomized, controlled, prospective, and open clinical trial, the effectiveness of RFA combined with second-line chemotherapy + bevacizumab on unresectable CRLM is going to be evaluated compared with that of second-line chemotherapy + bevacizumab. After screened by inclusion and exclusion criteria, the eligible subjects will be randomly allocated into the experimental group-with the treatment of RFA + second-line chemotherapy + bevacizumab and control group-with the treatment of second-line chemotherapy + bevacizumab equally.
As a leading cause of death around the world, the mobility and mortality of CRC also increase
in china with aging. Currently, distant organ metastasis, most commonly appearing in liver,
diminishes the life expectancy in more than 50% of CRC patients. Surgical resection of the
tumor primaries and metastases has been the first choice of patients with CRLM with five-year
survival rate of 44.2%. With only 25% resectable CRLM, however, most patients lose the
operation chance at diagnosis.
In the past two decades, RFA in CRLM treatment has been gradually approved and showed great
value in clinic. According to some retrospective researches, for small metastases, the
effectiveness of RFA is not inferior to surgery. However, what really makes sense is to
ensure if patients with unresectable metastases could benefit from RFA. The results from some
former researches and CLOCC study in 2017 noticeably reflected that RFA enabled to prolong
the survival significantly in unresectable CRLM patients, which determined its essential role
in clinical application.
As a humanized monoclonal antibody against vascular endothelial growth factor (VEGF),
bevacizumab shows great potential in tumor therapy: pruning the tumor vessels rapidly by
blocking VEGF signaling pathway; straightening and normalizing tumor vessels which ensure the
effective perfusion of chemotherapeutics. In addition, depending on durable angiogenesis
inhibition, bevacizumab restrains tumor growth and metastasis. To date, bevacizumab combined
with chemotherapy is approved in metastatic CRC treatment.
For long term survival, patients with CRLM can benefit from bevacizumab combined with
sencond-line chemotherapy basing on the strong evidence from above researches. While the role
that RFA plays in this therapeutic regimen is still confused. In this designed clinical
trial, the main purpose is to evaluate the effectiveness of RFA combined with second-line
chemotherapy + bevacizumab on CRLM patients plans, which is expected to polish up the
clinical treatment approaches.
This study is a randomized, controlled, prospective, open, and two-center clinical experiment
for patients with metastatic CRC. After screened by inclusion and exclusion criteria, the
eligible subjects will be randomly allocated into the experimental group and control group
equally. Liver biopsy or specimens of liver metastases are required in all eligible patients
for the second pathologic diagnosis by pathology department in Nanfang hospital, Southern
Medical University.
Supported by Logrank test in PASS II software, this study will compare the survival
differences between experimental and control group. In CLOCC study, the ratio between hazard
ratio (HR) of chemotherapy bevacizumab combined with RFA and that of chemotherapy bevacizumab
was 0.58. Considering that the subjects in this study are after second-line therapy and
extrahepatic metastases are allowed, so the HR will supposedly achieve 0.62. In addition,
with the four stratified blocks and 5% expulsion rate in both experimental and control
groups, 80 subjects in each group (total 160 subjects) are needed to detect the difference
with 80% confidence at the a=0.05 (bilateral) significant level.
In control group, subjects are treated with bevacizumab + second-line chemotherapy, while
treated with RFA + bevacizumab + second-line chemotherapy in experimental group. The detailed
descriptions of these interventions are as follow. Bevacizumab is given to patients in all
arms every 2 weeks (5mg/kg) or 3 weeks (7.5mg/kg), intravenous drip(VD). The second-line
chemotherapies depending on the judgement of researchers and the wills of subjects include
FOLFIRI [Irinotecan 180 mg/m2 D1+Calcium folinatc 400 mg/m2 or Calcium Levofolinate 200 mg/m2
D1+5-FU 400 mg/m2 D1, 2400 mg/m2 D1-2(46-48h), q2W] or irinotecan monotherapy (125 mg/m2 D1,
8, q3W or 180 mg/m2 D1, q2W) with the historical first-line treatment of oxaliplatin but not
irinotecan, mFOLFOX6 [Oxaliplatin 85 mg/m2 D1+Calcium folinatc 400 mg/m2 or Calcium
Levofolinate 200 mg/m2 D1+5-FU 400 mg/m2 D1, 2400 mg/m2 D1-2(46-48h), q2W] or CapeOX
(Oxaliplatin 130 mg/m2 D1+Capecitabine 1000 mg/m2 Bid D1-14, q3W) with the historical
first-line treatment of irinotecan but not oxaliplatin, and mFOLFOX6, CapeOX, FOLFIRI,
irinotecan monotherapy or irinotecan+oxaliplatin (Oxaliplatin 85 mg/m2 D1+Irinotecan 200
mg/m2 D1, q3W) with the historical first-line treatment of fluorouracil but not oxaliplatin
and irinotecan. Among these strategies, the treatment cycle of FOLFIRI, irinotecan
monotherapy and mFOLFOX6 is two weeks, while three weeks in CapeOX and irinotecan +
oxaliplatin. Navigated by CT-ultrasound merged images, RFA is taken in the experimental arm
at the first day of the first cycle during the second-line therapy. The initial power is 30w
and increases 20w per minute until 90w is reached. Then the operation will last for 15
minutes or until the power fall to 0w. If any severe unfit or abnormal vital signs occur in
subjects during the process and cannot be improved by symptomatic treatment, RFA should be
stopped immediately. After ensuring that the ablation area assessed by the hyperechoic area
in ultrasound has reached the intended target, the operation finishes successfully and
postoperative observation (including pulse, breath, and blood pressure etc.) is needed in all
experimental patients. To make the residual volumes of metastases as small as possible,
repeated RFA can be operated within 1 week after initial RFA treatment if the criteria of
normal coagulation function, platelets (PLT) 80/L and neutrophils 1.5/L, and RFA related
adverse events grade 1 are satisfied, but at most 3 times.
Tumor burden will be evaluated by imaging according to RECIST 1.1. For the assessment of
baseline level and at the first day ( 3 days) of the second cycle, PET-CT is designated.
While the subsequent method-enhanced CT or MRI is determined by researchers. Thoracic,
abdominal and pelvic examinations are involved at each assessment. And the evaluation should
be taken every 2 months ( 7 days) until progression or deaths occur. Baseline assessment
refers to whole body PET-CT, and additional head CT/MRI or bone scanning are required if
suspected brain or osseous metastases exist.
The safety will be evaluated through the analysis of adverse events (AE), severe adverse
events (SAE) and laboratory abnormalities, especially the specific events-hemorrhage and
elevated transaminase. The observational parameters include the type, incidence, severity,
time, correlation, risk factors, measurements and outcomes. The severity of every AE will be
classified into 5 grades according to National Cancer Institute (NCI-CTCAE), v 4.03. Main
researcher will be responsible for the documentation of AE and SAE.
The study will conduct at 24-month baseline and 36-month follow-up, and the anticipated
duration is 5 years.
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