Stereotactic MR-guided On-table Adaptive Radiation Therapy (SMART) for Borderline Resectable and Locally Advanced Pancreatic Cancer: A Multi-center, Open-label Phase 2 Study

Overview

Journal Radiother Oncol

Specialties Oncology
Radiology

Date 2023 Dec 22

PMID 38135187

Authors

Michael D Chuong

Percy Lee

Daniel A Low

Joshua Kim

Kathryn E Mittauer

Michael F Bassetti

Carri K Glide-Hurst

Ann C Raldow

Yingli Yang

Lorraine Portelance

Kyle R Padgett

Bassem Zaki

Rongxiao Zhang

Hyun Kim

Lauren E Henke

Alex T Price

Joseph D Mancias

Christopher L Williams

John Ng

Ryan Pennell

M Raphael Pfeffer

Daphne Levin

Adam C Mueller

Karen E Mooney

Patrick Kelly

Amish P Shah

Luca Boldrini

Lorenzo Placidi

Martin Fuss

Parag Jitendra Parikh

Affiliations

Soon will be listed here.

Abstract

Background And Purpose: Radiation dose escalation may improve local control (LC) and overall survival (OS) in select pancreatic ductal adenocarcinoma (PDAC) patients. We prospectively evaluated the safety and efficacy of ablative stereotactic magnetic resonance (MR)-guided adaptive radiation therapy (SMART) for borderline resectable (BRPC) and locally advanced pancreas cancer (LAPC). The primary endpoint of acute grade ≥ 3 gastrointestinal (GI) toxicity definitely related to SMART was previously published with median follow-up (FU) 8.8 months from SMART. We now present more mature outcomes including OS and late toxicity.

Materials And Methods: This prospective, multi-center, single-arm open-label phase 2 trial (NCT03621644) enrolled 136 patients (LAPC 56.6 %; BRPC 43.4 %) after ≥ 3 months of any chemotherapy without distant progression and CA19-9 ≤ 500 U/mL. SMART was delivered on a 0.35 T MR-guided system prescribed to 50 Gy in 5 fractions (biologically effective dose [BED] = 100 Gy). Elective coverage was optional. Surgery and chemotherapy were permitted after SMART.

Results: Mean age was 65.7 years (range, 36-85), induction FOLFIRINOX was common (81.7 %), most received elective coverage (57.4 %), and 34.6 % had surgery after SMART. Median FU was 22.9 months from diagnosis and 14.2 months from SMART, respectively. 2-year OS from diagnosis and SMART were 53.6 % and 40.5 %, respectively. Late grade ≥ 3 toxicity definitely, probably, or possibly attributed to SMART were observed in 0 %, 4.6 %, and 11.5 % patients, respectively.

Conclusions: Long-term outcomes from the phase 2 SMART trial demonstrate encouraging OS and limited severe toxicity. Additional prospective evaluation of this novel strategy is warranted.

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