Somatic POLE proofreading domain mutation, immune response, and prognosis in colorectal cancer: a retrospective, pooled biomarker study

Enric Domingo; Luke Freeman-Mills; Emily Rayner; Mark Glaire; Sarah Briggs; Louis Vermeulen; Evelyn Fessler; Jan Paul Medema; Arnoud Boot; Hans Morreau; Tom van Wezel; Gerrit-Jan Liefers; Ragnhild A Lothe; Stine A Danielsen; Anita Sveen; Arild Nesbakken; Inti Zlobec; Alessandro Lugli; Viktor H Koelzer; Martin D Berger; Sergi Castellví-Bel; Jenifer Muñoz; Epicolon consortium; Marco de Bruyn; Hans W Nijman; Marco Novelli; Kay Lawson; Dahmane Oukrif; Eleni Frangou; Peter Dutton; Sabine Tejpar; Mauro Delorenzi; Rachel Kerr; David Kerr; Ian Tomlinson; David N Church

doi:10.1016/S2468-1253(16)30014-0

Somatic POLE proofreading domain mutation, immune response, and prognosis in colorectal cancer: a retrospective, pooled biomarker study

Lancet Gastroenterol Hepatol. 2016 Nov;1(3):207-216. doi: 10.1016/S2468-1253(16)30014-0. Epub 2016 Jul 20.

Authors

Enric Domingo¹, Luke Freeman-Mills², Emily Rayner², Mark Glaire³, Sarah Briggs², Louis Vermeulen⁴, Evelyn Fessler⁴, Jan Paul Medema⁴, Arnoud Boot⁵, Hans Morreau⁵, Tom van Wezel⁵, Gerrit-Jan Liefers⁶, Ragnhild A Lothe⁷, Stine A Danielsen⁷, Anita Sveen⁷, Arild Nesbakken⁸, Inti Zlobec⁹, Alessandro Lugli⁹, Viktor H Koelzer¹⁰, Martin D Berger¹¹, Sergi Castellví-Bel¹², Jenifer Muñoz¹²; Epicolon consortium; Marco de Bruyn¹³, Hans W Nijman¹³, Marco Novelli¹⁴, Kay Lawson¹⁴, Dahmane Oukrif¹⁴, Eleni Frangou¹⁵, Peter Dutton¹⁵, Sabine Tejpar¹⁶, Mauro Delorenzi¹⁷, Rachel Kerr¹⁸, David Kerr¹⁹, Ian Tomlinson²⁰, David N Church²¹

Affiliations

¹ Molecular and Population Genetics Laboratory, University of Oxford, Oxford, UK; Oxford Centre for Cancer Gene Research and NIHR Comprehensive Biomedical Research Centre, The Wellcome Trust Centre for Human Genetics, University of Oxford, Oxford, UK; Department of Oncology, University of Oxford, Oxford, UK.
² Molecular and Population Genetics Laboratory, University of Oxford, Oxford, UK.
³ Cancer Genomics and Immunology Group, University of Oxford, Oxford, UK.
⁴ Academic Medical Center Amsterdam, Center for Experimental Molecular Medicine, Amsterdam, Netherlands.
⁵ Department of Pathology, Leiden, Netherlands.
⁶ Leiden University Medical Center, Leiden, Netherlands.
⁷ K G Jebsen Colorectal Cancer Research Centre, Oslo, Norway; Department of Molecular Oncology, Institute for Cancer Research, Oslo University Hospital, Oslo, Norway.
⁸ K G Jebsen Colorectal Cancer Research Centre, Oslo, Norway; Department of Gastrointestinal Surgery, Institute for Cancer Research, Oslo University Hospital, Oslo, Norway.
⁹ Institute of Pathology, University of Bern, Bern, Switzerland.
¹⁰ Molecular and Population Genetics Laboratory, University of Oxford, Oxford, UK; Institute of Pathology, University of Bern, Bern, Switzerland.
¹¹ Department of Medical Oncology, University Hospital of Bern, Bern, Switzerland.
¹² Gastroenterology Department, Hospital Clínic, Institut d'Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS), Centro de Investigación Biomédica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD), University of Barcelona, Barcelona, Spain.
¹³ Department of Obstetrics and Gynecology, University Medical Center Groningen, University of Groningen, Groningen, Netherlands.
¹⁴ Department of Histopathology, UCL, London, UK.
¹⁵ Centre for Statistics in Medicine, Nuffield Department of Orthopaedics, Rheumatology and Musculoskeletal Sciences, University of Oxford, Oxford, UK.
¹⁶ Department of Molecular Digestive Oncology, University of Leuven, Leuven, Belgium.
¹⁷ Ludwig Center for Cancer Research, University of Lausanne, Epalinges, Switzerland; Department of Oncology, Faculty of Biology and Medicine, University of Lausanne, Lausanne, Switzerland; SIB Swiss Institute Bioinformatics, Lausanne, Switzerland.
¹⁸ Department of Oncology, University of Oxford, Oxford, UK; Oxford Cancer Centre, Churchill Hospital, Oxford Radcliffe Hospitals NHS Trust, University of Oxford, Oxford, UK.
¹⁹ Oxford Cancer Centre, Churchill Hospital, Oxford Radcliffe Hospitals NHS Trust, University of Oxford, Oxford, UK; Radcliffe Department of Medicine, University of Oxford, Oxford, UK.
²⁰ Molecular and Population Genetics Laboratory, University of Oxford, Oxford, UK; Oxford Centre for Cancer Gene Research and NIHR Comprehensive Biomedical Research Centre, The Wellcome Trust Centre for Human Genetics, University of Oxford, Oxford, UK.
²¹ Cancer Genomics and Immunology Group, University of Oxford, Oxford, UK; Oxford Cancer Centre, Churchill Hospital, Oxford Radcliffe Hospitals NHS Trust, University of Oxford, Oxford, UK. Electronic address: dchurch@well.ox.ac.uk.

PMID: 28404093
DOI: 10.1016/S2468-1253(16)30014-0

Abstract

Background: Precision cancer medicine depends on defining distinct tumour subgroups using biomarkers that may occur at very modest frequencies. One such subgroup comprises patients with exceptionally mutated (ultramutated) cancers caused by mutations that impair DNA polymerase epsilon (POLE) proofreading.

Methods: We examined the association of POLE proofreading domain mutation with clinicopathological variables and immune response in colorectal cancers from clinical trials (VICTOR, QUASAR2, and PETACC-3) and colorectal cancer cohorts (Leiden University Medical Centre 1 and 2, Oslo 1 and 2, Bern, AMC-AJCC-II, and Epicolon-1). We subsequently investigated its association with prognosis in stage II/III colorectal cancer by Cox regression of pooled individual patient data from more than 4500 cases from these studies.

Findings: Pathogenic somatic POLE mutations were detected in 66 (1·0%) of 6517 colorectal cancers, and were mutually exclusive with mismatch repair deficiency (MMR-D) in the 6277 cases for whom both markers were determined (none of 66 vs 833 [13·4%] of 6211; p<0·0001). Compared with cases with wild-type POLE, cases with POLE mutations were younger at diagnosis (median 54·5 years vs 67·2 years; p<0·0001), were more frequently male (50 [75·8%] of 66 vs 3577 [55·5%] of 6445; p=0·0010), more frequently had right-sided tumour location (44 [68·8%] of 64 vs 2463 [39·8%] of 6193; p<0·0001), and were diagnosed at an earlier disease stage (p=0·006, χ² test for trend). Compared with mismatch repair proficient (MMR-P) POLE wild-type tumours, POLE-mutant colorectal cancers displayed increased CD8+ lymphocyte infiltration and expression of cytotoxic T-cell markers and effector cytokines, similar in extent to that observed in immunogenic MMR-D cancers. Both POLE mutation and MMR-D were associated with significantly reduced risk of recurrence compared with MMR-P colorectal cancers in multivariable analysis (HR 0·34 [95% CI 0·11-0·76]; p=0·0060 and 0·72 [0·60-0·87]; p=0·00035), although the difference between the groups was not significant.

Interpretation: POLE proofreading domain mutations identify a subset of immunogenic colorectal cancers with excellent prognosis. This association underscores the importance of rare biomarkers in precision cancer medicine, but also raises important questions about how to identify and implement them in practice.

Funding: Cancer Research UK, Academy of Medical Sciences, Health Foundation, EU, ERC, NIHR, Wellcome Trust, Dutch Cancer Society, Dutch Digestive Foundation.

Publication types

Meta-Analysis
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Aged, 80 and over
Biomarkers, Tumor / genetics*
Colorectal Neoplasms / diagnosis
Colorectal Neoplasms / genetics*
Colorectal Neoplasms / immunology
Colorectal Neoplasms / mortality
DNA Polymerase II / genetics*
Female
Humans
Male
Middle Aged
Mutation
Poly-ADP-Ribose Binding Proteins / genetics*
Prognosis
Retrospective Studies
Survival Analysis

Substances

Biomarkers, Tumor
Poly-ADP-Ribose Binding Proteins
DNA Polymerase II
POLE protein, human

Abstract

Publication types

MeSH terms

Substances

Grants and funding