Your search keyword '"Rodman JH"' showing total 74 results

1. Pharmacokinetics of oral zidovudine administered during labour: a preliminary study*

Author

Mirochnick, M, primary, Rodman, JH, additional, Robbins, BL, additional, Fridland, A, additional, Gandía, J, additional, Hitti, J, additional, Bardeguez, A, additional, Rathore, MH, additional, Gonzalez Garcia, A, additional, Cababasay, M, additional, Samson, P, additional, Mofenson, L, additional, Bryson, YJ, additional, and Dorenbaum, A, additional

Published

2007

2. RELATIONSHIP BETWEEN DOSE-RATE OF (6RS)LEUCOVORIN ADMINISTRATION, PLASMA-CONCENTRATIONS OF REDUCED FOLATES, AND POOLS OF 5,10-METHYLENETETRAHYDROFOLATES AND TETRAHYDROFOLATES IN HUMAN COLON ADENOCARCINOMA XENOGRAFTS

Author

HOUGHTON, JA, WILLIAMS, LG, DEGRAAF, SSN, CHESHIRE, PJ, RODMAN, JH, MANEVAL, DC, WAINER, IW, JADAUD, P, and HOUGHTON, PJ

Published

1990

3. Pharmacokinetics of subcutaneous recombinant human granulocyte colony- stimulating factor in children

Author

Stute, N, primary, Santana, VM, additional, Rodman, JH, additional, Schell, MJ, additional, Ihle, JN, additional, and Evans, WE, additional

Published

1992

4. Abacavir and metabolite pharmacokinetics in HIV-1-infected children and adolescents.

Author

Cross SJ, Rodman JH, Lindsey JC, Robbins BL, Rose CH, Yuen GJ, and D'angelo LJ

Subjects

Administration, Oral, Adolescent, Age Factors, Anti-HIV Agents administration & dosage, Anti-HIV Agents metabolism, Child, Dideoxynucleosides administration & dosage, Dideoxynucleosides metabolism, Female, HIV Infections drug therapy, Humans, Male, Metabolic Clearance Rate, Anti-HIV Agents pharmacokinetics, Dideoxynucleosides pharmacokinetics, HIV Infections metabolism, HIV-1

Abstract

Objectives: Abacavir (ABC) oral clearance, adjusted for body size, is approximately 2 times higher for children than adults with a corresponding difference in dose regimens. However, there are limited data available in the adolescent population. The pharmacokinetics (PKs) of ABC and primary metabolites were determined in HIV-1-infected children and adolescents to evaluate age and patient characteristics as a basis for adjusting ABC dose regimens and to assess the influence of metabolite formation on PK parameters., Methods: Pediatric subjects 9-18 years of age receiving antiretroviral therapy for HIV-1 infection were stratified by Tanner stage and given a single 8 mg/kg dose of ABC oral solution. Blood samples (n = 10) were obtained over 8 hours and measured for ABC, glucuronide, and carboxylate metabolites using high-performance liquid chromatography. PK parameters for children (Tanner stages 1-2; TS1) and adolescents (Tanner stages 3-5; TS2) were compared., Results: Twenty-five subjects were enrolled. ABC mean (range) maximum concentration (Cmax; microg/mL), area under the curve (microg.hr/mL), half-life (hours), and apparent clearance (CL/F; mL/min per kg) for TS1 and TS2 were 3.5 (1.2-5.6) vs 3.4 (1.8-5.9), 8.0 (2.1-18.6) vs 8.9 (3.1-17.2), 1.3 (0.7-2.5) vs 1.4 (0.9-1.9), and 22.1 (7.0-59.2) vs 18.4 (7.7-42.9) and not significantly different. Age, Tanner stage, and sex were not correlated with ABC clearance by univariate analysis. The ratios of metabolites to ABC area under the curve were correlated with ABC clearance as were the ratios of metabolites to ABC concentrations at the 6-hour time point., Conclusions: ABC oral clearance in HIV-1-infected pediatric patients does not change during puberty, is similar to younger children, and is higher than previously published in adults. Therefore, dosing adolescents as adults should be reexamined. Intersubject PK variability is substantial and is not correlated with body size or age but more likely due to differences in metabolite formation that may be genetic in origin.

Published

2009

5. Pharmacokinetics, safety and efficacy of lopinavir/ritonavir in infants less than 6 months of age: 24 week results.

Author

Chadwick EG, Capparelli EV, Yogev R, Pinto JA, Robbins B, Rodman JH, Chen J, Palumbo P, Serchuck L, Smith E, and Hughes M

Subjects

Antiretroviral Therapy, Highly Active, Brazil, CD4 Lymphocyte Count, Child, Preschool, Drug Administration Schedule, Female, HIV Protease Inhibitors administration & dosage, HIV Protease Inhibitors adverse effects, Humans, Infant, Lopinavir, Male, Prospective Studies, Pyrimidinones administration & dosage, Pyrimidinones adverse effects, Ritonavir administration & dosage, Ritonavir adverse effects, Treatment Outcome, United States, HIV Infections drug therapy, HIV Infections metabolism, HIV Protease Inhibitors pharmacokinetics, HIV Protease Inhibitors therapeutic use, HIV-1, Pyrimidinones pharmacokinetics, Pyrimidinones therapeutic use, Ritonavir pharmacokinetics, Ritonavir therapeutic use

Abstract

Objective: To investigate pharmacokinetics, safety and efficacy of lopinavir/ritonavir (LPV/r)-based therapy in HIV-1-infected infants 6 weeks to 6 months of age., Methods: A prospective, multicenter, open-label trial of 21 infants with HIV-1 RNA > 10 000 copies/ml and treated with LPV/r 300/75 mg/m twice daily plus two nucleoside reverse transcriptase inhibitors. Intensive pharmacokinetic sampling was performed at 2 weeks and predose concentrations were collected every 8 weeks; safety and plasma HIV-1 RNA were monitored every 4-12 weeks for 24 weeks., Results: Median age at enrollment was 14.7 weeks (range, 6.9-25.7) and 19/21 completed > or= 24 weeks of study. Although LPV/r apparent clearance was slightly higher than in older children, the median area under the concentration-time curve 0-12 h (67.5 mug.h/ml) was in the range reported from older children taking the recommended dose of 230/57.5 mg/m. Predose concentrations stabilized at a higher level after the first 2 weeks of study. In as-treated analysis at week 24, 10/19 (53%) had plasma HIV-1 RNA < 400 copies/ml (median change, -3.33 log10 copies/ml); poor adherence contributed to delayed viral suppression, which improved with longer follow-up. Three infants (14%) had transient adverse events of grade 3 or more that were possibly related to study treatment but did not require permanent treatment discontinuation., Conclusion: Despite higher clearance in infants 6 weeks to 6 months of age, a twice daily dose of 300/75 mg/m LPV/r provided similar exposure to that in older children, was well tolerated and provided favorable virological and clinical efficacy.

Published

2008

6. Simultaneous measurement of intracellular triphosphate metabolites of zidovudine, lamivudine and abacavir (carbovir) in human peripheral blood mononuclear cells by combined anion exchange solid phase extraction and LC-MS/MS.

Author

Robbins BL, Poston PA, Neal EF, Slaughter C, and Rodman JH

Subjects

HIV Infections blood, Humans, Reference Standards, Chromatography, High Pressure Liquid methods, Dideoxynucleosides blood, Lamivudine blood, Phosphates blood, Reverse Transcriptase Inhibitors blood, Tandem Mass Spectrometry methods, Zidovudine blood

Abstract

All nucleoside reverse transcriptase inhibitors (NRTI) must first be metabolized to their triphosphate forms in order to be active against HIV. Zidovudine (ZDV), abacavir (ABC) and lamivudine (3TC) have proven to be an efficacious combination. In order simultaneously to measure intracellular levels of the triphosphates (-TP) of ZDV, ABC (carbovir, CBV) and 3TC, either together or individually, we have developed a cartridge-LC-MS/MS method. The quantitation range was 2.5-250 pg/microl for 3TC-TP, 0.1-10.0 pg/microl for ZDV-TP and 0.05-5.00 pg/microl for CBV-TP. This corresponds to 0.1-11.0 pmol 3TC-TP per million cells, 4-375 fmol ZDV-TP per million cells and 2-200 fmol CBV-TP per million cells, extracted from 10 million cells. Patient samples demonstrated measured levels in the middle regions of our standard curves both at pre-dose and 4h post-dose times.

Published

2007

7. Model for intracellular Lamivudine metabolism in peripheral blood mononuclear cells ex vivo and in human immunodeficiency virus type 1-infected adolescents.

Author

Zhou Z, Rodman JH, Flynn PM, Robbins BL, Wilcox CK, and D'Argenio DZ

Subjects

Adolescent, Adult, Anti-HIV Agents pharmacokinetics, Bayes Theorem, Cross-Over Studies, HIV Infections metabolism, Humans, Lamivudine administration & dosage, Lamivudine pharmacokinetics, Models, Biological, Reverse Transcriptase Inhibitors pharmacokinetics, Anti-HIV Agents metabolism, HIV Infections drug therapy, HIV-1, Lamivudine metabolism, Leukocytes, Mononuclear metabolism, Reverse Transcriptase Inhibitors metabolism

Abstract

The pharmacologic variability of nucleoside reverse transcriptase inhibitors such as lamivudine (3TC) includes not only systemic pharmacokinetic variability but also interindividual differences in cellular transport and metabolism. A modeling strategy linking laboratory studies of intracellular 3TC disposition with clinical studies in adolescent patients is described. Data from ex vivo laboratory experiments using peripheral blood mononuclear cells (PBMCs) from uninfected human subjects were first used to determine a model and population parameter estimates for 3TC cellular metabolism. Clinical study data from human immunodeficiency virus type 1-infected adolescents were then used in a Bayesian population analysis, together with the prior information from the ex vivo analysis, to develop a population model for 3TC systemic kinetics and cellular kinetics in PBMCs from patients during chronic therapy. The laboratory results demonstrate that the phosphorylation of 3TC is saturable under clinically relevant concentrations, that there is a rapid equilibrium between 3TC monophosphate and diphosphate and between 3TC diphosphate and triphosphate, and that 3TC triphosphate is recycled to 3TC monophosphate through a 3TC metabolite that remains to be definitively characterized. The resulting population model shows substantial interindividual variability in the cellular kinetics of 3TC with population coefficients of variation for model parameters ranging from 47 to 87%. This two-step ex vivo/clinical modeling approach using Bayesian population modeling of 3TC that links laboratory and clinical data has potential application for other drugs whose intracellular pharmacology is a major determinant of activity and/or toxicity.

Published

2006

8. Ritonavir-based highly active antiretroviral therapy in human immunodeficiency virus type 1-infected infants younger than 24 months of age.

Author

Chadwick EG, Rodman JH, Britto P, Powell C, Palumbo P, Luzuriaga K, Hughes M, Abrams EJ, Flynn PM, Borkowsky W, and Yogev R

Subjects

Age Factors, Antiretroviral Therapy, Highly Active adverse effects, Child, Preschool, Dose-Response Relationship, Drug, Drug Administration Schedule, Female, Follow-Up Studies, HIV Infections mortality, HIV Infections physiopathology, HIV-1 isolation & purification, Humans, Infant, Infant, Newborn, Lamivudine administration & dosage, Lamivudine pharmacokinetics, Male, Maximum Tolerated Dose, Prospective Studies, Risk Assessment, Severity of Illness Index, Single-Blind Method, Survival Rate, Treatment Outcome, Zidovudine administration & dosage, Zidovudine pharmacokinetics, Antiretroviral Therapy, Highly Active methods, HIV Infections congenital, HIV Infections drug therapy, HIV-1 drug effects, Ritonavir administration & dosage, Ritonavir pharmacokinetics

Abstract

Background: Few data are available regarding clinical outcomes or dosing requirements for the protease inhibitor ritonavir in human immunodeficiency virus (HIV)-infected children younger than under 24 months of age., Methods: This prospective, multicenter phase I/II open label treatment trial used ritonavir, zidovudine and lamivudine to treat protease inhibitor-naive, HIV-infected infants between the ages of 4 weeks and 24 months. Two sequential dosing cohorts were treated with 350 or 450 mg/m(2) ritonavir every 12 hours; this report includes results of pharmacokinetics, safety, tolerability and efficacy through 104 weeks of follow-up of all subjects., Results: Fifty HIV-infected children were treated. By week 16, 36 had achieved HIV-1 RNA <400 copies/mL (72% intent-to-treat, 84% as-treated analysis); by week 104, 18 maintained durable viral suppression (36% intent-to-treat, 46% as-treated). Poor medication adherence by caregiver report contributed to virologic failure. Few subjects experienced treatment-limiting toxicity: emesis or ritonavir refusal in 6 (12%); and severe but reversible anemia or elevated serum hepatic transaminases in 1 (4%) each. Apparent oral clearance was higher and the median predose concentrations were substantially lower than those found in adults. Median z scores for weight and height for age/gender were below normal at baseline but improved by week 104., Conclusions: A combination regimen of ritonavir, zidovudine and lamivudine was generally safe and produced sustained viral suppression in more than one-third of infants who initiated therapy before 2 years of age. Improved palatability of liquid preparations of protease inhibitors, supporting infrastructure and behavioral approaches to improve medication adherence with antiretrovirals will likely be necessary to further improve efficacy.

Published

2005

9. Metabolism of tenofovir and didanosine in quiescent or stimulated human peripheral blood mononuclear cells.

Author

Robbins BL, Wilcox CK, Fridland A, and Rodman JH

Subjects

Adenine chemistry, Anti-HIV Agents chemistry, Cells, Cultured, Chromatography, High Pressure Liquid, Culture Media, Didanosine chemistry, Drug Interactions, Humans, Organophosphorus Compounds chemistry, Phosphorylation, Tenofovir, Adenine analogs & derivatives, Adenine metabolism, Anti-HIV Agents metabolism, Didanosine metabolism, Leukocytes, Mononuclear metabolism, Organophosphonates, Organophosphorus Compounds metabolism

Abstract

Objective: As tenofovir disoproxil fumarate substantially increases plasma concentrations of didanosine in patients with human immunodeficiency virus-1 infection, we sought to determine whether tenofovir and didanosine showed a similar intracellular interaction in human peripheral blood mononuclear cells (PBMCs)., Design: Comparative in vitro incubation of two antiretrovirals in lymphocytes., Setting: Clinical research laboratory., Material: Radiolabeled tenofovir and didanosine in human PBMCs., Measurements and Main Results: Phosphorylation of 2 and 20 microM didanosine to dideoxyadenosine triphosphate (ddATP) was determined in quiescent and stimulated PBMCs in the presence or absence of 5 microM tenofovir. Similarly, phosphorylation of 5 microM tenofovir to tenofovir diphosphate (TFVpp) was examined in the presence or absence of 2 and 20 microM didanosine. Intracellular amounts of ddATP and TFVpp were determined by incubating PBMCs with radiolabeled tenofovir or didanosine alone and together for up to 16 hours and then separating the anabolites by high-performance liquid chromatography for quantitation. The presence of tenofovir did not affect the amount of ddATP in quiescent or stimulated PBMCs with 2 or 20 microM didanosine. In addition, didanosine did not alter the amount of TFVpp that formed. The amount of ddATP was modestly (1.5-3-fold) but consistently higher in stimulated than in quiescent PBMCs, but the amount of TFVpp did not differ., Conclusion: There is no significant interaction between tenofovir and didanosine in human PBMCs as determined by the extent of formation of the phosphorylated anabolites. This suggests that adjusting didanosine dosage, when given with tenofovir, to achieve similar didanosine plasma concentrations, may be sufficient to accommodate the systemic drug interaction.

Published

2003

10. Design of antiretroviral clinical trials for HIV-1 infected pregnant women and their newborn infants.

Author

Rodman JH

Subjects

Acquired Immunodeficiency Syndrome prevention & control, Anti-HIV Agents pharmacokinetics, Female, Fetus drug effects, Humans, Infant, Newborn, Infectious Disease Transmission, Vertical, Pregnancy, Acquired Immunodeficiency Syndrome drug therapy, Acquired Immunodeficiency Syndrome transmission, Anti-HIV Agents adverse effects, Anti-HIV Agents therapeutic use, Clinical Trials as Topic, Pregnancy Complications, Infectious virology

Abstract

Antiretroviral therapy has been highly successful in reducing mother to child transmission of human immunodeficiency virus-1 infection in pregnant women. However, the treatment regimens are intensive, difficult to deliver in less developed countries, and there are limited pharmacology studies addressing critical questions regarding maternal safety and fetal risk. There are currently 3 pharmacologically diverse classes of antiretroviral agents with inadequate information available to define drug disposition necessary to determine appropriate dose regimens and limited data on long-term adverse events. This article summarizes representative clinical studies for selected antiretrovirals that provide a framework for continuing the necessary clinical research to extend successful outcomes in developed countries to human immunodeficiency virus-1 infected pregnant women and infants world-wide and minimize the risk of long-term adverse effects.

Published

2001

11. Single-dose pharmacokinetics and safety of the oral antiviral compound adefovir dipivoxil in children infected with human immunodeficiency virus type 1. The Pediatrics AIDS Clinical Trials Group.

Author

Hughes WT, Shenep JL, Rodman JH, Fridland A, Willoughby R, Blanchard S, Purdue L, Coakley DF, Cundy KC, Culnane M, Zimmer B, Burchett S, and Read JS

Subjects

Adenine adverse effects, Adenine pharmacokinetics, Adenine therapeutic use, Adolescent, Antiviral Agents adverse effects, Antiviral Agents therapeutic use, Area Under Curve, Child, Child, Preschool, Female, HIV Infections drug therapy, Half-Life, Humans, Infant, Male, Adenine analogs & derivatives, Antiviral Agents pharmacokinetics, HIV Infections metabolism, HIV-1, Organophosphonates

Abstract

The acyclic phosphonate analog adefovir is a potent inhibitor of retroviruses, including human immunodeficiency virus (HIV) type 1, and, unlike some antiviral nucleosides, does not require the initial phosphorylation step for its activity. Two oral dosages of the adefovir prodrug adefovir dipivoxil were evaluated in a phase I study with children with HIV infection. A total of 14 patients were stratified into age groups ranging from 6 months to 18 years of age. Eight patients received 1.5 mg of adefovir dipivoxil per kg of body weight, and six patients received 3.0 mg of adefovir dipivoxil per kg. Serum samples were obtained at intervals during the 8 h postdosing and were analyzed for adefovir concentrations. Patients were monitored for adverse effects. All samples collected resulted in quantifiable levels of adefovir (lower limit of quantitation, 25 ng/ml) from each patient. The areas under the concentration-versus-time curves (AUCs) were similar (P = 0.85) for the 1.5- and 3.0-mg/kg doses, while the apparent oral clearance (CL/F) was significantly higher (P = 0.05) for the 3-mg/kg dose. Pharmacokinetic parameters differed by patient age. In comparing those children older and younger than the median age of 5.1 years, AUC (P = 0.03), maximum concentration of drug in serum (P = 0.004), and the concentration at 8 h postdosing (P = 0.02) were significantly lower for the younger children. There were no significant differences for apparent volume of distribution and CL/F normalized to body surface area, but there was a suggestive difference in half-life (P = 0.07) among the subjects in the older and younger age groups. No significant adverse events were encountered. These data provide the basis for a multidose phase II study of adefovir dipivoxil in HIV-infected infants and children.

Published

2000

12. Effect of food and pharmacokinetic variability on didanosine systemic exposure in HIV-infected children. Pediatric AIDS Clinical Trials Group Protocol 144 Study Team.

Author

Stevens RC, Rodman JH, Yong FH, Carey V, Knupp CA, and Frenkel LM

Subjects

Administration, Oral, Adolescent, Area Under Curve, Biological Availability, Child, Child, Preschool, Didanosine blood, Double-Blind Method, Fasting blood, Female, HIV Infections blood, HIV Infections drug therapy, Humans, Infant, Infant, Newborn, Male, Randomized Controlled Trials as Topic, Reverse Transcriptase Inhibitors blood, Didanosine pharmacokinetics, Food, HIV Infections metabolism, HIV-1, Reverse Transcriptase Inhibitors pharmacokinetics

Abstract

The effect of food on didanosine bioavailability and interpatient pharmacokinetic variability was examined in children infected with human immunodeficiency virus type 1 (HIV-1). Didanosine pharmacokinetics were determined during fasting and fed conditions in HIV-infected children enrolled in the Pediatric AIDS Clinical Trials Group Protocol 144 randomized to receive didanosine at 50 mg/m2 or 150 mg/m2 orally every 12 hr. Pharmacokinetic parameters from patients in the low (n = 39) and high (n = 38) dosing groups were not significantly different, but intersubject variability was substantial. The fraction absorbed was higher while fasting than with food (0.27+/-0.13 versus 0.19+/-0.09, p < 0.0001); the zero order absorption rate was faster (0.48+/-0.31 versus 0.76+/-0.72 hr, p = 0.003); and the plasma half-life was shorter (0.93+/-0.43 versus 1.39+/-0.65 hr, p < 0.0001). The lower fraction absorbed with food was offset by the absorption rate becoming rate limiting for elimination, resulting in similar areas under the concentration-time curves (normalized to 100 mg/m2) when fasted (853.9+/-465.8 microg/liter-hr) versus fed (796.3+/-367.5 microg/liter x hr). Oral clearances during fasting (152.5+/-81.7 liters/hr/m2) and fed states (163.6+/-99.3 liters/hr/m2) were similar, but these values in children are substantially higher than previously reported for adults. The systemic exposure (i.e., AUC) of didanosine was highly variable in children but similar in the presence and absence of food. Administration of didanosine with food in children may be permissible if total systemic exposure rather than maximum plasma concentration is sufficient for antiretroviral activity. The higher oral clearance and substantial pharmacokinetic variability suggest the need to reexamine current didanosine dose recommendations for HIV-infected children.

Published

2000

13. Systemic pharmacokinetics and cellular pharmacology of zidovudine in human immunodeficiency virus type 1-infected women and newborn infants.

Author

Rodman JH, Flynn PM, Robbins B, Jimenez E, Bardeguez AD, Rodriguez JF, Blanchard S, and Fridland A

Subjects

Adolescent, Adult, Anti-HIV Agents blood, Anti-HIV Agents therapeutic use, Dideoxynucleotides, Female, Fetal Blood chemistry, Fetal Blood virology, HIV Infections blood, HIV Infections transmission, HIV Infections virology, Humans, Infant, Infant, Newborn, Infectious Disease Transmission, Vertical, Phosphorylation, Pregnancy, Pregnancy Complications, Infectious virology, Reverse Transcriptase Inhibitors blood, Reverse Transcriptase Inhibitors pharmacokinetics, Reverse Transcriptase Inhibitors therapeutic use, Thymine Nucleotides blood, Zidovudine analogs & derivatives, Zidovudine blood, Zidovudine therapeutic use, Anti-HIV Agents pharmacokinetics, HIV Infections drug therapy, HIV-1, Pregnancy Complications, Infectious drug therapy, Zidovudine pharmacokinetics

Abstract

Systemic and intracellular pharmacokinetics of zidovudine were determined for 28 human immunodeficiency virus type 1-infected pregnant women and their newborn infants. Plasma zidovudine and intracellular zidovudine monophosphate and triphosphate concentrations were determined in serial maternal samples and cord blood at delivery. Higher levels of cord blood zidovudine were associated with lower maternal zidovudine clearance and longer infusion times. Median levels of zidovudine monophosphate and triphosphate in maternal (1556 and 67 fmol/106 cells) and cord (1464 and 70 fmol/106 cells) blood were similar but highly variable. Intersubject pharmacokinetic variability for zidovudine is substantial, but intravenous therapy provides plasma concentrations and intracellular zidovudine triphosphate levels consistent with high antiviral activity. The substantial amount of intracellular zidovudine triphosphate in cord blood provides an explanation for the clinical success of zidovudine in reducing vertical transmission. Studies of simpler oral regimens of zidovudine can now be evaluated regarding the ability to achieve these pharmacologic end points associated with highly effective parenteral therapy.

Published

1999

14. Cyclophosphamide for the treatment of progressive low-grade astrocytoma: a Pediatric Oncology Group phase II Study.

Author

Kadota RP, Kun LE, Langston JW, Burger PC, Cohen ME, Mahoney DH, Walter AW, Rodman JH, Parent A, Buckley E, Kepner JL, and Friedman HS

Subjects

Carboplatin administration & dosage, Child, Child, Preschool, Humans, Infant, Survival Analysis, Vincristine administration & dosage, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Astrocytoma drug therapy, Brain Neoplasms drug therapy, Cyclophosphamide administration & dosage

Abstract

Purpose: Results of a phase II trial of cyclophosphamide (CPM) for children with progressive low-grade astrocytoma are reported., Patients and Methods: Fifteen patients with a median age of 39 months (range, 2 to 71) were included in this study. The tumors of 11 children were located in the optic pathway, hypothalamus, or thalamus. Four courses of intravenous CPM 1.2 g/m2 were administered every 3 weeks during the upfront window portion of this protocol. Subsequently, chemotherapy was to continue with CPM, vincristine, and carboplatin for 2 years., Results: By study design, the first 14 patients were centrally reviewed after completion of the initial 4 CPM courses. Toxicity was primarily hematologic. One patients had a complete response, 8 had stable disease, and 5 had progressive disease (PD). The excessive number of children with PD prompted study closure., Conclusion: CPM as used in this protocol showed insufficient activity against astrocytoma to justify further patient accrual.

Published

1999

15. High dose chemotherapy with autologous peripheral blood progenitor cell transplantation in an anephric child with multiply recurrent Wilms tumor.

Author

Dagher R, Kreissman S, Robertson KA, Provisor A, Bergstein J, Burke K, Rodman JH, Emanuel D, and Smith FO

Subjects

Antineoplastic Combined Chemotherapy Protocols adverse effects, Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Carboplatin administration & dosage, Carboplatin pharmacokinetics, Combined Modality Therapy, Cyclophosphamide administration & dosage, Cyclophosphamide pharmacokinetics, Dactinomycin administration & dosage, Doxorubicin administration & dosage, Drug Administration Schedule, Fatal Outcome, Female, Humans, Infant, Kidney Neoplasms radiotherapy, Kidney Neoplasms surgery, Metabolic Clearance Rate, Neoplasm Recurrence, Local radiotherapy, Nephrectomy, Peritoneal Dialysis, Salvage Therapy, Transplantation Conditioning, Vincristine administration & dosage, Wilms Tumor radiotherapy, Wilms Tumor surgery, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Hematopoietic Stem Cell Transplantation, Kidney Neoplasms drug therapy, Neoplasm Recurrence, Local drug therapy, Wilms Tumor drug therapy

Abstract

Purpose: An autologous peripheral blood progenitor cell (APBPC) transplant in an anephric child with multiply recurrent Wilms tumor using a conditioning regimen of high dose chemotherapy in conjunction with hemodialysis (HD) and peritoneal dialysis is described., Patient and Methods: The child had a left nephrectomy at 9 months of age for a stage II Wilms tumor. At 6 years of age, she required a right nephrectomy because of progressive, recurrent disease unresponsive to treatment with doxorubicin, actinomycin, and vincristine. She was maintained on peritoneal dialysis. Salvage chemotherapy consisted of 5 cycles of carboplatin and cyclophosphamide after APBPCs were collected after granulocyte colony-stimulating factor mobilization. After a preparative regimen of carboplatin, cyclophosphamide, and etoposide with closely timed HD, peripheral blood progenitor cells were infused and peritoneal dialysis was resumed., Results: No nonhematopoietic toxicity occurred. Pharmacokinetic studies demonstrated that HD effectively eliminated carboplatin and provided safe, effective plasma concentrations in this anephric patient. Trilineage engraftment occurred by day +10 and the child was discharged from the hospital on day +14. She had a local recurrence on day +194 and died of progressive disease on day +660., Conclusions: With dialysis support and dose modification, high-dose chemotherapy followed by APBPC transplantation can be successfully performed in the anephric child. Given the lack of organ toxicity in this patient, increased doses of the drugs used in this preparative regimen may be possible for anephric children.

Published

1998

16. Conventional compared with individualized chemotherapy for childhood acute lymphoblastic leukemia.

Author

Evans WE, Relling MV, Rodman JH, Crom WR, Boyett JM, and Pui CH

Subjects

Adolescent, Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Child, Child, Preschool, Cytarabine administration & dosage, Cytarabine pharmacokinetics, Female, Humans, Infant, Leukemia, B-Cell drug therapy, Male, Metabolic Clearance Rate, Methotrexate administration & dosage, Methotrexate pharmacokinetics, Patient Care Planning, Precursor Cell Lymphoblastic Leukemia-Lymphoma mortality, Proportional Hazards Models, Prospective Studies, Remission Induction, Survival Analysis, Teniposide administration & dosage, Teniposide pharmacokinetics, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy

Abstract

Background: The rate of clearance of antileukemic agents differs by a factor of 3 to 10 among children with acute lymphoblastic leukemia. We hypothesized that the outcome of treatment would be improved if doses were individualized to prevent low systemic exposure to the drugs in patients with fast drug clearance., Methods: We stratified and randomly assigned 182 children with newly diagnosed acute lymphoblastic leukemia to postremission regimens that included high-dose methotrexate and teniposide plus cytarabine. The doses of these drugs were based on body-surface area (in the conventional-therapy group) or the rates of clearance of the three medications in each patient (in the individualized-treatment group). In the individualized-treatment group, doses were increased in patients with rapid clearance and decreased in patients with very slow clearance., Results: Patients who received individualized doses had significantly fewer courses of treatment with systemic exposures below the target range than did patients who received conventional doses (P<0.001 for each medication). Among the patients with B-lineage leukemia, those who received individualized therapy had a significantly better outcome than those given conventional therapy (P=0.02); the mean (+/-SE) rates of continuous complete remission at five years were 76+/-6 percent and 66+/-7 percent, respectively. There was no significant difference between treatments for patients with T-lineage leukemia (P=0.54). In a proportional-hazards model, the time-dependent systemic exposure to methotrexate, but not to teniposide or cytarabine, was significantly related to the risk of early relapse in children with B-lineage leukemia., Conclusions: Adjusting the dose of methotrexate to account for the patient's ability to clear the drug can improve the outcome in children with B-lineage acute lymphoblastic leukemia.

Published

1998

17. Clinical effects and pharmacokinetics of the fusion protein PIXY321 in children receiving myelosuppressive chemotherapy.

Author

Furman WL, Rodman JH, Tonda ME, Luo X, Arnold B, Marina N, Garrison L, Hanna R, Pratt CB, and Meyer WH

Subjects

Adolescent, Adult, Child, Child, Preschool, Cisplatin administration & dosage, Drug Administration Schedule, Etoposide administration & dosage, Female, Granulocyte-Macrophage Colony-Stimulating Factor adverse effects, Half-Life, Humans, Ifosfamide administration & dosage, Infant, Interleukin-3 adverse effects, Male, Metabolic Clearance Rate, Neoplasms metabolism, Neutropenia chemically induced, Recombinant Fusion Proteins administration & dosage, Recombinant Fusion Proteins adverse effects, Recombinant Fusion Proteins pharmacokinetics, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Granulocyte-Macrophage Colony-Stimulating Factor administration & dosage, Granulocyte-Macrophage Colony-Stimulating Factor pharmacokinetics, Interleukin-3 administration & dosage, Interleukin-3 pharmacokinetics, Neoplasms drug therapy

Abstract

Unlabelled: A hemopoietin with the ability to accelerate both platelet and granulocyte recovery after intensive chemotherapy would have great clinical utility. The recombinant fusion protein composed of human granulocyte-macrophage colony-stimulating factor and interleukin-3 (PIXY321), showed some promise in early adult trials. However, studies for pediatric patients are limited, and there are no systematic data on the pharmacokinetics of PIXY321 given over prolonged periods at current dosage levels., Purpose: To determine the safety, clinical effects and plasma concentrations of increasing doses of PIXY321 in children treated with myelosuppressive chemotherapy., Methods: A total of 39 children with relapsed or high-risk solid tumors were enrolled in this phase I/II study. PIXY321 was administered once or twice daily by subcutaneous injection in total doses of 500 to 1000 microg/m2 per day for 14 days after each course of chemotherapy with ifosfamide, carboplatin, and etoposide (ICE). Pharmacokinetic studies were performed on day 1 of the first course in 33 patients and repeated on day 14 in 13 patients (once-daily schedule only)., Results: Although mild local skin reactions and fever were frequent, no dose-limiting toxicity was identified at the maximum dose studied (1000 microg/m2 per day). There were no statistically significant differences in chemotherapy-induced hematologic toxicity with increasing doses of PIXY321 or with twice-daily vs once-daily dosing. On day 1, the median PIXY321 clearance was 657 ml/min per m2 (range 77 1804 ml/min per m2) and the median half-life was 3.7 h (range 2.1-20.8 h). On day 14, clearance increased in all patients studied (median increase 63%), with a corresponding decrease in the median 12-h concentration (from 1.2 to 0.25 ng/ml). Maximum concentrations were < 1 ng/ml in 81% of patients, and only two patients had maximum plasma concentrations equivalent to those required for consistent activity in vitro., Conclusions: The recombinant fusion protein PIXY321 proved safe in children treated with myelosuppressive ICE chemotherapy but had no demonstrable clinical benefits. The pharmacokinetic studies suggest that the observed lack of hematologic benefit may be explained by low plasma concentrations resulting from increased clearance with prolonged administration. Moreover, the significant increase in PIXY321 systemic clearance in the absence of increased circulating myeloid cells suggests that the upregulation of either extravascular compartment hematopoietic progenitor cells or nonhematopoietic cells may play an important role in controlling circulating concentrations of this unique cytokine. These findings highlight the importance of a thorough assessment of the systemic disposition of cytokines when determining the dose and schedule necessary to achieve clinical activity in patients.

Published

1998

18. Pharmacokinetics of azithromycin after single- and multiple-doses in children.

Author

Stevens RC, Reed MD, Shenep JL, Baker DK, Foulds G, Luke DR, Blumer JL, and Rodman JH

Subjects

Adolescent, Aging metabolism, Anti-Bacterial Agents administration & dosage, Anti-Bacterial Agents adverse effects, Area Under Curve, Azithromycin administration & dosage, Azithromycin adverse effects, Child, Child, Preschool, Female, Half-Life, Humans, Infant, Male, Models, Biological, Neoplasms metabolism, Anti-Bacterial Agents pharmacokinetics, Azithromycin pharmacokinetics

Abstract

Study Objective: To characterize the disposition and tolerance of azithromycin after single and multiple oral doses of 12 mg/kg in children with and without cancer., Design: Open-label, nonrandomized pharmacokinetic study., Setting: Two pediatric hospitals., Patients: Twelve children with cancer admitted to the inpatient unit for empiric antibiotic treatment of febrile neutropenia, and 16 hospitalized patients receiving antibiotic therapy, Interventions: Patients received azithromycin suspension either as a single dose or daily dose every morning for 5 consecutive days. Serial blood samples were collected up to 120 hours after a single dose or during and after multiple doses to characterize the pharmacokinetic parameters estimated for a two-compartment absorption model., Measurements and Main Results: All 28 patients were evaluable for safety. Azithromycin was well tolerated except in one patient with cancer who experienced abdominal cramps and withdrew from the study. Pharmacokinetic results were not determined in five patients because of insufficient concentration-time data. The mean +/- SD estimates of oral clearance, terminal half-life, maximum concentration in serum (Cmax), and time to achieve Cmax in the 23 evaluable patients were 4.83 +/- 3.59 L/hour/kg, 54.5 +/- 36.4 hours, 318.2 +/- 174.5 microg/L, and 2.4 +/- 1.1 hours, respectively. These estimates did not differ between single-dose (14 patients) and multiple-dose (9 patients) groups. Pharmacokinetic parameters were not different between the 11 children with cancer and the 12 without cancer., Conclusion: Azithromycin 12 mg/kg results in proportionately higher serum concentrations than previously published results for lower doses (5 mg/kg). Variability in concentration profiles among patients is substantial, and age or other yet unidentified clinical factors may explain some of the differences observed.

Published

1997

19. ACCP strategic planning conference: issues and trends in clinical pharmacy research. American College of Clinical Pharmacy.

Author

Rodman JH

Subjects

Societies, Pharmaceutical, United States, Health Planning, Pharmacy trends, Research trends

Published

1997

20. Fentanyl pharmacokinetics in patients undergoing renal transplantation.

Author

Koehntop DE and Rodman JH

Subjects

Adolescent, Adult, Biological Availability, Blood Urea Nitrogen, Female, Half-Life, Humans, Male, Metabolic Clearance Rate, Middle Aged, Renal Insufficiency blood, Renal Insufficiency therapy, Serum Albumin analysis, Triglycerides blood, Adjuvants, Anesthesia pharmacokinetics, Analgesics, Opioid pharmacokinetics, Fentanyl pharmacokinetics, Kidney Transplantation, Renal Insufficiency metabolism

Abstract

Study Objective: To describe the pharmacokinetics of fentanyl in patients undergoing renal transplantation., Design: Prospective., Setting: A large university teaching hospital., Patients: Eight patients (mean +/- SD age 35.5 +/- 11.5 yrs, weight 73.4 +/- 24.8 kg) with end-stage renal failure receiving kidneys from a living relative; three patients were never dialyzed, three were receiving peritoneal dialysis, and two were receiving hemodialysis., Interventions: Plasma was sampled before and at intervals up to 8 hours after intravenous injection of fentanyl 25 microg/kg before skin incision., Measurements and Main Results: Mean +/- SD (range) preoperative values were blood urea nitrogen (BUN) 66 +/- 30 (35-111) mg/dl; albumin 3.6 +/- 0.7 (2.6-4.5) g/dl; and triglycerides 414 +/- 352 (156-1270) mg/dl. Elimination half-life was 382 +/- 205 minutes; volume of distribution for the central compartment 0.74 +/- 0.48 L/kg; volume of distribution at steady state (Vd(ss)) 3.1 +/- 2.0 L/kg; total body clearance 7.5 +/- 5.1 ml x kg(-1) x min(-1). A significant inverse relationship between degree of azotemia and fentanyl clearance was found. The two patients with the highest preoperative BUNs had the lowest multiple of clearance and Vd(ss), and were also the only ones to require postoperative mechanical ventilation., Conclusion: Although all patients received a kidney that functioned well after revascularization, the large intersubject variability in fentanyl kinetics may, in part, reflect their heterogeneity in dialysis status and renal failure-induced abnormalities. Marked decreases in fentanyl clearance do occur in these patients, appear to be related to very high BUN concentrations, and can lead to prolonged postoperative ventilatory depression.

Published

1997

21. Effect of acute phase response on phenytoin metabolism in neurotrauma patients.

Author

McKindley DS, Boucher BA, Hess MM, Rodman JH, Feler C, and Fabian TC

Subjects

Adolescent, Adult, Albumins metabolism, Anticonvulsants therapeutic use, Biological Availability, Craniocerebral Trauma complications, Cytokines blood, Female, Humans, Male, Middle Aged, Orosomucoid, Phenytoin therapeutic use, Prospective Studies, Acute-Phase Reaction metabolism, Anticonvulsants pharmacokinetics, Craniocerebral Trauma metabolism, Epilepsy, Post-Traumatic prevention & control, Phenytoin pharmacokinetics

Abstract

The purpose of this prospective study was to correlate measures of the acute phase response, associated therapeutic interventions, and other clinical variables with the process of altered drug metabolism previously observed in patients with severe neurotrauma. Nine patients with severe head injury (Glasgow Coma Scale < or = 8) requiring intravenous phenytoin were included in the study. A loading dose of phenytoin was followed by daily maintenance doses. Serial blood samples were taken after the loading dose and every even-numbered study day for 10 to 14 days for measurement of total and unbound concentrations of phenytoin, interleukin-1 beta, interleukin-6 (IL-6), tumor necrosis factor alpha, alpha 1-acid-glycoprotein, C-reactive protein, and albumin. Time-invariant and time-variant Michaelis-Menten models were fit to the phenytoin concentration-time data. Protein intake was closely monitored. The mean (+/- SEM) unbound fraction of phenytoin increased from 0.17 +/- 0.02 on day 1 to 0.24 +/- 0.04 on day 10 (P < 0.05). The time-variant model was superior in describing the concentration-time data of unbound phenytoin in eight of nine patients. Mean (+/- SEM) pharmacokinetic parameter estimates for unbound phenytoin were: Vmax delta = 605 +/- 92 mg/day, VmaxB = 149 +/- 26.3 mg/day, K(ind) = 0.013 +/- 0.004 hr-1. Interleukin-6 was the only cytokine with significant concentration changes over time; it was inversely correlated with Vmax,t. Peak concentrations of interleukin-6 also proved to be inversely correlated with VmaxB. The daily amount of protein administered was significantly correlated with Vmax,t. Significant alterations in the metabolism of phenytoin occur after severe neurotrauma. The etiology of these changes is probably multifaceted. These results suggest that low initial phenytoin Vmax may be explained by the presence of interleukin-6. An increase in oxidative metabolism that correlated with nutritional protein administration was observed later in these patients.

Published

1997

22. A systemic and cellular model for zidovudine plasma concentrations and intracellular phosphorylation in patients.

Author

Rodman JH, Robbins B, Flynn PM, and Fridland A

Subjects

Adolescent, Adult, Female, Humans, Leukocytes, Mononuclear metabolism, Lymphocyte Count, Male, Models, Biological, Phosphorylation, HIV Infections drug therapy, Zidovudine blood, Zidovudine pharmacokinetics

Abstract

In a pharmacokinetic model for the systemic and cellular disposition of zidovudine in patients, serial measurements of plasma zidovudine and intracellular metabolites were used to simultaneously characterize systemic pharmacokinetics and intracellular phosphorylation in 6 human immunodeficiency virus-infected patients. First-order processes are sufficient to describe zidovudine monophosphate kinetics in peripheral blood mononuclear cells (PBMC), and the pharmacokinetic model provided reliable parameter estimates for each subject. The amount of zidovudine monophosphate in PBMC was inversely correlated with plasma zidovudine concentrations, and patients with higher systemic clearance had less intracellular zidovudine monophosphate. Zidovudine triphosphate values were measurable but not different at each time point. Lower lymphocyte counts were associated with higher intracellular zidovudine monophosphate but lower zidovudine triphosphate. The pharmacokinetic model proposed provides a quantitative link between systemic zidovudine concentrations and zidovudine monophosphate in PBMC from patients that will be useful in evaluating alternative therapeutic strategies.

Published

1996

23. Formation of platinum-DNA adducts in pediatric patients receiving carboplatin.

Author

Tonda ME, Murry DJ, and Rodman JH

Subjects

Adult, Antineoplastic Agents blood, Antineoplastic Agents therapeutic use, Carboplatin blood, Carboplatin therapeutic use, Child, Child, Preschool, Cisplatin metabolism, Female, Humans, Infant, Leukocytes chemistry, Male, Neoplasms drug therapy, Prospective Studies, Antineoplastic Agents metabolism, Carboplatin metabolism, DNA Adducts metabolism, Leukocytes metabolism, Platinum metabolism

Abstract

Study Objective: To determine the extent of platinum-DNA (Pt-DNA) adduct formation in peripheral white blood cells of children with cancer., Design: Prospective study., Setting: Pediatric research hospital., Patients: Twenty-seven children receiving carboplatin as part of therapy as defined by clinical research protocols., Interventions: Patients received various dosages of carboplatin over 1, 3, or 24 hours as a primary component of combination chemotherapy for pediatric solid tumors, brain tumors, or large cell lymphoma., Measurements and Main Results: The Pt-DNA adducts were detectable in 10 (37%) of 27 patients. The median value was 3.4 fmol Pt/micrograms DNA (range 1.7-31.2 fmol) in patients with measurable values., Conclusion: The Pt-DNA adducts were detected less frequently in pediatric patients than reported in adults. Variables that influenced their detection were higher carboplatin dosages or systemic exposure and short (1-3 hrs) versus prolonged (24 hrs) infusions.

Published

1996

24. Carboplatin pharmacokinetics in young children with brain tumors.

Author

Tonda ME, Heideman RL, Petros WP, Friedman HS, Murry DJ, and Rodman JH

Subjects

Adolescent, Antineoplastic Combined Chemotherapy Protocols adverse effects, Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Carboplatin administration & dosage, Child, Child, Preschool, Cyclophosphamide administration & dosage, Etoposide administration & dosage, Glomerular Filtration Rate drug effects, Hematologic Diseases chemically induced, Humans, Prospective Studies, Reproducibility of Results, Statistics, Nonparametric, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Brain Neoplasms drug therapy, Carboplatin pharmacokinetics

Abstract

Purpose: The pharmacokinetic parameters and maximal tolerated systemic exposure were determined for carboplatin in young children given in combination with cyclophosphamide and etoposide., Patients and Methods: Carboplatin was administered as part of a multiagent chemotherapy regimen to 21 pediatric patients less than 5 years of age with newly diagnosed, malignant central nervous system tumors. Patients, received cyclophosphamide, 1.2 g/m2, on day 1 and carboplatin on day 2 followed by etoposide, 100 mg/m2, each day. Carboplatin doses were calculated to achieve a targeted area under the serum concentration versus time curve (TAUC) of 5, 6.5 or 8 mg/ml.min based on each patient's measured glomerular filtration rate (GFR). Carboplatin pharmacokinetic parameters were determined after course 1 and then after every third course of therapy., Results: The median carboplatin clearance and GFR after course 1 were 118 and 98 ml/min per m2, respectively. Targeted doses based on measured GFR reliably achieved the TAUC for carboplatin. The median (range) carboplatin clearance for four children less than 1 year of age was 76 (66-84) ml/min per m2, significantly lower (P = 0.05) than the value of 131 (80-158) ml/min per m2 for children from 1 to 4 years of age. The mean carboplatin clearance declined by 23% in 12 patients studied from course 1 to course 4 of therapy. The decrease was greater than 20% (range 20-53%) in 7 of the 12 patients studied., Conclusion: Carboplatin clearance for children aged between 1 and 4 years at diagnosis is approximately 45% higher than previously reported for pediatric patients, but declines after four courses of therapy. For children less than 1 year of age, carboplatin clearance per square meter is approximately 40% lower than patients 1 to 4 years of age. There are corresponding differences in GFR that provide a plausible explanation for the age and therapy-related changes in carboplatin clearance. Toxicity was acceptable for patients treated at a TAUC of 6.5 mg/ml.min for carboplatin given with etoposide and cyclophosphamide. The average carboplatin dose required for this AUC was 767 mg/m2.

Published

1996

25. Renal function and methotrexate clearance in children with newly diagnosed leukemia.

Author

Murry DJ, Synold TW, Pui CH, and Rodman JH

Subjects

Administration, Oral, Adolescent, Child, Child, Preschool, Creatinine blood, Female, Hospitals, Pediatric, Humans, Infant, Infusions, Intravenous, Male, Metabolic Clearance Rate, Methotrexate administration & dosage, Methotrexate therapeutic use, Precursor Cell Lymphoblastic Leukemia-Lymphoma metabolism, Precursor Cell Lymphoblastic Leukemia-Lymphoma physiopathology, Prospective Studies, Glomerular Filtration Rate, Methotrexate pharmacokinetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy

Abstract

Study Objectives: To determine whether glomerular filtration rate (GFR) changes during induction chemotherapy in children with leukemia, and to examine GFR as a determinant of pharmacokinetic variability of methotrexate clearance., Design: Prospective, unblinded observational study in consecutive patients., Setting: A research hospital., Patients: Thirty-eight children newly diagnosed with acute lymphoblastic leukemia., Interventions: The patients received either high-dose methotrexate 1 g/m2 intravenously over 24 hours or low-dose methotrexate 30 mg/m2 orally every 6 hours for six doses; both regimens were followed by an intensive six-drug chemotherapy regimen given over 6 weeks. Glomerular filtration rate was determined in each subject before and at the conclusion of induction therapy., Measurements and Main Results: The GFR was determined from 99mTc-DTPA serum clearance in all patients, and methotrexate clearance was estimated from serial serum concentrations in 18 of these children who received high-dose methotrexate. Median values for GFR at diagnosis (131 ml/min/1.73 m2) and after induction therapy (120 ml/min/1.73 m2) were not significantly different (p = 0.26) but were highly variable (range 49-274 ml/min/1.73 m2). Body size, age, and serum creatinine were correlated significantly with GFR at diagnosis. Amphotericin B therapy (6 patients) significantly decreased GFR (p = 0.046) without a corresponding increase in serum creatinine. Methotrexate clearance (58-155 ml/min/m2) was significantly (p = 0.007) correlated with GFR, but GFR accounted for only 37% of the variability of methotrexate clearance., Conclusions: The GFR was normal but highly variable in these children with leukemia and was significantly altered by amphotericin. Our results explain little of the intersubject variability in methotrexate clearance.

Published

1995

26. Pharmacokinetic variability in the adolescent: implications of body size and organ function for dosage regimen design.

Author

Rodman JH

Subjects

Adult, Age Factors, Body Constitution, Body Height, Body Surface Area, Body Weight, Child, Child, Preschool, Clinical Trials as Topic, Female, Humans, Kidney metabolism, Kidney physiology, Liver metabolism, Liver physiology, Male, Adolescent, Pharmaceutical Preparations administration & dosage, Pharmacokinetics

Abstract

Although there are convincing clinical studies demonstrating important pharmacokinetic differences between the adult and pediatric patient, guidelines for adjusting the dosages of specific drugs are often based on empirical and limited data. Adult doses often provide the reference point for therapy in children with adjustment for body size. Both body weight and body surface area (BSA) are commonly used to adjust adult doses for pediatric patients but yield substantially different absolute doses. For the child age five years, the BSA-based dose will be more than 50 percent greater than the dose adjusted for body weight. The choice of weight or BSA is often arbitrary and may be an important confounding variable when evaluating drugs over wide ranges of age in pediatric patients or comparing two drugs for which doses are not adjusted in a similar manner. For example, comparative trials for HIV-infected pediatric patients are evaluating zidovudine dosed by BSA with zalcitabine dosed by body weight. Organ function changes with age in pediatric patients yet little information is available on the effects of maturation on hepatic or renal function and the consequences for drug disposition. The use of model substrates for organ function offers potential for elucidating organ function relative to maturation and, in particular, to those functional capacities associated with the onset of puberty and gender differentiation.

Published

1994

27. Altered etoposide pharmacokinetics and time to engraftment in pediatric patients undergoing autologous bone marrow transplantation.

Author

Rodman JH, Murry DJ, Madden T, and Santana VM

Subjects

Adolescent, Adult, Anticonvulsants therapeutic use, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Carboplatin adverse effects, Carboplatin pharmacokinetics, Carboplatin therapeutic use, Child, Child, Preschool, Drug Interactions, Etoposide adverse effects, Etoposide therapeutic use, Half-Life, Humans, Infant, Metabolic Clearance Rate, Neoplasms drug therapy, Transplantation, Autologous, Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Bone Marrow Transplantation, Etoposide pharmacokinetics, Neoplasms therapy

Abstract

Purpose: To determine the pharmacokinetics and clinical response of high-dose etoposide in combination with carboplatin for pediatric cancer patients undergoing autologous bone marrow transplant., Patients and Methods: Pharmacokinetic parameters for etoposide were determined at doses of 960, 1,200, and 1,500 mg/m2 when given with high-dose carboplatin and followed by autologous marrow rescue. Twenty-nine patients (age 1.6 to 23 years) with refractory or relapsed solid tumors were studied. Etoposide was administered in three divided doses as a 6-hour infusion on alternate days with carboplatin. Etoposide concentrations (n = 14) were determined during and following each of three doses. Patient characteristics, drug dose, and pharmacokinetic parameters were examined as predictors of marrow engraftment as reflected by recovery of granulocytes and platelets., Results: The median values for clearance (Cl) and terminal half-life (T1/2 beta) of etoposide were 14.3 mL/min/m2 (range, 6.8 to 29.6) and 5.9 hours (range, 3.7 to 39). After adjustment for body size, Cl and volume of distribution did not correlate with any laboratory parameter or patient characteristic. However, seven patients who received concomitant anticonvulsant therapy had significantly higher (P < .01) average etoposide Cl values (23.7 mL/min/m2) than 22 patients who did not receive drugs known to alter hepatic metabolism (13.4 mL/min/m2). The median etoposide Cl value in patients who received concurrent carboplatin but no anticonvulsant agents is substantially lower than values previously reported in either children or adults. Higher etoposide concentrations were significantly associated with longer times to recovery of granulocyte and platelet counts., Conclusion: Etoposide Cl is significantly higher in patients who receive concomitant anticonvulsant therapy, which is consistent with clinically important hepatic enzyme induction. The lower etoposide Cl associated with high-dose carboplatin suggests that carboplatin may impair etoposide metabolism. Furthermore, high etoposide concentrations appeared to prolong time to recovery of hematopoietic function.

Published

1994

28. Patient characteristics associated with high-risk methotrexate concentrations and toxicity.

Author

Relling MV, Fairclough D, Ayers D, Crom WR, Rodman JH, Pui CH, and Evans WE

Subjects

Child, Child, Preschool, Female, Fluid Therapy, Humans, Hydrogen-Ion Concentration, Infusions, Intravenous, Leucovorin administration & dosage, Male, Methotrexate administration & dosage, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Risk Factors, Urine, Vomiting blood, Methotrexate adverse effects, Methotrexate blood, Precursor Cell Lymphoblastic Leukemia-Lymphoma blood

Abstract

Purpose: Following high-dose methotrexate (HD-MTX) treatment, delayed MTX elimination is an important problem because it necessitates increased leucovorin rescue and additional hospitalization for hydration and urinary alkalinization. Our purpose was to identify factors associated with high-risk MTX plasma concentrations (defined by plasma concentration > or = 1.0 mumol/L at 42 hours from the start of MTX) and with toxicity., Patients and Methods: Variables associated with MTX concentrations and toxicity were assessed in 134 children treated with one to five courses of HD-MTX (900 to 3,700 mg/m2 intravenously [i.v.] over 24 hours for a total of 481 courses) for acute lymphoblastic leukemia (ALL)., Results: High-risk MTX concentrations, toxicity (usually mild mucositis), and delay in resuming continuation chemotherapy occurred in 106 (22%), 123 (26%), and 66 (14%) of 481 courses, respectively. Using a mixed effects model for repeated measures, high-risk MTX concentrations were significantly associated with a higher MTX area-under-the-concentration-time curve (AUC), low urine pH, emesis, low MTX clearance, low urine output relative to intake, use of antiemetics during the MTX infusion, and concurrent intrathecal therapy (all p values < .01). Clinical toxicities and delay in resumption of continuation chemotherapy due to myelosuppression were more common in those with high 42-hour MTX concentrations, despite increased leucovorin rescue for all patients with high-risk MTX concentrations. However, with individualized rescue, no patient developed life-threatening toxicity. A more aggressive hydration and alkalinization regimen for subsequent courses reduced the frequency of high-risk MTX concentrations to 7% of courses (13 of 183) (P = .0001), and the frequency of toxicity decreased to 11% of courses (P = .0074)., Conclusion: This study identified several clinical variables that influence MTX disposition that, when modified, can reduce the frequency of high-risk MTX concentrations and toxicity.

Published

1994

29. Phase I study of escalating targeted doses of carboplatin combined with ifosfamide and etoposide in treatment of newly diagnosed pediatric solid tumors.

Author

Marina NM, Rodman JH, Murry DJ, Shema SJ, Bowman LC, Jones DP, Furman W, Meyer WH, and Pratt CB

Subjects

Antineoplastic Combined Chemotherapy Protocols adverse effects, Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Bone Marrow Diseases chemically induced, Carboplatin administration & dosage, Child, Child, Preschool, Etoposide administration & dosage, Female, Humans, Ifosfamide administration & dosage, Infant, Male, Neoplasms metabolism, Treatment Outcome, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Neoplasms drug therapy

Abstract

Background: The combination of carboplatin, ifosfamide, and etoposide has shown promising activity in a variety of relapsed childhood solid tumors but has not been studied in newly diagnosed patients., Purpose: The tolerance for and activity of escalating targeted doses of carboplatin combined with ifosfamide and etoposide (ICE) were assessed in children with advanced germ cell tumors or other rare solid tumors for which no standard therapy exists., Methods: Fifteen children with newly diagnosed solid tumors received ICE chemotherapy. Individualized carboplatin doses were calculated to achieve a target area under the concentration x time curve (AUC) and adjusted for the glomerular filtration rate (estimated by 99mTc-labeled diethylene-triamine pentaacetic acid clearance). Cohorts of at least three patients received carboplatin at an initial target AUC of 6 mg.min/mL, with escalations of 2 mg.min/mL in subsequent cohorts. Carboplatin was given on day 1, followed by ifosfamide at 2 g/m2 per day and etoposide at 100 mg/m2 per day on days 2 through 4. All patients received at least two courses of therapy in the absence of progressive disease, and as many as eight courses could be given., Results: The 15 patients received a total of 46 assessable courses of ICE. Myelosuppression was the dominant toxicity; 30 courses (67%) resulted in hospitalization for febrile neutropenia. Neutropenia was dose limiting at the carboplatin target AUC of 12 mg.min/mL. One complete and eight partial responses were seen in the 14 assessable patients; two additional patients had at least partial responses documented at surgery or autopsy. Six patients are without evidence of disease at a median of 548 days after diagnosis., Conclusion: ICE chemotherapy, with the carboplatin dose based on a target AUC of 10 mg.min/mL, is tolerable and has significant activity in a variety of rare malignancies, including extragonadal germ cell tumors., Implications: The combination of carboplatin, etoposide, and ifosfamide holds promise in the treatment of rare pediatric malignancies.

Published

1994

30. Superiority of aztreonam/clindamycin compared with gentamicin/clindamycin in patients with penetrating abdominal trauma.

Author

Fabian TC, Hess MM, Croce MA, Wilson RS, Wilson SE, Charland SL, Rodman JH, and Boucher BA

Subjects

Adult, Aztreonam pharmacokinetics, Aztreonam therapeutic use, Bacterial Infections drug therapy, Bacterial Infections etiology, Blood Transfusion, Clindamycin therapeutic use, Colon injuries, Double-Blind Method, Female, Gentamicins therapeutic use, Humans, Male, Prospective Studies, Risk Factors, Wounds, Gunshot complications, Abdominal Injuries complications, Bacterial Infections prevention & control, Drug Therapy, Combination therapeutic use, Wounds, Penetrating complications

Abstract

There were 73 evaluable patients entered into a prospective, double-blinded trial comparing aztreonam/clindamycin (A/C) to gentamicin/clindamycin (G/C) for the prevention of infection after penetrating abdominal trauma. Aztreonam was administered at a dosage of 2 g every 8 hours and gentamicin at 5 mg/kg for the first 24 hours and then adjusted by serum monitoring to a peak of 6 to 8 micrograms/mL and a trough of less than 2 micrograms/mL; all patients received 900 mg of clindamycin every 8 hours. Patients with colon wounds received 4 days of antibiotics, and the remaining patients received a 24-hour course. Gunshot wounds occurred in 69% of patients: 74% of all patients had some hollow viscus injury, and 26% had only solid viscus injury. The groups were well matched according to abdominal trauma index, percentage with colon injury, and transfusion requirements. Failures occurred in eight patients (11%): two wound infections, five intra-abdominal infections, and one case of necrotizing fasciitis. Seven infections occurred in 36 (19%) G/C patients compared with 1 in 37 (3%) A/C patients (p < 0.03). The hospital stay was 12 +/- 11 days for G/C patients and 8 +/- 7 for A/C patients (p < 0.12). The superiority of the A/C regimen may be partially attributable to relative underdosing of gentamicin (approximately half of the patients had inadequate levels after 24 hours) combined with a favorable pharmacokinetic profile (significantly prolonged half-life) of aztreonam in this clinical setting.

Published

1994

31. Opportunities for integration of pharmacokinetics, pharmacodynamics, and toxicokinetics in rational drug development.

Author

Peck CC, Barr WH, Benet LZ, Collins J, Desjardins RE, Furst DE, Harter JG, Levy G, Ludden T, and Rodman JH

Subjects

Animals, Clinical Trials, Phase I as Topic, Clinical Trials, Phase II as Topic, Clinical Trials, Phase III as Topic, Drug Evaluation, Preclinical, Drug Labeling, Humans, Drug Approval, Drugs, Investigational pharmacokinetics, Drugs, Investigational pharmacology, Drugs, Investigational toxicity

Published

1994

32. Stereoselective distribution of hydroxychloroquine in the rabbit following single and multiple oral doses of the racemate and the separate enantiomers.

Author

Ducharme J, Wainer IW, Parenteau HI, and Rodman JH

Subjects

Administration, Oral, Animals, Hydroxychloroquine administration & dosage, Male, Rabbits, Stereoisomerism, Hydroxychloroquine pharmacokinetics

Abstract

Hydroxychloroquine (HCQ) stereoselective distribution was investigated in rabbits after 20 mg/kg po of racemic-HCQ (rac-HCQ) and 20 mg/kg po of each enantiomer, 97% pure (-)-(R)-HCQ and 99% pure (+)-(S)-HCQ. Concentrations were 4 to 6 times higher in whole blood than in plasma. Melanin did not affect plasma and whole blood levels since concentrations did not differ between pigmented and nonpigmented animals. After single and multiple doses of the separate enantiomers, only 5-10% of the antipode could be measured, in blood or plasma. Therefore, there was no significant interconversion from one enantiomer into the other. Following rac-HCQ, plasma (+)-(S)-levels always surpassed (-)-(R)-ones while in whole blood, (-)-(R)-HCQ concentrations were always the highest. When the enantiomers were administered separately, blood concentrations achieved after (-)-(R)-HCQ were higher, especially after multiple doses. These observations suggest that (-)-(R)-HCQ is preferentially concentrated by cellular components of blood. This enantioselective distribution of HCQ could be secondary to a stereoselective protein binding to plasma proteins, although a more specific binding of (-)-(R)-HCQ to blood cells cannot be ruled out. Since in whole blood (-)-(R)-HCQ is retained in cellular components, metabolism would favour the more available (+)-(S)-enantiomer.

Published

1994

33. Successful treatment of acute lymphoblastic leukemia in a child with cystic fibrosis.

Author

Gururangan S, Horner M, Rodman JH, and Marina NM

Subjects

Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Asparaginase administration & dosage, Child, Preschool, Cytarabine administration & dosage, Daunorubicin administration & dosage, Female, Humans, Mercaptopurine administration & dosage, Methotrexate administration & dosage, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma etiology, Precursor Cell Lymphoblastic Leukemia-Lymphoma etiology, Prednisone administration & dosage, Remission Induction, Teniposide administration & dosage, Vincristine administration & dosage, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Cystic Fibrosis complications, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy

Abstract

A 3 1/2 year old girl with cystic fibrosis who underwent successful treatment for acute lymphoblastic leukemia remains in complete remission 36 months after diagnosis. We also report high clearance rates of three antineoplastic agents in this patient. Drug doses were adjusted to achieve optimal systemic exposure.

Published

1994

34. Pharmacokinetics and acute renal effects of continuously infused carboplatin.

Author

Murry DJ, Sandlund JT, Stricklin LM, and Rodman JH

Subjects

Adolescent, Burkitt Lymphoma drug therapy, Carboplatin administration & dosage, Child, Child, Preschool, Humans, Infusions, Intravenous, Least-Squares Analysis, Lymphoma, Large B-Cell, Diffuse drug therapy, Carboplatin pharmacokinetics, Carboplatin pharmacology, Glomerular Filtration Rate drug effects

Abstract

Carboplatin was given as a 24-hour infusion at high doses to pediatric patients with cancer (n = 11) and pharmacokinetic parameters and renal effects were determined. Median carboplatin clearance for course 1 (151 ml/min per 1.73 m2;) was not significantly different from clearance for course 2 (144 ml/min per 1.73 m2; p = 0.33). The median glomerular filtration rate measured before (159 ml/min per 1.73 m2) and after course 1 (161 ml/min per 1.73 m2) did not differ significantly (p = 0.4). Binding was time dependent but modest with a median free fraction at the end of infusion of 0.82. Pharmacokinetic parameters for continuous-infusion carboplatin are similar to those reported for short infusions, but the median dose of 817 mg/m2 required to achieve an acceptable systemic exposure in these patients was 45% greater than the previously suggested maximum tolerated dosage. Continuous infusion carboplatin did not alter carboplatin clearance or adversely effect glomerular filtration rate during a second course, showing the feasibility of this alternative dosage strategy to enhance therapeutic effects.

Published

1993

35. A randomized study of outpatient treatment with ceftriaxone for selected febrile children with sickle cell disease.

Author

Wilimas JA, Flynn PM, Harris S, Day SW, Smith R, Chesney PJ, Rodman JH, Eguiguren JM, Fairclough DL, and Wang WC

Subjects

Ambulatory Care, Bacteremia prevention & control, Child, Child, Preschool, Female, Hemoglobin SC Disease drug therapy, Hospitalization, Humans, Infant, Male, Pilot Projects, Prospective Studies, Random Allocation, beta-Thalassemia drug therapy, Anemia, Sickle Cell drug therapy, Ceftriaxone therapeutic use

Abstract

Background: Because of their susceptibility to pneumococcal sepsis, children with sickle cell disease and fever are usually hospitalized for antibiotic therapy. Outpatient treatment may be a safe and less expensive alternative for selected patients., Methods: After evaluation in the emergency room, children ranging from 6 months to 12 years of age who had sickle hemoglobinopathies and temperatures exceeding 38.5 degrees C were randomly assigned to treatment as either inpatients or outpatients. We excluded from randomization children at higher risk of sepsis (as defined by specific criteria, including temperature above 40 degrees C, white-cell count below 5000 per cubic millimeter or above 30,000 per cubic millimeter, and the presence of pulmonary infiltrates) or with complications of sickle cell disease (such as a hemoglobin level below 5 g per deciliter, dehydration, or severe pain); these children were treated as inpatients. All patients received an initial intravenous dose of ceftriaxone (50 mg per kilogram of body weight). Those treated as outpatients returned 24 hours later for a second dose of ceftriaxone, whereas the in patients were treated as directed by their physicians., Results: None of the 86 patients (with a total of 98 febrile episodes) in the randomized groups had sepsis, as compared with 6 of the 70 patients (7 of 86 episodes) excluded because of higher risk (P = 0.004). Among the 44 children (50 episodes) assigned to outpatient treatment, there were 11 hospitalizations (22 percent of episodes) within two weeks after treatment (95 percent confidence interval, 12 to 36 percent), whereas after inpatient care only a single patient (2 percent of episodes) was rehospitalized. When the randomized groups were compared, outpatient treatment saved a mean of $1,195 per febrile episode. The median hospital stay was 3 days (range, 1 to 6) for the children randomly assigned to inpatient care and 4 days (range, 1 to 18) for the higher-risk children treated as inpatients (P < 0.001)., Conclusions: With the use of conservative eligibility criteria, at least half the febrile episodes in children with sickle cell disease can be treated safely on an outpatient basis, with substantial reductions in cost.

Published

1993

36. Targeting the systemic exposure of teniposide in the population and the individual using a stochastic therapeutic objective.

Author

D'Argenio DZ and Rodman JH

Subjects

Drug Monitoring, Feedback, Humans, Models, Biological, Population, Teniposide administration & dosage, Teniposide pharmacokinetics, Treatment Outcome, Teniposide therapeutic use

Abstract

A stochastic control approach for dose regimen design is developed and applied to the problem of targeting the systemic exposure, defined as the area under the blood concentration-time curve (AUC), of the anticancer drug teniposide in both the population and individual patients. The control objective involves maximizing the probability that AUC is within a selected target interval given either the population distribution for the kinetic model parameters (a priori control) or the posterior distribution for an individual patient (feedback control). Results of a detailed simulation study are presented, illustrating the feasibility of applying stochastic control principles to the design of dose regimens. The predictive ability of the calculated distributions of AUC for the population and for individuals is evaluated in part by determining the percentage coverage of the computed 95% uncertainty intervals using the simulation results. For the a priori control phase, 94% of the simulated subjects had values of systemic exposure within the computed 95% uncertainty interval, while 93.4% of the simulated subjects had feedback control phase systemic exposure values within their computed 95% uncertainty intervals. Similar evaluation of the uncertainty intervals calculated for plasma concentrations further document the ability of the proposed stochastic control method to predict the uncertainty associated with future therapy.

Published

1993

37. Clinical pharmacokinetics and pharmacodynamics of anticancer drugs in children.

Author

Rodman JH, Relling MV, Stewart CF, Synold TW, McLeod H, Kearns C, Stute N, Crom WR, and Evans WE

Subjects

Adult, Bone Marrow Transplantation, Child, Child, Preschool, Humans, Leukemia drug therapy, Neoplasms drug therapy, Recombinant Proteins, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents pharmacology

Abstract

Pharmacokinetic variability in children with cancer is substantial and confounds drawing conclusions regarding optimal therapy based only on dose-response relationships. Careful pharmacokinetic studies performed during drug development in conjunction with an assessment of patient characteristics, such as age, renal and hepatic function, and concomitant therapy, is essential for defining those factors that may alter drug disposition. By integrating pharmacokinetic studies with measures of efficacy and toxicity, a pharmacodynamic framework can be established for guiding therapy to minimize differences in systemic exposure among subpopulations of patients (eg, impaired renal function and neonates). In selected instances when pharmacokinetic variability cannot be predicted by patient covariates, the potential for individualizing dosages based on patient-specific pharmacokinetic parameters is now a clinically feasible option. The need for and benefits of incorporating such strategies into routine therapy represents an exciting area for further clinical research.

Published

1993

38. Escalating teniposide systemic exposure to increase dose intensity for pediatric cancer patients.

Author

Rodman JH, Furman WL, Sunderland M, Rivera G, and Evans WE

Subjects

Adolescent, Adult, Bayes Theorem, Child, Child, Preschool, Drug Administration Schedule, Humans, Infant, Precursor Cell Lymphoblastic Leukemia-Lymphoma metabolism, Regression Analysis, Teniposide pharmacokinetics, Treatment Outcome, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Teniposide administration & dosage

Abstract

Purpose: The primary objective for this study was to determine whether controlling pharmacokinetic variability, by designing patient-specific dosage regimens for teniposide using a Bayesian estimation control strategy, would permit an increase in dose intensity without increased toxicity., Patients and Methods: Twenty patients with relapsed acute lymphocytic leukemia were given teniposide as part of their induction and maintenance therapy. Before beginning reinduction therapy, an intensive pharmacokinetic study was performed based on 12 measured teniposide plasma concentrations. Doses were determined to achieve a targeted systemic exposure defined by an area under the plasma concentration time curve (AUC) beginning at an AUC consistent with that predicted for a patient with average pharmacokinetic parameters receiving the currently accepted maximal-tolerated dose. The targeted systemic exposure was then escalated in increments of 25% in cohorts of at least three patients until unacceptable toxicity occurred. In 36 follow-up studies, when teniposide was administered during maintenance therapy, a Bayesian strategy based on only three or five measured drug concentrations was evaluated for precision and bias for achieving the targeted systemic exposure against the full pharmacokinetic study., Results: Teniposide clearance varied over a fivefold range (3.7 to 21.6 mL/min/m2). With the use of the patient-specific dosage regimens, the intensity of systemic exposure was increased 50% (1,656 mumol.h v 1,060 mumol/L.h) over that previously possible with standard fixed doses, with no increase in acute, nonhematologic toxicity. Teniposide concentrations (n = 265) were well predicted (R2 = .82) with as few as three measured values from the initial study., Conclusion: Targeting systemic exposure is clinically feasible, precise, and allows increased dose intensity for teniposide without increased risk of acute, nonhematologic toxicity, when compared with fixed-dose regimens.

Published

1993

39. Measurement of Tc-99m DTPA serum clearance for estimating glomerular filtration rate in children with cancer.

Author

Rodman JH, Maneval DC, Magill HL, and Sunderland M

Subjects

Adolescent, Child, Child, Preschool, Female, Humans, Male, Glomerular Filtration Rate, Neoplasms physiopathology, Technetium Tc 99m Pentetate blood

Abstract

Clearance of the radiopharmaceutical Tc-99m DTPA estimated from blood samples with no urine collection can provide a reliable estimate of glomerular filtration rate (GFR) in adults, but has not been well studied in children. The disposition of Tc-99m DTPA was determined in 17 children with cancer, and the influence of binding and study design on the estimates for serum clearance were evaluated. Nine blood samples were obtained over 6 hours in each patient, and serum was assayed for total and free Tc-99m. Free Tc-99m DTPA was determined by ultrafiltration. Estimates of clearance derived from a two-compartment model for ultrafiltrable Tc-99m DTPA were determined from all nine measured concentrations, and these results served as a reference value for GFR in each subject. Total Tc-99m DTPA concentrations also were best described by a two-compartment model, but the median total clearance (35 ml/min) was significantly (p < 0.01) lower than the ultrafiltrate clearance (58 ml/min). The effect of a simplified sampling schedule was assessed from clearance estimates based on a 3-point subset of the ultrafiltrable data. The median clearance of 69 ml/minute was significantly higher (p < 0.01) than the reference GFR. However with a correction factor included to account for the positive bias arising from the limited sampling schedule, the reference estimates for GFR were well predicted (r2 = 0.99) with no significant bias. Ultrafiltrable Tc-99m DTPA serum clearance using a limited sampling schedule can provide a consistent and clinically feasible estimate of glomerular filtration rate in children, but binding in serum and study design are potentially important confounding factors.

Published

1993

40. Disposition of antineoplastic agents in the very young child.

Author

McLeod HL, Relling MV, Crom WR, Silverstein K, Groom S, Rodman JH, Rivera GK, Crist WM, and Evans WE

Subjects

Age Factors, Antineoplastic Agents therapeutic use, Antineoplastic Agents toxicity, Blood Proteins metabolism, Child, Child, Preschool, Doxorubicin pharmacokinetics, Etoposide pharmacokinetics, Humans, Infant, Infant, Newborn, Liver drug effects, Liver pathology, Mercaptopurine pharmacokinetics, Methotrexate pharmacokinetics, Neoplasms blood, Nervous System drug effects, Nervous System pathology, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Teniposide pharmacokinetics, Antineoplastic Agents pharmacokinetics, Neoplasms drug therapy

Abstract

Maturation of physiologic process which govern the disposition of pharmacologic agents can yield significant changes in absorption, distribution, metabolism, and elimination of drugs in neonates, infants and children. However, there are very little data concerning the disposition of anticancer drugs in young children. Pharmacokinetic data for six anticancer agents were compared in infants less than 1 year of age and children greater than 1 year of age treated at St Jude Children's Research Hospital. No pharmacokinetic data were available for infants less than 2 months of age. Median methotrexate clearance tended to be lower in four infants (0.26-0.99 years) vs 108 children (1-19 years): 80 vs 103 ml min-1 m-2, respectively (P = 0.01). There was no difference in the median 42 h methotrexate concentration. Teniposide systemic clearance and terminal half-life and cytarabine systemic clearance were not different between the two groups. There was no significant difference in etoposide systemic clearance when normalised to body surface area (ml min-1 m-2), however a significantly lower systemic clearance relative to body weight (ml min-1 kg-1) was observed in two infants, 0.5 to 1 year of age, vs 23 children, 3-18 years of age. Doxorubicin systemic clearance was not significantly different between the two groups when systemic clearance was expressed in ml min-1 kg-1. However, there was a trend toward a lower rate of systemic clearance in ml min-1 m-2 in infants.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1992

41. The pharmacokinetics of high-dose carboplatin in pediatric patients with cancer.

Author

Madden T, Sunderland M, Santana VM, and Rodman JH

Subjects

Adolescent, Adult, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Carboplatin administration & dosage, Child, Child, Preschool, Dose-Response Relationship, Drug, Drug Administration Schedule, Etoposide administration & dosage, Female, Humans, Male, Neoplasms drug therapy, Carboplatin pharmacokinetics, Neoplasms metabolism

Abstract

Carboplatin disposition was studied in 18 pediatric patients with cancer over a dosage range of 400 to 700 mg/m2 given on an alternate-day schedule (total doses of 1200 to 2100 mg/m2) with high-dose etoposide. Median age was 7.7 years, hepatic functions were normal, and serum creatinine levels were less than or equal to 1.0 mg/dl. Carboplatin pharmacokinetics were determined by atomic absorption spectroscopy. Median pharmacokinetic parameters for ultrafilterable platinum were as follows: clearance 45.8 ml/min/m2 (range, 25.5 to 65.3 ml/min/m2) and a terminal half-life of 3.6 hours (range, 2.1 to 14.2 hours). Carboplatin clearance (CL) values and volume of distribution (VC) were highly correlated to body size (CL = 55 x Body surface area in [BSA, in square meters] - 6.7, r2 = 0.73; VC = 5 x BSA [in square meters] + 0.26, r2 = 0.69). However, carboplatin doses normalized to BSA still resulted in twofold to threefold variability in area under the concentration-time curve. Carboplatin CL was significantly lower in those subjects (n = 9) who had previously received cumulative cisplatin doses of greater than or equal to 960 mg/m2 (p less than 0.05) but was not influenced by age, gender, or diagnosis.

Published

1992

42. Opportunities for integration of pharmacokinetics, pharmacodynamics, and toxicokinetics in rational drug development.

Author

Peck CC, Barr WH, Benet LZ, Collins J, Desjardins RE, Furst DE, Harter JG, Levy G, Ludden T, and Rodman JH

Subjects

Animals, Clinical Trials as Topic, Drug Evaluation, Drug Evaluation, Preclinical, Drugs, Investigational pharmacokinetics, Drugs, Investigational toxicity, Humans, Drugs, Investigational pharmacology

Published

1992

43. Increased teniposide clearance with concomitant anticonvulsant therapy.

Author

Baker DK, Relling MV, Pui CH, Christensen ML, Evans WE, and Rodman JH

Subjects

Adolescent, Child, Child, Preschool, Chromatography, High Pressure Liquid, Drug Interactions, Female, Humans, Male, Metabolic Clearance Rate drug effects, Phenobarbital pharmacology, Phenytoin pharmacology, Teniposide therapeutic use, Anticonvulsants pharmacology, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Teniposide pharmacokinetics

Abstract

Purpose: A possible pharmacokinetic interaction between teniposide and anticonvulsant medications was evaluated in pediatric patients., Patients and Methods: The systemic clearance of teniposide was determined in six pediatric patients with acute lymphocytic leukemia receiving concomitant therapy with anticonvulsants. Clearance was then compared with a control group of patients treated with the same protocol therapy and matched for age at diagnosis, sex, and race but not receiving anticonvulsants or other agents known to induce hepatic metabolism or alter protein binding of drugs. Eight blood samples were obtained during and after 4-hour infusions of teniposide, and plasma concentrations were measured by a specific high-performance liquid chromatography (HPLC) assay. A two-compartment model was fitted to each subject's data., Results: The mean systemic clearance (range) for the six anticonvulsant-treated patients studied during 22 courses of therapy was 32 mL/min/m2 (range, 21 to 54 mL/min/m2), significantly higher (P less than .001) than the mean value of 13 mL/min/m2 (range, 7 to 17 mL/min/m2) for the control patients studied during 26 courses of therapy. Clearance estimates for control patients were similar to previously published values for pediatric patients., Conclusion: These data indicate that the systemic clearance of teniposide is consistently increased two- to three-fold by concomitant phenobarbital or phenytoin therapy. The consequent substantial reduction in systemic exposure may reduce teniposide's efficacy.

Published

1992

44. Variability in teniposide plasma protein binding is correlated with serum albumin concentrations.

Author

Petros WP, Rodman JH, Relling MV, Christensen M, Pui CH, Rivera GK, and Evans WE

Subjects

Adolescent, Adult, Body Weight, Child, Child, Preschool, Female, Humans, Infant, Male, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Protein Binding, Remission Induction, Teniposide therapeutic use, Blood Proteins metabolism, Precursor Cell Lymphoblastic Leukemia-Lymphoma metabolism, Serum Albumin analysis, Teniposide metabolism

Abstract

Teniposide is a widely used anticancer drug that is extensively bound to plasma proteins (greater than 95%). We evaluated the drug's plasma protein binding in nine patients with acute lymphocytic leukemia who were in their first complete remission, and in a second group of nine patients at the time of relapse and subsequently after achieving another complete remission. Plasma protein binding was assessed by equilibrium dialysis, with direct high-performance liquid chromatographic measurement of total and free teniposide. The mean unbound fraction was 0.44% (0.21-0.88%) in the plasma of patients in first remission. It was significantly higher in patients at the time of relapse (mean = 0.86%; range 0.68-1.08%) and after achieving another complete remission (mean = 1.25%; range 0.51-2.11%). Serum albumin values were significantly lower at the time of relapse (mean = 4.6 vs 4.0 mg/dl; p less than 0.014), and decreased further during intensive postremission therapy containing L-asparaginase (mean = 3.2; p less than 0.05). For all 18 patients, a significant negative correlation (r2 = 0.667; p less than 0.001) was found between serum albumin and unbound teniposide, with low albumin being associated with higher unbound fraction. Such patients have higher systemic exposure to unbound (presumably active) teniposide at any given total plasma concentration of the agent.

Published

1992

45. Differences in teniposide disposition and pharmacodynamics in patients with newly diagnosed and relapsed acute lymphocytic leukemia.

Author

Evans WE, Rodman JH, Relling MV, Petros WP, Stewart CF, Pui CH, and Rivera GK

Subjects

Adolescent, Adult, Bilirubin blood, Blood Proteins metabolism, Child, Child, Preschool, Female, Humans, Infant, Male, Precursor Cell Lymphoblastic Leukemia-Lymphoma blood, Protein Binding, Remission Induction, Serum Albumin metabolism, Teniposide pharmacology, Precursor Cell Lymphoblastic Leukemia-Lymphoma metabolism, Teniposide pharmacokinetics

Abstract

Teniposide, a widely used investigational anticancer drug, is extensively bound to plasma proteins (greater than 95%). The present study evaluated the clearance and pharmacodynamics of total and unbound teniposide in patients with acute lymphocytic leukemia who were either in first complete remission or who had relapsed and achieved a subsequent complete remission. When compared to values of patients in first remission, the mean total systemic clearance of teniposide in relapsed patients was significantly lower at the time remission reinduction therapy was initiated, but increased to values greater than first remission patients after a subsequent remission was achieved. However, the mean clearance of unbound teniposide (ml/min/m2) was 3-fold lower in relapsed patients during reinduction therapy (1224 vs. 4261, P less than .0001), and improved but remained low after these patients achieved a subsequent remission (1965, P = .025). Changes in plasma protein binding accounted for the increase in total clearance when unbound clearance decreased. Continuous therapy with L-asparaginase was the major treatment difference in those patients with hypoalbuminemia and lower clearance of unbound teniposide. In 15 evaluable patients in complete remission, there was a statistically significant (P = .039) linear correlation between the percentage decrease in white blood cell count and the systemic exposure (AUC) to unbound teniposide, with higher exposure associated with a greater decrease in white blood cell count. There was not a significant correlation between the percent decrease in white blood cell count and the dosage given or the systemic exposure to total teniposide.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1992

46. Developing a specialty structure for the pharmacy profession.

Author

Rodman JH

Subjects

Pharmacology, Clinical trends, Pharmacy classification, Pharmacy trends, Professional Practice trends, Societies, Pharmaceutical, United States, Pharmacy organization & administration, Specialization

Published

1991

47. Hypersensitivity reactions to epipodophyllotoxins in children with acute lymphoblastic leukemia.

Author

Kellie SJ, Crist WM, Pui CH, Crone ME, Fairclough DL, Rodman JH, and Rivera GK

Subjects

Adolescent, Adrenal Cortex Hormones therapeutic use, Bronchial Spasm chemically induced, Child, Child, Preschool, Cyanosis chemically induced, Diphenhydramine therapeutic use, Dose-Response Relationship, Drug, Drug Hypersensitivity prevention & control, Etoposide administration & dosage, Female, Humans, Hypotension chemically induced, Infant, Male, Precursor Cell Lymphoblastic Leukemia-Lymphoma complications, Premedication, Teniposide administration & dosage, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Drug Hypersensitivity etiology, Etoposide adverse effects, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Teniposide adverse effects

Abstract

The incidence, clinical characteristics, and outcome of hypersensitivity reactions to teniposide (VM-26), etoposide (VP-16), or both were determined in 108 children with acute lymphoblastic leukemia (ALL) treated with a contemporary regimen of intensive multiagent chemotherapy. Fifty (46%) of the 108 patients had one or more hypersensitivity reactions. The risk of any child having an initial reaction over the cumulative dose range studied was 52% (95% confidence limits, 41% and 63%) for VM-26, compared with 34% (95% confidence limits, 24% and 44%) for VP-16. The risk of having an initial reaction to VM-26 or VP-16 was clearly related to the cumulative dose. This risk peaked at 1500 to 2000 mg/m2 for VM-26 and at 2000-3000 mg/m2 for VP-16. All reactions were Type 1 reactions according to the Gell and Coombs classification, characterized by urticaria, angioedema, flushing, rashes, or hypotension, and 86% of reactions were of Grade 1 or 2 severity according to standard criteria. There was no evidence of increasing clinical severity on repeated rechallenge with premedication, and no deaths occurred. The findings suggested that hypersensitivity reactions to epipodophyllotoxins in children with ALL are more common than previously reported, but only rarely constitute dose-limiting toxicity.

Published

1991

48. Somnolence, hypotension, and metabolic acidosis following high-dose teniposide treatment in children with leukemia.

Author

McLeod HL, Baker DK Jr, Pui CH, and Rodman JH

Subjects

Acidosis blood, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Child, Child, Preschool, Cytarabine administration & dosage, Diphenhydramine administration & dosage, Drug Administration Schedule, Female, Humans, Hypotension blood, Precursor Cell Lymphoblastic Leukemia-Lymphoma blood, Remission Induction, Sleep Wake Disorders blood, Teniposide administration & dosage, Teniposide blood, Acidosis chemically induced, Hypotension chemically induced, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Sleep Wake Disorders chemically induced, Teniposide adverse effects

Abstract

This report describes an unexpected adverse effect in three children receiving teniposide at 3-5 times the conventional dosage (i.e. 200 mg/m2) plus cytarabine as part of continuation therapy for acute lymphocytic leukemia. Pharmacokinetic studies in each patient had demonstrated high teniposide clearances, and thus the increased dosage requirements were necessary to attain plasma concentrations similar to those expected for patients with average drug clearance. At 3-4 h after the beginning of the 4-h simultaneous infusions of teniposide and cytarabine, these patients experienced somnolence, hypotension, and metabolic acidosis. The adverse events were associated with elevated teniposide plasma concentrations during the infusions compared with those in patients receiving similar doses without toxicity, and clinically significant ethanol concentrations, presumably from the teniposide formulation. Blood concentrations of cremophor and histamine, which are also constituents of the teniposide formulation, were not measured. In addition, concomitant therapy with antiemetic agents in patients who may have been mildly volume-depleted due to emesis may also play a contributory role. Prolonging the infusion time for patients receiving teniposide doses above 500 mg/m2 will avoid excessive teniposide and ethanol plasma concentrations and minimize the risk of this potentially serious side effect.

Published

1991

49. Pharmacokinetics of continuous-infusion amsacrine and teniposide for the treatment of relapsed childhood acute nonlymphocytic leukemia.

Author

Petros WP, Rodman JH, Mirro J Jr, and Evans WE

Subjects

Adolescent, Amsacrine administration & dosage, Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Child, Child, Preschool, Humans, Infant, Teniposide administration & dosage, Amsacrine pharmacokinetics, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Leukemia, Myeloid, Acute drug therapy, Teniposide pharmacokinetics

Abstract

The systemic disposition of both amsacrine and teniposide was determined in children receiving treatment for resistant acute nonlymphocytic leukemia. As part of a phase I-II study, amsacrine and teniposide were given as continuous 72-h i.v. infusions at doses of 75-150 and 150-250 mg m-2 day-1, respectively. Plasma samples obtained during steady state were analyzed for drug concentrations by high-performance liquid chromatography assays specific for each compound. Clearance and systemic exposure values for both amsacrine and teniposide were calculated for 14 patients, and data were available for teniposide alone in an additional 14 subjects. Interpatient variability in clearance was substantial for each drug, producing overlapping systemic exposure across dose levels. No evidence of dose-dependent drug clearance was evident. Clearance values for teniposide given in combination with amsacrine were similar to previous values obtained when teniposide was given in an identical manner but as a single agent. In all, 80% of patients experienced some degree of mucositis after chemotherapy administration. Severe mucositis (Pediatric Oncology Group grades 3-4) occurred in 18% of cases, all of whom showed teniposide steady-state plasma concentrations above the median population value (11.9 micrograms/ml; P less than 0.0001). A comparison of the results of the present study on teniposide combined with amsacrine with those previously obtained for single-agent teniposide suggest that amsacrine produced little additive gastrointestinal toxicity. The evaluation of anti-cancer drug pharmacokinetics in individual patients during combination chemotherapy regimens helps to determine the relative importance of each agent when toxicity patterns are similar.

Published

1991

50. Concept of maximum tolerated systemic exposure and its application to phase I-II studies of anticancer drugs.

Author

Evans WE, Rodman JH, Relling MV, Crom WR, Rivera GK, Pratt CB, and Crist WM

Subjects

Antineoplastic Agents pharmacokinetics, Antineoplastic Agents pharmacology, Dose-Response Relationship, Drug, Drug Evaluation, Humans, Antineoplastic Agents administration & dosage

Abstract

The traditional approach to conducting Phase I studies of anticancer drugs is to select a starting dosage for humans based on preclinical data (e.g., mg equivalent of 1/10 LD10 in mice), then empirically escalate dosages in cohorts of patients until the maximum tolerated dosage (MTD) is established. More recently, NCl and EORTC investigators have advocated the use of pharmacokinetic data from preclinical studies to facilitate more rapid dose escalation (e.g., double the dose until the area under the concentration-time curve [AUC] in humans equals the AUC in mice at the LD10). The present paper describes a strategy which builds on the above approach, by extending the application of pharmacokinetic principles to systematically escalate systemic exposure (AUC) instead of dosage in Phase I trials. Human trials are initiated at whatever patient-specific dosage is required to achieve an AUC equal to 1/10 the AUC in mice at the LD10, such that three patients at the first treatment level might receive three different dosages. If no dose-limiting toxicity is observed, the next cohort of patients receives whatever dosage is required to achieve 2 x AUC of the first dosage level, with AUC escalation continuing until the maximum tolerate systemic exposure (MTSE) is reached. By escalating systemic exposure instead of dosage, one adjusts for interpatient pharmacokinetic variability. This strategy will permit more rapid and precise dosage escalations and, more importantly, it should more precisely establish the maximum level of treatment intensity for future Phase II trials.

Published

1991