Validation of CIP2A as a Biomarker of Subsequent Disease Progression and Treatment Failure in Chronic Myeloid Leukaemia

It would be clinically useful to prospectively identify the risk of disease progression in chronic myeloid leukaemia (CML). Overexpression of cancerous inhibitor of protein phosphatase 2A (PP2A) (CIP2A) protein is an adverse prognostic indicator in many cancers. We examined CIP2A protein levels in d...

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Published inCancers Vol. 13; no. 9; p. 2155
Main Authors Clark, Richard E, Basabrain, Ammar A, Austin, Gemma M, Holcroft, Alison K, Loaiza, Sandra, Apperley, Jane F, Law, Christopher, Scott, Laura, Parry, Alexandra D, Bonnett, Laura, Lucas, Claire M
Format Journal Article
LanguageEnglish
Published Switzerland MDPI AG 29.04.2021
MDPI
Subjects
AKT protein
Biobanks
Biomarkers
blast crisis
Chronic myeloid leukemia
CIP2A
CML
Cytogenetics
dasatinib
Enzyme inhibitors
Flow cytometry
Imatinib
Kinases
Leukemia
Medical research
Patients
Phosphatase
Phosphoprotein phosphatase
Protein phosphatase
Protein-tyrosine kinase
Proteins
Risk assessment
SPIRIT2
Survival
United Kingdom > UK
SPIRIT2
CML
dasatinib
imatinib
CIP2A
disease progression
blast crisis
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Summary:It would be clinically useful to prospectively identify the risk of disease progression in chronic myeloid leukaemia (CML). Overexpression of cancerous inhibitor of protein phosphatase 2A (PP2A) (CIP2A) protein is an adverse prognostic indicator in many cancers. We examined CIP2A protein levels in diagnostic samples from the SPIRIT2 trial in 172 unselected patients, of whom 90 received imatinib and 82 dasatinib as first-line treatment. High CIP2A levels correlated with inferior progression-free survival ( = 0.04) and with worse freedom from progression ( = 0.03), and these effects were confined to dasatinib recipients. High CIP2A levels were associated with a six-fold higher five-year treatment failure rate than low CIP2A levels (41% vs. 7.5%; = 0.0002), in both imatinib (45% vs. 11%; = 0.02) and dasatinib recipients (36% vs. 4%; = 0.007). Imatinib recipients with low CIP2A levels had a greater risk of treatment failure ( = 0.0008). CIP2A levels were independent of Sokal, Hasford, EUTOS (EUropean Treatment and Outcome Study), or EUTOS long-term survival scores (ELTS) or the presence of major route cytogenetic abnormalities. No association was seen between CIP2A levels and time to molecular response or the levels of the CIP2A-related proteins PP2A, SET, SET binding protein 1 (SETBP1), or AKT. These data confirm that high diagnostic CIP2A levels correlate with subsequent disease progression and treatment failure. CIP2A is a simple diagnostic biomarker that may be useful in planning treatment strategies.
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ISSN:2072-6694
2072-6694
DOI:10.3390/cancers13092155