Your search keyword '"Balis FM"' showing total 277 results

1. Clinical Drug Development for Childhood Cancers

Author

Balis, FM, primary, Fox, E, additional, Widemann, BC, additional, and Adamson, PC, additional

Published

2009

2. 92. Capacity-limited metabolism of all-trans-retinoic add and the time course of enzyme induction of the non-human primate

Author

Adamson, PC, primary, Balis, FM, additional, Smith, MA, additional, Murphy, RF, additional, Godwin, KA, additional, Boylan, JF, additional, Gudas, LJ, additional, and Poplack, DG, additional

Published

1992

3. A phase I trial and pharmacokinetic study of a 24-hour infusion of trabectedin (Yondelis®, ET-743) in children and adolescents with relapsed or refractory solid tumors.

Author

Chuk MK, Aikin A, Whitcomb T, Widemann BC, Zannikos P, Bayever E, Balis FM, Fox E, Chuk, Meredith K, Aikin, Alberta, Whitcomb, Trish, Widemann, Brigitte C, Zannikos, Peter, Bayever, Eliel, Balis, Frank M, and Fox, Elizabeth

Published

2012

4. Plasma and CNS pharmacokinetics of O4-benzylfolic acid (O4BF) and metabolite in a non-human primate model.

Author

Chuk MK, Cole DE, McCully C, Loktionova NA, Pegg AE, Parker RJ, Pauly G, Widemann BC, Balis FM, Fox E, Chuk, Meredith K, Cole, Diane E, McCully, Cynthia, Loktionova, Natalia A, Pegg, Anthony E, Parker, Robert J, Pauly, Gary, Widemann, Brigitte C, Balis, Frank M, and Fox, Elizabeth

Abstract

Purpose: O(6)-alkylguanine-DNA alkyltransferase (AGT) repairs DNA damage from alkylating agents by transferring the alkyl adducts from the O(6)-position of guanine in DNA to AGT. The folate analog O(4)-benzylfolic acid (O(4)BF) is an inhibitor of AGT with reported selectivity of the alpha-folate receptor in tumors. We studied plasma and cerebrospinal fluid (CSF) pharmacokinetics and CSF penetration of O(4)BF in a non-human primate model.Methods: Rhesus monkeys (Macaca mulatta) received O(4)BF (10-50 mg/kg) intravenously, and serial blood and CSF samples were obtained. Analyte concentrations in plasma were measured by HPLC/photo diode array, and an HPLC/MS/MS assay was used for CSF samples.Results: A putative metabolite of O(4)BF was detected in plasma and CSF. O(4)BF and the metabolite inactivated purified AGT with ED(50) of 0.04 mcM. The median clearance of O(4)BF was 8 ml/min/kg and half-life was 1.1 h. The metabolite had a substantially longer half-life (>20 h) and greater AUC than O(4)BF. The AUC of the metabolite increased disproportionately to the dose of O(4)BF, suggesting saturable elimination. CSF penetration of O(4)BF and its metabolite was < 1%. At the 50 mg/kg dose level, the C(max) in CSF for O(4)BF was less than 0.09 mcM and for the metabolite the C(max) ranged from 0.02 to 0.04 mcM (O(4)BF equivalents).Conclusions: Concentrations of O(4)BF and the metabolite in CSF exceeded the ED(50) of AGT; however, recently reported lack of receptor specificity and pharmacokinetic data suggesting saturable elimination of both O(4)BF and its metabolite may limit dose-escalation and future clinical development of this agent. [ABSTRACT FROM AUTHOR]

Published

2011

5. A phase 1 trial and pharmacokinetic study of cediranib, an orally bioavailable pan-vascular endothelial growth factor receptor inhibitor, in children and adolescents with refractory solid tumors.

Author

Fox E, Aplenc R, Bagatell R, Chuk MK, Dombi E, Goodspeed W, Goodwin A, Kromplewski M, Jayaprakash N, Marotti M, Brown KH, Wenrich B, Adamson PC, Widemann BC, Balis FM, Fox, Elizabeth, Aplenc, Richard, Bagatell, Rochelle, Chuk, Meredith K, and Dombi, Eva

Published

2010

6. Pharmacokinetics of temozolomide administered in combination with O6-benzylguanine in children and adolescents with refractory solid tumors.

Author

Meany HJ, Warren KE, Fox E, Cole DE, Aikin AA, Balis FM, Meany, Holly J, Warren, Katherine E, Fox, Elizabeth, Cole, Diane E, Aikin, Alberta A, and Balis, Frank M

Abstract

Purpose: Temozolomide pharmacokinetics were evaluated in children receiving concurrent O(6)-benzylguanine (O(6)BG), which enhanced the hematological toxicity of temozolomide.Methods: Temozolomide was administered orally, daily for 5 days starting at 28 mg/m(2) per day with escalations to 40, 55, 75 and 100 mg/m(2) per day with O(6)BG intravenously daily for 5 days at doses of 60, 90 or 120 mg/m(2) per day. Plasma samples were drawn over 48 h after the day 5 dose. Temozolomide was quantified with a validated HPLC/tandem mass spectroscopic assay.Results: Temozolomide was rapidly absorbed (mean T (max), 2.1 h). The mean apparent clearance (CL/F) (96 mL/min/m(2)) was similar to the CL/F for temozolomide alone and was not age- or gender-dependent. There was minimal inter-patient variability.Conclusions: The enhanced hematologic toxicity resulting from combining O(6)BG with temozolomide does not appear to be the result of a pharmacokinetic interaction between the agents. [ABSTRACT FROM AUTHOR]

Published

2009

7. Characteristics of children enrolled in treatment trials for NF1-related plexiform neurofibromas.

Author

Kim A, Gillespie A, Dombi E, Goodwin A, Goodspeed W, Fox E, Balis FM, Widemann BC, Kim, A, Gillespie, A, Dombi, E, Goodwin, A, Goodspeed, W, Fox, E, Balis, F M, and Widemann, B C

Published

2009

8. Phase I trial and pharmacokinetic study of ixabepilone administered daily for 5 days in children and adolescents with refractory solid tumors.

Author

Widemann BC, Goodspeed W, Goodwin A, Fojo T, Balis FM, Fox E, Widemann, Brigitte C, Goodspeed, Wendy, Goodwin, Anne, Fojo, Tito, Balis, Frank M, and Fox, Elizabeth

Published

2009

9. A phase 2 trial of all-trans-retinoic acid in combination with interferon-alpha2a in children with recurrent neuroblastoma or Wilms tumor: A Pediatric Oncology Branch, NCI and Children's Oncology Group Study.

Author

Adamson PC, Matthay KK, O'Brien M, Reaman GH, Sato JK, Balis FM, Adamson, Peter C, Matthay, Katherine K, O'Brien, Michelle, Reaman, Gregory H, Sato, Judith K, and Balis, Frank M

Published

2007

10. Substitution of oral and intravenous thioguanine for mercaptopurine in a treatment regimen for children with standard risk acute lymphoblastic leukemia: a collaborative Children's Oncology Group/National Cancer Institute pilot trial (CCG-1942)

Author

Jacobs SS, Stork LC, Bostrom BC, Hutchinson R, Holcenberg J, Reaman GH, Erdmann G, Franklin J, Neglia JP, Steinberg SM, Balis FM, and Adamson PC

Published

2007

11. Expression of the mdr-1/P-170 gene in patients with acute lymphoblastic leukemia

Author

Rothenberg, ML, Mickley, LA, Cole, DE, Balis, FM, Tsuruo, T, Poplack, DG, and Fojo, AT

Abstract

Increased expression of the multidrug resistance gene (mdr-1/P-170) and the dihydrofolate reductase (DHFR) gene have been implicated in the development of in vitro drug resistance. Overexpression, with or without gene amplification, is seen in the development of drug resistance in culture and it has been postulated that genetic modulation of mdr-1/P-170 and DHFR may also be involved in the development of clinical drug resistance. We screened lymphoblasts from 28 patients with acute lymphoblastic leukemia (ALL) for evidence of overexpression of mdr-1/P-170 using RNAse protection, RNA in situ hybridization and immunohistochemistry. Overexpression of mdr-1/P-170 without gene amplification was detected in samples from four patients (three after multiple relapses, one at presentation). Overexpression of mdr-1/P-170 was heterogeneous within the population of malignant lymphoblasts as demonstrated by RNA in situ hybridization, immunohistochemistry, and drug uptake using daunomycin autofluorescence analysis. There was no evidence of overexpression of DHFR in any of the eight patient samples tested by RNAse protection nor was there any evidence of gene amplification in 11 patient samples on Southern blot analysis. From these observations it appears that overexpression without gene amplification of mdr-1/P-170 may be one mechanism of clinical drug resistance in ALL.

Published

1989

12. Effect of continuous intravenous infusion of zidovudine (AZT) in children with symptomatic HIV infection

Author

Pizzo, PA, primary, Eddy, J, additional, Falloon, J, additional, Balis, FM, additional, Murphy, RF, additional, Moss, H, additional, Wolters, P, additional, Brouwers, P, additional, Jarosinski, P, additional, Rubin, M, additional, Broder, S, additional, Yarchoan, R, additional, Brunetti, A, additional, Maha, M, additional, Nusinoff-Lehrman, S, additional, and Poplack, DG, additional

Published

1989

13. Tenofovir disoproxil fumarate and an optimized background regimen of antiretroviral agents as salvage therapy for pediatric HIV infection.

Author

Hazra R, Gafni RI, Maldarelli F, Balis FM, Tullio AN, DeCarlo E, Worrell CJ, Steinberg SM, Flaherty J, Yale K, Kearney BP, and Zeichner SL

Published

2005

14. Roadmap for the next generation of Children's Oncology Group rhabdomyosarcoma trials.

Author

Metts JL, Aye JM, Crane JN, Oberoi S, Balis FM, Bhatia S, Bona K, Carleton B, Dasgupta R, Dela Cruz FS, Greenzang KA, Kaufman JL, Linardic CM, Parsons SK, Robertson-Tessi M, Rudzinski ER, Soragni A, Stewart E, Weigel BJ, Wolden SL, Weiss AR, Venkatramani R, and Heske CM

Subjects

Child, Humans, Clinical Trials as Topic, Quality of Life, Rhabdomyosarcoma diagnosis, Rhabdomyosarcoma drug therapy

Abstract

Clinical trials conducted by the Intergroup Rhabdomyosarcoma (RMS) Study Group and the Children's Oncology Group have been pivotal to establishing current standards for diagnosis and therapy for RMS. Recent advancements in understanding the biology and clinical behavior of RMS have led to more nuanced approaches to diagnosis, risk stratification, and treatment. The complexities introduced by these advancements, coupled with the rarity of RMS, pose challenges to conducting large-scale phase 3 clinical trials to evaluate new treatment strategies for RMS. Given these challenges, systematic planning of future clinical trials in RMS is paramount to address pertinent questions regarding the therapeutic efficacy of drugs, biomarkers of response, treatment-related toxicity, and patient quality of life. Herein, the authors outline the proposed strategic approach of the Children's Oncology Group Soft Tissue Sarcoma Committee to the next generation of RMS clinical trials, focusing on five themes: improved novel agent identification and preclinical to clinical translation, more efficient trial development and implementation, expanded opportunities for knowledge generation during trials, therapeutic toxicity reduction and quality of life, and patient engagement., (© 2024 American Cancer Society.)

Published

2024

15. Population modeling analyses of crizotinib in pediatric patients with ALK-positive advanced cancers.

Author

Jerry L, Swan L, Dana N, Balis FM, Greengard E, and Huiping X

Subjects

Humans, Child, Female, Male, Adolescent, Child, Preschool, Neoplasms drug therapy, Neoplasms pathology, Lymphoma, Large-Cell, Anaplastic drug therapy, Lymphoma, Large-Cell, Anaplastic pathology, Young Adult, Infant, Crizotinib therapeutic use, Crizotinib pharmacokinetics, Anaplastic Lymphoma Kinase antagonists & inhibitors, Anaplastic Lymphoma Kinase genetics, Protein Kinase Inhibitors therapeutic use, Protein Kinase Inhibitors pharmacokinetics, Protein Kinase Inhibitors adverse effects

Abstract

Background: Alterations in the ALK (anaplastic lymphoma kinase) gene play a critical role in pathogenesis of anaplastic large cell lymphoma (ALCL). Crizotinib is a small molecule competitive inhibitor of ALK, ROS1, and MET kinases and was approved for pediatric patients with ALK-positive relapsed or refractory, systemic ALCL, and ALK-positive unresectable, recurrent, or refractory inflammatory myofibroblastic tumors (IMT)., Procedure: Crizotinib data from pediatric patients with relapsed or refractory solid tumors, IMT, or ALCL were included in the analyses. All patients received crizotinib orally at doses ranging from 100 to 365 mg/m 2 twice daily (BID). PopPK analyses were conducted to characterize crizotinib disposition in pediatric patients. Exposure-response (ER) safety and antitumor analyses were conducted to characterize relationships between crizotinib dose or exposure with safety and antitumor activity endpoints of interest., Results: The population pharmacokinetic (popPK), ER safety, and ER antitumor analysis included 98, 110, and 36 pediatric patients, respectively. A one-compartment pharmacokinetic model with allometric scaling, first-order elimination, and first-order absorption with lag time adequately described the data. Natural log-transformed model-predicted crizotinib AUC ss (steady-state area under the concentration-time curve) demonstrated a significant, positive relationship with Grade ≥3 NEUTROPENIA and Any Grade VISION DISORDER. Crizotinib dose demonstrated a positive relationship with objective response rate., Conclusions: No significant differences in PK were identified across a wide range of ages or across tumor types, suggesting body surface area (BSA)-based dosing adequately adjusted for differences in patient size to achieve similar systemic crizotinib exposures across young children and adolescent pediatric patients. None of the myelosuppressive events except Grade ≥3 NEUTROPENIA had significant relationships identified with crizotinib dose or exposure, suggesting crizotinib is a tolerable treatment with less hematological toxicity than traditional chemotherapy regimens for pediatric patients with ALK-mutated cancers. Results from the presented analyses support the pediatric dosing recommendations in the product label., (© 2024 Wiley Periodicals LLC.)

Published

2024

16. Phase 1 study of high-dose DFMO, celecoxib, cyclophosphamide and topotecan for patients with relapsed neuroblastoma: a New Approaches to Neuroblastoma Therapy trial.

Author

Hogarty MD, Ziegler DS, Franson A, Chi YY, Tsao-Wei D, Liu K, Vemu R, Gerner EW, Bruckheimer E, Shamirian A, Hasenauer B, Balis FM, Groshen S, Norris MD, Haber M, Park JR, Matthay KK, and Marachelian A

Subjects

Child, Humans, Antineoplastic Combined Chemotherapy Protocols adverse effects, Celecoxib therapeutic use, Cyclophosphamide therapeutic use, Topotecan therapeutic use, Child, Preschool, Adolescent, Young Adult, Adult, Neoplasm Recurrence, Local drug therapy, Neuroblastoma drug therapy, Neuroblastoma genetics

Abstract

Background: MYC genes regulate ornithine decarboxylase (Odc) to increase intratumoral polyamines. We conducted a Phase I trial [NCT02030964] to determine the maximum tolerated dose (MTD) of DFMO, an Odc inhibitor, with celecoxib, cyclophosphamide and topotecan., Methods: Patients 2-30 years of age with relapsed/refractory high-risk neuroblastoma received oral DFMO at doses up to 9000 mg/m 2 /day, with celecoxib (500 mg/m 2 daily), cyclophosphamide (250 mg/m 2 /day) and topotecan (0.75 mg/m 2 /day) IV for 5 days, for up to one year with G-CSF support., Results: Twenty-four patients (median age, 6.8 years) received 136 courses. Slow platelet recovery with 21-day courses (dose-levels 1 and 2) led to subsequent dose-levels using 28-day courses (dose-levels 2a-4a). There were three course-1 dose-limiting toxicities (DLTs; hematologic; anorexia; transaminases), and 23 serious adverse events (78% fever-related). Five patients (21%) completed 1-year of therapy. Nine stopped for PD, 2 for DLT, 8 by choice. Best overall response included two PR and four MR. Median time-to-progression was 19.8 months, and 3 patients remained progression-free at >4 years without receiving additional therapy. The MTD of DFMO with this regimen was 6750 mg/m 2 /day., Conclusion: High-dose DFMO is tolerable when added to chemotherapy in heavily pre-treated patients. A randomized Phase 2 trial of DFMO added to chemoimmunotherapy is ongoing [NCT03794349]., (© 2024. The Author(s).)

Published

2024

17. Altered Peripheral Blood Gene Expression in Childhood Cancer Survivors With Anthracycline-Induced Cardiomyopathy - A COG-ALTE03N1 Report.

Author

Singh P, Shah DA, Jouni M, Cejas RB, Crossman DK, Magdy T, Qiu S, Wang X, Zhou L, Sharafeldin N, Hageman L, McKenna DE, Armenian SH, Balis FM, Hawkins DS, Keller FG, Hudson MM, Neglia JP, Ritchey AK, Ginsberg JP, Landier W, Bhatia R, Burridge PW, and Bhatia S

Subjects

Humans, Child, Matrix Metalloproteinase 8 genetics, Matrix Metalloproteinase 8 therapeutic use, Matrix Metalloproteinase 9, Anthracyclines adverse effects, Case-Control Studies, Antibiotics, Antineoplastic adverse effects, Myocytes, Cardiac, RNA, Messenger, Gene Expression, Cancer Survivors, Neoplasms drug therapy, Neoplasms genetics, Neoplasms complications, Cardiomyopathies chemically induced, Cardiomyopathies genetics

Abstract

Background Anthracycline-induced cardiomyopathy is a leading cause of premature death in childhood cancer survivors, presenting a need to understand the underlying pathogenesis. We sought to examine differential blood-based mRNA expression profiles in anthracycline-exposed childhood cancer survivors with and without cardiomyopathy. Methods and Results We designed a matched case-control study (Children's Oncology Group-ALTE03N1) with mRNA sequencing on total RNA from peripheral blood in 40 anthracycline-exposed survivors with cardiomyopathy (cases) and 64 matched survivors without (controls). DESeq2 identified differentially expressed genes. Ingenuity Pathway Analyses (IPA) and Gene Set Enrichment Analyses determined the potential roles of altered genes in biological pathways. Functional validation was performed by gene knockout in human-induced pluripotent stem cell-derived cardiomyocytes using CRISPR/Cas9 (clustered regularly interspaced short palindromic repeats/CRISPR-associated protein 9) technology. Median age at primary cancer diagnosis for cases and controls was 8.2 and 9.7 years, respectively. Thirty-six differentially expressed genes with fold change ≥±2 were identified; 35 were upregulated. IPA identified "hepatic fibrosis" and "iron homeostasis" pathways to be significantly modulated by differentially expressed genes, including toxicology functions of myocardial infarction, cardiac damage, and cardiac dilation. Leading edge analysis from Gene Set Enrichment Analyses identified lactate dehydrogenase A ( LDHA ) and cluster of differentiation 36 ( CD36 ) genes to be significantly upregulated in cases. Interleukin 1 receptor type 1, 2 ( IL1R1 , IL1R2 ), and matrix metalloproteinase 8, 9 ( MMP8, MMP9 ) appeared in multiple canonical pathways. LDHA -knockout human-induced pluripotent stem cell-derived cardiomyocytes showed increased sensitivity to doxorubicin. Conclusions We identified differential mRNA expression profiles in peripheral blood of anthracycline-exposed childhood cancer survivors with and without cardiomyopathy. Upregulation of LDHA and CD36 genes suggests metabolic perturbations in a failing heart. Dysregulation of proinflammatory cytokine receptors IL1R1 and IL1R2 and matrix metalloproteinases, MMP8 and MMP9 indicates structural remodeling that accompanies the clinical manifestation of symptomatic cardiotoxicity.

Published

2023

18. Utilizing RENAL nephrometry in pediatric patients undergoing nephron-sparing surgery for renal tumors: A single-institutional cohort.

Author

Mittal S, Long C, El-Ali A, Talwar R, Lattanzio K, Lawton B, Hamdan D, Balis FM, Mattei P, Back SJ, and Kolon TF

Subjects

Adult, Humans, Child, Infant, Child, Preschool, Nephrectomy methods, Research Design, Nephrons surgery, Nephrons pathology, Retrospective Studies, Treatment Outcome, Kidney diagnostic imaging, Kidney surgery, Kidney pathology, Kidney Neoplasms surgery, Kidney Neoplasms pathology

Abstract

Introduction: RENAL Nephrometry is a complexity score validated in adults with renal tumors and describes the likelihood of complication after partial nephrectomy (PN). Utilization in pediatrics has been limited. Thus, our goal is to quantify inter-rater agreement as well as determine how scores correlate with outcomes. We hypothesize that the RENAL Nephrometry Score is reproducible in children with renal tumors and is related to perioperative and post-operative complications., Methods: All pediatric patients who underwent PN for a renal mass from 2006 to 2019 were identified. Patient data, operative details, and outcomes were aggregated. Pre-operative CT/MR imaging was anonymized and scored by 2 pediatric radiologists and 2 pediatric urologists using RENAL Nephrometry metrics. Statistical analysis utilized Fleiss' kappa and the intraclass correlation coefficient (ICC). Comparative analyses were performed based on Nephrometry Score <9 and ≥ 9., Results: 28 patients undergoing 33 PN were identified. Median age at surgery was 3.2 years (IQR 1.8-4.0). There is moderate-good agreement across scorers on the domains of RENAL Nephrometry Score, with the lowest agreement noted for anterior vs posterior tumors. Comparing patients with scores <9 and ≥ 9, there was increased operative time (357 vs 267 min, p = 0.003) and LOS for those with a higher score, but no difference in the incidence of 30-day complications., Conclusion: RENAL Nephrometry Score is an easily reproducible complexity score for renal tumors in pediatric patients. Higher scores are associated with increased length of stay and estimated blood loss but not complications. Reporting of nephrometry scores in future publications on pediatric renal tumors should become standard in the literature., Competing Interests: Conflicts of interest There are no conflicts of interest., (Copyright © 2023 Journal of Pediatric Urology Company. Published by Elsevier Ltd. All rights reserved.)

Published

2023

19. Identification of novel hypermethylated or hypomethylated CpG sites and genes associated with anthracycline-induced cardiomyopathy.

Author

Singh P, Zhou L, Shah DA, Cejas RB, Crossman DK, Jouni M, Magdy T, Wang X, Sharafeldin N, Hageman L, McKenna DE, Horvath S, Armenian SH, Balis FM, Hawkins DS, Keller FG, Hudson MM, Neglia JP, Ritchey AK, Ginsberg JP, Landier W, Burridge PW, and Bhatia S

Subjects

Adult, Humans, Anthracyclines adverse effects, Case-Control Studies, Genome-Wide Association Study, DNA Methylation, Epigenesis, Genetic, DNA, CpG Islands, Antibiotics, Antineoplastic, Carrier Proteins genetics, Membrane Proteins genetics, Induced Pluripotent Stem Cells, Cardiomyopathies chemically induced, Cardiomyopathies genetics

Abstract

Anthracycline-induced cardiomyopathy is a leading cause of late morbidity in childhood cancer survivors. Aberrant DNA methylation plays a role in de novo cardiovascular disease. Epigenetic processes could play a role in anthracycline-induced cardiomyopathy but remain unstudied. We sought to examine if genome-wide differential methylation at 'CpG' sites in peripheral blood DNA is associated with anthracycline-induced cardiomyopathy. This report used participants from a matched case-control study; 52 non-Hispanic White, anthracycline-exposed childhood cancer survivors with cardiomyopathy were matched 1:1 with 52 survivors with no cardiomyopathy. Paired ChAMP (Chip Analysis Methylation Pipeline) with integrated reference-based deconvolution of adult peripheral blood DNA methylation was used to analyze data from Illumina HumanMethylation EPIC BeadChip arrays. An epigenome-wide association study (EWAS) was performed, and the model was adjusted for GrimAge, sex, interaction terms of age at enrollment, chest radiation, age at diagnosis squared, and cardiovascular risk factors (CVRFs: diabetes, hypertension, dyslipidemia). Prioritized genes were functionally validated by gene knockout in human induced pluripotent stem cell cardiomyocytes (hiPSC-CMs) using CRISPR/Cas9 technology. DNA-methylation EPIC array analyses identified 32 differentially methylated probes (DMP: 15 hyper-methylated and 17 hypo-methylated probes) that overlap with 23 genes and 9 intergenic regions. Three hundred and fifty-four differential methylated regions (DMRs) were also identified. Several of these genes are associated with cardiac dysfunction. Knockout of genes EXO6CB, FCHSD2, NIPAL2, and SYNPO2 in hiPSC-CMs increased sensitivity to doxorubicin. In addition, EWAS analysis identified hypo-methylation of probe 'cg15939386' in gene RORA to be significantly associated with anthracycline-induced cardiomyopathy. In this genome-wide DNA methylation profile study, we observed significant differences in DNA methylation at the CpG level between anthracycline-exposed childhood cancer survivors with and without cardiomyopathy, implicating differential DNA methylation of certain genes could play a role in pathogenesis of anthracycline-induced cardiomyopathy., (© 2023. Springer Nature Limited.)

Published

2023

20. Haptoglobin Gene Expression and Anthracycline-Related Cardiomyopathy in Childhood Cancer Survivors: A COG-ALTE03N1 Report.

Author

Singh P, Crossman DK, Zhou L, Wang X, Sharafeldin N, Hageman L, Blanco JG, Burridge PW, Armenian SH, Balis FM, Hawkins DS, Keller FG, Hudson MM, Neglia JP, Ritchey AK, Ginsberg JP, Landier W, and Bhatia S

Abstract

Background: Anthracycline-related cardiomyopathy is a leading cause of premature death in childhood cancer survivors. The high interindividual variability in risk suggests the need to understand the underlying pathogenesis., Objectives: The authors interrogated differentially expressed genes (DEGs) to identify genetic variants serving regulatory functions or genetic variants not easily identified when using genomewide array platforms. Using leads from DEGs, candidate copy number variants (CNVs) and single-nucleotide variants (SNVs) were genotyped., Methods: Messenger RNA sequencing was performed on total RNA from peripheral blood of 40 survivors with cardiomyopathy (cases) and 64 matched survivors without cardiomyopathy (control subjects). Conditional logistic regression analysis adjusting for sex, age at cancer diagnosis, anthracycline dose, and chest radiation was used to assess the associations between gene expression and cardiomyopathy and between CNVs and SNVs and cardiomyopathy., Results: Haptoglobin ( HP ) was identified as the top DEG. Participants with higher HP gene expression had 6-fold greater odds of developing cardiomyopathy (OR: 6.4; 95% CI: 1.4-28.6). The HP2 -specific allele among the HP genotypes (HP1-1, HP1-2, and HP2-2) had higher transcript levels, as did the G allele among SNVs previously reported to be associated with HP gene expression (rs35283911 and rs2000999). The HP1-2 and HP2-2 genotypes combined with the G/G genotype for rs35283911 and/or rs2000999 placed the survivors at 4-fold greater risk (OR: 3.9; 95% CI: 1.0-14.5) for developing cardiomyopathy., Conclusions: These findings provide evidence of a novel association between HP2 allele and cardiomyopathy. HP binds to free hemoglobin to form an HP-hemoglobin complex, thereby preventing oxidative damage from free heme iron, thus providing biological plausibility to the mechanistic basis of the present observation., Competing Interests: This research is supported by the National Cancer Institute (R35CA220502; principal investigator [PI], S. Bhatia), Leukemia and Lymphoma Society (6563-19; PI, S. Bhatia), and the V Foundation (DT2019-010; PI, S. Bhatia). The Children’s Oncology Group study (COG-ALTE03N1 [NCT00082745]; PI, S. Bhatia) reported here is supported by the National Clinical Trials Network Operations Center Grant (U10CA180886; PI, D.S. Hawkins), the National Clinical Trials Network Statistics & Data Center Grant (U10CA180899; PI, Alonzo), the Children’s Oncology Group Chair’s Grant (U10CA098543; PI, Adamson), the Children’s Oncology Group Statistics & Data Center Grant (U10CA098413; PI, Anderson), the National Cancer Institute Community Oncology Research Program Grant (UG1CA189955; PI, Pollock), and the Community Clinical Oncology Program Grant (U10CA095861; PI, Pollock), and the St. Baldrick’s Foundation through an unrestricted grant. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. The authors have reported that they have no relationships relevant to the contents of this paper to disclose., (© 2023 The Authors.)

Published

2023

21. An enhanced recovery after surgery protocol in children who undergo nephrectomy for Wilms tumor safely shortens hospital stay.

Author

Moon JK, Hwang R, Balis FM, and Mattei P

Subjects

Child, Child, Preschool, Humans, Ketorolac, Length of Stay, Male, Nephrectomy methods, Postoperative Complications epidemiology, Postoperative Complications etiology, Postoperative Complications prevention & control, Retrospective Studies, Review Literature as Topic, Enhanced Recovery After Surgery, Kidney Neoplasms pathology, Kidney Neoplasms surgery, Wilms Tumor pathology, Wilms Tumor surgery

Abstract

Background: Pediatric unilateral renal tumors in the US are treated with upfront nephrectomy and surgical staging. We applied enhanced recovery after surgery (ERAS) principles in care of children after Wilms nephrectomy., Methods: We reviewed records of pediatric unilateral nephrectomies for Wilms tumors, and analyzed tumor stage, surgical approach, length of operation, use of anesthesia adjuncts and catheters, diet advancement, hospital length of stay (LOS), and complications. Our ERAS protocol includes: parental education regarding discharge criteria and anticipated LOS, avoiding thoraco abdominal incisions, avoiding routine nasogastric tubes, clear liquids starting day of surgery, minimizing opiates, routine IV ketorolac use, and avoiding routine ICU stay. We examined the effects of our protocol on postoperative hospital LOS and complication rates., Results: Sixty six children (31 boys, mean age 3.8y, range 0-11.9) underwent unilateral total nephrectomy for Wilms tumor. Mean nephrectomy duration was 2.7 h. Post operatively, seven (11%) had temporary gastric tubes and 24 (36%) had epidural catheters. Ten (15%) recovered in the ICU. Patients were given regular diets mean of 1.9 days post op. Mean LOS was 3.7 days, with 56% of patients being discharged within 2-3 days. Presence of tumor thrombus, longer epidural catheter duration, delayed diet advancement, and total IV narcotic usage were associated with longer LOS. Routine use of IV ketorolac was associated with shorter LOS., Conclusions: Use of an ERAS protocol in children undergoing nephrectomy for Wilms tumor is safe, resulting in rapid return to regular diet and compared to the published literature, shorter postoperative LOS without an increase in complications or return to ED/OR., Level of Evidence: Level III., Competing Interests: Declaration of Competing Interest None, (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

22. Age-dependent reference intervals in children for the disialoganglioside, G D2 , a circulating tumor biomarker for the childhood cancer, neuroblastoma.

Author

Busch CM and Balis FM

Subjects

Age Factors, Biomarkers, Tumor blood, Child, Child, Preschool, Female, Gangliosides blood, Humans, Infant, Infant, Newborn, Male, Reference Values, Biomarkers, Tumor standards, Gangliosides standards, Neuroblastoma blood

Abstract

Background: The disialoganglioside G D2 is a circulating tumor biomarker for the childhood cancer, neuroblastoma. This study establishes reference intervals for G D2 concentration in children within the age range where neuroblastoma commonly occurs., Methods: Leftover plasma samples taken for routine clinical laboratory tests from children without cancer were collected and assayed for the 18-carbon fatty acid chain length lipoform of G D2 using a validated high-pressure liquid chromatography tandem mass spectrometry method with a lower limit of quantification of 3 nM. Samples were stratified into 5 age cohorts (0-6 months, 6-12 months, 12-36 months, 3-10 years and > 10 years). Non-parametric statistical methods were used to define the upper bound of the reference interval for each age cohort., Results: G D2 was measurable in 90% of samples from children < 10 years of age and G D2 concentration was age-dependent, peaking at 9 months followed by a gradual decline. G D2 was below the lower limit of quantification in 55% of samples in the > 10 years cohort. Upper bounds of reference intervals were 15.5 nM in 0-6 month cohort, 35.1 nM in 6-12 month cohort, 24.9 nM in 12-36 month cohort, 18.4 in 3-10 year cohort and 10.4 nM in > 10 year cohort., Conclusions: Age-dependent reference intervals were defined for circulating G D2 in children. G D2 concentration was highest in the 6-12 month age cohort, which is below the age of most children with high-risk neuroblastoma. The peak G D2 concentration at 9 months may reflect neurodevelopmental events in the brain., (Copyright © 2021 The Canadian Society of Clinical Chemists. Published by Elsevier Inc. All rights reserved.)

Published

2022

23. Pharmacokinetics of the disialoganglioside, G D2 , a circulating tumor biomarker for neuroblastoma, in nonhuman primates.

Author

Balis FM, McCully CL, Busch CM, Fox E, and Warren KE

Abstract

Competing Interests: Conflict of interest: The authors declare no conflict of interest.

Published

2021

24. Activity of Crizotinib in Patients with ALK-Aberrant Relapsed/Refractory Neuroblastoma: A Children's Oncology Group Study (ADVL0912).

Author

Foster JH, Voss SD, Hall DC, Minard CG, Balis FM, Wilner K, Berg SL, Fox E, Adamson PC, Blaney SM, Weigel BJ, and Mossé YP

Subjects

Anaplastic Lymphoma Kinase genetics, Child, Crizotinib therapeutic use, Humans, Neoplasm Recurrence, Local drug therapy, Neoplasm Recurrence, Local genetics, Protein Kinase Inhibitors adverse effects, Lung Neoplasms drug therapy, Neuroblastoma drug therapy, Neuroblastoma genetics

Abstract

Purpose: Anaplastic lymphoma kinase (ALK) aberrations are a promising target for patients with neuroblastoma. We assessed the activity of first-generation ALK inhibitor crizotinib in patients with no known curative treatments and whose tumors harbored an activating ALK alteration., Patients and Methods: Twenty patients with relapsed/refractory ALK-positive neuroblastoma received crizotinib at the recommended phase II dose of 280 mg/m 2 /dose. A Simon two-stage design was used to evaluate the antitumor activity of crizotinib monotherapy. Response evaluation occurred after cycles 1, 3, 5, 7, and then every 3 cycles. Correlation of ALK status and response was a secondary aim of the study., Results: The objective response rate for patients with neuroblastoma was 15% [95% confidence interval (CI): 3.3%-34.3%]: two with partial responses and 1 with a complete response. All three patients had a somatic ALK Arg1275Gln mutation, the most common ALK hotspot mutation observed in neuroblastoma and the only mutation predicted to be sensitive to ALK inhibition with crizotinib. Two patients had prolonged stable disease (10 and 13 cycles, respectively); both harbored an ALK Arg1275Gln mutation. Three patients with ALK Phe1174Leu mutations progressed during cycle 1 of therapy, and one patient with an ALK Phe1174Val received three cycles before disease progression. The two patients with ALK amplification had no response. The most common adverse event was a decrease in neutrophil count., Conclusions: Despite limited activity seen in this trial, we conclude that this is more likely due to an inability to reach the higher concentrations of crizotinib needed to overcome the competing ATP affinity. See related commentary by Schulte and Eggert, p. 3507 ., (©2021 American Association for Cancer Research.)

Published

2021

25. The ganglioside G D2 as a circulating tumor biomarker for neuroblastoma.

Author

Balis FM, Busch CM, Desai AV, Hibbitts E, Naranjo A, Bagatell R, Irwin M, and Fox E

Subjects

Case-Control Studies, Child, Follow-Up Studies, Humans, Neuroblastoma blood, Prognosis, Retrospective Studies, Biomarkers, Tumor blood, Gangliosides blood, Neuroblastoma diagnosis

Abstract

Background: G D2 is a ganglioside that is ubiquitously expressed in the plasma membrane of neuroblastoma and is shed into the circulation., Procedure: G D2 was measured with a high-pressure liquid chromatography/tandem mass spectrometry assay in serum or plasma from 40 children without cancer (controls) and in biobanked samples from 128 (73 high-risk) children with neuroblastic tumors at diagnosis, 56 children with relapsed neuroblastoma, 14 children with high-risk neuroblastoma after treatment, and 8 to 12 children each with 10 other common childhood cancers at diagnosis., Results: The C 18 (18 carbon fatty acid) lipoform was the predominant circulating form of G D2 in controls and in patients with neuroblastoma. The median concentration of G D2 in children with high-risk neuroblastoma at diagnosis was 167 nM (range, 16.1-1060 nM), which was 30-fold higher than the median concentration (5.6 nM) in controls. G D2 was not elevated in serum from children with the differentiated neuroblastic tumors, ganglioneuroma (n = 10) and ganglioneuroblastoma-intermixed subtype (n = 12), and in children with 10 other childhood cancers. G D2 concentrations were significantly higher in serum from children with MYCN-amplified tumors (P = 0.0088), high-risk tumors (P < 0.00001), International Neuroblastoma Staging System (INSS) stage 4 tumors (P < 0.00001), and in children who died (P = 0.034)., Conclusions: Circulating G D2 appears to be a specific and sensitive tumor biomarker for high-risk/high-stage neuroblastoma and may prove to be clinically useful as a diagnostic or prognostic circulating tumor biomarker. G D2 will be measured prospectively and longitudinally in children enrolled on a high-risk neuroblastoma treatment trial to assess its ability to measure response to treatment and predict survival., (© 2019 Wiley Periodicals, Inc.)

Published

2020

26. Exceptional Response to Nivolumab in a 13-Year-Old Female with Metastatic HPV-Negative Cervical Carcinoma.

Author

Oved JH, Graul A, Burger RA, Schwartz LE, Reyes MC, and Balis FM

Subjects

Adolescent, Carboplatin therapeutic use, Carcinoma secondary, Carcinoma surgery, Female, Gamma Rays therapeutic use, Humans, Hysterectomy, Liver Neoplasms secondary, Liver Neoplasms surgery, Lung Neoplasms secondary, Lung Neoplasms surgery, Lymph Node Excision, Ovariectomy, Paclitaxel therapeutic use, Papillomaviridae, Salpingectomy, Treatment Outcome, Uterine Cervical Neoplasms pathology, Uterine Cervical Neoplasms surgery, Antineoplastic Agents, Immunological therapeutic use, Carcinoma therapy, Liver Neoplasms therapy, Lung Neoplasms therapy, Nivolumab therapeutic use, Uterine Cervical Neoplasms therapy

Abstract

Cervical carcinoma is associated with high-risk human papillomavirus (HPV) DNA integration and usually occurs after age 21 (peak 45 years), as reflected in screening guidelines. Between 1999 and 2008, cervical carcinoma rate in adolescents aged 15-19 years was 0.15 per 100,000. HPV-negative cervical carcinoma is rare in adolescents. The youngest previously reported case was 15 years old. Treatment options for cervical carcinoma are limited after first-line therapy. Immune checkpoint inhibitors blocking programmed death receptor (PD-1) and its ligand, PD-L1, have shown objective clinical responses and are tolerable in adults with gynecologic cancers. This class of agents is well tolerated in pediatric patients. PD-1/PD-L1 is commonly expressed in gynecologic cancers but its expression may not predict clinical response. We describe an exceptional response to single agent nivolumab postradiation therapy in a 13-year-old adolescent with poorly differentiated cervical carcinoma and widespread metastatic disease.

Published

2019

27. Fundamental problems with pediatric adaptive dosing of carboplatin using nuclear-medicine-based estimates of renal function.

Author

Adamson PC, Veal GJ, Womer RB, Meany HJ, Bernhardt MB, Frazier AL, and Balis FM

Subjects

Algorithms, Antineoplastic Agents administration & dosage, Area Under Curve, Carboplatin administration & dosage, Child, Follow-Up Studies, Glomerular Filtration Rate, Humans, Kidney diagnostic imaging, Kidney drug effects, Neoplasms metabolism, Neoplasms pathology, Prognosis, Antineoplastic Agents pharmacokinetics, Carboplatin pharmacokinetics, Kidney physiopathology, Neoplasms drug therapy, Nuclear Medicine, Radionuclide Imaging methods

Abstract

Background: Carboplatin is often adaptively dosed based on glomerular filtration rate (GFR), usually estimated by nuclear medicine tests. At least five pediatric adaptive dosing formulas have been developed. In an effort to standardize dosing in Children's Oncology Group protocols, we explored methodologic variation in GFR estimation and adaptive-dosing formula performance., Procedure: Nuclear medicine GFR data from published series of ≥100 children with cancer were compared. Data from patients for whom body surface area, weight, GFR, and tracer half-life were available were used to compare formulas., Results: Differences in methods used to estimate GFR in children with cancer resulted in highly variable population results, with median GFRs ranging from 96 to 150 mL/min/1.73m 2 . The choice of adaptive formula had a major impact on calculated dose. When targeting an area under the curve of 7.9 mg/mL • min, the median difference between the formula yielding the lowest and highest carboplatin dose for individual subjects was 289 (range 96-1 737) mg/m 2 ., Conclusions: Wide variation in GFR obtained with nuclear-medicine-based tests in children with cancer primarily results from systematic methodologic errors. Formulas for calculating carboplatin dose produce additional and substantial variation that may place children with cancer at unnecessary risk for excessive toxicity or underdosing. These findings indicate a need for the development of a uniform, validated method for GFR determination in children that should be utilized in all centers. Currently, adaptive dosing of carboplatin based on GFR has serious limitations and in most clinical settings should arguably not be used in place of body-surface-area-based dosing., (© 2019 Wiley Periodicals, Inc.)

Published

2019

28. A validated HPLC-MS/MS method for estimating the concentration of the ganglioside, G D2 , in human plasma or serum.

Author

Busch CM, Desai AV, Moorthy GS, Fox E, and Balis FM

Subjects

Humans, Limit of Detection, Linear Models, Reproducibility of Results, Chromatography, High Pressure Liquid methods, Gangliosides blood, Tandem Mass Spectrometry methods

Abstract

G D2 is a ganglioside found in the plasma membrane of the neural crest-derived cancer, neuroblastoma. G D2 is shed into the circulation of patients with neuroblastoma and could serve as a tumor biomarker to monitor tumor burden or response to treatment. We developed and validated a high-performance liquid chromatography tandem mass spectrometry (HPLC-MS/MS) method to quantify the D18:1-18:0 (C18) and the D18:1-20:0 (C20) lipoforms of G D2 in human plasma and serum. Human brain derived G D2 containing a mixture of C18 and C20 was used as the analytical standard. Samples were extracted with methanol containing dueterated-G M1 (internal standard), and analytes were separated on a Phenomenex Kinetex C 18 column eluted with a gradient mobile phase composed of ammonium acetate buffer, methanol and isopropanol. An AB Sciex 4500 QTRAP mass spectrometer in negative ion mode was used to quantify the doubly charged G D2 C18 and C20 lipoform precursor ions (m/z 836.8 and m/z 850.8) that both yield a product ion of m/z 290.0. The calibration curves were linear from 4-1000 ng/mL and 6-1500 ng/mL for G D2 C18 and C20 lipoforms respectively. Inter-day and intra-day accuracy were within the acceptable validation range in plasma and serum., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

29. Diagnosis of Beckwith-Wiedemann syndrome in children presenting with Wilms tumor.

Author

MacFarland SP, Duffy KA, Bhatti TR, Bagatell R, Balamuth NJ, Brodeur GM, Ganguly A, Mattei PA, Surrey LF, Balis FM, and Kalish JM

Subjects

Child, Child, Preschool, Female, Humans, Infant, Infant, Newborn, Male, Beckwith-Wiedemann Syndrome complications, Beckwith-Wiedemann Syndrome diagnosis, Kidney Neoplasms genetics, Wilms Tumor genetics

Abstract

Beckwith-Wiedemann syndrome (BWS) is a genetic syndrome associated with overgrowth and cancer predisposition, including predisposition to Wilms tumor (WT). Patients with BWS and BWS spectrum are screened from birth to age 7 years for BWS-associated cancers. However, in some cases a BWS-associated cancer may be the first recognized manifestation of the syndrome. We describe 12 patients diagnosed with BWS after presenting with a WT. We discuss the features of BWS in these patients and hypothesize that earlier detection of BWS by attention to its subtler manifestations could lead to earlier detection of children at risk for associated malignancies., (© 2018 Wiley Periodicals, Inc.)

Published

2018

30. Case Report: Nephron-sparing Surgery in a Patient With Bilateral Multifocal Wilms Tumor.

Author

Bowen DK, Long CJ, Balis FM, and Kolon TF

Subjects

Humans, Infant, Male, Nephrons, Kidney Neoplasms surgery, Nephrectomy methods, Organ Sparing Treatments, Wilms Tumor surgery

Abstract

We present a case of bilateral multifocal Wilms tumor in a nonsyndromic 12-month-old male. Our management approach included 12 weeks of preoperative chemotherapy for maximal tumor shrinkage and, despite the central location of the tumors, successful staged bilateral nephron-sparing surgery. We advocate for a broader application of nephron-sparing surgery in Wilms tumor cases with the goal of preserving renal function without compromising oncologic outcomes., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

31. Outcomes of Children and Adolescents with Advanced Hereditary Medullary Thyroid Carcinoma Treated with Vandetanib.

Author

Kraft IL, Akshintala S, Zhu Y, Lei H, Derse-Anthony C, Dombi E, Steinberg SM, Lodish M, Waguespack SG, Kapustina O, Fox E, Balis FM, Merino MJ, Meltzer PS, Glod JW, Shern JF, and Widemann BC

Subjects

Adolescent, Carcinoma, Medullary drug therapy, Carcinoma, Medullary genetics, Carcinoma, Medullary pathology, Child, Disease Progression, Disease-Free Survival, Female, Germ-Line Mutation, Humans, Male, Multiple Endocrine Neoplasia Type 2a genetics, Multiple Endocrine Neoplasia Type 2a pathology, Outcome Assessment, Health Care, Protein Kinase Inhibitors therapeutic use, Thyroid Neoplasms genetics, Thyroid Neoplasms pathology, Carcinoma, Medullary congenital, Multiple Endocrine Neoplasia Type 2a drug therapy, Piperidines therapeutic use, Quinazolines therapeutic use, Thyroid Neoplasms drug therapy

Abstract

Purpose: Vandetanib is well-tolerated in patients with advanced medullary thyroid carcinoma (MTC). Long-term outcomes and mechanisms of MTC progression have not been reported previously. Experimental Design: We monitored toxicities and disease status in patients taking vandetanib for hereditary, advanced MTC. Tumor samples were analyzed for molecular mechanisms of disease progression. Results: Seventeen patients [8 male, age 13 (9-17)* years] enrolled; 16 had a RET p.Met918Thr germline mutation. The duration of vandetanib therapy was 6.1 (0.1-9.7+)* years with treatment ongoing in 9 patients. Best response was partial response in 10, stable disease in 6, and progressive disease in one patient. Duration of response was 7.4 (0.6-8.7+)* and 4.9 (0.6-7.8+)* years in patients with PR and SD, respectively. Six patients died 2.0 (0.4-5.7)* years after progression. Median progression-free survival (PFS) was 6.7 years [95% confidence interval (CI): 2.3 years-undefined] and 5-year overall survival (OS) was 88.2% (95% CI: 60.6%-96.9%). Of 16 patients with a RET p.Met918Thr mutation, progression-free survival was 6.7 years (95% CI: 3.1-undefined) and 5-year overall survival was 93.8% (95% CI: 63.2%-99.1%). No patients terminated treatment because of toxicity. DNA sequencing of tissue samples ( n = 11) identified an increase in copy number alterations across the genome as a potential mechanism of drug resistance [*median (range)]. Conclusions: This study demonstrates that vandetanib is safe and results in sustained responses in children and adolescents with hereditary MTC. Our preliminary molecular data suggest that an increase in copy number abnormalities may be associated with tumor progression in hereditary MTC patients treated with vandetanib. Clin Cancer Res; 24(4); 753-65. ©2017 AACR ., (©2017 American Association for Cancer Research.)

Published

2018

32. Consensus Guideline for Use of Glucarpidase in Patients with High-Dose Methotrexate Induced Acute Kidney Injury and Delayed Methotrexate Clearance.

Author

Ramsey LB, Balis FM, O'Brien MM, Schmiegelow K, Pauley JL, Bleyer A, Widemann BC, Askenazi D, Bergeron S, Shirali A, Schwartz S, Vinks AA, and Heldrup J

Subjects

Acute Kidney Injury chemically induced, Antimetabolites, Antineoplastic administration & dosage, Consensus, Dose-Response Relationship, Drug, Follow-Up Studies, Humans, Methotrexate administration & dosage, Neoplasms pathology, Recombinant Proteins therapeutic use, Acute Kidney Injury drug therapy, Antimetabolites, Antineoplastic adverse effects, Methotrexate adverse effects, Neoplasms drug therapy, Practice Guidelines as Topic standards, gamma-Glutamyl Hydrolase therapeutic use

Abstract

Acute kidney injury due to high-dose methotrexate (HDMTX) is a serious, life-threatening toxicity that can occur in pediatric and adult patients. Glucarpidase is a treatment approved by the Food and Drug Administration for high methotrexate concentrations in the context of kidney dysfunction, but the guidelines for when to use it are unclear. An expert panel was convened to provide specific, expert consensus guidelines for the use of glucarpidase in patients who develop HDMTX-induced nephrotoxicity and delayed methotrexate excretion. The guideline provides recommendations to identify the population of patients who would benefit from glucarpidase rescue by more precisely defining the absolute methotrexate concentrations associated with risk for severe or life-threatening toxicity at several time points after the start of an HDMTX infusion. For an HDMTX infusion ≤24 hours, if the 36-hour concentration is above 30 µM, 42-hour concentration is above 10 µM, or 48-hour concentration is above 5 µM and the serum creatinine is significantly elevated relative to the baseline measurement (indicative of HDMTX-induced acute kidney injury), glucarpidase may be indicated. After a 36- to 42-hour HDMTX infusion, glucarpidase may be indicated when the 48-hour methotrexate concentration is above 5 µM. Administration of glucarpidase should optimally occur within 48-60 hours from the start of the HDMTX infusion, because life-threatening toxicities may not be preventable beyond this time point., Implications for Practice: Glucarpidase is a rarely used medication that is less effective when given after more than 60 hours of exposure to high-dose methotrexate, so predicting early which patients will need it is imperative. There are no currently available consensus guidelines for the use of this medication. The indication on the label does not give specific methotrexate concentrations above which it should be used. An international group of experts was convened to develop a consensus guideline that was specific and evidence-based to identify the population of patients who would benefit from glucarpidase., Competing Interests: Disclosures of potential conflicts of interest may be found at the end of this article., (© AlphaMed Press 2017.)

Published

2018

33. Modernizing Clinical Trial Eligibility: Recommendations of the American Society of Clinical Oncology-Friends of Cancer Research Minimum Age Working Group.

Author

Gore L, Ivy SP, Balis FM, Rubin E, Thornton K, Donoghue M, Roberts S, Bruinooge S, Ersek J, Goodman N, Schenkel C, and Reaman G

Subjects

Age Factors, Humans, United States, Biomedical Research methods, Clinical Trials as Topic, Medical Oncology methods

Abstract

Purpose Children have historically been excluded from first-in-human studies of promising new cancer drugs and later phase adult clinical trials. Delays in evaluation may result in off-label use without dosing information as the only access to new drugs. A multistakeholder workshop was convened in May 2016 by ASCO and Friends of Cancer Research to identify opportunities for when it would be scientifically appropriate to expand trial eligibility to include children younger than age 18 years in first-in-human and other adult cancer clinical trials. Methods This group convened experts from academia, government, and industry to review barriers to enrolling children and adolescents in oncology clinical trials. We evaluated the historical context, published literature, regulatory considerations, and myriad risks and benefits associated with lowering the age of enrollment on oncology clinical trials. Results We conclude that many of the historical concerns about including children early in oncology clinical trials do not apply in the current scientific and clinical environment of pediatric oncology and drug development; we provide specific recommendations for how the inclusion of children in early-phase investigational cancer drug trials might be accomplished. Automatic inclusion of pediatric patients is appropriate in early-phase trials that assess dose, safety, and pharmacokinetics in a variety of tumor types and later phase trials that assess efficacy in a specific disease that spans adult and pediatric populations. Conclusion Including children in appropriately designed adult clinical oncology trials is feasible and can be done in a way that enhances their access to these agents without compromising safety or development strategies.

Published

2017

34. Dosing anticancer drugs in infants: Current approach and recommendations from the Children's Oncology Group's Chemotherapy Standardization Task Force.

Author

Balis FM, Womer RB, Berg S, Winick N, Adamson PC, and Fox E

Subjects

Antineoplastic Agents administration & dosage, Child, Preschool, Dose-Response Relationship, Drug, Female, Humans, Infant, Infant, Newborn, Male, Neoplasms pathology, Prognosis, Antineoplastic Agents standards, Neoplasms drug therapy, Practice Guidelines as Topic standards

Abstract

An analysis of dose modifications for infants in 29 Children's Oncology Group protocols across 10 cancer types revealed 11 sets of criteria defining the infant population using age, weight, body surface area (BSA), or a combination of these parameters and eight dose modification methods. A new method of dosing anticancer drugs in infants was developed based on the rationale that prior modifications were implemented to reduce toxicity, which is not cancer-specific. The new method uses BSA dose banding in dosing tables for infants and children with a BSA <0.6 m 2 and gradually transitions from body weight based to BSA-based dosing., (© 2017 Wiley Periodicals, Inc.)

Published

2017

35. First-dose and steady-state pharmacokinetics of orally administered crizotinib in children with solid tumors: a report on ADVL0912 from the Children's Oncology Group Phase 1/Pilot Consortium.

Author

Balis FM, Thompson PA, Mosse YP, Blaney SM, Minard CG, Weigel BJ, and Fox E

Subjects

Administration, Oral, Adolescent, Adult, Child, Child, Preschool, Crizotinib, Female, Humans, Lymphoma, Large-Cell, Anaplastic drug therapy, Male, Protein Kinase Inhibitors administration & dosage, Pyrazoles administration & dosage, Pyridines administration & dosage, Neoplasms drug therapy, Protein Kinase Inhibitors pharmacokinetics, Pyrazoles pharmacokinetics, Pyridines pharmacokinetics

Abstract

Purpose: Characterize the pharmacokinetics of oral crizotinib in children with cancer., Methods: Sixty-four children with solid tumors or anaplastic large-cell lymphoma (ALCL) enrolled on a phase 1/2 trial of the ALK, MET and ROS1 inhibitor, crizotinib, had pharmacokinetic sampling after the first dose (n = 15) or at steady state (n = 49). Dose levels studied were 100, 130, 165, 215, 280 and 365 mg/m 2 /dose administered twice daily. Two capsule and two oral liquid formulations were used over the course of the trial. Crizotinib was quantified with a validated HPLC/tandem mass spectrometry method with a lower limit of detection of 0.2 ng/mL. Pharmacokinetic parameters were derived using non-compartmental analysis., Results: Time to peak plasma concentration was 4 h. At 280 mg/m 2 (MTD), mean (±SD) steady-state peak plasma concentration was 717 ± 201 ng/mL, and steady-state trough plasma concentration was 480 ± 176 ng/mL. At steady state, AUC 0-τ was proportional to dose over the dose range of 215-365 mg/m 2 /dose. Apparent clearance of crizotinib was 731 ± 241 mL/min/m 2 . Steady-state AUC 0-τ at 280 mg/m 2 /dose was 2.5-fold higher than the AUC 0-∞ in adults receiving 250 mg (~140 mg/m 2 ). Age, sex and drug formulation do not account for the inter-subject variability in AUC 0-τ at steady state. The accumulation index was 4.9, and the half-life estimated from the accumulation index was 36 h., Conclusions: The pharmacokinetics of oral crizotinib in children is similar to that in adults. Steady-state trough-free crizotinib concentrations in plasma at the MTD exceed inhibitory concentrations of crizotinib in ALCL cell lines. CLINICALTRIALS., Gov Identifier: NCT00939770., Competing Interests: F. Balis has research funding from United Therapeutics Corp.; Y. Mosse has research funding from Pfizer, Inc. and Novartis; E. Fox has research funding from Glaxo Smith Kline, Merck and Incyta. Ethical approval The phase 1 clinical trial of crizotinib was reviewed and approved by the Institutional Review Boards at each participating institution, and the clinical trial was conducted in accordance with the ethical standards outlined in the Declaration of Helsinki and the US Federal Regulations governing research in human subjects.

Published

2017

36. 15-0600-Dr. Fox's response to letter to the editor.

Author

Fox E and Balis FM

Published

2016

37. Pharmacokinetic and pharmacodynamic study of tariquidar (XR9576), a P-glycoprotein inhibitor, in combination with doxorubicin, vinorelbine, or docetaxel in children and adolescents with refractory solid tumors.

Author

Fox E, Widemann BC, Pastakia D, Chen CC, Yang SX, Cole D, and Balis FM

Subjects

ATP Binding Cassette Transporter, Subfamily B metabolism, Adolescent, Anemia chemically induced, Antineoplastic Combined Chemotherapy Protocols adverse effects, Area Under Curve, Child, Child, Preschool, Docetaxel, Dose-Response Relationship, Drug, Doxorubicin administration & dosage, Doxorubicin adverse effects, Drug Resistance, Neoplasm, Female, Humans, Male, Metabolic Clearance Rate, Neoplasms metabolism, Neoplasms pathology, Neutropenia chemically induced, Quinolines administration & dosage, Quinolines adverse effects, Taxoids administration & dosage, Taxoids adverse effects, Treatment Outcome, Vinblastine administration & dosage, Vinblastine adverse effects, Vinblastine analogs & derivatives, Vinorelbine, Vomiting chemically induced, ATP Binding Cassette Transporter, Subfamily B antagonists & inhibitors, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Neoplasms drug therapy, Quinolines pharmacokinetics

Abstract

Purpose: P-glycoprotein (Pgp), an ATP-dependent transport protein, confers multidrug resistance in cancer cells. Tariquidar binds and inhibits Pgp. To assess the toxicity, pharmacokinetics (PK), and pharmacodynamics of tariquidar, we conducted a phase I trial of tariquidar in combination with doxorubicin, docetaxel, or vinorelbine in children and adolescents with recurrent or refractory solid tumors., Methods: Patients less than 19 years of age with refractory or recurrent solid tumors were eligible. Tariquidar (1, 1.5, or 2 mg/kg) was administered alone and in combination with doxorubicin, docetaxel, or vinorelbine. PK of tariquidar and cytotoxic drugs was performed. Pgp function was assessed by a rhodamine efflux assay and (99m)Tc-sestamibi scintigraphy. Tumor Pgp expression was assessed by immunohistochemistry. Response was assessed using Response Evaluation Criteria in Solid Tumors., Results: Twenty-nine subjects were enrolled. No tariquidar-related dose-limiting toxicity (DLT) was observed. DLT related to cytotoxic drugs occurred in 12 % of subjects receiving tariquidar 2 mg/kg. When administered in combination with tariquidar, the clearance of docetaxel and vinorelbine was reduced compared to prior studies. Inhibition of rhodamine efflux was dose dependent. After tariquidar administration, (99m)Tc-sestamibi accumulation in tumor increased by 22 %. Objective responses (1 complete, 2 partial) were observed. There was no association between tumor Pgp expression and response., Conclusion: A tolerable and biologically active dose of tariquidar was established in children and adolescents. This trial demonstrates that modulators of resistance can be evaluated in combination with chemotherapy, and pharmacokinetic and pharmacodynamic endpoints can be useful in determination of recommended dose in children and adolescents.

Published

2015

38. Phase II/III trial of a pre-transplant farnesyl transferase inhibitor in juvenile myelomonocytic leukemia: a report from the Children's Oncology Group.

Author

Stieglitz E, Ward AF, Gerbing RB, Alonzo TA, Arceci RJ, Liu YL, Emanuel PD, Widemann BC, Cheng JW, Jayaprakash N, Balis FM, Castleberry RP, Bunin NJ, Loh ML, and Cooper TM

Subjects

Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Cytarabine administration & dosage, Disease-Free Survival, Enzyme Inhibitors administration & dosage, Female, Hematopoietic Stem Cell Transplantation, Humans, Infant, Isotretinoin administration & dosage, Leukemia, Myelomonocytic, Juvenile enzymology, Leukemia, Myelomonocytic, Juvenile mortality, Leukemia, Myelomonocytic, Juvenile pathology, Male, Middle Aged, Survival Rate, Vidarabine administration & dosage, Vidarabine analogs & derivatives, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Farnesyl-Diphosphate Farnesyltransferase antagonists & inhibitors, Leukemia, Myelomonocytic, Juvenile drug therapy, Quinolones administration & dosage

Abstract

Background: Juvenile myelomonocytic leukemia (JMML) is not durably responsive to chemotherapy, and approximately 50% of patients relapse after hematopoietic stem cell transplant (HSCT). Here we report the activity and acute toxicity of the farnesyl transferase inhibitor tipifarnib, the response rate to 13-cis retinoic acid (CRA) in combination with cytoreductive chemotherapy, and survival following HSCT in children with JMML., Procedure: Eighty-five patients with newly diagnosed JMML were enrolled on AAML0122 between 2001 and 2006. Forty-seven consented to receive tipifarnib in a phase II window before proceeding to a phase III trial of CRA in combination with fludarabine and cytarabine followed by HSCT and maintenance CRA. Thirty-eight patients enrolled only in the phase III trial., Results: Overall response rate was 51% after tipifarnib and 68% after fludarabine/cytarabine/CRA. Tipifarnib did not increase pre-transplant toxicities. Forty-six percent of the 44 patients who received protocol compliant HSCT relapsed. Five-year overall survival was 55 ± 11% and event-free survival was 41 ± 11%, with no significant difference between patients who did or did not receive tipifarnib., Conclusions: Administration of tipifarnib in the window setting followed by HSCT in patients with newly diagnosed JMML was safe and yielded a 51% initial response rate as a single agent, but failed to reduce relapse rates or improve long-term overall survival., (© 2014 Wiley Periodicals, Inc.)

Published

2015

39. Pharmacokinetics of the chimeric anti-GD2 antibody, ch14.18, in children with high-risk neuroblastoma.

Author

Desai AV, Fox E, Smith LM, Lim AP, Maris JM, and Balis FM

Subjects

Algorithms, Antibodies, Monoclonal blood, Antibodies, Monoclonal genetics, Area Under Curve, Child, Child, Preschool, Female, Humans, Immunoassay methods, Infant, Male, Metabolic Clearance Rate, Models, Biological, Neuroblastoma blood, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins pharmacokinetics, Risk Factors, Treatment Outcome, Antibodies, Monoclonal pharmacokinetics, Gangliosides immunology, Neuroblastoma drug therapy, Neuroblastoma metabolism

Abstract

Purpose: Ch14.18 improves survival in children with high-risk neuroblastoma but is associated with substantial toxicity. Ch14.18 pharmacokinetics were previously reported to be highly variable and characterized by a higher clearance in children than in adults, and a large volume of distribution. Identifying factors responsible for its variability could lead to alternative dosing strategies that reduce toxicity., Methods: Plasma sampling was performed prior to, during, and for 25 days after four daily 10-h infusions of 25 mg/m(2) of ch14.18 administered with sargramostim. Ch14.18 concentrations were quantified with an electrochemiluminescence immunoassay, and pharmacokinetic parameters were derived using non-compartmental methods and from fitting a two-compartment model. Human anti-chimeric antibody (HACA) was measured before each course., Results: Fourteen subjects (median age, 4.3 years) were enrolled; seven had sampling on two courses to assess intra-subject variability. Mean peak ch14.18 plasma concentration was 11 µg/mL, and disappearance was biexponential with half-life of 7 days. Mean trough (day 28) concentration was 0.2 µg/mL. Mean AUC0-∞ was 1,380 µg h/mL and was less variable than previously reported (CV 29 %). Intra-patient variability was also minimal, but one subject who developed HACA had a 41 % decrease in AUC 0-tlast from courses 1 to 3. Clearance (2 L/day m(2)) was fourfold higher in children than in adults and appeared to be age dependent. Steady state volume of distribution was 0.4 L/kg. Two-compartment model parameters were used to simulate alternative dosing schedules., Conclusions: Ch14.18 disposition in children is less variable than previously reported. Clearance is age dependent and more rapid in younger children.

Published

2014

40. Phase II trial of pirfenidone in children and young adults with neurofibromatosis type 1 and progressive plexiform neurofibromas.

Author

Widemann BC, Babovic-Vuksanovic D, Dombi E, Wolters PL, Goldman S, Martin S, Goodwin A, Goodspeed W, Kieran MW, Cohen B, Blaney SM, King A, Solomon J, Patronas N, Balis FM, Fox E, Steinberg SM, and Packer RJ

Subjects

Adolescent, Adult, Child, Child, Preschool, Disease Progression, Female, Follow-Up Studies, Humans, Male, Neoplasm Staging, Neurofibroma, Plexiform mortality, Neurofibroma, Plexiform pathology, Neurofibromatosis 1 mortality, Neurofibromatosis 1 pathology, Prognosis, Quality of Life, Survival Rate, Time Factors, Young Adult, Antineoplastic Agents therapeutic use, Neurofibroma, Plexiform drug therapy, Neurofibromatosis 1 drug therapy, Pyridones therapeutic use, Tumor Necrosis Factor-alpha antagonists & inhibitors

Abstract

Background: Pirfenidone, an oral anti-inflammatory, antifibrotic agent with activity in idiopathic pulmonary fibrosis, may mediate anti-tumor activity in neurofibromatosis type 1 (NF1) and plexiform neurofibromas (PN) by inhibition of fibroblast proliferation and collagen synthesis. The primary objective of this open label, single arm phase II trial was to evaluate the activity of pirfenidone in children and young adults with inoperable PN., Procedure: Patients (3-21 years) with NF1-related progressive PN received pirfenidone at the previously determined optimal dose (500 mg/m(2) orally, q8h) on a continuous dosing schedule (one cycle = 28 days). Volumetric MRI analysis was used to assess response. Progression was defined as ≥ 20% PN volume increase compared to baseline. Pirfenidone would be considered active if it doubled the median time to progression (TTP) compared to the TTP on the placebo arm of a phase II trial with the farnesyltransferase inhibitor tipifarnib, which used near identical eligibility criteria. Toxicities, objective response rate, and quality of life (QOL) also were evaluated., Results: Thirty-six patients were enrolled and tolerated pirfenidone well with intermittent nausea and vomiting as the most frequent toxicities. A dose reduction was required in only three patients. The median TTP for pirfenidone was 13.2 months compared to 10.6 months for the placebo control group from the tipifarnib trial (two-tailed P = 0.92; one-tailed P = 0.46). No objective responses were observed., Conclusions: Pirfenidone was well tolerated, but did not demonstrate activity as defined in this trial and does not warrant further evaluation in children with NF1 and progressive PN., (© 2014 Wiley Periodicals, Inc.)

Published

2014

41. Vandetanib successfully controls medullary thyroid cancer-related Cushing syndrome in an adolescent patient.

Author

Nella AA, Lodish MB, Fox E, Balis FM, Quezado MM, Whitcomb PO, Derdak J, Kebebew E, Widemann BC, and Stratakis CA

Subjects

Adolescent, Adrenocorticotropic Hormone metabolism, Carcinoma, Neuroendocrine, Clinical Trials, Phase I as Topic, Clinical Trials, Phase II as Topic, Humans, Male, Neoplasms, Second Primary metabolism, Neoplasms, Second Primary secondary, Thyroid Neoplasms metabolism, Thyroid Neoplasms secondary, Cushing Syndrome etiology, Multiple Endocrine Neoplasia Type 2b complications, Neoplasms, Second Primary complications, Piperidines therapeutic use, Protein-Tyrosine Kinases antagonists & inhibitors, Quinazolines therapeutic use, Thyroid Neoplasms complications

Abstract

Context: Ectopic Cushing syndrome due to ACTH secretion from metastatic medullary thyroid cancer (MTC) is associated with significant morbidity and mortality., Objective: The aim of the study was to describe the first case of Cushing syndrome associated with MTC in a pediatric patient and the successful reversal of Cushing syndrome with tyrosine kinase inhibitor (vandetanib) therapy., Patient and Methods: A 17-year-old Brazilian adolescent presented with metastatic MTC and associated ACTH-dependent ectopic Cushing syndrome in the context of multiple endocrine neoplasia type 2B. When the patient was treated with the tyrosine kinase inhibitor vandetanib, rapid decrease in serum cortisol and improvement of clinical symptoms were observed., Conclusion: We describe the first pediatric case of clinical and biochemical improvement of paraneoplastic MTC-related Cushing syndrome after treatment with vandetanib. Vandetanib and possibly other tyrosine kinase inhibitors may be a novel beneficial option in patients with neuroendocrine tumor-related ectopic Cushing syndrome.

Published

2014

42. Time to disease progression in children with relapsed or refractory neuroblastoma treated with ABT-751: a report from the Children's Oncology Group (ANBL0621).

Author

Fox E, Mosse' YP, Meany HM, Gurney JG, Khanna G, Jackson HA, Gordon G, Shusterman S, Park JR, Cohn SL, Adamson PC, London WB, Maris JM, and Balis FM

Subjects

Adolescent, Antineoplastic Agents adverse effects, Antineoplastic Agents pharmacokinetics, Biomarkers, Capsules, Child, Child, Preschool, Combined Modality Therapy, Disease Progression, Disease-Free Survival, Female, Gastrointestinal Diseases chemically induced, Hematologic Diseases chemically induced, Humans, Male, Nervous System Diseases chemically induced, Neuroblastoma therapy, Quality of Life, Recurrence, Sulfonamides adverse effects, Sulfonamides pharmacokinetics, Suspensions, Treatment Failure, Antineoplastic Agents therapeutic use, Neuroblastoma drug therapy, Salvage Therapy, Sulfonamides therapeutic use, Tubulin Modulators therapeutic use

Abstract

Background: ABT-751, an orally bioavailable sulfonamide binds the colchicine site of beta-tubulin and inhibits microtubule polymerization. Prior phase I studies established the recommended dose in children with solid tumors as 200 mg/m(2) PO daily × 7 days every 21 days and subjects with neuroblastoma experienced prolonged stable disease. We conducted a phase 2 study (NCT00436852) in children and adolescents with progressive neuroblastoma to determine if ABT-751 prolonged the time to progression (TTP) compared to a hypothesized standard based on a historical control population., Procedure: Children and adolescents (n = 91) with a median (range) age 7.7 (2.3-21.5) years and progressive neuroblastoma were enrolled and stratified by disease status into disease measureable by CT/MRI (n = 47) or disease assessable by (123) I-metaiodobenzylguanine scintigraphy (MIBG, n = 44). Response was evaluated using RECIST for measureable disease and the Curie score for MIBG-avid disease., Results: ABT-751 was well tolerated. The objective response rate was 7%. The median TTP was 42 days (95% CI: 36, 56) in the measureable disease stratum and 45 days (95% CI: 42, 85) in the MIBG-avid disease stratum. TTP was similar to the historical control group (n = 136, median TTP 42 days). For the combined strata (n = 91), 1-year progression free survival (PFS) was 13 ± 4% and overall survival (OS) was 48 ± 5%., Conclusions: The low objective response rate and failure to prolong TTP indicate that ABT-751 is not sufficiently active to warrant further development for neuroblastoma. However, this trial demonstrates the utility of TTP as the primary endpoint in phase 2 trials in children and adolescents with neuroblastoma., (© 2013 Wiley Periodicals, Inc.)

Published

2014

43. Phase 2 randomized, flexible crossover, double-blinded, placebo-controlled trial of the farnesyltransferase inhibitor tipifarnib in children and young adults with neurofibromatosis type 1 and progressive plexiform neurofibromas.

Author

Widemann BC, Dombi E, Gillespie A, Wolters PL, Belasco J, Goldman S, Korf BR, Solomon J, Martin S, Salzer W, Fox E, Patronas N, Kieran MW, Perentesis JP, Reddy A, Wright JJ, Kim A, Steinberg SM, and Balis FM

Subjects

Adolescent, Adult, Child, Child, Preschool, Cross-Over Studies, Disease Progression, Double-Blind Method, Female, Humans, Male, Treatment Outcome, Young Adult, Antineoplastic Agents therapeutic use, Enzyme Inhibitors therapeutic use, Farnesyltranstransferase antagonists & inhibitors, Neurofibroma, Plexiform drug therapy, Neurofibromatosis 1 drug therapy, Quinolones therapeutic use

Abstract

Background: RAS is dysregulated in neurofibromatosis type 1 (NF1) related plexiform neurofibromas (PNs). The activity of tipifarnib, which blocks RAS signaling by inhibiting its farnesylation, was tested in children and young adults with NF1 and progressive PNs., Methods: Patients aged 3-25 years with NF1-related PNs and imaging evidence of tumor progression were randomized in a double-blinded fashion to receive tipifarnib (200 mg/m(2) orally every 12 h) or placebo (phase A) and crossed over to the opposite treatment arm at the time of tumor progression (phase B). PN volumes were measured with MRI, and progression was defined as ≥20% volume increase. Time to progression (TTP) in phase A was the primary endpoint, and the trial was powered to detect whether tipifarnib doubled TTP compared with placebo. Toxicity, response, and quality of life were also monitored., Results: Sixty-two patients were enrolled. Tipifarnib and placebo were well tolerated. On phase A, the median TTP was 10.6 months on the placebo arm and 19.2 months on the tipifarnib arm (P = .12; 1-sided). Quality of life improved significantly compared with baseline on the tipifarnib arm but not on the placebo arm. Volumetric tumor measurement detected tumor progression earlier than conventional 2-dimensional (WHO) and 1-dimensional (RECIST) methods., Conclusions: Tipifarnib was well tolerated but did not significantly prolong TTP of PNs compared with placebo. The randomized, flexible crossover design and volumetric PN assessment provided a feasible and efficient means of assessing the efficacy of tipifarnib. The placebo arm serves as an historical control group for phase 2 single-arm trials directed at progressive PNs.

Published

2014

44. Vandetanib in children and adolescents with multiple endocrine neoplasia type 2B associated medullary thyroid carcinoma.

Author

Fox E, Widemann BC, Chuk MK, Marcus L, Aikin A, Whitcomb PO, Merino MJ, Lodish M, Dombi E, Steinberg SM, Wells SA, and Balis FM

Subjects

Adolescent, Carcinoma, Medullary genetics, Carcinoma, Neuroendocrine, Child, Child, Preschool, Drug-Related Side Effects and Adverse Reactions pathology, Gene Expression Regulation, Neoplastic, Germ-Line Mutation, Humans, Multiple Endocrine Neoplasia Type 2b genetics, Multiple Endocrine Neoplasia Type 2b pathology, Neoplasm Metastasis, Neoplasm Recurrence, Local drug therapy, Neoplasm Recurrence, Local pathology, Piperidines adverse effects, Protein-Tyrosine Kinases genetics, Proto-Oncogene Mas, Proto-Oncogene Proteins c-ret genetics, Quinazolines adverse effects, Thyroid Neoplasms genetics, Thyroid Neoplasms pathology, Carcinoma, Medullary drug therapy, Multiple Endocrine Neoplasia Type 2b drug therapy, Piperidines administration & dosage, Quinazolines administration & dosage, Thyroid Neoplasms drug therapy

Abstract

Purpose: Medullary thyroid carcinoma (MTC) is a manifestation of multiple endocrine neoplasia type 2 (MEN2) syndromes caused by germline, activating mutations in the RET (REarranged during Transfection) proto-oncogene. Vandetanib, a VEGF and EGF receptor inhibitor, blocks RET tyrosine kinase activity and is active in adults with hereditary MTC., Experimental Design: We conducted a phase I/II trial of vandetanib for children (5-12 years) and adolescents (13-18 years) with MTC to define a recommended dose and assess antitumor activity. The starting dose was 100 mg/m(2) administered orally, once daily, continuously for 28-day treatment cycles. The dose could be escalated to 150 mg/m(2)/d after two cycles. Radiographic response to vandetanib was quantified using RECIST (v1.0), biomarker response was measured by comparing posttreatment serum calcitonin and carcinoembryonic antigen (CEA) levels to baseline, and a patient-reported outcome was used to assess clinical benefit., Results: Sixteen patients with locally advanced or metastatic MTC received vandetanib for a median (range) 27 (2-52) cycles. Eleven patients remain on protocol therapy. Diarrhea was the primary dose-limiting toxicity. In subjects with M918T RET germline mutations (n = 15) the confirmed objective partial response rate was 47% (exact 95% confidence intervals, 21%-75%). Biomarker partial response was confirmed for calcitonin in 12 subjects and for CEA in 8 subjects., Conclusion: Using an innovative trial design and selecting patients based on target gene expression, we conclude that vandetanib 100 mg/m(2)/d is a well-tolerated and highly active new treatment for children and adolescents with MEN2B and locally advanced or metastatic MTC., (©2013 AACR.)

Published

2013

45. Safety and activity of crizotinib for paediatric patients with refractory solid tumours or anaplastic large-cell lymphoma: a Children's Oncology Group phase 1 consortium study.

Author

Mossé YP, Lim MS, Voss SD, Wilner K, Ruffner K, Laliberte J, Rolland D, Balis FM, Maris JM, Weigel BJ, Ingle AM, Ahern C, Adamson PC, and Blaney SM

Subjects

Adolescent, Age Factors, Anaplastic Lymphoma Kinase, Antineoplastic Agents administration & dosage, Antineoplastic Agents adverse effects, Antineoplastic Agents pharmacokinetics, Biomarkers, Tumor antagonists & inhibitors, Biomarkers, Tumor genetics, Biomarkers, Tumor metabolism, Child, Child, Preschool, Crizotinib, Disease Progression, Drug Administration Schedule, Female, Humans, Infant, Lymphoma, Large-Cell, Anaplastic enzymology, Lymphoma, Large-Cell, Anaplastic genetics, Lymphoma, Large-Cell, Anaplastic pathology, Male, Maximum Tolerated Dose, Molecular Targeted Therapy, Mutation, Neoplasms enzymology, Neoplasms genetics, Neoplasms pathology, Protein Kinase Inhibitors administration & dosage, Protein Kinase Inhibitors adverse effects, Protein Kinase Inhibitors pharmacokinetics, Pyrazoles adverse effects, Pyrazoles pharmacokinetics, Pyridines adverse effects, Pyridines pharmacokinetics, Receptor Protein-Tyrosine Kinases antagonists & inhibitors, Receptor Protein-Tyrosine Kinases genetics, Receptor Protein-Tyrosine Kinases metabolism, Time Factors, Treatment Outcome, Young Adult, Antineoplastic Agents therapeutic use, Drug Resistance, Neoplasm genetics, Lymphoma, Large-Cell, Anaplastic drug therapy, Neoplasms drug therapy, Protein Kinase Inhibitors therapeutic use, Pyrazoles therapeutic use, Pyridines therapeutic use

Abstract

Background: Various human cancers have ALK gene translocations, amplifications, or oncogenic mutations, such as anaplastic large-cell lymphoma, inflammatory myofibroblastic tumours, non-small-cell lung cancer (NSCLC), and neuroblastoma. Therefore, ALK inhibition could be a useful therapeutic strategy in children. We aimed to determine the safety, recommended phase 2 dose, and antitumour activity of crizotinib in children with refractory solid tumours and anaplastic large-cell lymphoma., Methods: In this open-label, phase 1 dose-escalation trial, patients older than 12 months and younger than 22 years with measurable or evaluable solid or CNS tumours, or anaplastic large-cell lymphoma, refractory to therapy and for whom there was no known curative treatment were eligible. Crizotinib was given twice daily without interruption. Six dose levels (100, 130, 165, 215, 280, 365 mg/m(2) per dose) were assessed in the dose-finding phase of the study (part A1), which is now completed. The primary endpoint was to estimate the maximum tolerated dose, to define the toxic effects of crizotinib, and to characterise the pharmacokinetics of crizotinib in children with refractory cancer. Additionally, patients with confirmed ALK translocations, mutations, or amplification (part A2 of the study) or neuroblastoma (part A3) could enrol at one dose level lower than was currently given in part A1. We assessed ALK genomic status in tumour tissue and used quantitative RT-PCR to measure NPM-ALK fusion transcript in bone marrow and blood samples of patients with anaplastic large-cell lymphoma. All patients who received at least one dose of crizotinib were evaluable for response; patients completing at least one cycle of therapy or experiencing dose limiting toxicity before that were considered fully evaluable for toxicity. This study is registered with ClinicalTrials.gov, NCT00939770., Findings: 79 patients were enrolled in the study from Oct 2, 2009, to May 31, 2012. The median age was 10.1 years (range 1.1-21.4); 43 patients were included in the dose escalation phase (A1), 25 patients in part A2, and 11 patients in part A3. Crizotinib was well tolerated with a recommended phase 2 dose of 280 mg/m(2) twice daily. Grade 4 adverse events in cycle 1 were neutropenia (two) and liver enzyme elevation (one). Grade 3 adverse events that occurred in more than one patient in cycle 1 were lymphopenia (two), and neutropenia (eight). The mean steady state peak concentration of crizotinib was 630 ng/mL and the time to reach this peak was 4 h (range 1-6). Objective tumour responses were documented in 14 of 79 patients (nine complete responses, five partial responses); and the anti-tumour activity was enriched in patients with known activating ALK aberrations (eight of nine with anaplastic large-cell lymphoma, one of 11 with neuroblastoma, three of seven with inflammatory myofibroblastic tumour, and one of two with NSCLC)., Interpretation: The findings suggest that a targeted inhibitor of ALK has antitumour activity in childhood malignancies harbouring ALK translocations, particularly anaplastic large-cell lymphoma and inflammatory myofibroblastic tumours, and that further investigation in the subset of neuroblastoma harbouring known ALK oncogenic mutations is warranted., Funding: Pfizer and National Cancer Institute grant to the Children's Oncology Group., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

46. Phase I trial and pharmacokinetic study of sorafenib in children with neurofibromatosis type I and plexiform neurofibromas.

Author

Kim A, Dombi E, Tepas K, Fox E, Martin S, Wolters P, Balis FM, Jayaprakash N, Turkbey B, Muradyan N, Choyke PL, Reddy A, Korf B, and Widemann BC

Subjects

Adolescent, Antineoplastic Agents administration & dosage, Antineoplastic Agents adverse effects, Child, Child, Preschool, Female, Humans, Male, Maximum Tolerated Dose, Neurofibroma, Plexiform etiology, Neurofibromatosis 1 complications, Niacinamide administration & dosage, Niacinamide adverse effects, Niacinamide pharmacokinetics, Phenylurea Compounds administration & dosage, Phenylurea Compounds adverse effects, Sorafenib, Antineoplastic Agents pharmacokinetics, Neurofibroma, Plexiform drug therapy, Neurofibromatosis 1 drug therapy, Niacinamide analogs & derivatives, Phenylurea Compounds pharmacokinetics

Abstract

Background: Sorafenib targets multiple pathways thought to be crucial in growth of plexiform neurofibroma (PN) in children with neurofibromatosis type 1 (NF1). Sorafenib has been tolerated with manageable toxicities in adults and children with refractory cancer. We conducted a separate study in this population. Monitoring long-term toxicities such as effects on growth and obtaining additional pharmacokinetic data were of importance due to the young age and long duration of therapy seen in previous phase I trials in children with NF1., Procedure: Children ≥3 and ≤18-year-old with NF1 and inoperable PN were eligible. Sorafenib was administered orally twice daily for consecutive 28-day cycles. Maximum tolerated dose (MTD) was determined from toxicities observed during the first three cycles., Results: Nine children enrolled, median age 8 (6-12) years. At the starting 115 mg/m(2) /dose (n = 5), two experienced dose-limiting grade 3 pain in their PN. At the de-escalated 80 mg/m(2) /dose (n = 4), approximately 40% of the pediatric solid tumor MTD, two had dose-limiting toxicity (grade 3 rash and grade 4 mood alteration), exceeding the MTD. At 80 mg/m(2) /dose, the median AUC(0-12 hours) at steady-state was 39.5 µg hours/ml. Toxicities appeared to correspond with decreases in quality of life (QOL). No tumor shrinkage was observed., Conclusions: Children with NF1 and PN did not tolerate sorafenib at doses substantially lower than the MTD in children and adults with malignant solid tumors. Future trials with targeted agents for children with NF1 may require a more conservative starting dose and separate definitions of dose limiting toxicities (DLT) than children with cancer., (Copyright © 2012 Wiley Periodicals, Inc.)

Published

2013

47. A phase I trial and pharmacokinetic study of sorafenib in children with refractory solid tumors or leukemias: a Children's Oncology Group Phase I Consortium report.

Author

Widemann BC, Kim A, Fox E, Baruchel S, Adamson PC, Ingle AM, Glade Bender J, Burke M, Weigel B, Stempak D, Balis FM, and Blaney SM

Subjects

Adolescent, Antineoplastic Agents adverse effects, Antineoplastic Agents pharmacokinetics, Child, Child, Preschool, Female, Humans, Male, Niacinamide pharmacokinetics, Niacinamide therapeutic use, Phenylurea Compounds pharmacokinetics, Protein Kinase Inhibitors adverse effects, Protein Kinase Inhibitors pharmacokinetics, Sorafenib, Treatment Outcome, Young Adult, Antineoplastic Agents therapeutic use, Leukemia drug therapy, Neoplasms drug therapy, Niacinamide analogs & derivatives, Phenylurea Compounds therapeutic use, Protein Kinase Inhibitors therapeutic use

Abstract

Purpose: To determine the dose-limiting toxicities (DLT), maximum tolerated dose (MTD), pharmacokinetics, and pharmacodynamics of sorafenib in children with refractory extracranial solid tumors and evaluate the tolerability of the solid tumor MTD in children with refractory leukemias., Experimental Design: Sorafenib was administered orally every 12 hours for consecutive 28-day cycles. Pharmacokinetics (day 1 and steady-state) and pharmacodynamics were conducted during cycle 1., Results: Of 65 patients enrolled, 60 were eligible. In the solid tumor cohort (n = 49), 4 of 6 patients experienced a DLT [hypertension, pain, rash/urticaria, thrombocytopenia, alanine aminotransferase (ALT)/aspartate aminotransferase (AST)] at the starting dose (150 mg/m(2)/dose) which resulted in de-escalation to 105 mg/m(2)/dose. After eligibility criteria modification and dose re-escalation, the MTD was 200 mg/m(2)/dose for solid tumors and 150 mg/m(2)/dose for leukemias. Sorafenib exposure was highly variable between patients but was within the ranges reported in adults. The apparent sorafenib clearance increased with patient age. Diarrhea, rash, fatigue, and increased ALT/AST were the most common sorafenib-related toxicities. Stable disease for 4 or more cycles was observed in 14 solid tumor patients, and 2 patients with acute myeloid leukemia (AML) and FLT3 internal tandem duplication (FLT3ITD) experienced a decrease in bone marrow blasts to less than 5%., Conclusions: The recommended phase II dose of sorafenib administered every 12 hours continuously for children with solid tumors is 200 mg/m(2)/dose and 150 mg/m(2)/dose for children with leukemias. Sorafenib toxicities and distribution in children are similar to adults. The activity of sorafenib in children with AML and FLT3ITD is currently being evaluated, and a phase II study for select solid tumors is ongoing., (©2012 AACR.)

Published

2012

48. The plasma and cerebrospinal fluid pharmacokinetics of sorafenib after intravenous administration in non-human primates.

Author

Kim A, McCully C, Cruz R, Cole DE, Fox E, Balis FM, and Widemann BC

Subjects

Animals, Antineoplastic Agents blood, Antineoplastic Agents cerebrospinal fluid, Area Under Curve, Benzenesulfonates blood, Benzenesulfonates cerebrospinal fluid, Blood-Brain Barrier metabolism, Capillary Permeability, Chromatography, High Pressure Liquid, Half-Life, Infusions, Intravenous, Macaca mulatta, Male, Metabolic Clearance Rate, Models, Animal, Models, Biological, Niacinamide analogs & derivatives, Phenylurea Compounds, Protein Binding, Protein Kinase Inhibitors blood, Protein Kinase Inhibitors cerebrospinal fluid, Pyridines blood, Pyridines cerebrospinal fluid, Sorafenib, Tandem Mass Spectrometry, Antineoplastic Agents administration & dosage, Antineoplastic Agents pharmacokinetics, Benzenesulfonates administration & dosage, Benzenesulfonates pharmacokinetics, Protein Kinase Inhibitors administration & dosage, Protein Kinase Inhibitors pharmacokinetics, Pyridines administration & dosage, Pyridines pharmacokinetics

Abstract

Purpose: Sorafenib is a small molecule inhibitor of multiple signaling kinases thought to contribute to the pathogenesis of many tumors including brain tumors. Clinical trials with sorafenib in primary and metastatic brain tumors are ongoing. We evaluated the plasma and cerebrospinal fluid (CSF) pharmacokinetics (PK) of sorafenib after an intravenous (IV) dose in a non-human primate (NHP) model., Methods: 7.3 mg/kg of sorafenib free base equivalent solubilized in 20% cyclodextrin was administered IV over 1 h to three adult rhesus monkeys. Serial paired plasma and CSF samples were collected over 24 h. Sorafenib was quantified with a validated HPLC/tandem mass spectrometry assay. PK parameters were estimated using non-compartmental methods. CSF penetration was calculated from the AUC(CSF) : AUC(plasma)., Results: Peak plasma concentrations after IV dosing ranged from 3.4 to 7.6 μg/mL. The mean ± standard deviation (SD) area under the plasma concentration from 0 to 24 h was 28 ± 4.3 μg • h/mL, which is comparable to the exposure observed in humans at recommended doses. The mean ± SD clearance was 1.7 ± 0.5 mL/min/kg. The peak CSF concentrations ranged from 0.00045 to 0.00058 μg/mL. The mean ± SD area under the CSF concentration from 0 to 24h was 0.0048 ± 0.0016 μg•h/mL. The mean CSF penetration of sorafenib was 0.02% and 3.4% after correcting for plasma protein binding., Conclusion: Sorafenib is well tolerated in NHP and measurable in CSF after an IV dose. The CSF penetration of sorafenib is limited relative to total and free drug exposure in plasma.

Published

2012

49. Retained platinum uptake and indifference to p53 status make novel transplatinum agents active in platinum-resistant cells compared to cisplatin and oxaliplatin.

Author

Murphy RF, Komlodi-Pasztor E, Robey R, Balis FM, Farrell NP, and Fojo T

Subjects

Antineoplastic Agents chemistry, Apoptosis drug effects, Cell Cycle Checkpoints drug effects, Cell Line, Tumor, Cisplatin chemistry, DNA chemistry, DNA metabolism, Drug Resistance, Neoplasm drug effects, Humans, Organoplatinum Compounds chemistry, Oxaliplatin, Antineoplastic Agents toxicity, Cisplatin toxicity, Organoplatinum Compounds toxicity, Tumor Suppressor Protein p53 metabolism

Abstract

Despite the clinical success of platinum-containing drugs in the treatment of solid tumors, acquired resistance remains a major obstacle. We previously identified a group of novel transplanaramine or transplatinum compounds based on distinct activity profiles in the NCI-60 panel. In the present study, parental KB-3.1 cells with wild-type p53 and its cisplatin- and oxaliplatin-resistant sublines harboring mutant p53 proteins were used to contrast several transplatinum compounds with cisplatin and oxaliplatin. The transplatinum compounds retained cytotoxic activity in the resistant cell lines. While intracellular accumulation and DNA platination of cisplatin and oxaliplatin was decreased in the resistant cells, the transplatinum compounds both accumulated intracellularly and platinated DNA at comparable levels in all cell lines. Cytoflow analysis confirmed that cisplatin and oxaliplatin alter the cell cycle distribution and result in apoptosis; however, at comparably toxic concentrations, the transplatinum compounds did not alter the cell cycle distribution. Analysis of the cytoplasmic fraction treated with acetone showed that cisplatin and oxaliplatin readily bound to macromolecules in the pellet, whereas a larger percentage of the transplatinum compounds remained in the supernatant. We concluded that, distinct from platinum compounds currently in use, transplatinum compounds accumulate intracellularly in resistant cells at levels comparable to those in drug-sensitive cells, do not affect the cell cycle and thus retain cytotoxicity independent of p53 status and likely have cytoplasmic targets that are important in their activity.

Published

2012

50. A phase II study of O6-benzylguanine and temozolomide in pediatric patients with recurrent or progressive high-grade gliomas and brainstem gliomas: a Pediatric Brain Tumor Consortium study.

Author

Warren KE, Gururangan S, Geyer JR, McLendon RE, Poussaint TY, Wallace D, Balis FM, Berg SL, Packer RJ, Goldman S, Minturn JE, Pollack IF, Boyett JM, and Kun LE

Subjects

Adolescent, Brain Stem Neoplasms mortality, Child, Child, Preschool, DNA Modification Methylases metabolism, DNA Repair Enzymes metabolism, Dacarbazine therapeutic use, Drug Therapy, Combination methods, Female, Glioma mortality, Guanine therapeutic use, Humans, Kaplan-Meier Estimate, Ki-67 Antigen metabolism, Male, Proportional Hazards Models, Retrospective Studies, Temozolomide, Tumor Suppressor Proteins metabolism, Young Adult, Antineoplastic Agents therapeutic use, Brain Stem Neoplasms drug therapy, Dacarbazine analogs & derivatives, Glioma drug therapy, Guanine analogs & derivatives

Abstract

To estimate the sustained (≥8 weeks) objective response rate in pediatric patients with recurrent or progressive high-grade gliomas (HGG, Stratum A) or brainstem gliomas (BSG, Stratum B) treated with the combination of O6-benzylguanine (O6BG) and temozolomide(®) (TMZ). Patients received O6BG 120 mg/m(2)/d IV followed by TMZ 75 mg/m(2)/d orally daily for 5 consecutive days of each 28-day course. The target objective response rate to consider the combination active was 17%. A two-stage design was employed. Forty-three patients were enrolled; 41 were evaluable for response, including 25 patients with HGG and 16 patients with BSG. The combination of O6BG and TMZ was tolerable, and the primary toxicities were myelosuppression and gastrointestinal symptoms. One sustained (≥8 weeks) partial response was observed in the HGG cohort; no sustained objective responses were observed in the BSG cohort. Long-term (≥6 courses) stable disease (SD) was observed in 4 patients in Stratum A and 1 patient in Stratum B. Of the 5 patients with objective response or long-term SD, 3 underwent central review with 2 reclassified as low-grade gliomas. The combination of O6BG and TMZ did not achieve the target response rate for activity in pediatric patients with recurrent or progressive HGG and BSG.

Published

2012