Chemoradiation and Consolidation Chemotherapy With or Without Oxaliplatin for Distal Rectal Cancer and Watch and Wait
216 patients around the world
Available in Brazil, Uruguay
Patients and Methods
Patients with distal rectal cancer will be eligible for the study after initial clinical,
endoscopic and radiological assessment. At this point, patients will be offered to
participate in the study and after informed consent, randomized to control or experimental
arms as follows.
Endpoints
Primary endpoint: Decision to Watch and Wait due to clinical complete response achieved at 18
weeks from last date of radiation using clinical (DRE), endoscopic and radiological criteria
(mrTRG grade) or near-complete clinical response (no progressive disease clinically,
endoscopically or radiologically)
Definition of clinical complete response (cCR) available below and at the discretion of the
attending surgeon.
Definition of radiological complete response as described below (centralized).
Patients will be counted as event if at 18 weeks the decision is to interrupt Watch and Wait
and proceed to surgery (any kind) because of overt incomplete clinical response. In order to
standardize assessment of response and reduce inter-observer variability, the decision to
continue on Watch and Wait (or not) will be at the discretion of the central committee during
central revision of studies.
Secondary endpoints:
- Surgery-free survival at 3 years
- TME-free survival at 3 years
- Distant metastases free survival at 3 years
- Local regrowth-free survival at 3 years
- Colostomy-free survival at 3 years
Definitions
Definition of cCR:
- Endoscopic: white scar, teleangiectasia, absence of ulceration and/or mass 6
- Clinical: no irregularity, firm area with minor induration6
- Radiological: mrTRG1: fibrosis with low signal intensity seen on T2 weighted images
replacing the primary tumor; no restricted diffusion on diffusion weighted images; no
nodes with border irregularity or mixed signal intensity; no extramural vascular
invasion23-26
Definition of near-complete response:
- Endoscopic: residual tumor size ≤2cm (or reduction of ≥70% original tumor volume/size)
4,27,28
- Clinical: only superficial ulceration or minor (questionable) irregularities of the
mucosal/rectal wall
- Radiological: mrTRG2 predominant fibrosis with low signal with foci of intermediate
tumor signal intensity seen on T2 weighted images with or without restricted diffusion;
mrTRG1: fibrosis with low signal intensity seen on T2 weighted images replacing the
primary tumor with restricted diffusion; no nodes with border irregularity or mixed
signal intensity; no extramural vascular invasion 27
Central Committee
The central committee is multidisciplinary group of surgeons, medical oncologists and
radiologists previously appointed at the beginning of the recruitment of patients and with
previous experience with organ preservation.2, 21 This group of specialist will be
responsible to assess the baseline staging and define if the patients fulfill all the
inclusion/exclusion criteria prior to randomization. The committee will also be responsible
to evaluate the endoscopic and radiological tumor re-assessment studies at 12 and 18 weeks
from radiation completion. The definition to continue on the Watch and Wait pathway or not
will be at the discretion of this committee.
Technical aspects of assessment tests:
Suggested MR protocol:
1.5T - FRFSE; TR/TE: 3300/120 (ms); slice thickness/gap: 3.0/0; Matrix: 256 x 256; NSA 8)
3.0T - FRFSE; TR/TE: 8000/150 (ms); slice thickness/gap: 3.0/0; Matrix: 288 x 288; NSA 5) DWI
- inclusion of a high b-value of at least 800
Suggested Endoscopic assessment:
Endoscopic assessment using a flexible scope (gastroscope preferred for retroflexion); direct
endoscopic and retroflexion view of the primary tumor/scar; endoscopic biopsies at discretion
of participating center.
Radiotherapy
Preoperative radiotherapy will be delivered on a linear accelerator in prone or supine
position, preferably with full bladder. The use of a belly board is allowed. Isocentric 3 or
4 fields, as well as an IMRT technique is allowed, as long as all beams are treated on a
daily basis. The dose distribution and calculation should be performed on CT or MRI and
specified according to the ICRU 50 guidelines.
Dose specification: All patients will receive 25 daily fractions of 1.8 Gy up to a total dose
of 45 Gy to the pelvic field including the tumor bed with a margin and the regional lymph
nodes. A field reduction after 45 Gy is recommended up to 54 Gy. The last 5 fractions will
then be given to the tumor bed with a margin.
Target volume:
Pelvic CTV
- The primary tumor
- Mesorectum: Distally, only lymph nodes or tumor deposits up to 4 cm are included. For
tumors in lower rectum this means that the entire mesorectum down to the pelvic floor is
included.
- Presacral nodes and nodes along the rectal superior artery: Since local recurrences are
very unusual above S1 - S2, lymph nodes above this level should not be included unless
there are signs of radiologically positive lymph nodes presacrally. If this is the case,
the cranial limit of CTV should be at least 1 cm above the most cranial radiologically
positive lymph node.
- Lateral lymph node stations: Until they reach the level of the obturator canal Internal
iliac artery up to the bifurcation from the external iliac artery. The cranial border
for the CTV is in most cases just below the bifurcation of the internal and external
iliac arteries. In most patients this is at the level of S1 - S2.
- Ischio-rectal fossa and the anal canal: Included in pelvic CTV only if the tumor grows
into the levators or down into the anal canal.
- Lymph nodes along the external iliac artery: Included if the tumor grows into anterior
organs like the prostate, urinary bladder, cervix, vagina or uterus to such an extent
that the external nodes are at risk for metastases.
Boost GTV:
GTV is the visible primary tumor and radiologically positive lymph nodes.
CTV boost:
GTV boost plus a margin of 2 cm within the same anatomical compartment as the tumour is in,
for the dose of 45 Gy, also around radiologically engaged lymph nodes.
PTV:
The above description relates to the CTV. A PTV should normally be defined and includes CTV
and internal target volume (ITV) and a margin necessary for the setup. These margins are
depending upon several factors that are related to the equipment at each radiotherapy center.
Chemotherapy Protocols
Concomitant chemotherapy:
Concomitant capecitabine: 825mg/m2 bid on the radiotherapy days only
Consolidation chemotherapy:
1. Consolidation capecitabine (alone): 1000mg/m2 bid, for 14 days, in a 3 week cycle, for 4
cycles
2. Consolidation options with oxaliplatin:
2.1. mFOLFOX6: Oxaliplatin 85mg/m2 plus Leucovorin 400mg/m2 on a concomitant 2 hours
infusion. 5FU 400mg/m2 on a bolus infusion, followed by 5FU 2400mg/m2 in 46 hours infusion,
every 2 weeks, for 6 cycles 2.2. CAPOX: Oxaliplatin 130mg/m2 on a 2 hours infusion.
Capecitabine 1000mg/m2 bid daily, for 14 days, starting on the evening of the oxaliplatin
infusion. Repeat every 3 weeks, for 4 cycles
Assessment of Response
Assessment of response will be performed at 12 weeks (and 18 weeks from last date of
radiation therapy if cCR or near-complete response is detected at 12 weeks). All patients
will undergo endoscopic reassessment, DRE and high-resolution MR. Endoscopic biopsies will be
at the discretion of the attending surgeon/endoscopist.
Patients with complete or near-complete clinical response at 12 weeks will be recommended
reassessment at 18 weeks from RT. Patients with clinically overt incomplete clinical response
at 12 or 18 weeks will be referred to immediate radical surgery.
Randomization
Individuals will be randomized and allocated at a 1:1 ratio to the two groups (control and
experimental) using a permuted block design with a random block size of 4, 6, and 8. (1-3) A
randomization list will be generated electronically using appropriate software immediately
after being considered eligible.
Protocol Blinding
Patients and attending physicians will not be blinded to the treatment arm randomized for
each patient. However, as a strategy to reduce investigator's expectations and reduce
inherent bias, the central committee will be blinded to the treatment arm. It is expected
that blinding the central committee, who will be responsible for assessing the primary
endpoint, any bias related to the investigator's expectation about the treatment arm and the
chances of Watch and Wait will be nulled.
Sample size calculation
The primary endpoint (decision to WW due to cCR/near CR) was observed in 55% and 85% at 12
weeks (in contrast to the 18 weeks used in the present trial) among patients with early cT3
and cT2 rectal cancer respectively.29 In this study, there was a distribution of 66% of cT3
and 33% cT2. Therefore, response rates appear to be highly dependent on exact T-stage
distribution. Considering the expected inclusion of more advanced disease (late mrT3 or even
mrT4 rectal cancers) the investigators expect 40% cCR/near-CR in the control arm. A similar
difference 60% versus 40% was achieved in the preliminary report of the outcomes of the OPRA
trial. This difference in TME-free survival at 3 years was statistically significant favoring
patients undergoing nCRT with cCT in comparison to nCRT preceded by induction chemotherapy
(both regimens incorporating oxaliplatin). In this setting, if experimental results in ≥60%
cCR/near-CR, the study will be considered POSITIVE. The incorporation of oxaliplatin to a
consolidation CRT regimen that results in ≥20% increase in cCR/near-CR exceeds the potential
disadvantages of treatment-related toxicity.
The investigators will assume that the primary outcome will occur in 40% of individuals in
control group and 60% in the experimental group, which corresponds to an absolute difference
in proportions of 20%. It is estimated that a sample of 194 (97 per group) provides 80%
statistical power to detect this difference at a significance level of 5% using the
Chi-square test and assuming a two-sided significance hypothesis and considering a 1:1
allocation. The estimated dropout rate is 10% in each group, so it is expected to include 216
individuals (108 per group). The sample size calculation was performed using SAS 9.4 (PROC
POWER procedure).
Time-table
Patient accrual: 2 years and 6 months Patient/institution/year: 5-6 (20 institutions:
100-120/year - 2 years n=200-240)
Interim analysis:
If the arm of two drugs during consolidation shows ≥25% response rate after 72 patients,
study will be interrupted (efficacy). If the arm of two drugs shows less than 5% response
rate after 72 patients, the study will be interrupted.