Somatic variants in epigenetic modifiers can predict failure of response to imatinib but not to second-generation tyrosine kinase inhibitors

Georgios Nteliopoulos; Alexandra Bazeos; Simone Claudiani; Gareth Gerrard; Edward Curry; Richard Szydlo; Mary Alikian; Hui En Foong; Zacharoula Nikolakopoulou; Sandra Loaiza; Jamshid S. Khorashad; Dragana Milojkovic; Danilo Perrotti; Robert Peter Gale; Letizia Foroni; Jane F. Apperley

doi:10.3324/haematol.2018.200220

Haematologica (Dec 2019)

Somatic variants in epigenetic modifiers can predict failure of response to imatinib but not to second-generation tyrosine kinase inhibitors

Georgios Nteliopoulos,
Alexandra Bazeos,
Simone Claudiani,
Gareth Gerrard,
Edward Curry,
Richard Szydlo,
Mary Alikian,
Hui En Foong,
Zacharoula Nikolakopoulou,
Sandra Loaiza,
Jamshid S. Khorashad,
Dragana Milojkovic,
Danilo Perrotti,
Robert Peter Gale,
Letizia Foroni,
Jane F. Apperley

Affiliations

Georgios Nteliopoulos: Centre for Haematology, Department of Medicine, Imperial College, London, UK
Alexandra Bazeos: Centre for Haematology, Department of Medicine, Imperial College, London, UK
Simone Claudiani: Centre for Haematology, Department of Medicine, Imperial College, London, UK;Imperial College Healthcare NHS Trust, London, UK
Gareth Gerrard: Centre for Haematology, Department of Medicine, Imperial College, London, UK;Sarah Cannon Molecular Diagnostics, HCA Healthcare UK, London, UK
Edward Curry: Department of Surgery and Cancer, Ovarian Cancer Action Research Centre, Imperial College, London, UK
Richard Szydlo: Centre for Haematology, Department of Medicine, Imperial College, London, UK
Mary Alikian: Centre for Haematology, Department of Medicine, Imperial College, London, UK;Imperial College Healthcare NHS Trust, London, UK
Hui En Foong: Imperial College Healthcare NHS Trust, London, UK
Zacharoula Nikolakopoulou: Centre for Haematology, Department of Medicine, Imperial College, London, UK;Lungs for Living Research Centre, UCL Respiratory, University College London, London, UK
Sandra Loaiza: Centre for Haematology, Department of Medicine, Imperial College, London, UK;Imperial College Healthcare NHS Trust, London, UK
Jamshid S. Khorashad: Centre for Haematology, Department of Medicine, Imperial College, London, UK;Imperial College Healthcare NHS Trust, London, UK
Dragana Milojkovic: Centre for Haematology, Department of Medicine, Imperial College, London, UK;Imperial College Healthcare NHS Trust, London, UK
Danilo Perrotti: Centre for Haematology, Department of Medicine, Imperial College, London, UK;Greenebaum Cancer Center, University of Maryland School of Medicine, Baltimore MD, USA
Robert Peter Gale: Centre for Haematology, Department of Medicine, Imperial College, London, UK
Letizia Foroni: Centre for Haematology, Department of Medicine, Imperial College, London, UK
Jane F. Apperley: Centre for Haematology, Department of Medicine, Imperial College, London, UK;Imperial College Healthcare NHS Trust, London, UK

DOI: https://doi.org/10.3324/haematol.2018.200220
Journal volume & issue: Vol. 104, no. 12

Abstract

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There are no validated molecular biomarkers to identify newly-diagnosed individuals with chronic-phase chronic myeloid leukemia likely to respond poorly to imatinib and who might benefit from first-line treatment with a more potent second-generation tyrosine kinase inhibitor. Our inability to predict these ‘high-risk’ individuals reflects the poorly understood heterogeneity of the disease. To investigate the potential of genetic variants in epigenetic modifiers as biomarkers at diagnosis, we used Ion Torrent next-generation sequencing of 71 candidate genes for predicting response to tyrosine kinase inhibitors and probability of disease progression. A total of 124 subjects with newly-diagnosed chronic-phase chronic myeloid leukemia began with imatinib (n=62) or second-generation tyrosine kinase inhibitors (n=62) and were classified as responders or non-responders based on the BCRABL1 transcript levels within the first year and the European LeukemiaNet criteria for failure. Somatic variants affecting 21 genes (e.g. ASXL1, IKZF1, DNMT3A, CREBBP) were detected in 30% of subjects, most of whom were non-responders (41% non-responders, 18% responders to imatinib, 38% non-responders, 25% responders to second-generation tyrosine kinase inhibitors). The presence of variants predicted the rate of achieving a major molecular response, event-free survival, progression-free survival and chronic myeloid leukemia-related survival in the imatinib but not the second-generation tyrosine kinase inhibitors cohort. Rare germline variants had no prognostic significance irrespective of treatment while some pre-leukemia variants suggest a multi-step development of chronic myeloid leukemia. Our data suggest that identification of somatic variants at diagnosis facilitates stratification into imatinib responders/non-responders, thereby allowing earlier use of second-generation tyrosine kinase inhibitors, which, in turn, may overcome the negative impact of such variants on disease progression.

Published in Haematologica

ISSN: 0390-6078 (Print); 1592-8721 (Online)
Publisher: Ferrata Storti Foundation
Country of publisher: Italy
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the blood and blood-forming organs
Website: http://www.haematologica.org

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