Neoadjuvant FOLFOXIRI prior to chemoradiotherapy for high-risk (“ugly”) locally advanced rectal cancer: study protocol of a single-arm, multicentre, open-label, phase II trial (MEND-IT)
K. van den Berg,
D. P. Schaap,
E. L. K. Voogt,
T. E. Buffart,
H. M. W. Verheul,
J. W. B. de Groot,
C. Verhoef,
J. Melenhorst,
J. M. L. Roodhart,
J. H. W. de Wilt,
H. L. van Westreenen,
A. G. J. Aalbers,
M. van ‘t Veer,
C. A. M. Marijnen,
J. Vincent,
L. H. J. Simkens,
N. A. J. B. Peters,
M. Berbée,
I. M. Werter,
P. Snaebjornsson,
H. M. U. Peulen,
I. G. van Lijnschoten,
M. J. Roef,
G. A. P. Nieuwenhuijzen,
J. G. Bloemen,
J. M. W. E. Willems,
G. J. M. Creemers,
J. Nederend,
H. J. T. Rutten,
J. W. A. Burger
Affiliations
K. van den Berg
Department of Medical Oncology, Catharina Hospital
D. P. Schaap
Department of Surgery, Catharina Hospital
E. L. K. Voogt
Department of Surgery, Catharina Hospital
T. E. Buffart
Department of Gastrointestinal Oncology, Netherlands Cancer Institute
H. M. W. Verheul
Department of Medical Oncology, Radboud University Medical Centre
J. W. B. de Groot
Department of Medical Oncology, Isala Oncology Centre
C. Verhoef
Department of Surgical Oncology, Erasmus MC Cancer Institute
J. Melenhorst
Department of Surgery, Maastricht University Medical Centre
J. M. L. Roodhart
Department of Medical Oncology, University Medical Centre Utrecht
J. H. W. de Wilt
Department of Surgery, Radboud University Medical Centre
H. L. van Westreenen
Department of Surgery
A. G. J. Aalbers
Department of Surgical Oncology, Netherlands Cancer Institute
M. van ‘t Veer
Department of Research and Education, Catharina Hospital
C. A. M. Marijnen
Department of Radiation Oncology, Netherlands Cancer Institute
J. Vincent
Department of Medical Oncology, Elkerliek Hospital
L. H. J. Simkens
Department of Medical Oncology, Maxima Medical Centre
N. A. J. B. Peters
Department of Medical Oncology, St. Jans Hospital
M. Berbée
Department of Radiation Oncology (MAASTRO), GROW School for Oncology and Reproduction, Maastricht University Medical Centre+
I. M. Werter
Department of Medical Oncology, Rijnstate Hospital
P. Snaebjornsson
Department of Pathology, Netherlands Cancer Institute
H. M. U. Peulen
Department of Radiation Oncology, Catharina Hospital
I. G. van Lijnschoten
Department of Pathology, PAMM Laboratory for Pathology and Medical Microbiology
M. J. Roef
Department of Nuclear Medicine, Catharina Hospital
G. A. P. Nieuwenhuijzen
Department of Surgery, Catharina Hospital
J. G. Bloemen
Department of Surgery, Catharina Hospital
J. M. W. E. Willems
Department of Medical Oncology, Anna Hospital
G. J. M. Creemers
Department of Medical Oncology, Catharina Hospital
Abstract Background The presence of mesorectal fascia (MRF) invasion, grade 4 extramural venous invasion (EMVI), tumour deposits (TD) or extensive or bilateral extramesorectal (lateral) lymph nodes (LLN) on MRI has been suggested to identify patients with indisputable, extensive locally advanced rectal cancer (LARC), at high risk of treatment failure. The aim of this study is to evaluate whether or not intensified chemotherapy prior to neoadjuvant chemoradiotherapy improves the complete response (CR) rate in these patients. Methods This multicentre, single-arm, open-label, phase II trial will include 128 patients with non-metastatic high-risk LARC (hr-LARC), fit for triplet chemotherapy. To ensure a study population with indisputable, unfavourable prognostic characteristics, hr-LARC is defined as LARC with on baseline MRI at least one of the following characteristics; MRF invasion, EMVI grade 4, enlarged bilateral or extensive LLN at high risk of an incomplete resection, or TD. Exclusion criteria are the presence of a homozygous DPD deficiency, distant metastases, any chemotherapy within the past 6 months, previous radiotherapy within the pelvic area precluding standard chemoradiotherapy, and any contraindication for the planned treatment. All patients will be planned for six two-weekly cycles of FOLFOXIRI (5-fluorouracil, leucovorin, oxaliplatin and irinotecan) prior to chemoradiotherapy (25 × 2 Gy or 28 × 1.8 Gy with concomitant capecitabine). A resection will be performed following radiological confirmation of resectable disease after the completion of chemoradiotherapy. A watch and wait strategy is allowed in case of a clinical complete response. The primary endpoint is the CR rate, described as a pathological CR or a sustained clinical CR one year after chemoradiotherapy. The main secondary objectives are long-term oncological outcomes, radiological and pathological response, the number of resections with clear margins, treatment-related toxicity, perioperative complications, health-related costs, and quality of life. Discussion This trial protocol describes the MEND-IT study. The MEND-IT study aims to evaluate the CR rate after intensified chemotherapy prior to concomitant chemoradiotherapy in a homogeneous group of patients with locally advanced rectal cancer and indisputably unfavourable characteristics, defined as hr-LARC, in order to improve their prognosis. Trial registration Clinicaltrials.gov: NCT04838496 , registered on 02–04-2021 Netherlands Trial Register: NL9790. Protocol version Version 3 dd 11–4-2022.
