Journal article

Targeted therapy and disease monitoring in CNTRL-FGFR1-driven leukaemia

LM Brown, RC Bartolo, NM Davidson, B Schmidt, I Brooks, J Challis, V Petrovic, DA Khuong-Quang, F Mechinaud, SL Khaw, IJ Majewski, A Oshlack, PG Ekert

Pediatric Blood and Cancer | WILEY | Published : 2019

DOI: 10.1002/pbc.27897

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Abstract

We report two patients with leukaemia driven by the rare CNTRL-FGFR1 fusion oncogene. This fusion arises from a t(8;9)(p12;q33) translocation, and is a rare driver of biphenotypic leukaemia in children. We used RNA sequencing to report novel features of expressed CNTRL-FGFR1, including CNTRL-FGFR1 fusion alternative splicing. From this knowledge, we designed and tested a Droplet Digital PCR assay that detects CNTRL-FGFR1 expression to approximately one cell in 100 000 using fusion breakpoint-specific primers and probes. We also utilised cell-line models to show that effective tyrosine kinase inhibitors, which may be included in treatment regimens for this disease, are only those that block F..

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Keywords

Science & Technology
3211 Oncology and Carcinogenesis
Orphan Drug
Oncology
Biotechnology
32 Biomedical and Clinical Sciences
Pediatric Research Initiative
Fgfr1
Genetics
Tyrosine Kinase
8p11 Myeloproliferative Syndrome
Hematology
Pediatrics
5.1 Pharmaceuticals
Fusion Gene
Minimal Residual Disease Monitoring
Fusion
Leukaemia
Disorder
Cancer
2.1 Biological and Endogenous Factors
4.1 Discovery and Preclinical Testing of Markers and Technologies
Life Sciences & Biomedicine
Rare Diseases
Targeted Therapies