Systemic Exposure to Thiopurines and Risk of Relapse in Children With Acute Lymphoblastic Leukemia

Bhatia, Smita; Landier, Wendy; Hageman, Lindsey; Chen, Yanjun; Kim, Heeyoung; Sun, Can Lan; Kornegay, Nancy; Evans, William E.; Angiolillo, Anne; Bostrom, Bruce; Casillas, Jacqueline; Lew, Glen; Maloney, Kelly W.; Mascarenhas, Leo; Ritchey, A. Kim; Termuhlen, Amanda; Carroll, William L.; Wong, F. Lennie; Relling, Mary V.

doi:10.1001/jamaoncol.2015.0245

Cited by 122 publications

(167 citation statements)

References 28 publications

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“…Although the participation rate of study participants across the 87 participating institutions is not available, we have previously shown that the AALL03N1 study participants were comparable to patients enrolled on the relevant parent COG therapeutic first-line ALL protocols. 15 Only patients who had both evaluable MEMS and self-report data were included in this analysis.…”

Section: Study Participantsmentioning

confidence: 99%

Comparison of self-report and electronic monitoring of 6MP intake in childhood ALL: a Children’s Oncology Group study

Landier

Chen

Hageman

et al. 2017

Blood

Self Cite

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• Self-report overestimated electronically monitored 6MP adherence at least some of the time in a large majority of patients (84.4%).• Nonadherers were more likely to overreport 6MP intake (47%) compared with adherent patients (8%).Adequate exposure to oral 6-mercaptopurine (6MP) during maintenance therapy for childhood acute lymphoblastic leukemia (ALL) is critical for sustaining durable remissions; accuracy of self-reported 6MP intake is unknown. We aimed to directly compare self-report to electronic monitoring (Medication Event Monitoring System [MEMS]) and identify predictors of overreporting in a cohort of 416 children with ALL in first remission over 4 study months (1344 patient-months for the cohort) during maintenance therapy. Patients were classified as "perfect reporters" (self-report agreed with MEMS), "overreporters" (self-report was higher than MEMS by ‡5 days/month for ‡50% of study months), and "others" (not meeting criteria for perfect reporter or overreporter). Multivariable logistic regression examined sociodemographic and clinical characteristics, 6MP dose intensity, TPMT genotype, thioguanine nucleotide levels, and 6MP nonadherence (MEMS-based adherence <95%) associated with the overreporter phenotype; generalized estimating equations compared 6MP intake by self-report and MEMS. Self-reported 6MP intake exceeded MEMS at least some of the time in 84% of patients. Fifty patients (12%) were classified as perfect reporters, 98 (23.6%) as overreporters, 2 (0.5%) as underreporters, and 266 (63.9%) as others. In multivariable analysis, the following variables were associated with the overreporter phenotype: non-white race: Hispanic, odds ratio (OR), 2.4, P 5 .02; Asian, OR, 3.1, P 5 .02; African American, P < .001; paternal education less than college (OR, 1.4, P 5 .05);

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Section: Study Participantsmentioning

confidence: 99%

Comparison of self-report and electronic monitoring of 6MP intake in childhood ALL: a Children’s Oncology Group study

Landier

Chen

Hageman

et al. 2017

Blood

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“…These include inferior geographic access to care, 3 insurance, 3 tolerance of therapy, 4 and treatment adherence. 5 There appear to be biological differences in some histologically similar malignancies presenting in pediatric, AYA, and older patients. 6 In addition, there likely are substantial developmental differences in pharmacokinetics/pharmacodynamics that influence toxicity and efficacy.…”

Section: Introductionmentioning

confidence: 99%

Enhancing Adolescent and Young Adult Oncology Research Within the National Clinical Trials Network: Rationale, Progress, and Emerging Strategies

Weiss

Nichols

Freyer

2015

Seminars in Oncology

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Adolescent and young adult oncology (AYAO, including patients 15-39 years of age) is an emerging discipline in the field of cancer treatment and research. Poorer survival outcomes for this population and characteristic age-related challenges in care have called attention to the need for increased AYAO research. This chapter outlines pressing questions and reviews recent progress in AYAO research within the current organizational structure of the federal clinical trials enterprise, emphasizing how the United States National Cancer Institute's National Clinical Trials Network (NCTN) has created novel opportunities for collaborative AYAO research among the pediatric and adult NCTN groups. Potential strategies for expanding collaborative AYAO research, both within the NCTN and with other partners in the federal and advocacy domains are identified.

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“…Anyway, the CACE approach was used to estimate the true effect in the presence of noncompliance. 32 The current EFS results do not support the routine use of cyclophosphamide and methotrexate as metronomic agents after standard chemotherapy for nonmetastatic OST. Compliance is a major concern when one considers cancer treatments and more specifically long-term treatments.…”

Section: Discussionmentioning

confidence: 60%

Results of a randomized, prospective clinical trial evaluating metronomic chemotherapy in nonmetastatic patients with high‐grade, operable osteosarcomas of the extremities: A report from the Latin American Group of Osteosarcoma Treatment

Senerchia

Macedo

Ferman

et al. 2016

Cancer

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Systemic Exposure to Thiopurines and Risk of Relapse in Children With Acute Lymphoblastic Leukemia

Cited by 122 publications

References 28 publications

Comparison of self-report and electronic monitoring of 6MP intake in childhood ALL: a Children’s Oncology Group study

Comparison of self-report and electronic monitoring of 6MP intake in childhood ALL: a Children’s Oncology Group study

Enhancing Adolescent and Young Adult Oncology Research Within the National Clinical Trials Network: Rationale, Progress, and Emerging Strategies

Results of a randomized, prospective clinical trial evaluating metronomic chemotherapy in nonmetastatic patients with high‐grade, operable osteosarcomas of the extremities: A report from the Latin American Group of Osteosarcoma Treatment

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