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Intracellular cytarabine triphosphate in circulating blasts post-treatment predicts remission status in patients with acute myeloid leukemia

Anderson, Elizabeth; Rees, Barbara; Hull, Jonathon; Heywood, Jonathan; Preston, Andrea; Protheroe, Rachel; Foulstone, E.; Greenwood, Rosemary; Salisbury, Vyv; Mehta, Priyanka

Authors

Barbara Rees

Profile image of Jonathon Hull

Jonathon Hull Jonathon2.Hull@uwe.ac.uk
Senior Lecturer in Biomedical Sci (Biochemistry)

Jonathan Heywood

Andrea Preston

Rachel Protheroe

E. Foulstone

Rosemary Greenwood

Vyv Salisbury

Priyanka Mehta



Abstract

© 2019 Cytarabine remains the backbone of therapy in acute myeloid leukemia (AML). The ability to assess intracellular cytarabine triphosphate (ara-CTP) levels in patients receiving cytarabine represents a major goal in the prediction of treatment response. This study, conducted within a clinical setting, aimed to assess ara-CTP levels in circulating peripheral blasts from non-M3 AML patients receiving cytarabine at one of three dosing levels, using a novel biosensor assay. Results from the initial 72 hours post-commencement were correlated with day 28 remission status, with feasibility parameters concurrently assessed. Intracellular ara-CTP was detectable in ex vivo blasts post-treatment for standard-dose (SD) and high-dose (HD) patients (p < 0.05), and quantification revealed a 27-fold increase in intracellular steady-state concentration between the two dosing levels. For low-dose cytarabine, high rates of patient discharge and low intracellular concentrations limited analysis; however, assessment of intracellular ara-CTP concentration was achievable in a dwindling population of blasts for SD and HD treatment cohorts, with 4 hours post-treatment commencement potentially being most predictive of clinical response (r = –0.912, p = 0.0113). Concurrent assessment of peripheral leukemia-associated immunophenotype (LAIP)-positive cells revealed a decline in burden (0–72 hours), which correlated with remission status (p < 0.05). Unexpectedly high rates of night sampling led to challenges associated with sampling rates, but did not have an impact on patient compliance. Additional training of night staff improved feasibility substantially. Multiple peripheral sampling during the initial 72 hours of treatment is feasible in newly diagnosed patients, and ara-CTP is detectable over the initial 24 hours, facilitating prediction of chemosensitivity of leukemic blasts to cytarabine.

Journal Article Type Article
Acceptance Date Apr 25, 2019
Online Publication Date May 2, 2019
Publication Date Jun 1, 2019
Deposit Date Apr 29, 2019
Publicly Available Date May 3, 2020
Journal Experimental Hematology
Print ISSN 0301-472X
Electronic ISSN 1873-2399
Publisher Elsevier
Peer Reviewed Peer Reviewed
Volume 74
Pages 13-18.e3
DOI https://doi.org/10.1016/j.exphem.2019.04.005
Public URL https://uwe-repository.worktribe.com/output/847364
Publisher URL https://doi.org/10.1016/j.exphem.2019.04.005
Additional Information Additional Information : This is the author's accepted manuscript. The final published version is available here: https://doi.org/10.1016/j.exphem.2019.04.005
Contract Date Apr 29, 2019

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