2012
DOI: 10.1038/leu.2012.85
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Early molecular and cytogenetic response is predictive for long-term progression-free and overall survival in chronic myeloid leukemia (CML)

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Cited by 379 publications
(316 citation statements)
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“…In our experience, the proportions of patients who achieved an EMR and a deep EMR after 3 months of treatment were higher than those reported by Millot et al (2014) in a comparable cohort of children and similar to those observed in adults treated with high-dose IM (600-800 mg/daily) (Hanfstein et al, 2012;Jain et al, 2013;Deininger et al, 2014;Hughes et al, 2014). These findings suggest that IM exposure is an important factor influencing early treatment response in CP-CML patients.…”
contrasting
confidence: 52%
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“…In our experience, the proportions of patients who achieved an EMR and a deep EMR after 3 months of treatment were higher than those reported by Millot et al (2014) in a comparable cohort of children and similar to those observed in adults treated with high-dose IM (600-800 mg/daily) (Hanfstein et al, 2012;Jain et al, 2013;Deininger et al, 2014;Hughes et al, 2014). These findings suggest that IM exposure is an important factor influencing early treatment response in CP-CML patients.…”
contrasting
confidence: 52%
“…In our experience the BCR-ABL1 IS values at 3 months are not predictive of overall MMR, MR and CMR rates, or outcomes. Indeed, the PFS probabilities were not influenced by an EMR at 3 months, as reported both in adults treated with high-dose IM (Hanfstein et al, 2012;Jain et al, 2013;Deininger et al, 2014;Hughes et al, 2014) and in children receiving standard doses of IM (Millot et al, 2014).…”
mentioning
confidence: 58%
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“…Whereas approximately one‐third of patients with dose escalation due to BCR‐ABL1 IS > 10% at 3 months achieved MMR, ≈80% of those with dose escalation due to lack of MMR at 12 months or loss of MMR went on to achieve MMR after their dose was escalated. The importance of achieving BCR‐ABL1 IS  ≤ 10% at 3 months is well established (Hanfstein et al , 2012; Marin et al , 2012; Hughes et al , 2014a; Hochhaus et al , 2016b), and this response milestone has been incorporated into CML management guidelines from the European LeukemiaNet and the National Comprehensive Cancer Network (Baccarani et al , 2013; National Comprehensive Cancer Network, 2017); however, optimal management strategies for patients who do not meet this milestone remain unclear. Overall among patients with BCR‐ABL1 IS  > 10% at 3 months (regardless of dose escalation), the rate of MMR by 24 months (36·1%) was comparable to that in the nilotinib 300‐mg twice‐daily arm of ENESTnd (29%) (Hughes et al , 2014a).…”
Section: Discussionmentioning
confidence: 99%
“…Several clinical studies have demonstrated that achievement of early molecular responses (e.g., BCR-ABL1 transcript reduction to 10% after 3 months of TKI therapy) is associated with improved [22,32], patients treated with nilotinib following imatinib resistance or intolerance [33], and patients treated with second-line nilotinib or dasatinib [34]. Achievement of MMR is associated with improved survival, and achievement of deeper molecular responses beyond MMR may also be associated with improved long-term outcomes.…”
Section: Importance Of Achieving Deep Molecular Responses To Tki Therapymentioning
confidence: 99%