S130

ESTRO 35 2016

_____________________________________________________________________________________________________

PV-0281

(ICORG 05-03): Radiotherapy in malignant spinal cord

compression; The quality of life analysis

K. Lee

1

St Luke's Radiation Oncology Network, Radiation Oncology,

Dublin, Ireland Republic of

1

, C. Small

2,3

, P. Kelly

2,4

, O. McArdle

1,2

, J. O'Sullivan

2,5

,

D. Hacking

2,6

, M. Pomeroy

2,3

, M. Stevenson

2

, J. Armstrong

1,2

,

M. Moriarty

1,2

, M. Dunne

7

, A. Clayton-Lea

2,8

, I. Parker

2

, C.

Collins

9

, P. Thirion

1,2

2

All Ireland Cooperative Oncology Research Group, Radiation

Oncology, Dublin, Ireland Republic of

3

Galway University Hospital, Radiation Oncology, Galway,

Ireland Republic of

4

Cork University Hospital, Radiation Oncology, Cork, Ireland

Republic of

5

Belfast City Hospital, Radiation Oncology, Belfast, United

Kingdom

6

Whitfield Clinic, Radiation Oncology, Waterford, Ireland

Republic of

7

St Luke's Radiation Oncology Network, Clinical Trials,

Dublin, Ireland Republic of

8

St Luke's Radiation Oncology Network, Operational Services,

Dublin, Ireland Republic of

9

St Luke's Radiation Oncology Network, Radiology, Dublin,

Ireland Republic of

Purpose or Objective:

To compare Quality of Life (QoL)

outcomes in patients (pts) with Malignant Spinal Cord

Compression (MSCC) not proceeding with surgical

decompression and treated by External Beam Radiation

Therapy (EBRT) with one of two Fractionation Schedules (FS).

Material and Methods:

ICORG 05-03 was an ICH-GCP

compliant prospective (1.1) randomised non-inferiority phase

III trial comparing two FS: arm 1 (control): 20Gy/5 Fractions

(#) vs. arm 2 (experimental): 10Gy/1#, with 80% power, 5%

significant level and 0.4 non-inferiority margin. While the

primary end point of this trial (previously presented (ASTRO

2014)) was change in mobility at 5 weeks (wks), the current

focus is on a secondary endpoint, QoL (EORTC QLQ-C30

questionnaire).

Results:

From 2006 to 2014, 5 institutions accrued 115

eligible pts (2 non-eligible pts, no treatment allocation

violation). 70 pts with QoL data at 5 wks were evaluable.

Baseline characteristics were balanced between arms [

♀

/

♂

:

30/40, median age: 69 (range: 30-87)]. Analysis showed a

statistically significant benefit of radiotherapy (RT) for ‘Pain

interfered with daily activities’ but not for Overall OoL.

There was no statistically significant benefit between arms

for either: 1. Overall QoL (mean change from pre-treatment

.52 in arm 1 vs. .21 in arm 2; 95% CI: -0.84 – 1.45, p = 0.596);

2. Pain interfered with daily activities (mean change: .84 in

arm 1 vs. 1.00 in arm 2; 95% CI: -0.66 – .98, p = 0.698). A

non-planned exploratory regression analysis checked for

independent prognostic factors for less pain at 5 wks.

Multiple regression analysis revealed baseline pain as the

strongest unique and statistically significant contributor to

explaining less pain at 5-wks (beta = -0.63; p=0.002).

Exploratory analyses were also conducted to characterise pts

dying at <5 wks,who might not benefit from RT. Primary

malignancy (Chi-square test: Χ2 (3, n=106) = 15.6, p = 0.001,

phi = 0.38) and initial mobility status (Chi-square test, Χ2 (2,

n=106) = 11.0, p = 0.004, phi = 0.32.) were found to be

associated with a life expectancy <5 wks. 67% of lung and 13%

of breast cancer pts died before 5 wks, as did 49% of bed-

bound and 15% of pts who could walk unaided.

Conclusion:

With respect to QoL, primary RT significantly

improves the pain related variables used in the trial, with

10Gy/1# FS being at least equivalent to 20Gy/5#. Baseline

pain is the most significant independent prognostic factor for

less pain at 5 wks. Tumour site and mobility should be

considered when offering RT treatment to similar pts.

Proffered Papers: Donal Hollywood Award

OC-0282

FLAME randomised trial: 95Gy MRI-boost vs 77Gy prostate

radiotherapy: toxicity and quality of life

M. Van Vulpen

1

UMC Utrecht, Radiation Oncology, Utrecht, The Netherlands

1

, J. Van Loon

1

, F. Pos

2

, K. Haustermans

3

, R.

Smeenk

4

, L. Van den Bergh

3

, S. Isebaert

3

, G. McColl

4

, M.

Kunze-Busch

4

, B. Doodeman

2

, J. Noteboom

1

, E. Monninkhof

5

,

U. Van der Heide

2

2

AvL/NKI, Radiation Oncology, Amsterdam, The Netherlands

3

UZ Leuven, Radiation Oncology, Leuven, Belgium

4

Radboud UMC, Radiation Oncology, Nijmegen, The

Netherlands

5

UMC Utrecht, Julius Center for methodology, Utrecht, The

Netherlands

Purpose or Objective:

The aim of this study was to compare

treatment related side-effects and quality of life of an MRI-

based 95Gy boost to the multi-parametric MRI visible tumor

with 77Gy whole prostate external beam radiotherapy in

patients with intermediate or high risk localized prostate

cancer.

Material and Methods:

FLAME (NCT01168479) was a phase 3,

single blind, multi-center randomized controlled trial.

Patients with biopsy proven intermediate and high risk

prostate cancer (D’Amico risk classification) were randomly

assigned and stratified per center. Analysis was done by

intention to treat. The control group received a dose to the

entire prostate of 77Gy in 35 fractions. The experimental arm

received an additional integrated boost up to 95 Gy to the

mp-MRI-visible lesions. Treatment related toxicity was

measured by the Common Toxicity Criteria for adverse events

version 3.0 (CTCAE). Quality of Life (QoL) was measured by

SF-36, EORTC QLQ-C30 and EORTC QLQ-PR25. All items and

scale scores were linearly transformed to a 0–100 scale, with

higher scores reflecting either more symptoms or higher

levels of functioning. Clinical relevance was considered a

difference of more than 10 points between arms. Mean

differences between groups were calculated using a linear

mixed model with adjustment for baseline values. Statistical

significance was considered P<0.01.

Results:

Between 2009 and 2015 287 patients were assigned

to the control group and 284 to the dose-escalated (FLAME)

arm. Mean follow up was 22 months. In both arms, 84% of

patients had high risk disease. Regarding GU toxicity, 134

patients (47.2%) in the FLAME arm and 147 patients (51.4%) in

de control arm experienced any grade 2 or higher toxicity.

Grade 3 GU toxicity occurred in 15 patients (5.3%) in the

FLAME arm and 12 patients (4.2%) in the control arm.

Regarding GI toxicity, 60 patients (21.1%) in the FLAME arm

and 47 patients (16.4%) in the control arm experienced grade

2 or higher toxicity. Grade 3 toxicity occurred in 2 patients

(0.7%) in the FLAME arm and in 5 patients (1.7%) in the

control arm. None of these differences were statistically

significant. For all quality of life measures no statistically

significant or clinical relevant differences were observed.