Spinal Cord Compression Due to Metastasis to Spine Clinical Trial
Official title:
High-precision Radiotherapy of Motor Deficits Due to Metastatic Spinal Cord Compression
The major goal of this clinical study is to investigate to which extent high-precision radiotherapy (RT) with modern techniques can prevent progression or recurrence of motor deficits (weakness) of the legs following RT. In addition, it will be evaluated to which extent RT can lead to improvement of motor function, ambulatory status, sensory function and sphincter dysfunction, to pain relief and to improvement in quality of life, side effects and overall survival. For this purpose 44 patients who will receive modern high-precision RT treatment for the metastases on their vertebral bodies will be included into this phase 2 study. The results of the high-precision RT with a treatment of 5x5 Gray (Gy) in 1 week will be compared to data of a historical control group. The data set of the historical control group consists of more than 500 patients who received conventional RT with 5x4 Gy. The data collected in 1 week treatment will be compared. It is intended to show superiority regarding the local progression-free survival (LPFS) for the high-precision RT when compared with the conventional RT.
This is a multinational, multicenter study (single arm) supplemented by a comparison to a
historical, propensity score matched control group (superiority study).
A total of 44 patients (40 patients + 10% for potential drop-outs) who will receive modern
high-precision radiotherapy (RT) treatment for the metastases on their vertebral bodies are
planned to take part in the clinical study. The historical control group treated with 5x4 Gy
of conventional RT between 2001 and 2016 consists of more than 500 patients The primary aim
of this study is to investigate the local progression-free survival (LPFS) of metastatic
spinal cord compression (MSCC) after 5x5 Gray (Gy) of high-precision RT and to demonstrate
that this regimen results in significantly better 6-month LPFS than conventional RT with 5x4
Gy. For the high-precision RT volumetric modulated arc therapy (VMAT), stereotactic body
radiotherapy (SBRT) is allowed for treatment of patients with involvement of only one
vertebra, if the required constraints can be met. LPFS is defined as freedom from progression
of motor deficits during RT and freedom from an in-field recurrence of MSCC (i.e. freedom
from motor deficits due to a recurrence of MSCC in the previously irradiated parts of the
spine) following RT. The LPFS rate will be assessed 6 months after the end of RT.
In patients treated with RT alone for MSCC, conventional RT with 10x3 Gy in 2 weeks results
in similar motor function but significantly better LPFS than conventional RT with 5x4 Gy in 1
week. Since patients with MSCC are often significantly impaired, a RT regimen with an overall
treatment time of only 1 week would be preferable if it resulted in similar LPFS as 10x3 Gy
in 2 weeks. This may be achieved with 5x5 Gy in 1 week, since the equivalent dose in 2 Gy
fractions (EQD2) with respect to tumor cell kill of 5x5 Gy and 10x3 Gy are similar. The
tolerance dose of the spinal cord, 5x5 Gy can be safely administered with high-precision RT
such as VMAT (or SBRT). Therefore, the present study investigates the LPFS after
high-precision RT with 5x5 Gy in 1 week. To demonstrate superiority the patients of this
study will be compared to a historical control group receiving conventional RT with 5x4 Gy in
1 week. If superiority regarding LPFS can be shown for high-precision RT with 5x5 Gy,
patients with MSCC would benefit from this regimen, since they can achieve high LPFS rates
with an RT regimen lasting only 1 week (5x5 Gy) instead of 2 weeks (10x3 Gy). This study aims
to make a significant contribution to the most appropriate RT schedule for patients with
MSCC.
In accordance with a previous study assessing local control of MSCC, the following patient
characteristics will be recorded to allow adequate comparison with the historical,
propensity-score matched control group:
- Age (2 groups, depending on median age)
- Gender
- Type of primary tumor (breast cancer vs. prostate cancer vs. myeloma/lymphoma vs. lung
cancer vs. other tumors)
- Interval from tumor diagnosis to MSCC (≤15 months vs. >15 months)
- Number of involved vertebrae (1-2 vs. ≥3)
- Other bone metastases at the time of RT (no vs. yes)
- Visceral metastases at the time of RT (no vs. yes)
- Time developing motor deficits prior to RT (1-7 days vs. 8-14 days vs. >14 days)
- Ambulatory status prior to RT (no vs. yes)
- Eastern Cooperative Oncology Group (ECOG) performance score (1-2 vs. 3-4) Study arm: 5x5
Gy of high-precision RT in 1 week Historical control: 5x4 Gy of conventional RT in 1
week Follow-up directly and at 1, 3 and 6 months following RT RT is administered as
high-precision RT with 25.0 Gy in 1 week, i.e. with 5.0 Gy per fraction on 5 days per
week (representing an EQD2 of 43.8 Gy for radiation myelopathy). An EQD2 of 45 Gy is
estimated to be associated with a risk of radiation-related myelopathy of 0.03% and is
therefore considered safe. The clinical target volume (CTV) includes the vertebral and
soft tissue tumor as seen on the planning computed tomography and diagnostic MR-imaging,
the spinal canal, the width of the involved vertebrae, and half a vertebra above and
below those vertebrae involved by MSCC. The planning target volume (PTV) should include
the CTV plus 0.8 cm and should be covered by the 95%-isodose. The maximum relative dose
allowed to the spinal cord is 101.5% of the prescribed dose (representing an EQD2 of
44.9 Gy for radiation myelopathy). This maximum dose is estimated to be associated with
a risk of radiation-related of <0.03% and is, therefore, also considered safe. Both the
EQD2 of the prescribed dose (41.7 Gy) and the EQD2 of the maximum dose (43.8 Gy) are
well below the tolerance dose of bone. In accordance with the Quantitative Analyses of
Normal Tissue Effects in the Clinic (QUANTEC) data, the mean doses EQD2 for esophagus,
heart and lung must be <34 Gy, <26 Gy and ≤7 Gy, respectively. Taking into account a
radiation regimen of five fractions, the corresponding mean doses per fraction are 4.5
Gy, 3.8 Gy and 1.54 Gy, respectively. MSCC may affect single or multiple spinal sites.
All sites need to be treated with high-precision RT following the dose prescriptions and
constraints given above.
It is recommended that the patients receive concomitant treatment with dexamethasone during
the period of radiotherapy if indicated.
Quality assurance plan:
Monitoring: The Centre for Clinical Trials Lübeck will conduct clinical on-site monitoring at
the German sites according to Good Clinical Practice and written standard operating
procedures (SOPs) to ensure the patients' rights and safety as well as the reliability of
trial results.
The frequency of monitoring visits per site will be defined depending on the recruitment rate
and the quality of data.
Patient Registration:
The patients were assigned 2 code numbers, the number of the contributing center plus a
patient identification number starting with 001 and chronologically ongoing.
Coordination and supervision of the inclusion of the patients will be performed by the
Department of Radiation Oncology of the University of Lübeck, Germany.
Sample size calculation:
The primary goal of this study is to assess high-precision RT with 5x5 Gy in 1 week with
respect to 6-month LPFS and to demonstrate that this rate is superior to conventional RT with
5x4 Gy with respect to LPFS of MSCC (hypothesis).
With respect to tumor cell kill, the EQD2 of 5x5 Gy is similar to the EQD2 of 10x3 Gy (31.3
Gy vs. 32.5 Gy) and higher than the EQD2 of 5x4 Gy (23.3 Gy) . In a previous prospective
non-randomized study, the 6-month LPFS rates were 86% after longer-course RT and 67% after
short-course RT, respectively (p=0.034). In that study, 95 of 117 patients (81%) in the
longer-course RT group had received 10x3 Gy, and 91 of 114 patients (80%) in the short-course
RT group had received 5x4 Gy. Thus, assuming - for the present study - that conventional RT
with 5x4 Gy in fact results in a 6-month LPFS rate of 67%, an increase by roughly 20
percentage point is considered to be clinically minimal relevant and even appears to be
realistic when applying high-precision RT with 5x5 Gy.
The sample size is chosen to obtain prospective data that can be interpreted on its own and
to allow for comparison with historical data:
- A sample size of at least 40 eligible patients is needed to estimate the probability of
LPFS at 6 month with adequate precision, based on the following assumptions:
- 6-month LPFS can be assumed to be 87%
- 6-month LPFS is to be estimated with a precision of plus/minus 20 percentage points
expressed as the half length of the associated two-sided confidence interval with a
confidence coefficient of 95%.
- The power -i.e. the probability to obtain this precision, should be at least 80%
- Confidence limits are used as the approach for sample size. Assuming that roughly
10% of enrolled patients will not be eligible for efficacy analysis due to early
lost-to-follow-up or due to premature discontinuation of high-precision RT, a total
of 44 patients should be enrolled in the prospective part of the trial.
- The aim of the confirmatory study is to compare the prospectively collected data with a
historical, propensity-score matched cohort collected up to the time of data analysis.
Assuming for simplicity and conservative power calculation that this comparison could be
conducted with a simple Pearson-Chi-Square test using a two-sided significance level of
5% (10%), a power of 79% (86%) is reached, if 40 patients are treated with
high-precision RT and roughly 400 patients of the historical control group qualify for
Propensity-Score adjusted comparison and assuming that the expected 6-month LPFS are 87%
and 67%, respectively. Taking into account that the more sophisticated propensity-score
adjusted statistical analysis will increase statistical power, the power for treatment
arm comparison reached with 40 eligible patients in the prospective part of the study
can be assumed to be at least 80%.
Primary endpoint:
The primary endpoint (LPFS of MSCC) will be evaluated based on the sample size calculations.
The evaluation will be performed in those patients, who are available for assessment of the
primary endpoint and have received at least 80% of the planned RT dose. Due to the open
nature of the study, a blind data review is not necessary. The safety population includes all
patients who have received at least 1 fraction of high-precision RT.
LPFS is defined as freedom from progression of motor deficits during RT and freedom from an
in-field recurrence of MSCC (i.e. freedom from motor deficits due to a recurrence of MSCC in
the previously irradiated parts of the spine) following RT. Deterioration of motor deficits
during RT will be counted as LPFS of 0 months. Freedom from an in-field recurrence following
RT will be referenced from the last day of RT. LPFS rates will be calculated for each
potential prognostic factor using the Kaplan-Meier method. Differences between the
Kaplan-Meier curves will be calculated with the log-rank test (univariate analysis). Factors
that achieve significance (p<0.05) or show a trend (p<0.06) on univariate analysis will be
additionally included in a multivariate analysis (Cox proportional hazards model).
Secondary endpoints:
The comparison of the high-precision RT group and the conventional RT group with respect to
their effect on motor function and sensory function (improvement, no further progression,
deterioration) will be evaluated with the ordered logit model adjusted for propensity score,
because the data for the impact of RT on motor and sensory function are ordinal (-1 =
deterioration, 0 = no further progression, 1 = improvement). An improvement or deterioration
of the motor function will be defined as a change of at least 1 point on a 5-point scale.
Post-RT ambulatory and sphincter dysfunction rates will be compared between both groups with
the Chi-square test stratified for propensity score. Effect of RT on motor function, post-RT
ambulatory rates, sensory function and sphincter dysfunction will be evaluated directly after
RT and at 1, 3 and 6 months following RT in those patients who are alive and available for
assessment. P-values of <0.05 are considered significant.
Overall survival (OS) will be counted from the last day of RT. OS rates will be calculated
with the Kaplan-Meier-method. Differences between Kaplan-Meier curves will be analyzed with
the log-rank test. Again, p-values of <0.05 are considered significant. Factors that achieve
significance or show a trend (p<0.06) on univariate analysis will be included in a
multivariate analysis (Cox proportional hazards model). The analysis of OS will be conducted
in the intent-to-treat population.
Data regarding pain, quality of life and toxicity will only be assessed in the study group.
;
Status | Clinical Trial | Phase | |
---|---|---|---|
Recruiting |
NCT04043156 -
RAdiotherapy for Metastatic Spinal Cord Compression With Increased Radiation dosES
|
N/A |