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Copenhagen, Denmark
Onsite/Online

ESTRO 2022

Session Item

Saturday
May 07
10:30 - 11:30
Room D3
Late-breaking
Anna Kirby, United Kingdom;
Ben Slotman, The Netherlands
1220
Proffered Papers
Clinical
11:00 - 11:10
SCALOP2:A multicenter randomized trial of RT dose escalation and nelfinavir in pancreatic cancer
Somnath Mukherjee, United Kingdom
OC-0103

Abstract

SCALOP2:A multicenter randomized trial of RT dose escalation and nelfinavir in pancreatic cancer
Authors:

Somnath Mukherjee1, Cathy Qi2, Rachel Shaw3, John Bridgewater4, Ganesh Radhakrishna5, Neel Patel6, Bethan Tranter7, Philip Parsons8, Stephen Falk9, Harpreet Wasan10, Daniel Holyoake11, Rajarshi Roy12, Martin Scott-Brown13, Chris Hurt14, David Sebag-Montefiore15, Tim Maughan16, Maria Hawkins17, Pippa Corrie18

1Oxford University Hospital NHS Trust, Oncology, Oxford, United Kingdom; 2Centre for Statistics in Medicine, University of Oxford, Statistics, Oxford, United Kingdom; 3University of Oxford, Oxford Clinical Trials Unit, Oxford, United Kingdom; 4University College London Cancer Institute, Oncology, London, United Kingdom; 5The Christie NHS Foundation Trust, Oncology, Manchester, United Kingdom; 6Oxford University Hospitals NHS Foundation Trust, Radiology, Oxford, United Kingdom; 7Velindre Hospital NHS Foundation Trust, Pharmacy, Cardiff, United Kingdom; 8Velindre Hospital NHS Foundation Trust, Radiotherapy Physics, Cardiff, United Kingdom; 9Bristol Oncology Centre, Oncology, Bristol, United Kingdom; 10Hammersmith Hospital, Imperial College London, Division of Cancer, London, United Kingdom; 11Norfolk and Norwich University Hospitals NHS Foundation Trust, Oncology, Norwich, United Kingdom; 12Hull University Teaching Hospitals NHS Trust, Oncology, Hull, United Kingdom; 13University Hospital Coventry and Warwickshire, Oncology, Coventry, United Kingdom; 14Cardiff University, Centre for Trials Research, Cardiff, United Kingdom; 15St. James's University Hospital, Institute of Oncology, , Leeds, United Kingdom; 16MRC Oxford Institute for Radiation Oncology, University of Oxford, Oncology, Oxford, United Kingdom; 17University College London, Dept of Med Phys & Biomedical Eng, London, United Kingdom; 18Cambridge University Hospitals NHS Foundation Trust, Oncology, Cambridge, United Kingdom

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Purpose or Objective

The anti-retroviral agent, nelfinavir (N), demonstrated radiosensitising properties in pre-clinical models and showed promising activity in single arm phase I/II trials in combination with CRT for LAPC. RT dose escalation (BED10 >70) may be associated with improved survival. SCALOP2 was a phase 1/randomized phase II study. The phase I component established the MTD of nelfinavir in combination with capecitabine-based CRT following gemcitabine+nab-paclitaxel (GEMABX) induction chemotherapy in LAPC (previously reported). The 2 x 2 randomized phase II component evaluated whether (1) RT dose escalation from 50.4Gy/28 fractions [standard dose (SD)] to 60Gy/30 fractions [high dose (HD)], combined with capecitabine improved OS and (2) adding nelfinavir to CRT improved PFS.

Material and Methods

Patients with unresectable, histologically/cytologically proven LAPC and WHO PS 0-1 received 3 cycles of induction GEMABX (standard dose and schedule) followed by restaging. Progression-free patients were randomized to 1 further cycle of GEMABX followed by A (SD+N), B (SD = control arm), C (HD +N), D (HD), or E (GEMABX x 2 cycles = calibration arm). CRT capecitabine dose was 830mg/m2 bd on days of RT, nelfinavir 1250mg bd started 7 days before CRT until completing CRT.

Results

Between March 2016 and March 2020, 186 patients were recruited from 21 centres in the UK (phase 1=27; phase 2=159). 106/159 patients were randomized (A=19, B=26, C=19, D=27, E=15). Arm E closed in Nov 2019, taking into consideration data from the LAPACT trial. The ISDMC recommended closure of the nelfinavir arms in Feb 2020 due to futility. At the time of analysis, 64/91 patients randomized to CRT arms had died. Median OS was 15.6 mo (60% CI 14.3,18.2) in the SD arms and 16.9 mo (16.2, 17.7) in the HD arms, HR (60% CI) 1.11(0.89,1.38), adjusted one-sided p=Not significant (NS). Of the 76 patients eligible for randomization to N-containing arms, median PFS was 11.1 (10.3, 12.8) in the CRT-only arms (HR (60% CI) 1.84(1.47,2.3) and 10 mo (60% CI 9.9,10.2) in the CRT+N arms, adjusted one-sided p=NS. Secondary endpoints: Grade 3-4 serious adverse reactions during CRT were reported as follows: 5/45 (11.1%) in SD arms, 4/46 (8.7%) in HD arms, 5/38 (13.2%) in CRT+N arms and 4/38 (10.5%) in CRT-only arms. 1-year local progression (with/without metastasis) and local-only (no metastasis) progression rate was 33.3% and 26.7% (SD arms) and 23.9% and 15.2% (HD arms) respectively. Overall resection rate (11%) and quality of life were similar for all arms.

Conclusion

The addition of nelfinavir and/or RT dose escalation to 60Gy failed to improve outcomes in LAPC. RT dose escalation to 60Gy was well tolerated.