Quantitative modeling of chronic myeloid leukemia: insights from radiobiology

Radivoyevitch, Tomas; Hlatky, Lynn; Landaw, Julian; Sachs, Rainer K.

doi:10.1182/blood-2011-09-381855

Cited by 24 publications

(14 citation statements)

References 94 publications

(136 reference statements)

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“…Sampling from a distribution of CML latency times as reported by Radivoyevitch et al . 27 [median latency time = 6.9 years, IQR (5.0,10.1)] ( Online Supplementary Figure S6B ) and taking into account the observed TKI response, we obtained an individual distribution of possible proliferation rates p Y for each patient ( Online Supplementary Figure S6C ). In other words, we fit our mathematical model several times under different, plausible assumptions about the aggressiveness of the underlying leukemia.…”

Section: Resultsmentioning

confidence: 99%

Reduced tyrosine kinase inhibitor dose is predicted to be as effective as standard dose in chronic myeloid leukemia: a simulation study based on phase III trial data

et al. 2018

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Continuing tyrosine kinase inhibitor (TKI)-mediated targeting of the BCR-ABL1 oncoprotein is the standard therapy for chronic myeloid leukemia (CML) and allows for a sustained disease control in the majority of patients. While therapy cessation for patients appeared as a safe option for about half of those patients with optimal response, no systematic assessment of long-term TKI dose de-escalation has been made. We use a mathematical model to analyze and consistently describe biphasic treatment responses from TKI-treated patients from two independent clinical phase III trials. Scale estimates reveal that drug efficiency determines the initial response while the long-term behavior is limited by the rare activation of leukemic stem cells. We use this mathematical framework to investigate the influence of different dosing regimens on the treatment outcome. We provide strong evidence to suggest that TKI dose de-escalation (at least 50%) does not lead to a reduction of long-term treatment efficiency for most patients, who have already achieved sustained remission, and maintains the secondary decline of BCR-ABL1 levels. We demonstrate that continuous BCR-ABL1 monitoring provides patient-specific predictions of an optimal reduced dose without decreasing the anti-leukemic effect on residual leukemic stem cells. Our results are consistent with the interim results of the DESTINY trial and provide clinically testable predictions. Our results suggest that dose-halving should be considered as a long-term treatment option for CML patients with good response under continuing maintenance therapy with TKIs. We emphasize the clinical potential of this approach to reduce treatment-related side-effects and treatment costs.

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Section: Resultsmentioning

confidence: 99%

Reduced tyrosine kinase inhibitor dose is predicted to be as effective as standard dose in chronic myeloid leukemia: a simulation study based on phase III trial data

et al. 2018

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“…In patients with blood cancers, the observation of normal blood counts months to years prior to diagnosis has led to the prediction that tumour development occurs quickly, and therefore driver mutations must occur late in life. Estimates from cancer incidences in Japanese atomic survivors who developed chronic myeloid leukaemia have suggested a mean latency time of only 8 years between BCR-ABL1 induction and clinical presentation 6 . However, the presence of driver mutations in normal tissues [7][8][9][10][11][12] , including blood from healthy individuals who harbor age-related clonal haematopoiesis (CH) [13][14][15][16][17] , some of whom subsequently develop malignancies, supports a longer multi-hit evolutionary trajectory of cancer.…”

Section: Introductionmentioning

confidence: 99%

Phylogenetic reconstruction of myeloproliferative neoplasm reveals very early origins and lifelong evolution

Williams

Lee

Moore

et al. 2020

Preprint

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Mutations in cancer-associated genes drive tumour outgrowth. However, the timing of driver mutations and dynamics of clonal expansion that lead to human cancers are largely unknown. We used 448,553 somatic mutations from whole-genome sequencing of 843 clonal haematopoietic colonies to reconstruct the phylogeny of haematopoiesis, from embryogenesis to clinical disease, in 10 patients with myeloproliferative neoplasms which are blood cancers more common in older age. JAK2V617F, the pathognomonic mutation in these cancers, was acquired in utero or childhood, with upper estimates of age of acquisition ranging between 4.1 months and 11.4 years across 5 patients. DNMT3A mutations, which are associated with age-related clonal haematopoiesis, were also acquired in utero or childhood, by 7.9 weeks of gestation to 7.8 years across 4 patients. Subsequent driver mutation acquisition was separated by decades. The mean latency between JAK2V617F acquisition and clinical presentation was 31 years (range 12-54 years). Rates of clonal expansion varied substantially (<10% to >200% expansion/year), were affected by additional driver mutations, and predicted latency to clinical presentation. Driver mutations and rates of expansion would have been detectable in blood one to four decades before clinical presentation. This study reveals how driver mutation acquisition very early in life with life-long growth and evolution drive adult blood cancer, providing opportunities for early detection and intervention, and a new paradigm for cancer development.

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“…Because CML is a comparatively well-characterized neoplasm, many mechanistic mathematical models of CML have been developed (Radivoyevitch et al 2012). …”

Section: Introductionmentioning

confidence: 99%

Sex differences in the incidence of chronic myeloid leukemia

Radivoyevitch

Janković²,

Tiu

et al. 2013

Radiat Environ Biophys

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The incidence of chronic myeloid leukemia (CML), which is caused by BCR/ABL chimeric oncogene formation in a pluripotent hematopoietic stem cell (HSC), increases with age and exposure to ionizing radiation. CML is a comparatively well-characterized neoplasm, important for its own sake and useful for insights into other neoplasms. Here, Surveillance, Epidemiology and End Results (SEER) CML data are analyzed after considering possible misclassification of chronic myelo-monocytic leukemia as CML. For people older than 25 years, plots of male and female CML log incidences versus age at diagnosis are approximately parallel straight lines with males either above or to the left of females. This is consistent with males having a higher risk of developing CML or a shorter latency from initiation to diagnosis of CML. These distinct mechanisms cannot be distinguished using SEER data alone. Therefore, CML risks among male and female Japanese A-bomb survivors are also analyzed. The present analyses suggest that sex differences in CML incidence more likely result from differences in risk than in latency. The simplest but not the sole interpretation of this is that males have more target cells at risk to develop CML. Comprehensive mathematical models of CML could lead to a better understanding of the role of HSCs in CML and other preleukemias that can progress to acute leukemia.

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Quantitative modeling of chronic myeloid leukemia: insights from radiobiology

Cited by 24 publications

References 94 publications

Reduced tyrosine kinase inhibitor dose is predicted to be as effective as standard dose in chronic myeloid leukemia: a simulation study based on phase III trial data

Reduced tyrosine kinase inhibitor dose is predicted to be as effective as standard dose in chronic myeloid leukemia: a simulation study based on phase III trial data

Phylogenetic reconstruction of myeloproliferative neoplasm reveals very early origins and lifelong evolution

Sex differences in the incidence of chronic myeloid leukemia

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