Laying the foundation for genomically-based risk assessment in chronic myeloid leukemia

Susan Branford; Dennis Dong Hwan Kim; Jane F Apperley; Christopher A Eide; Satu Mustjoki; S Tiong Ong; Georgios Nteliopoulos; Thomas Ernst; Charles Chuah; Carlo Gambacorti-Passerini; Michael J Mauro; Brian J Druker; Dong-Wook Kim; Francois-Xavier Mahon; Jorge Cortes; Jerry P Radich; Andreas Hochhaus; Timothy P Hughes; International CML Foundation Genomics Alliance

doi:10.1038/s41375-019-0512-y

Laying the foundation for genomically-based risk assessment in chronic myeloid leukemia

Leukemia. 2019 Aug;33(8):1835-1850. doi: 10.1038/s41375-019-0512-y. Epub 2019 Jun 17.

Authors

Susan Branford^{1

2

3}, Dennis Dong Hwan Kim⁴, Jane F Apperley⁵, Christopher A Eide^{6

7}, Satu Mustjoki^{8

9}, S Tiong Ong^{10

11}, Georgios Nteliopoulos⁵, Thomas Ernst¹², Charles Chuah^{10

11}, Carlo Gambacorti-Passerini¹³, Michael J Mauro¹⁴, Brian J Druker^{6

7}, Dong-Wook Kim^{15

16}, Francois-Xavier Mahon¹⁷, Jorge Cortes¹⁸, Jerry P Radich¹⁹, Andreas Hochhaus¹², Timothy P Hughes^{20

21

22}; International CML Foundation Genomics Alliance

Affiliations

¹ Department of Genetics and Molecular Pathology, Centre for Cancer Biology, SA Pathology, Adelaide, Australia. susan.branford@sa.gov.au.
² School of Pharmacy and Medical Science, University of South Australia, Adelaide, Australia. susan.branford@sa.gov.au.
³ School of Medicine, University of Adelaide, Adelaide, Australia. susan.branford@sa.gov.au.
⁴ Department of Medical Oncology and Hematology, Princess Margaret Cancer Centre, University Health Network, University of Toronto, Toronto, Canada.
⁵ Centre for Haematology, Hammersmith Hospital, Imperial College, London, UK.
⁶ Division of Hematology and Medical Oncology, Oregon Health & Science University Knight Cancer Institute, Portland, OR, USA.
⁷ Howard Hughes Medical Institute, Portland, 97239, OR, USA.
⁸ Hematology Research Unit Helsinki, Helsinki University Hospital Comprehensive Cancer Center, Helsinki, Finland.
⁹ Translational Immunology Research Program and Department of Clinical Chemistry and Hematology, University of Helsinki, Helsinki, Finland.
¹⁰ Cancer and Stem Cell Biology Signature Research Program, Duke-NUS Medical School, Singapore, Singapore.
¹¹ Department of Haematology, Singapore General Hospital, Singapore, Singapore.
¹² Abteilung Hämatologie und Internistische Onkologie, Klinik für Innere Medizin II, Universitätsklinikum Jena, Jena, Germany.
¹³ University of Milano Bicocca, San Gerardo Hospital, Monza, Italy.
¹⁴ Myeloproliferative Neoplasms Program, Leukemia Service, Memorial Sloan Kettering Cancer Center, New York, NY, USA.
¹⁵ Catholic Leukemia Research Institute, The Catholic University of Korea, Seoul, Korea.
¹⁶ Department of Hematology, Seoul St. Mary's Hospital, The Catholic University of Korea, Seoul, Korea.
¹⁷ Bergonié Cancer Institute, Inserm Unit 916, University of Bordeaux, Bordeaux, France.
¹⁸ Department of Leukemia, The University of Texas MD Anderson Cancer Center, Houston, TX, USA.
¹⁹ Fred Hutchinson Cancer Research Center, Seattle, WA, USA.
²⁰ School of Medicine, University of Adelaide, Adelaide, Australia.
²¹ South Australian Health & Medical Research Institute, Adelaide, Australia.
²² Department of Haematology, SA Pathology, Adelaide, Australia.

Abstract

Outcomes for patients with chronic myeloid leukemia (CML) have substantially improved due to advances in drug development and rational treatment intervention strategies. Despite these significant advances there are still unanswered questions on patient management regarding how to more reliably predict treatment failure at the time of diagnosis and how to select frontline tyrosine kinase inhibitor (TKI) therapy for optimal outcome. The BCR-ABL1 transcript level at diagnosis has no established prognostic impact and cannot guide frontline TKI selection. BCR-ABL1 mutations are detected in ~50% of TKI resistant patients but are rarely responsible for primary resistance. Other resistance mechanisms are largely uncharacterized and there are no other routine molecular testing strategies to facilitate the evaluation and further stratification of TKI resistance. Advances in next-generation sequencing technology has aided the management of a growing number of other malignancies, enabling the incorporation of somatic mutation profiles in diagnosis, classification, and prognostication. A largely unexplored area in CML research is whether expanded genomic analysis at diagnosis, resistance, and disease transformation can enhance patient management decisions, as has occurred for other cancers. The aim of this article is to review publications that reported mutated cancer-associated genes in CML patients at various disease phases. We discuss the frequency and type of such variants at initial diagnosis and at the time of treatment failure and transformation. Current limitations in the evaluation of mutants and recommendations for future reporting are outlined. The collective evaluation of mutational studies over more than a decade suggests a limited set of cancer-associated genes are indeed recurrently mutated in CML and some at a relatively high frequency. Genomic studies have the potential to lay the foundation for improved diagnostic risk classification according to clinical and genomic risk, and to enable more precise early identification of TKI resistance.

Publication types

Research Support, Non-U.S. Gov't
Review

MeSH terms

Genes, Neoplasm
Hematopoiesis
Humans
Leukemia, Myelogenous, Chronic, BCR-ABL Positive / drug therapy
Leukemia, Myelogenous, Chronic, BCR-ABL Positive / etiology
Leukemia, Myelogenous, Chronic, BCR-ABL Positive / genetics*
Mutation
Protein Kinase Inhibitors / therapeutic use
Protein-Tyrosine Kinases / antagonists & inhibitors
Repressor Proteins / genetics
Risk Assessment

Substances

ASXL1 protein, human
Protein Kinase Inhibitors
Repressor Proteins
Protein-Tyrosine Kinases

Abstract

Publication types

MeSH terms

Substances

Grants and funding