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Int. J. Radiation Oncology Biol. Phys., Vol. 79, No. 4, pp. 1151–1157, 2011Copyright � 2011 Elsevier Inc.
Printed in the USA. All rights reserved0360-3016/$–see front matter
jrobp.2009.12.038
doi:10.1016/j.iCLINICAL INVESTIGATION Metastasis
PREDICTORS OF LOCAL CONTROL AFTER SINGLE-DOSE STEREOTACTICIMAGE-GUIDED INTENSITY-MODULATED RADIOTHERAPY FOR
EXTRACRANIAL METASTASES
CARLO GRECO, M.D.,* MICHAEL J. ZELEFSKY, M.D.,* MICHAEL LOVELOCK, PH.D.,y ZVI FUKS, M.D.,*
MARGIE HUNT, M.S.,y KENNETH ROSENZWEIG, M.D.,* JOAN ZATCKY, B.S., N.P.,* BALEM KIM, B.A.,*
AND YOSHIYA YAMADA, M.D.*
Departments of *Radiation Oncology and yMedical Physics, Memorial Sloan-Kettering Cancer Center, New York, NY
ReprinRadiation1275 Yor639-6802
Purpose: To report tumor local control after treatment with single-dose image-guided intensity-modulated radio-therapy (SD-IGRT) to extracranial metastatic sites.Methods and Materials: A total of 126 metastases in 103 patients were treated with SD-IGRT to prescription dosesof 18–24 Gy (median, 24 Gy) between 2004 and 2007.Results: The overall actuarial local relapse–free survival (LRFS) rate was 64% at a median follow-up of 18 months(range, 2–45 months). The median time to failure was 9.6 months (range, 1–23 months). On univariate analysis,LRFS was significantly correlated with prescription dose (p = 0.029). Stratification by dose into high (23 to 24Gy), intermediate (21 to 22 Gy), and low (18 to 20 Gy) dose levels revealed highly significant differences inLRFS between high (82%) and low doses (25%) (p < 0.0001). Overall, histology had no significant effect onLRFS (p = 0.16). Renal cell histology displayed a profound dose–response effect, with 80% LRFS at the highdose level (23 to 24 Gy) vs. 37% with low doses (#22 Gy) (p = 0.04). However, for patients who received thehigh dose level, histology was not a statistically significant predictor of LRFS (p = 0.90). Target organ (bone vs.lymph node vs. soft tissues) (p = 0.5) and planning target volume size (p = 0.55) were not found to be associatedwith long-term LRFS probability. Multivariate Cox regression analysis confirmed prescription dose to be a signif-icant predictor of LRFS (p = 0.003).Conclusion: High-dose SD-IGRT is a noninvasive procedure resulting in high probability of local tumor control.Single-dose IGRT may be effectively used to locally control metastatic deposits regardless of histology and targetorgan, provided sufficiently high doses (> 22 Gy) of radiation are delivered. � 2011 Elsevier Inc.
Image-guided radiotherapy, IMRT, Single fraction, Metastases.
INTRODUCTION
One of the basic tenets of classic clinical radiobiology is that
fractionation of the radiation optimizes outcomes because it
affords protection to normal tissues relative to the targeted tu-
mor. For radiotherapy to extracranial disease sites, the pres-
ence of dosimetric and treatment delivery uncertainties,
largely due to organ motion, have traditionally necessitated
the use of considerable safety margins around the target vol-
ume, leading to greater exposure of normal tissues to higher
radiation doses. Until recently, in the extracranial setting,
treatment with ultra-hypofractionated or single-dose regi-
mens has often been regarded as unfeasible owing to the
potential increased risk for radiation-induced complications.
During the last 5–10 years, advances in radiotherapy plan-
ning and delivery have led to a major paradigm shift in radio-
therapy practice. Treatment plans featuring steep dose
t requests to: Michael J. Zelefsky, M.D., Department ofOncology, Memorial Sloan-Kettering Cancer Center,
k Avenue, Box 22, New York, NY 10065. Tel: (212); Fax: (212) 639-8876; E-mail: zelefskm@mskcc.org
1151
gradients at the planning target volume (PTV) edge can be
achieved with intensity modulation of the radiation beams,
thereby maximally reducing exposure to adjacent nontarget
tissues. More recently, the advent of image-guided radiother-
apy (IGRT) has made it possible to achieve near-real-time
quality assurance of the treatment plan, enabling safe deliv-
ery of unprecedented dose exposures (>10 Gy) with single-
dose or ultra-hypofractionated regimens (1). Evidence of
the feasibility and effectiveness of this approach is rapidly
emerging in the scientific literature, mostly in the field of
hypofractionated stereotactic body radiotherapy (SBRT).
Reports on SBRT for lung, liver, and bone metastases have
consistently shown improved tumor-control outcomes with
regimens using higher hypofractionated biologically equiva-
lent doses compared with lower dose levels (2–7). Hereto-
fore, published clinical experience using single-dose
Conflict of interest: none.Received Sept 30, 2009, and in revised form Dec 4, 2009.
Accepted for publication Dec 4, 2009.
Table 1. Patient characteristics
All lesions (n = 124) n
GenderMale 71Female 32
Age (y), median (range) 64 (33–91)Treatment site
Bone 94Lymph node 14Lung 8Liver 6Other soft tissues 2
Histologic typeProstate 42Renal cell 35Colorectal 15Sarcoma 5Non–small cell lung cancer 4Cholangiocarcinoma 4Breast 3Melanoma 3Bladder 2Leydig cell 2Small-cell lung cancer 2Thyroid cancer 2Esophageal 1Germ cell 1Chordoma 1Ovarian 1Pancreatic 1
1152 I. J. Radiation Oncology d Biology d Physics Volume 79, Number 4, 2011
image-guided intensity-modulated radiotherapy (SD-IGRT)
has been far more limited, and the optimal dose required
for local tumor control is not yet defined (8, 9). Stereotactic
radiosurgery of intracranial tumors using single doses of
18–24 Gy is an established mode of treatment and results
in remarkable outcomes. A dose–response relationship has
been reported for single-dose stereotactic radiosurgery of
brain metastases, with approximately 50% freedom from lo-
cal relapse at 1 to 2 years after 15–18 Gy compared with
$80% after 22–24 Gy, regardless of the histologic phenotype
of the primary tumor (10, 11). Similar dose–response data for
extracranial sites are not available. Recent studies using sin-
gle doses of 24 to 25 Gy have shown $80% local control
rates for inoperable primary lung cancer (12–14) and oligo-
metastatic disease (4, 15, 16). Results from our institution re-
ported by Yamada et al. (16) have shown improved outcomes
for metastatic spinal lesions using SD-IGRT of $22 Gy
compared with lower doses. The present study reports on
our experience using SD-IGRT for nonspinal lesions; initial
single-dose levels used ranged from 18 to 20 Gy, and subse-
quently, as part of a Phase I dose-escalation study, doses of
22 and 24 Gy were used. Our findings indicate that higher
doses were associated with improved and durable tumor-con-
trol outcomes irrespective of histology and lesion size.
METHODS AND MATERIALS
Between February 2004 and December 2007, 103 consecutive pa-
tients with a total of 124 lesions underwent SD-IGRT directed to fo-
cal metastatic disease within bone, lymph nodes, or soft tissue using
prescription doses ranging between 18 Gy and 24 Gy. Patients were
initially treated to dose levels of 18–20 Gy and, beginning in 2006,
a Phase I dose-escalation study was activated at 22 Gy. The intent of
this dose-escalation study was to determine the maximally tolerated
dose of single-fraction high-dose IGRT to soft tissues, lymph node,
and bone lesions. Once 20 patients were treated at this dose level
with a minimum follow-up of 6 months, subsequent eligible patients
were accrued to the next dose level of 24 Gy. Although the Phase I
trial is currently accruing patients at the 26-Gy level, the present re-
port includes patients treated with dose ranges of 18–24 Gy until De-
cember 2007. The study was internally approved by the Memorial
Sloan-Kettering Cancer Center Research Board, and all patients
signed informed consent forms. No patient had undergone surgical
resection of the lesion of interest or prior radiotherapy to this region,
and adequate cross-sectional imaging was acquired before treat-
ment.
The clinical characteristics of these patients are summarized in
Table 1. The most frequently treated metastatic lesion was of pros-
tate origin (n = 42), followed by kidney (n = 35) and colorectal (n =
15). The median follow-up was 18 months (range, 2–45 months).
No patient has been lost to follow-up.
Treatment planningThe techniques used for treatment planning and delivery of IGRT
at our institution have been previously described (16, 17). All pa-
tients were immobilized in a customized cradle developed at our in-
stitution for IGRT to prevent any inadvertent patient motion. Before
simulation, if deemed necessary, the patient underwent implantation
of radio-opaque fiducial markers in the vicinity of the target lesion to
ensure target localization before treatment delivery. Patients were
simulated in the cradle using 2-mm slice thickness CT images. Dur-
ing treatment, patient movement was monitored with infrared ste-
reoscopic cameras, and if any motion was noted the treatment was
temporarily stopped and only continued when movement was no
longer observed.
Prescription doseTreatment planning was generated on in-house software using an
inverse treatment algorithm. The dose was prescribed to the 100%
maximum isodose line, which completely encompassed the PTV.
The prescribed doses in these patients ranged between 18 and
24 Gy. The planning target volume was created with a 2-mm expan-
sion around the clinical target volume. Dose constraints of <12 Gy
were set as the maximum allowable dose to the spinal cord contour
and of #16 Gy to bowel, rectum, bladder, and other identified rele-
vant normal tissue structures. This was determined using a standard-
ized best-fit inverse optimization process that takes into account
normal tissue constraints, clinical target volume, and PTV coverage.
Typically, seven to nine coplanar fields were set to a single isocenter
using dynamic multileaf collimation. Six- and/or 15-MV photons
were used to provide optimal coverage and normal tissue sparing.
IGRT techniqueImage verification was performed by creating digitally recon-
structed radiographs from the simulation studies for each field’s
beam’s eye view, which were used as the gold standard of compar-
ison. Linear accelerator on-board cone-beam CT was used for veri-
fication. These images were digitally overlaid with the reference
images to calculate isocenter corrections. The calculated corrections
were then verified for each field before actual treatment.
Table 2. Distribution by prescription dose (all lesions,n = 124)
Planning target volume dose (Gy) n
18 1020 221 322 3823 124 70
Fig. 1. Actuarial local control (Kaplan-Meir method) by dose level.Y axis represents local relapse-free survival (%).
Fig. 2. Actuarial local control (Kaplan-Meir method) by histology.Y axis represents local relapse-free survival (%).
Predictors of local control after SD-IGRT for extracranial metastases d C. GRECO et al. 1153
Intrafraction motion was monitored with infrared stereoscopic cam-
eras. Four spherical infrared reflectors were placed on the patient
above and below the treated region to track intrafractional motion.
If motion >2 mm was detected, treatment was temporarily stopped
and the position was verified again with both two-dimensional kilo-
voltage and three-dimensional beam CT imaging for accurate repo-
sitioning. A cone-beam CT scan was also acquired to verify
positioning after treatment was completed.
EndpointsIn general, patients were examined 8 weeks after treatment.
Repeat diagnostic CT, magnetic resonance imaging, and positron
emission tomography/CT scans were acquired at approximately 3
to 4-month intervals to assess local control for the first 2 years. Local
response to treatment was scored as complete response, stable
disease, or failure on the basis of a thorough assessment of all
cross-sectional imaging/metabolic studies available. Local failure
was scored as an event if a lesion increased in size by $20% accord-
ing to the Response Evaluation Criteria in Solid Tumors and when-
ever persistence of disease was confirmed pathologically (18).
Estimates of local relapse-free survival (LRFS) were calculated us-
ing the Kaplan-Meier method (19).
RESULTS
The overall 2-year actuarial local control rate for all treated
lesions was 64%. The median time to local failure was 9.6
months (range, 0.8–23.5 months). Overall, 76% of the treated
lesions (95 of 124) showed durable local control. Complete
responses occurred in 22% of treatments (21 of 95) (1 lung
nodule, 9 lymph nodes, 11 skeletal lesions). No complete re-
sponses (0 of 12) were observed at lower dose levels (18–20
Gy), 25% (1 of 4) occurred at 21 Gy, 21% (8 of 38) at 22 Gy,
and 17% (12 of 71) at 24 Gy (p = 0.15). Of the 29 local fail-
ures, distribution by histology was as follows: 5 prostate, 8
renal cell, 8 colorectal, 4 sarcomas, 1 non–small-cell lung
cancer, 1 small-cell lung cancer, 1 breast, 1 ovarian. Colorec-
tal lesions fared significantly worse (p < 0.001) than prostate
vs. renal cell vs. all other histologies grouped together. In par-
ticular, four of five colorectal liver metastases recurred
despite receiving a prescription dose of 24 Gy.
Effect of doseThe distribution of numbers of cases at each prescription
dose is summarized in Table 2. Analysis of the effect of
dose on local response was carried out on a total of 118 le-
sions (with the exclusion of liver lesions). On univariate anal-
ysis, prescription dose significantly correlated with LRFS
(p = 0.029). For this analysis patients were stratified into three
dose groups: high (23 to 24 Gy), intermediate (21 to 22 Gy),
and low (18–20 Gy). Figure 1 shows actuarial LRFS curves
as a function of dose. The difference between high dose
(82%) vs. low dose (25%) was highly significant (p <
0.0001), indicating a steep dose–response curve. The local
control rates for lesions treated with intermediate (69%) vs.
low doses (25%) was also significantly different (p = 0.04).
HistologyFigure 2 demonstrates the Kaplan-Meier overall probabil-
ities of LRFS by histology (p = 0.16).
Because of the relatively small number of cases treated at
doses between 18 and 20 Gy, subset analysis of the effect of
dose on different histologic phenotypes was carried out di-
chotomically for high (23 to 24 Gy) vs. low (#22 Gy) dose
levels. No correlation of dose and LRFS probability was ob-
served for prostate cancer (not shown; p = 0.8), whereas renal
cell histology (Fig. 3) displayed significantly improved local
control at higher doses (80%) vs. lower doses (37%) (p =
0.04). For the highest dose level only, analysis of LRFS prob-
abilities showed no statistical significance as a function of
histology (p = 0.90) (Fig. 4), with local control rates of
Fig. 3. Actuarial local control (Kaplan-Meir method) showing theeffect of high dose vs. lower doses in renal cell histology. Y axis rep-resents local relapse-free survival (%).
Fig. 5. Actuarial local control (Kaplan-Meir method) as a functionof lesion location. Y axis represents local relapse-free survival (%;p = 0.50).
1154 I. J. Radiation Oncology d Biology d Physics Volume 79, Number 4, 2011
85%, 80%, 75%, and 72% for prostate, renal cell, colorectal,
and other histologies, respectively.
Target organsNinety-four lesions were osseous, 14 were located in
lymph nodes, 8 in the lungs, 6 in the liver, 1 in the adrenal
gland, and 1 was subcutaneous. Four of the liver lesions re-
curred early on, and no patients with hepatic metastases
were alive beyond the median survival of 18 months owing
to systemic progression. Fig. 5 shows the Kaplan-Meier
LRFS probabilities for bone, lymph node, and lung lesions
(p = 0.5).
The relatively large number of bone lesions allowed fur-
ther analysis of the effect of dose and histology in this site.
A positive association (Fig. 6) between dose and actuarial
LRFS was observed in bone metastases (p = 0.019). More-
over, the difference between high dose (83%) vs. intermedi-
ate dose (60%) was also significant (p = 0.04). At the high
dose level, 2-year actuarial LRFS probabilities of osseous
metastases were 86% for prostate, 80% for renal cell, 75%
for colorectal, and 83% for all other histologies combined
(p = 0.89).
Fig. 4. Actuarial local control (Kaplan-Meir method) at the highdose level for all histologies. Y axis represents local relapse-free sur-vival (%; p = 0.90).
Effect of lesion sizeMean PTV volume was 104.8 cm3 (median, 54.9 cm3;
range, 8.5–1150 cm3). No correlation between PTV and
LRFS as a function of prescribed dose was found (p = 0.55).
Multivariate analysisMultivariate analysis was performed using the Cox propor-
tional hazards multiple regression model with prescription
dose, PTV size, histology and target organ as covariates. Pre-
scription dose retained significance as a predictor of long-
term LRFS (p = 0.003).
ToxicityTreatment was generally well tolerated. Gastrointestinal
Grade 3 acute toxicity was observed in 2 cases (1 patient
treated to a dose of 24 Gy for a liver metastasis, and 1 treated
to 22 Gy for a T6 lesion). Grade $2 late toxicity was ob-
served in 11 of 103 patients. Grade 2 dermatitis with telan-
gectasias was observed in 4 cases. One case of Grade 3
gastrointestinal toxicity (esophageal stricture) occurred after
severe acute toxicity after 22 Gy. Grade 2 radiculopathy was
Fig. 6. Actuarial local control (Kaplan-Meir method) of bone le-sions as a function of dose. Y axis represents local relapse-free sur-vival (%).
Predictors of local control after SD-IGRT for extracranial metastases d C. GRECO et al. 1155
observed in 3 cases. Three patients treated in the pelvic re-
gion developed a radiation-induced Grade 3 peripheral neu-
ritis syndrome (1 at 22 Gy and 2 at 24 Gy). Two of three
cases gradually improved with time and aggressive physical
therapy interventions. The overall incidence of Grade 3 late
toxicity was <4%.
DISCUSSION
Similar to other recent reports, the results of the present
analysis confirm that SD-IGRT is a powerful tool for achiev-
ing long-term local control of metastatic lesions. One of the
most important findings in the present series was the recogni-
tion of a dose–response relationship, with a highly statisti-
cally significant difference in tumor control between high
vs. low single doses (p < 0.0001). A significant difference be-
tween intermediate and low dose (p = 0.04) was also ob-
served, indicating the presence of a steep dose–response
curve. These findings are consistent with results from our in-
stitution published by Yamada et al. (16) which showed
higher doses (24 Gy vs. #23 Gy) to be a predictor of
improved local control (p = 0.03) for metastatic spinal
lesions.
It is noteworthy that an overall actuarial LRFS of 82% was
observed at the high dose level regardless of tumor histology,
lesion size, and target tissue. Analysis of the effect of histol-
ogy on the likelihood of local control revealed a pronounced
dose effect for renal cell histologies, a known radioresistant
histology according to classic radiobiologic ranking. A sim-
ilar effect was not observed for any other histology, likely
owing to the relatively small number of lesions treated at
lower doses in this series. This finding, however, is of great
interest in light of the fact that inherent radioresistance of re-
nal cell cancer seemed to be overcome at a dose of 24 Gy, for
which LRFS rates similar to those of other histologies were
achieved.
The finding of poor local control rates for colorectal liver
metastases after high-dose single-fraction irradiation is not
unexpected. Herfarth et al. (15) carried out a prospective
Phase I/II trial for limited hepatic metastases with dose esca-
lation from 14 Gy to 26 Gy using a single-fraction regimen.
In the initial report actuarial freedom from local failure for the
entire group was 67% at 18 months, but in a subsequent up-
date of the study higher failure rates were observed, suggest-
ing that the single-fraction dose level should be further
escalated (3). Wulf et al. (4), however, reported an 82% actu-
arial local control at 24 months after a single fraction of 26 Gy
in 9 patients. This finding may be due to the steep dose–
response curve of single-dose irradiation, whereby relatively
moderate increases may lead to significant improvements in
outcome. The disappointing local control for colorectal liver
metastases observed in our limited series warrants further in-
vestigation of its underlying causes. Aside from liver loca-
tions, in our cohort, colorectal metastases seemed to
respond relatively well, suggesting that colorectal histology
per se is likely not responsible for the poor outcome.
The findings of the present report and of similar studies re-
porting on high-dose-per-fraction irradiation defy the princi-
ples of classic radiobiology. There are abundant experimental
and clinical data to show that the standard linear-quadratic
(LQ) model performs well for comparison of isoeffective
doses in fractionated radiotherapy up to 8 Gy per fraction.
However, the biologically equivalent doses calculated by
LQ modeling are inconsistent with the clinical outcomes of
1–5 fractions exceeding 12 Gy each (20). It has been disputed
that the LQ model overestimates cell killing at high single
doses (21). Moreover, if the effect of hypoxia is taken into ac-
count, a single dose of 20 Gy is expected to result in a surviv-
ing fraction of 10�3 with 20% hypoxic tumor cells vs.
a survival of 10�6 after 30 fractions of 2 Gy, assuming full
reoxygenation of the tumor (22). On the basis of these as-
sumptions, 40 Gy in a single fraction would be isoeffective
to 60 Gy in 2-Gy fractions (23). Experimental models and
emerging clinical data, however, consistently show that sig-
nificantly lower single exposures are able to achieve high lo-
cal control rates, leading to the hypothesis that the underlying
mechanisms of tumor-cell killing may be different from frac-
tionated radiotherapy.
The biologic foundation of radiation-induced cell death af-
ter high-dose radiation exposure (>10 Gy per fraction) is be-
ginning to be unraveled. Recent studies have challenged the
prevailing hypothesis that at high-dose exposures tissue stem
cell clonogens represent exclusive and independent targets
for radiation-induced tissue damage through reproductive
cell death. There is emerging evidence that tumor endothe-
lium may be impacted to a greater degree with high radiation
doses, resulting in apoptosis, microvasculature dysfunction,
and cell death through parallel and independent pathways
(24–27).
The efficacy of SD-IGRT seems to be durable, suggesting
that the patients most likely to benefit are those with limited
metastatic disease. The beneficial impact of achieving local
control in patients with limited metastases is corroborated
by extensive surgical series of complete excision of brain,
pulmonary, and liver metastases with long-term survival
(28–33). The term oligometastases was coined to indicate
a state of limited metastatic progression in which overt wide-
spread dissemination of the disease has not yet occurred (34).
According to this hypothesis, a disease state, comprised be-
tween locoregionally confined and widely disseminated,
may exist early on in the evolution of metastatic progression,
in which only a limited number of lesions and/or destination
organs are present (35–37). A window of therapeutic oppor-
tunity, therefore, may be exploited in carefully selected pa-
tients who may still benefit from a local form of treatment.
This therapeutic approach may achieve long-term survival
of patients who have been historically considered incurable.
Indeed, if the detected lesions represent the only sites of dis-
tant disease, effective local therapy may result in cure (38,
39) and potentially prevent further disease dissemination
(40).
In our experience, SD-IGRT is extremely well tolerated
and results in minimal radiation-induced morbidity, provided
1156 I. J. Radiation Oncology d Biology d Physics Volume 79, Number 4, 2011
strict dose/volume constraints for the critical structures are
complied with. Overall, Grade 3 complications were <4%
in this series. The instance of a Grade 3 esophageal stricture
occurred in early 2005, before adequate dose/volume con-
straints had been established. A thorough analysis of thoracic
toxicity in paraspinal SD-IGRT recently carried out at our in-
stitution showed a low rate of treatment-related toxicity and
overall safety of this therapeutic approach (41).
Because treatment is administered in 1 day, SD-IGRT also
has practical advantages and seems particularly appealing in
the context of metastatic disease (42, 43). Furthermore, SD-
IGRT is also less likely to conflict with systemic therapy
schedules. As treatment procedures become more stream-
lined, single-fraction radiotherapy will allow improved pa-
tient throughput per treatment machine.
CONCLUSIONS
The present series suggests that SD-IGRT is a highly effec-
tive intervention regardless of target tissue, lesion size, and
histology, provided high enough doses of radiation are deliv-
ered. Further investigation on the clinical role of SD-IGRT is
warranted to ascertain whether dose escalation beyond 24 Gy
improves outcome in specific clinical settings.
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