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102. Cardiac toxicity associated with intravenous erythromycin lactobionate

Author

Jeffrey L. Blumer, Henry C. Farrar, Kay Kyllonen, and Michele C. Walsh-sukys

Subjects
Male, Microbiology (medical), medicine.medical_specialty, Heart disease, medicine.medical_treatment, Infant, Premature, Diseases, Erythromycin Lactobionate, Gastroenterology, Ureaplasma, Internal medicine, Cardiac toxicity, Bradycardia, medicine, Humans, Infusions, Intravenous, Chemotherapy, biology, business.industry, Ureaplasma Infections, Infant, Newborn, medicine.disease, biology.organism_classification, Erythromycin, Heart Arrest, Surgery, Infectious Diseases, Recien nacido, Pediatrics, Perinatology and Child Health, Toxicity, Female, Hypotension, business, Ureaplasma urealyticum, Infant, Premature
Published
1993
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103. Pharmacokinetics and tolerability of single-dose intravenous ertapenem in infants, children, and adolescents

Author

Yang Xu, Anup K. Majumdar, Gary A. Herman, Susan M. Abdel-Rahman, Santiago Topelberg, Jeffrey L. Blumer, John A. Wagner, Michelle Groff, Chester J. Kitchen, Richard F. Jacobs, Gregory L. Kearns, and Goutam C. Mistry

Subjects
Microbiology (medical), Ertapenem, Male, Carbapenem, Pediatrics, medicine.medical_specialty, Adolescent, medicine.drug_class, Antibiotics, Pharmacology, beta-Lactams, Article, chemistry.chemical_compound, Broad spectrum, Plasma, Pharmacotherapy, Pharmacokinetics, polycyclic compounds, medicine, Humans, Child, Chromatography, High Pressure Liquid, Antibacterial agent, business.industry, Infant, Anti-Bacterial Agents, body regions, Infectious Diseases, chemistry, Tolerability, Child, Preschool, Pediatrics, Perinatology and Child Health, Female, business, medicine.drug
Abstract

Ertapenem is a carbapenem antibiotic with broad spectrum activity and a pharmacokinetic profile that favors once-daily administration in adults.This investigation was designed to evaluate the dose-exposure profile of ertapenem in children from infancy through adolescence.Eighty-four children (3 months-16 years) requiring antibiotic therapy were enrolled in this multicenter trial. Children received a single intravenous dose of ertapenem at 15, 20, or 40 mg/kg followed by repeated blood sampling for 24 hours. Free and total plasma ertapenem concentrations were quantitated by high-performance liquid chromatography, and the pharmacokinetics were determined using a model-independent approach.Ertapenem exposure increased proportionally with increasing dose; however, achievable concentrations were influenced by age. Children older than 12 years attained higher dose-normalized concentrations at the end of the infusion (concentration at the end of the infusion [Ceoi]: 8.7 ± 1.9 mg/L per mg/kg dose) and total body exposure (area under the curve area under the plasma concentration-time curve [AUC]0-∞: 34.7 ± 14.7 mg hr/L per mg/kg dose) as compared with children 2 to 12 years (Ceoi: 6.9 ± 2.4 mg/L per mg/kg dose, AUC0-∞: 18.4 ± 8.0 mg hr/L per mg/kg dose) and children younger than 2 years (Ceoi: 6.1 ± 2.2 mg/L per mg/kg dose, AUC0-∞: 17.0 ± 5.4 mg hr/L per mg/kg dose). These findings were accounted for by age-dependent changes in ertapenem clearance and distribution volume. In 3 children adverse events (nausea, n = 2; injection site reaction, n = 1) were considered related to study drug administration.Children younger than 12 years require dosing more frequently than once daily to achieve optimal efficacy when treating organisms with a minimum inhibitory concentration near the susceptibility breakpoint.

Published
2010

105. Determination of platelet monoamine oxidase activity by high-performance liquid chromatography with electrochemical detection

Author

Takayuki Ogata, Jeffrey L. Blumer, and Carolyn Myers

Subjects
Blood Platelets, Tris, Chromatography, Elution, Monoamine oxidase, Dopamine, Substrate (chemistry), General Chemistry, Hydrogen-Ion Concentration, Michaelis–Menten kinetics, High-performance liquid chromatography, chemistry.chemical_compound, Adsorption, chemistry, Electrochemistry, Humans, Perchloric acid, Monoamine Oxidase, Chromatography, High Pressure Liquid
Abstract

A procedure for determining human platelet monoamine oxidase (MAO) with dopamine (DA) as substrate is described. High-performance liquid chromatography (HPLC) with electrochemical detection (ED) was used to separate and detect components of the reaction mixture. The method for platelet preparation was also improved and only 2 ml of blood were required. Following a 10-min incubation of the platelet preparation with DA in 0.1 M Tris buffer (pH 9.0), excess DA substrate was removed by adsorption on a cation-exchange resin. The reaction product, 3,4-dihydroxyphenylacetaldehyde, was adsorbed on acid-washed alumina, eluted with 0.1 M perchloric acid and analyzed by HPLC. Simple, clean chromatograms were obtained with good reproducibility using 3,4-dihydroxybenzylamine as an internal standard. The within-sample, between-samples and between-day relative standard deviations were 0.9, 3.7 and 6.1%, respectively. The apparent Michaelis constant and maximum velocity were 0.10 mM and 0.37 nmol/min.mg protein, respectively. This HPLC-ED method offers a good alternative to methods using radioactivity.

Published
1992
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106. An Open-Label Study of Aripiprazole: Pharmacokinetics, Tolerability, and Effectiveness in Children and Adolescents with Conduct Disorder

Author

Vaishali P Sahasrabudhe, Georgia Kollia, Ralph E. Kauffman, Robert D. McQuade, Daniel E. Salazar, Nimish N. Vachharajani, David M. Kornhauser, David W. Boulton, Jeffrey L. Blumer, Taro Iwamoto, Sheila Assunção-Talbott, Robert L. Findling, Floyd R. Sallee, Suresh Mallikaarjun, and University of Groningen

Subjects
Conduct Disorder, Male, Pediatrics, medicine.medical_specialty, Bipolar I disorder, Adolescent, Vomiting, Sedation, Aripiprazole, Schizoaffective disorder, PLACEBO-CONTROLLED 26-WEEK, Quinolones, Piperazines, DOUBLE-BLIND, ANTIPSYCHOTIC ARIPIPRAZOLE, Tremor, INTRAMUSCULAR ARIPIPRAZOLE, medicine, Humans, Pharmacology (medical), Prospective Studies, Adverse effect, Psychiatry, Child, ADJUNCTIVE THERAPY, PARTIAL AGONIST, MAJOR DEPRESSIVE DISORDER, ACUTE AGITATION, Age Factors, medicine.disease, Psychiatry and Mental health, Tolerability, Conduct disorder, Pediatrics, Perinatology and Child Health, Major depressive disorder, Female, BIPOLAR-I-DISORDER, medicine.symptom, Psychology, SCHIZOAFFECTIVE DISORDER, medicine.drug, Antipsychotic Agents, Follow-Up Studies
Abstract

This study evaluated flexible-dose pharmacokinetics, safety, and effectiveness of aripiprazole in children and adolescents with conduct disorder (CD).This open-label, 15-day, three-center study with an optional 36-month extension enrolled a total of 23 patients: 12 children (6-12 years) and 11 adolescents (13-17 years) with CD and a score of 2-3 on the Rating of Aggression Against People and/or Property (RAAPP). Initially, the protocol used the following dosing: subjects25 kg, 2 mg/day; subjects 25-50 kg, 5 mg/day; subjects50-70 kg, 10 mg/day; and subjects70 kg, 15 mg/day. Due to vomiting and sedation, this schedule was revised to:25 kg, 1 mg/day; 25-50 kg, 2 mg/day;50-70 kg, 5 mg/day; and70 kg, 10 mg/day.Aripiprazole pharmacokinetics were linear, and steady state appeared to be attained within 14 days. Both groups demonstrated improvements in RAAPP scores and Clinical Global Impressions-Severity (CGI-S) scores. Adverse events were similar to the known profile for aripiprazole in adults.The pharmacokinetics of aripiprazole in children and adolescents are linear and comparable with those in adults. Aripiprazole was generally well-tolerated in patients with CD, particularly after protocol adjustments, with improvements in aggressive behavior.

Published
2009

107. Tinea capitis: predictive value of symptoms and time to cure with griseofulvin treatment

Author

Mary Ann O'Riordan, Lydia Furman, Jeffrey L. Blumer, Kelly C. Lorch Dauk, and Elana Comrov

Subjects
Male, medicine.medical_specialty, Antifungal Agents, Time Factors, Population, Hair Preparations, Administration, Oral, medicine.disease_cause, Administration, Cutaneous, Drug Administration Schedule, Griseofulvin, chemistry.chemical_compound, Trichophyton, Predictive Value of Tests, medicine, Humans, Prospective Studies, education, Prospective cohort study, Child, Selenium Compounds, Tinea Capitis, education.field_of_study, biology, Dose-Response Relationship, Drug, business.industry, Infant, biology.organism_classification, medicine.disease, Dermatology, Surgery, Clinical trial, Treatment Outcome, chemistry, Predictive value of tests, Child, Preschool, Pediatrics, Perinatology and Child Health, Dermatophyte, Tinea capitis, Female, business
Abstract

Objectives. To describe ( a) the predictive value of symptoms for diagnosis of tinea capitis and ( b) the rate and timing of cure with high-dose griseofulvin treatment. Methods. This prospective open-label study enrolled children aged 1 to 12 years with clinical tinea capitis. Participants with a positive dermatophyte culture received oral griseofulvin (20-25 mg/kg/day) and topical selenium sulfide shampoo for 6 weeks. Main outcome measures. The rate of symptoms of tinea capitis, and rates of mycologic and clinical cure. Results. The positive predictive values of any 1, 2, 3, or 4 symptoms for a positive culture were 88%, 82%, 78%, and 77%, respectively. The observed rates of mycologic, clinical, and complete cure were 89%, 66%, and 49%, respectively. Conclusion. In a high-risk population it is reasonable to diagnose tinea capitis using one or more cardinal symptoms. Oral griseofulvin at 20 to 25 mg/ kg/day with adjunctive shampooing for 6 weeks is moderately successful as treatment.

Published
2009

109. CONTRIBUTORS

Author

John G. Aaskov, Susan M. Abdel-Rahman, Christoph Aebi, Marvin E. Ament, Marsha S. Anderson, Stephen S. Arnon, Ann M. Arvin, Jane T. Atkins, Robert L. Atmar, Carol J. Baker, Robert S. Baltimore, Stephen J. Barenkamp, Elizabeth D. Barnett, Robert D. Basow, William R. Beisel, Beth P. Bell, Gil Benard, David I. Bernstein, Kathrin M. Bernt, Andrea A. Berry, Charles D. Bluestone, Jeffrey L. Blumer, Robert Bortolussi, Bobby L. Boyanton, Kenneth M. Boyer, John S. Bradley, Michael T. Brady, William J. Britt, Annemarie Broderick, David E. Bronstein, David A. Bruckner, Steven C. Buckingham, Ana Burgos, Carrie L. Byington, Judith R. Campbell, Samson Cantu, Mariam R. Chacko, Louisa E. Chapman, Rémi N. Charrel, Tempe K. Chen, James D. Cherry, P. Joan Chesney, Madhuri C. Chilakapati, Javier Chinen, Natascha Ching, H. Fred Clark, Thomas G. Cleary, David K. Coats, Armando G. Correa, J. Thomas Cross, William B. Cutrer, Ronald Dagan, David E. Dassey, Jeffrey P. Davis, Gail J. Demmler-Harrison, Penelope H. Dennehy, Minh L. Doan, Simon R. Dobson, Jan E. Drutz, Paul H. Edelstein, Kathryn M. Edwards, Morven S. Edwards, B. Keith English, Dora Estripeaut, Leland L. Fan, Ralph D. Feigin, George D. Ferry, Anthony E. Fiore, Philip R. Fischer, Randall G. Fisher, Patricia M. Flynn, Thomas R. Flynn, Lisa M. Frenkel, Ellen M. Friedman, Richard A. Friedman, Lynne S. Garcia, Patrick J. Gavin, Michael A. Gerber, Anne A. Gershon, Mark A. Gilger, Susan L. Gillespie, Daniel G. Glaze, W. Paul Glezen, Mary P. Glodé, Donald A. Goldmann, Ellie J.C. Goldstein, Nira A. Goldstein, Edmond T. Gonzales, Mark P. Gorman, Michael D. Green, David Greenberg, Andreas H. Groll, Charles Grose, Duane J. Gubler, Roberto A. Guerrero, Javier Nieto Guevara, Kathleen M. Gutierrez, Caroline Breese Hall, Scott B. Halstead, Shinjiro Hamano, Richard J. Hamill, Margaret R. Hammerschlag, I. Celine Hanson, Nada Harik, Rick E. Harrison, C. Mary Healy, Ulrich Heininger, Gloria P. Heresi, Peter W. Hiatt, Harry R. Hill, David C. Hilmers, Jill A. Hoffman, Ellis K.L. Hon, Margaret K. Hostetter, Peter J. Hotez, Walter T. Hughes, Kristina G. Hulten, David A. Hunstad, Eugene S. Hurwitz, W. Charles Huskins, David Y. Hyun, Mary Anne Jackson, Michael R. Jacobs, Richard F. Jacobs, Jenifer L. Jaeger, Ravi R. Jhaveri, Samantha Johnston, Maureen M. Jonas, Meena R. Julapalli, Edward L. Kaplan, Sheldon L. Kaplan, Saul J. Karpen, Gregory L. Kearns, Margaret A. Keller, Chaouki K. Khoury, Martin B. Kleiman, Jerome O. Klein, Mark W. Kline, Katherine M. Knapp, Heidi M. Kokkinos, Peter J. Krause, Leonard R. Krilov, Paul Krogstad, Thomas L. Kuhls, Xavier de Lamballerie, Timothy R. La Pine, Matthew B. Laurens, Charles T. Leach, Robert J. Leggiadro, Diana R. Lennon, Carolyn Lentzsch-Parcells, Eric Leroy, Chi Wai Leung, Moise L. Levy, Karen Lewis, Phyllis T. Losikoff, Timothy Edward Lotze, Adam W. Lowry, Timothy Mailman, Susan A. Maloney, Laurene Mascola, Edward O. Mason, David O. Matson, Alan N. Mayer, Marc A. Mazade, James B. McAuley, George H. McCracken, Kenneth McIntosh, James E. McJunkin, Kelly T. McKee, Rima L. McLeod, Valérie A. McLin, Maria José Soares Mendes-Giannini, Wayne M. Meyers, Marian G. Michaels, Ian C. Michelow, Vladana Milisavljevic, Aaron M. Miller, James N. Miller, Marjorie J. Miller, James N. Mills, Linda L. Minnich, Ann Moran, James R. Murphy, Pratip K. Nag, Joseph J. Nania, James P. Nataro, Roger K. Nicome, Karin Nielsen-Saines, Delma J. Nieves, Richard A. Oberhelman, Theresa J. Ochoa, Christopher M. Oermann, Alina Olteanu, Gary D. Overturf, Debra L. Palazzi, Pia S. Pannaraj, Janak A. Patel, Christian C. Patrick, Evelyn A. Paysse, Norma Pérez, C.J. Peters, William A. Petri, Brandon Lane Phillips, Larry K. Pickering, Joseph F. Piecuch, Francisco P. Pinheiro, Stanley A. Plotkin, Scott L. Pomeroy, Alice Pong, David L. Pugatch, Joan S. Purcell, Ramya Ramraj, Jack S. Remington, Carina A. Rodriguez, José R. Romero, Benjamin A. Ross, Lawrence A. Ross, Judith L. Rowen, Charles E. Rupprecht, Xavier Sáez-Llorens, Lisa Saiman, Joseph W. St. Geme, Pablo J. Sánchez, Laura A. Sass, Carlos A. Sattler, Danica J. Schulte, Gordon E. Schutze, Filiz O. Seeborg, Eugene D. Shapiro, Nina L. Shapiro, William T. Shearer, Ziad M. Shehab, Jerry L. Shenep, W. Donald Shields, Robyn Shimizu-Cohen, Stanford T. Shulman, Constantine Simos, Arnold L. Smith, Jason S. Soden, Mary Allen Staat, Jeffrey R. Starke, Barbara W. Stechenberg, William J. Steinbach, Paul G. Steinkuller, E. Richard Stiehm, Stephanie H. Stovall, Jeffrey Suen, Ciro V. Sumaya, Andrea P. Summer, Douglas S. Swanson, Tina Q. Tan, Herbert B. Tanowitz, Robert B. Tesh, Philip Toltzis, Richard G. Topazian, Michael F. Tosi, Amelia P.A. Travassos da Rosa, Theodore F. Tsai, Tulio A. Valdez, Jesus G. Vallejo, John A. Vanchiere, Pedro Fernando da C. Vasconcelos, Jorge J. Velarde, James Versalovic, Ellen R. Wald, Douglas S. Walsh, Edward E. Walsh, Thomas J. Walsh, Mark A. Ward, Richard L. Ward, Michelle Weinberg, Robert C. Welliver, J. Gary Wheeler, A. Clinton White, Suzanne Whitworth, Bernhard L. Wiedermann, Natalie Williams-Bouyer, Murray Wittner, Charles R. Woods, Kimberly G. Yen, Ram Yogev, Edward J. Young, and Theoklis E. Zaoutis

Published
2009
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110. Pharmacokinetics of Ceftriaxone

Author

Jeffrey L. Blumer

Subjects
medicine.drug_class, business.industry, Ceftriaxone, Antibiotics, Half-life, Bacterial Infections, General Medicine, 030204 cardiovascular system & hematology, Pharmacology, Total Daily Dose, Excretion, 03 medical and health sciences, 0302 clinical medicine, Single bolus, Pharmacokinetics, medicine, Humans, 030212 general & internal medicine, Dosing, business, Half-Life, Protein Binding, medicine.drug
Abstract

Ceftriaxone fulfills many of the qualities of an ideal antibiotic: a prolonged elimination half-life, which results from a "restrictive" excretion pattern; saturable protein binding, which provides the theoretical basis for administering the total daily dose as a single bolus; and once-a-day dosing, which provides plasma and tissue concentrations that exceed the MIC for most susceptible pathogens for 24 hours.

Published
1991
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111. Opioids and Other Analgesics

Author

Jeffrey L. Blumer and Marcia L. Buck

Subjects
Drug, medicine.medical_specialty, Resuscitation, Nonsteroidal, business.industry, media_common.quotation_subject, Binding properties, General Medicine, Critical Care and Intensive Care Medicine, Intensive care unit, law.invention, chemistry.chemical_compound, chemistry, law, Intensive care, medicine, Ketamine, Intensive care medicine, Adverse effect, business, medicine.drug, media_common
Abstract

Medications for pain relief are an important component of therapy for intensive care patients. Opioids, the most commonly used analgesics in the ICLJ setting, are associated with a large number of adverse effects that are related to their binding properties at opioid-receptor subtypes. Other analgesics, such as ketamine and nonsteroidal anti-inflammatory agents, may cause fewer cardiovascular and respiratory effects, but lead to other unwanted effects in ICU patients. In addition to a review of analgesic-associated adverse effects and drug interactions, guidelines for anticipating and monitoring these agents are presented.

Published
1991
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112. Phenothiazine-Associated Apnea in Two Siblings

Author

Jeffrey L. Blumer and Marcia L. Buck

Subjects
Male, Bradycardia, Meperidine, Apnea, Chlorpromazine, Promethazine Hydrochloride, Promethazine, 030226 pharmacology & pharmacy, Meperidine Hydrochloride, 03 medical and health sciences, Lethargy, 0302 clinical medicine, Phenothiazines, 030225 pediatrics, medicine, Humans, Family, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, Naloxone, business.industry, Infant, medicine.disease, Upper respiratory tract infection, Anesthesia, Urinary Tract Infections, Drug Therapy, Combination, Female, Premedication, medicine.symptom, business, medicine.drug
Abstract

A two-month-old white girl presented to our facility with increasing lethargy and new onset apnea and bradycardia following a week of upper respiratory tract infection symptoms. The patient had been receiving a cough syrup containing promethazine hydrochloride during the previous five days, which was temporally correlated with the onset of lethargy and apneic episodes. Upon further investigation, it was discovered that the patient's older sibling also may have experienced phenothiazine-associated apnea after receiving a combination of meperidine hydrochloride, promethazine hydrochloride, and chlorpromazine as a premedication prior to an endoscopic examination. In addition to the presentation of these cases, the literature pertaining to phenothiazine-associated apnea is reviewed.

Published
1991
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113. Influence of infusion pumps on the pharmacologic response to nitroprusside

Author

Allen Erenberg, Richard D. Leff, Michael D. Reed, Jill C. Hurlbut, Jeffrey L. Blumer, and Suzanne Thompson

Subjects
Male, Nitroprusside, Mean arterial pressure, business.industry, Coefficient of variation, Infant, Hemodynamics, Blood Pressure, Critical Care and Intensive Care Medicine, Crossover study, Random Allocation, Hemodynamically stable, Blood pressure, Child, Preschool, Anesthesia, Humans, Infusion pump, Medicine, Female, Prospective Studies, Child, business, Perfusion, Infusion Pumps
Abstract

OBJECTIVE To compare the relationship between variability in nitroprusside delivery from five infusion pumps and the resulting variability in mean arterial pressure (MAP). DESIGN Randomized, crossover study design. SETTING A pediatric ICU in a university hospital. PATIENTS Informed parental consent was obtained for six patients who were hemodynamically stable and receiving a continuous nitroprusside infusion for a clinical application. Subjects ranged in age from 11 months to 9 yr. INTERVENTIONS All of the subjects were administered nitroprusside using selected infusion pumps, which included Abbott (Micro), 3M/AVI (210), IMED (965), IVAC (565), and Kendall McGaw (MicroRate). MEASUREMENTS AND MAIN RESULTS After an initial equilibration interval for each device, MAP was measured and recorded at 10-sec intervals for greater than or equal to 90-min intervals using a computerized data collection technique. Variation in nitroprusside administration (flow continuity) for each infusion pump was determined in vitro using a computerized gravimetric technique. Variation in both MAP and flow continuity was mathematically expressed as the coefficient of variance (CV) of the measured values for each of the respective infusion pumps. For the Abbott, IMED, 3M/AVI, IVAC, and Kendall McGaw, infusion pumps, mean +/- SD continuity CV values were 85 +/- 31%, 39 +/- 26%, 19 +/- 8%, 17 +/- 3%, and 12 +/- 3%, respectively, and MAP CV values were 18 +/- 21%, 15 +/- 11%, 8 +/- 2%, and 16 +/- 10%, respectively. CONCLUSIONS An apparent direct relationship between MAP variability and flow continuity was observed. We speculate that variation in effect of potent short-acting drugs may, in part, be due to infusion pump operation.

Published
1991
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115. Pharmacokinetics of azithromycin in plasma and sinus mucosal tissue following administration of extended-release or immediate-release formulations in adult patients with chronic rhinosinusitis

Author

Bharat Damle, Annie F. Fang, Michael D. Campbell, James N. Palmer, Jeffrey L. Blumer, Penelope Crownover, and Alexander G. Chiu

Subjects
Microbiology (medical), Adult, Male, medicine.medical_specialty, Urology, Azithromycin, Dosage form, Mass Spectrometry, Plasma, Young Adult, Pharmacokinetics, Olfactory Mucosa, Blood plasma, medicine, Humans, Pharmacology (medical), Sinusitis, Sinus (anatomy), Antibacterial agent, Aged, Aged, 80 and over, Protein synthesis inhibitor, business.industry, General Medicine, Middle Aged, medicine.disease, Anti-Bacterial Agents, Infectious Diseases, medicine.anatomical_structure, Anesthesia, Delayed-Action Preparations, Female, business, medicine.drug, Chromatography, Liquid
Abstract

This study compared the pharmacokinetics of azithromycin (AZI) following administration of extended-release (ER) and immediate-release (IR) formulations in plasma and sinus mucosa in patients with chronic rhinosinusitis. Patients (n=71) were randomised 1:1 to receive a single dose of AZI-ER 2g or up to three doses of AZI-IR 500 mg daily. Paired plasma and sinus tissue samples were taken during endoscopic sinus surgery at 2-168 h (four patients per time point) after the first dose. Samples were measured by a validated liquid chromatography/mass spectrometry assay. Pharmacokinetics were determined using composite concentration-time profiles. Comparison between formulations showed that within the first 24 h, the AZI area under the plasma concentration-time curve (AUC(24)) for ER was 5.2- and 7.0-fold higher than IR in plasma and sinus tissue, respectively. Comparison between matrices showed that the AUC(24) and AUC(168) in sinus tissue were 28.2- and 62.2-fold higher than in plasma for the ER formulation, whilst the AUC(24) in sinus tissue was 21.1-fold higher than in plasma for IR formulation. These results indicated that AZI has good penetration into sinus tissue regardless of formulation; however, dosing of AZI-ER (2 g) increased AZI exposure within the first 24 h compared with the Day 1 dose of 500 mg IR regimen.

Published
2008

116. Acetaminophen-Associated Hepatic Injury: Evaluation of Acetaminophen Protein Adducts in Children and Adolescents With Acetaminophen Overdose

Author

Dean W. Roberts, Gregory L. Kearns, Pippa Simpson, Jacqueline Sullivan, Jeffrey L. Blumer, Lynda Letzig, Jan Hinson, Edmund V. Capparelli, and Leonard James

Subjects
Male, acetaminophen overdose, Adolescent, Drug Compounding, Population, Poison control, Pharmacology, Risk Assessment, Article, Statistics, Nonparametric, Transaminase, Cohort Studies, Pharmacokinetics, Predictive Value of Tests, Medicine, Humans, Pharmacology (medical), Antipyretic, Aspartate Aminotransferases, education, Child, Acetaminophen, Probability, education.field_of_study, biology, business.industry, digestive, oral, and skin physiology, Alanine Transaminase, Bayes Theorem, Alanine transaminase, Child, Preschool, biology.protein, Female, Chemical and Drug Induced Liver Injury, Drug Overdose, business, Biomarkers, Blood Chemical Analysis, medicine.drug, Half-Life
Abstract

Acetaminophen protein adducts (APAP adducts) were quantified in 157 adolescents and children presenting at eight pediatric hospitals with the chief complaint of APAP overdose. Two of the patients required liver transplantation, whereas all the others recovered spontaneously. Peak APAP adducts correlated with peak hepatic transaminase values, time-to-treatment with N-acetylcysteine (NAC), and risk determination per the Rumack-Matthews nomogram. A population pharmacokinetic analysis (NONMEM) was performed with post hoc empiric Bayesian estimates determined for the elimination rate constants (k(e)), elimination half-lives (t(1/2)), and maximum concentration of adducts (C(max)) of the subjects. The mean (+/-SD)k(e) and half-life were 0.486 +/- 0.084 days(-1) and 1.47+/- 0.30 days, respectively, and the C(max) was 1.2 (+/-2.92) nmol/ml serum. The model-derived, predicted adduct value at 48 h (Adduct 48) correlated with adductC(max), adduct T(max), Rumack-Matthews risk determination, peak aspartate aminotransferase (AST), and peak alanine aminotransferase (ALT). The pharmacokinetics and clinical correlates of APAP adducts in pediatric and adolescent patients with APAP overdose support the need for a further examination of the role of APAP adducts as clinically relevant and specific biomarkers of APAP toxicity.

Published
2008

117. Single-dose pharmacokinetics of oral and intravenous pantoprazole in children and adolescents

Author

Stephen M. Schexnayder, Laura P. James, Gregory L. Kearns, Andrea Gaedigk, James F. Daniel, Kim G. Adcock, Jeffrey L. Blumer, Jeffrey Paul, and Michael D. Reed

Subjects
Male, Adolescent, Population, Administration, Oral, CYP2C19, 2-Pyridinylmethylsulfinylbenzimidazoles, law.invention, Pharmacokinetics, Randomized controlled trial, law, Medicine, Humans, Pharmacology (medical), In patient, education, Adverse effect, Child, Infusions, Intravenous, Pantoprazole, Pharmacology, education.field_of_study, business.industry, Proton Pump Inhibitors, Tolerability, Anesthesia, Child, Preschool, Female, business, medicine.drug
Abstract

The primary objective was to determine the pharmacokinetics of single oral and intravenous doses of pantoprazole in children 2 to 16 years of age. The secondary objective was to assess the safety and tolerability of these doses. Male and female hospitalized and nonhospitalized patients from ages 5 to 16 years received single oral doses (20 mg or 40 mg), and those from ages 2 to 16 years received single intravenous doses (0.8 mg/kg or 1.6 mg/kg) of pantoprazole. The plasma concentration-time data for each patient were analyzed using noncompartmental methods. Routine safety and tolerability assessments were also obtained. The mean values for peak plasma concentration and total area under the plasma concentration-time curve increased with increasing dose. Pharmacokinetic values were similar in patients from ages 2 to 16 years and to those previously obtained in adults. Statistically significant differences were observed for dose-normalized pantoprazole area under the plasma concentration-time curve when compared between CYP2C19 extensive metabolizers with 1 versus 2 functional alleles. All adverse events were mild in severity and considered to be unrelated to study drug. The pharmacokinetic profile of oral and intravenous pantoprazole was similar in children ages 2 to 16 years. The doses used here were safe and well tolerated in this population.

Published
2008

118. A randomized comparative study of levofloxacin versus amoxicillin/clavulanate for treatment of infants and young children with recurrent or persistent acute otitis media

Author

Dainius Balis, Adriano Arguedas, Jeffrey L. Blumer, Partha Bagchi, Rama Melkote, Michael E. Pichichero, James Hedrick, Richard H. Schwartz, and Gary J. Noel

Subjects
Microbiology (medical), Male, medicine.medical_specialty, Ofloxacin, medicine.drug_class, Antibiotics, Levofloxacin, Amoxicillin-Potassium Clavulanate Combination, law.invention, Randomized controlled trial, law, Internal medicine, Clavulanic acid, medicine, Humans, Intensive care medicine, Antibacterial agent, business.industry, Infant, Newborn, Infant, Amoxicillin, Antimicrobial, Anti-Bacterial Agents, Otitis Media, Infectious Diseases, Treatment Outcome, El Niño, Child, Preschool, Pediatrics, Perinatology and Child Health, Female, business, medicine.drug
Abstract

The need for alternative antimicrobial therapy for recurrent and persistent acute otitis media (AOM) in children has raised interest in assessing the efficacy and safety of fluoroquinolones for treatment of these infections.In an evaluator-blinded, active-comparator, noninferiority, multicenter study, children (6 months to5 years) were randomized 1:1 to receive levofloxacin (10 mg/kg twice daily) or amoxicillin/clavulanate (14:1; amoxicillin 45 mg/kg twice daily) for 10 days, with evaluations 4-6 days of therapy (visit 2), 2-5 days after completing therapy (visit 3), and 10-17 days after last dose (visit 4). Primary outcome was clinical cure at visit 3 based on resolution of clinical signs and symptoms of AOM.A total of 1650 children were randomized and 1305 were clinically evaluable at visit 3 (630 levofloxacin, 675 comparator). Clinical cure rates were 72.4% (456 of 630) in levofloxacin-treated and 69.9% (472 of 675) in amoxicillin/clavulanate-treated children. Cure rates were also similar for levofloxacin and comparator for each age group (or =24 months: 68.9% versus 66.2%;24 months: 76.9% versus 75.1%; respectively). Cure rates at visit 4 were 74.9% and 73.8% in levofloxacin and amoxicillin/clavulanate groups, respectively. The upper limits of the confidence intervals were less than the noninferiority margin of 10% indicating that levofloxacin treatment is noninferior to comparator treatment overall and in both infants (6 months to 2 years) and children 2-5 years. No differences between treatment groups regarding the frequency or type of adverse events were apparent.Levofloxacin was not inferior to amoxicillin/clavulanate for the treatment of recurrent and/or persistent AOM in infants and children.

Published
2008

119. Pharmacokinetics, outcome of treatment, and toxic effects of amphotericin B and 5-fluorocytosine in neonates

Author

Robert M. Kliegman, Jill E. Baley, Jeffrey L. Blumer, Carolyn Meyers, and Michael R. Jacobs

Subjects
Birth weight, Flucytosine, Gestational Age, Pharmacology, Kidney, chemistry.chemical_compound, Pharmacokinetics, Oral administration, Amphotericin B, medicine, Humans, Blood urea nitrogen, Volume of distribution, Creatinine, business.industry, Candidiasis, Infant, Newborn, Infant, Low Birth Weight, Prognosis, Mycoses, chemistry, Pediatrics, Perinatology and Child Health, business, Infant, Premature, medicine.drug
Abstract

To determine the pharmacokinetics of amphotericin B and 5-fluorocytosine in neonates, we measured serum concentrations at first dose and after 5 days of therapy by high-performance liquid chromatography in 13 neonates (mean birth weight 1.2 +/- 0.8 kg). The dose of amphotericin B was serially increased from 0.1 to 0.5 mg/kg/day in 10 infants but was decreased from 0.8 to 1.0 to 0.5 mg/kg/day in three infants. Amphotericin B concentrations were not detectable in infants receiving 0.1 mg/kg/day. Amphotericin B cerebrospinal fluid concentrations were 40% to 90% of serum values obtained simultaneously. Serum concentrations after oral administration of 5-fluorocytosine (dose 25 to 100 mg/kg/day) were detectable in all infants. We found extreme interindividual variability for the half-life, volume of distribution, and clearance for both drugs. Four infants had minimal elimination for both drugs between doses, a finding that correlates with rises in serum creatinine (greater than 0.4 mg/dl, 40 mumol/L) and blood urea nitrogen (greater than 10 mg/dl, 3.6 mmol/L). We recommend that the dose of amphotericin B given on the first day of treatment be greater than the usual testing dose of 0.1 mg/kg/day. We also recommend an initial 24-hour dosing interval for amphotericin B and 5-fluorocytosine. Serum drug concentrations may need to be monitored in high-risk, low birth weight infants.

Published
1990
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120. Potential pharmacokinetic basis for zolpidem dosing in children with sleep difficulties

Author

Daniel G. Glaze, Carol L. Rosen, Mary Ann O'Riordan, Frank Steinberg, Michael L. Christensen, MA Springer, Jeffrey L. Blumer, and Reed

Subjects
Male, Zolpidem, Adolescent, medicine.drug_class, Pyridines, Polysomnography, Drug Administration Schedule, Hypnotic, Pharmacokinetics, Sleep Initiation and Maintenance Disorders, medicine, Humans, Hypnotics and Sedatives, Pharmacology (medical), Dosing, Child, Pharmacology, Volume of distribution, Analysis of Variance, medicine.diagnostic_test, Chemistry, Age Factors, Sedative, Anesthesia, Pharmacodynamics, Area Under Curve, Child, Preschool, Female, medicine.drug
Abstract

The pharmacokinetics of zolpidem was assessed in this open-label, dose-escalation study in children with insomnia. Twenty-one children, seven per age group (2-6, >6 to 12, >12 to 18 years), received a single dose of zolpidem at one of the three dose levels (0.125, 0.25, or 0.50 mg/kg (20 mg maximum dose)). Multiple pharmacokinetic measures were assessed at nine post-dose intervals and pharmacodynamics was assessed by polysomnography and actigraphy. Significant pharmacokinetic effects by dose were observed only as linear increases in maximum concentration (C(max), P

Published
2007

121. Change in pneumococcal susceptibility to azithromycin during treatment for acute otitis media

Author

Jeffrey L. Blumer, Philip Toltzis, and Michael Dul

Subjects
Microbiology (medical), medicine.drug_class, Acute otitis media, Antibiotics, Microbial Sensitivity Tests, Penicillins, Azithromycin, medicine.disease_cause, Pneumococcal Infections, Microbiology, Antibiotic resistance, Drug Resistance, Multiple, Bacterial, Streptococcus pneumoniae, medicine, Humans, Antibacterial agent, Protein synthesis inhibitor, biology, business.industry, bacterial infections and mycoses, Streptococcaceae, biology.organism_classification, Otitis Media, Infectious Diseases, Pediatrics, Perinatology and Child Health, Immunology, business, medicine.drug
Abstract

Authorities have suggested restriction of azithromycin use as a principal strategy to contain the spread of azithromycin-nonsusceptible Streptococcus pneumoniae (ANSP). In 83 children persistently colonized by pneumococcus during and after treatment of acute otitis media, 17 acquired a new strain, 9 of which were less susceptible to azithromycin than the original isolate. New appearance of ANSP was documented after both beta-lactam and azithromycin exposure. ANSP is likely to disseminate even with significant reduction of azithromycin use unless other antibiotic use is decreased as well.

Published
2007

122. Extracorporeal membrane oxygenation

Author

Jeffrey L. Blumer and Lia Lowrie

Subjects
medicine.medical_specialty, business.industry, medicine.medical_treatment, Extracorporeal membrane oxygenation, Medicine, Critical Care and Intensive Care Medicine, business, Intensive care medicine
Published
1998
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123. Evolution of a new drug formulation: the rationale for high-dose, short-course therapy with azithromycin

Author

Jeffrey L. Blumer

Subjects
Microbiology (medical), Drug, media_common.quotation_subject, Chemistry, Pharmaceutical, Pharmacology, Pharmaceutical formulation, Azithromycin, Pharmacokinetics, In vivo, medicine, Potency, Animals, Humans, Pharmacology (medical), Respiratory Tract Infections, media_common, Phagocytes, Dose-Response Relationship, Drug, business.industry, General Medicine, Microspheres, Anti-Bacterial Agents, Infectious Diseases, Tolerability, Pharmacodynamics, Area Under Curve, Immunology, business, medicine.drug, Half-Life
Abstract

The rationale for the use of high-dose, short-course azithromycin treatment regimens is based on the pharmacokinetic properties of azithromycin. Its long elimination half-life (approximately 60 h) and antibacterial potency make short-course (1-day) regimens feasible. Azithromycin is concentrated within phagocytic cells, which deliver it in a targeted manner to sites of infection. In vitro and in vivo models demonstrate that azithromycin is taken up, transported and released at the sites of infection by polymorphonuclear neutrophils and macrophages. Uptake is not saturable, so delivery of the total azithromycin therapeutic regimen as a single dose of azithromycin microspheres should lead to increased uptake and delivery of the drug to sites of infection. By achieving higher drug concentrations at the site of infection, a single, high dose of azithromycin microspheres should maximize efficacy. The new microsphere formulation allows for 'front loading' of the dose to achieve the highest drug levels early in the course of infection while maintaining favorable tolerability.

Published
2006

124. Serogroup 19 pneumococci containing both mef and erm macrolide resistance determinants in an American city

Author

Mary Ann O'Riordan, Michael R. Jacobs, Jeffrey L. Blumer, Michael Dul, and Philip Toltzis

Subjects
Microbiology (medical), Serotype, DNA, Bacterial, medicine.drug_class, Antibiotics, Drug resistance, Microbial Sensitivity Tests, Biology, Azithromycin, medicine.disease_cause, Polymerase Chain Reaction, Pneumococcal Infections, Microbiology, Antibiotic resistance, stomatognathic system, Bacterial Proteins, Streptococcus pneumoniae, Drug Resistance, Bacterial, otorhinolaryngologic diseases, medicine, Humans, Serotyping, Child, Antibacterial agent, Ohio, Molecular Epidemiology, Molecular epidemiology, Infant, Membrane Proteins, Methyltransferases, Sequence Analysis, DNA, biochemical phenomena, metabolism, and nutrition, Virology, DNA Fingerprinting, Anti-Bacterial Agents, Electrophoresis, Gel, Pulsed-Field, Otitis Media, Infectious Diseases, Genes, Bacterial, Child, Preschool, embryonic structures, Pediatrics, Perinatology and Child Health, Efflux
Abstract

Asia has experienced a striking incidence of infection by highly resistant pneumococi containing both principal macrolide resistance determinants, namely, the mef efflux pump and the erm ribosomal methylase. mef/erm-containing pneumococci have not been identified in significant numbers in North America.Pneumococci were isolated as part of a larger study in Cleveland, OH examining colonization patterns among children randomized to 1 of 4 outpatient antibiotics for acute otitis media. Azithromycin-resistant organisms were tested for the presence of mef and erm sequences by polymerase chain reaction. The clonal relationship of pneumococci containing both genes was determined by pulsed field gel electrophoresis and multilocus sequence testing. Selected characteristics of children harboring mef/erm-containing organisms were compared with other participants of the larger study.Of 221 children colonized by pneumococci, 17 (7.7%) were colonized with an organism containing both determinants. All mef/erm-positive organisms demonstrated azithromycin minimum inhibitory concentrationsor =256 microg/mL and were coresistant to all other agents tested. The mef/erm-containing organisms were serotype 19A and 19F, all but 1 of which manifested similar pulsed field gel electrophoresis patterns. Multilocus sequence testing analysis indicated a relationship to the Taiwan-14 macrolide-resistant strain that has spread throughout Eastern Asia. More than one-third of children colonized by a mef/erm-containing organism had receivedor =1 dose of conjugate pneumococcal vaccine, a significantly higher proportion than children carrying less resistant organisms (P0.01). No other characteristics distinguished children harboring a mef/erm-containing pneumococcus from other children enrolled in the larger study.Clonally related mef/erm-containing serogroup 19 pneumococci were prominent among otherwise healthy children in a North American metropolitan area. Our findings suggest that spread of these organisms may be poorly contained by immunization.

Published
2006

125. Contributors

Author

P. David Adelson, David B. Allen, Estella M. Alonso, Gülay Pinar Alper, Derek C. Angus, Sidney Anthone, Andrew Argent, John H. Arnold, Barbara Bambach, Hülya Bayir, Pierre Beaulieu, Laurie O. Beitz, Jorge R. Beltrán, Wade W. Benton, Robert A. Berg, Ira Bergman, Julie Blatt, Douglas L. Blowey, Jeffrey L. Blumer, John S. Bradley, Barbara W. Brandom, Martin L. Brecher, Richard J. Brilli, Guy F. Brisseau, Thomas V. Brogan, Timothy E. Bunchman, Sean P. Bush, Joseph Carcillo, Aaron L. Carrel, Hector Carrillo-Lopez, Victoria Cartwright, Hugo F. Carvajal, Leticia Castillo, Michael G. Caty, Pelin Cengiz, Anthony C. Chang, John R. Charpie, Adrián Chávez, Russell W. Chesney, Michael A. Cimino, Robert S.B. Clark, Jacqueline J. Coalson, D. Ryan Cook, Craig M. Coopersmith, Christopher P. Coppola, Seth J. Corey, Peter N. Cox, Kathleen Culver, James J. Cummings, Martha A.Q. Curley, Marek Czosnyka, Heidi J. Dalton, Stéphane Dauger, Peter J. Davis, Jenina Deshler, Sonny Dhanani, Rhonda M. Dick, Emily L. Dobyns, Elizabeth J. Donner, Didier Dreyfuss, Philippe Durand, Susan Duthie, Richard G. Ellenbogen, Jacqueline Evans, James C. Fackler, Kathryn Felmet, Jeffrey R. Fineman, Debra H. Fiser, Frank A. Fish, James E. Fletcher, J. Julio Pérez Fontán, Michael L. Forbes, Norman Fost, Joel E. Frader, Deborah Franzon, F. Jay Fricker, Aaron L. Friedman, Bradley P. Fuhrman, France Gauvin, Eli Gilad, James C. Gilbert, Brett P. Giroir, Stuart L. Goldstein, James Graham, Jerril W. Green, Thomas P. Green, Stephanie Greene, James A. Griffith, Mauro Grossi, Björn Gunnarsson, Scott A. Hagen, Cecil D. Hahn, Craig Hallstrom, Yong Y. Han, Cary O. Harding, William G. Harmon, Eric Harry, Mary E. Hartman, Christopher Heard, Lynn Hernan, Mark J. Heulitt, Robert W. Hickey, Julien I.E. Hoffman, Karen T. Hofmann, Gregory A. Hollman, James C. Huhta, Hector E. James, David Jardine, Alberto Jarillo, Etienne Javouey, James A. Johns, Kristin K. Johnson, Michael V. Johnston, Deborah P. Jones, Prashant Joshi, Prince J. Kannankeril, Robert K. Kanter, John A. Kellum, Michael Kelly, Patrick M. Kochanek, Samuel A. Kocoshis, Thomas J. Kulik, Vasanth H. Kumar, Jacques Lacroix, Yichen Lai, Joanne M. Langley, Stanley T. Lau, Peter Laussen, Yi-Horng Lee, Mary W. Lieh-Lai, D. Michael Lindsay, Catherine Litalien, Naomi L.C. Luban, Robert E. Lynch, Frank Maffei, James P. Marcin, Mary Michele Mariscalco, Barry P. Markovitz, Lynn D. Martin, Anne G. Matlow, John E. Mayer, Paula Mazur, E. Dean McKenzie, Gwenn E. McLaughlin, Nilesh Mehta, Renuka Mehta, Ann J. Melvin, Jean-Christophe Mercier, Kelly Michelson, Kelly A. Michienzi, Patricia A. Moloney-Harmon, Frederick C. Morin, Michele Moss, Vinay Nadkarni, Carol E. Nicholson, Victoria F. Norwood, Daniel Notterman, Alan Nugent, Peter Oishi, Victor Olivar, Richard A. Orr, Yves Ouellette, Daiva Parakininkas, Margaret M. Parker, Anthony L. Pearson-Shaver, Mary Jane F. Petruzzi, Maury N. Pinsk, Murray M. Pollack, Steven Pon, Alice Pong, Lara Primak, Audra Prince, Jean-Damien Ricard, Tom B. Rice, Gail E. Richards, Debra Ann Ridling, Joan Roberts, Kimberly Roth, Alexandre T. Rotta, Daniel Rubens, Jeffrey S. Rubenstein, Christopher M. Rubino, Randall Ruppel, Peter J. Safar, Ashok P. Sarnaik, Joel B. Sarner, Georges Saumon, Matthew C. Scanlon, Kenneth Schenkman, Stephen M. Schexnayder, Charles L. Schleien, Timothy A. Sentongo, Thomas P. Shanley, Frank Shann, Dennis W.W. Shaw, Sam D. Shemie, Peter Skippen, Anthony D. Slonim, Laurie Smith, Lincoln Smith, David M. Steinhorn, Waldemar E. Storm, Marc Sturgill, Marianne T. Sweetser, Jordan M. Symons, Robert C. Tasker, Ann E. Thompson, Ann Henderson Tilton, Nicole H. Tobin, I. David Todres, Peter Trinkaus, David J. Vaughan, Shekhar T. Venkataraman, Rapheus C.Q. Villanueva, Patricia C. Wankum, R. Scott Watson, Wayne R. Waz, Carl G.M. Weigle, Maria B. Weimer, Ed Weinberger, David L. Wessel, William T. West, Randall C. Wetzel, Dale Whitby, Hector R. Wong, Ellen G. Wood, Alan D. Woolf, James Woytash, Ofer Yanay, Arno Zaritsky, Danielle M. Zerr, and Jerry J. Zimmerman

Published
2006
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127. Cytokines and toxicity in acetaminophen overdose

Author

Janice E. Sullivan, Pippa Simpson, Michael D. Reed, Laura P. James, Henry C. Farrar, Jack A. Hinson, Gregory L. Kearns, Gary S. Wasserman, and Jeffrey L. Blumer

Subjects
Male, acetaminophen overdose, Adolescent, medicine.medical_treatment, Enzyme-Linked Immunosorbent Assay, Transaminase, medicine, Humans, Pharmacology (medical), Interleukin 8, Aspartate Aminotransferases, Interleukin 6, Child, Chemokine CCL2, Acetaminophen, Pharmacology, biology, business.industry, Interleukin-6, digestive, oral, and skin physiology, Interleukin-8, Infant, Newborn, Infant, Alanine Transaminase, Interleukin-10, Interleukin 10, Cytokine, Child, Preschool, Toxicity, Immunology, biology.protein, Linear Models, Prothrombin Time, Cytokines, Female, Drug Overdose, business, medicine.drug
Abstract

Several cytokines have been reported to have hepatoprotective properties in animal models of acetaminophen toxicity. To investigate the relationships of cytokines and toxicity in acetaminophen overdose, blood samples were collected from patients following acute ingestions of acetaminophen. Samples for cytokine analysis were collected at the time of routine clinical monitoring in 111 patients (90 females; mean age 13.6 years). Plasma concentrations of interleukin 6, interleukin 8, interleukin 10, and monocyte chemoattractant protein 1 were analyzed by enzyme-linked immunosorbent assay. Patients were stratified by toxicity severity, defined by the maximal values of hepatic transaminase elevation. Levels of interleukin 6, interleukin 8, and monocyte chemoattractant protein 1 were higher in patients with serum alanine aminotransferase > 1000 IU/L, and monocyte chemoattractant protein 1 had the strongest association with toxicity. Monocyte chemoattractant protein 1 values were higher in patients with greater delays in N-acetylcysteine treatment and in patients with higher values of prothrombin time. Monocyte chemoattractant protein 1 elevation in acetaminophen overdose may represent an innate, immunomodulary response of the liver to earlier events in the toxicity. An understanding of the role of cytokine responses in acetaminophen overdose may be relevant to the future development of new therapies for acetaminophen toxicity.

Published
2005

128. Fluticasone propionate plasma concentration and systemic effect: effect of delivery device and duration of administration

Author

Jeffrey L. Blumer, Richard J. Martin, Glenn J. Whelan, and Stanley J. Szefler

Subjects
Adult, medicine.medical_specialty, Time Factors, Hydrocortisone, medicine.drug_class, Immunology, Pharmacology, Fluticasone propionate, Pharmacokinetics, Internal medicine, Administration, Inhalation, medicine, Immunology and Allergy, Humans, Metered Dose Inhalers, Fluticasone, Clinical Trials as Topic, integumentary system, business.industry, Inhaler, Area under the curve, Metered-dose inhaler, Dry-powder inhaler, Asthma, Bronchodilator Agents, Androstadienes, Endocrinology, Corticosteroid, Powders, business, medicine.drug
Abstract

Inhaled corticosteroids are the preferred therapy in persistent asthma. Dry powder inhalers (DPIs) generate a larger particle size compared with metered-dose inhalers (MDIs), which affects pulmonary deposition, bioavailability, and subsequent systemic effects of fluticasone propionate (fluticasone).To examine the relationship of fluticasone pharmacokinetics and cortisol suppression for 2 fluticasone formulations (DPI and MDI) administered in adults over 1-week and 6-week treatment periods.Two previous studies conducted in adults by the Asthma Clinical Research Network examined relative efficacy and systemic effect of fluticasone from MDI and DPI. Sample sets (n=33) were analyzed for fluticasone after administration of 352 microg from the MDI, and 400 microg from the DPI formulation, twice daily, after a 1-week treatment period. The second study's sample sets (n=9) were analyzed for fluticasone after 6 weeks therapy at 352 microg twice daily from the MDI formulation, allowing achievement of steady state.ANOVA revealed a significant trend of increasing fluticasone area under the curve from 0 to time t (AUC(0--t)) when comparing DPI with MDI for 1 week with MDI for 6 weeks (P.0001). Similarly, ANOVA revealed increasing cortisol suppression between these groups (P=.007). Linear regression demonstrated that increasing fluticasone AUC(0--t) was significantly correlated with cortisol suppression (P.0001; r(2)=0.41). MDI for 6 weeks showed increasing fluticasone AUC (P=.0008, t test) compared with MDI for 1 week, suggesting accumulation.Fluticasone plasma concentrations are significantly greater after MDI compared with DPI, and cortisol suppression is associated with fluticasone plasma concentrations. Accumulation of fluticasone concentrations suggests that time to steady state exceeds 1 week of treatment with MDI.

Published
2005

129. Levofloxacin pharmacokinetics in children

Author

Gregory L. Kearns, Samuel Maldonado, Jaya Natarajan, Gary J. Noel, John S. Bradley, Thomas G. Wells, Jeffrey L. Blumer, Joseph A. Bocchini, and Shuchean Chien

Subjects
Pediatrics, medicine.medical_specialty, Ofloxacin, Adolescent, Metabolic Clearance Rate, Administration, Oral, Biological Availability, Levofloxacin, Drug Administration Schedule, Fluoroquinolone Antibiotic, Age groups, Pharmacokinetics, Anti-Infective Agents, medicine, Humans, Pharmacology (medical), Dosing, Child, Infusions, Intravenous, Pharmacology, Inpatients, business.industry, Body Weight, Age Factors, Infant, Clinical trial, Multicenter study, Area Under Curve, Child, Preschool, Injections, Intravenous, business, Biological availability, medicine.drug
Abstract

Levofloxacin is a broad-spectrum fluoroquinolone antibiotic with activity against many pathogens that cause bacterial infections in children, including penicillin-resistant pneumococci. To provide dosing guidance for children, 3 single-dose, multicenter pharmacokinetic studies were conducted in 85 children in 5 age groups: 6 months to2 years, 2 to5 years, 5 to10 years, 10 to12 years, and 12 to 16 years. Each child received a single 7-mg/kg dose of levofloxacin (not to exceed 500 mg) intravenously or orally. Plasma and urine samples were collected through 24 hours after dose. Pharmacokinetic parameters were estimated and compared among the 5 age groups and to previously collected adult data. Levofloxacin absorption (as indicated by C(max) and t(max)) and distribution in children are not age dependent and are comparable to those in adults. Levofloxacin elimination (reflected by t1/2 and clearance), however, is age dependent. Children younger than 5 years of age clear levofloxacin nearly twice as fast (intravenous dose, 0.32+/-0.08 L/h/kg; oral dose, 0.28+/-0.05 L/h/kg) as adults and, as a result, have the total systemic exposure (area under the plasma drug concentration-time curve) approximately one half that of adults. The levofloxacin area under the plasma drug concentration-time curve (dose normalized) in children receiving a single dose of the oral liquid formulation is comparable to that in children receiving the intravenous formulation. To provide compatible levofloxacin exposures associated with clinical effectiveness and safety in adults, childrenor =5 years need a daily dose of 10 mg/kg, whereas children 6 months to5 years should receive 10 mg/kg every 12 hours.

Published
2005

130. Propofol Bashing

Author

Michael D. Reed and Jeffrey L. Blumer

Subjects
business.industry, medicine, Medical emergency, Critical Care and Intensive Care Medicine, medicine.disease, Propofol, business, medicine.drug
Published
1996
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131. Rationale for single and high dose treatment regimens with azithromycin

Author

Emma M. Gordon and Jeffrey L. Blumer

Subjects
Microbiology (medical), Male, Maximum Tolerated Dose, medicine.drug_class, medicine.medical_treatment, Antibiotics, Biological Availability, Azithromycin, Risk Assessment, Drug Administration Schedule, Pharmacokinetics, In vivo, medicine, Humans, Child, Respiratory Tract Infections, Antibacterial agent, Randomized Controlled Trials as Topic, Chemotherapy, Dose-Response Relationship, Drug, business.industry, Regimen, Infectious Diseases, Treatment Outcome, Pharmacodynamics, Child, Preschool, Pediatrics, Perinatology and Child Health, Immunology, Female, business, medicine.drug
Abstract

The rationale for the use of single dose and shorter course azithromycin treatment regimens is based on the pharmacokinetic properties of azithromycin. The drug has a long elimination half-life (>50 h), which enables short course 1- or 3-day dose regimens to be clinically effective. Azithromycin is concentrated within phagocytic cells and tissues and it achieves targeted delivery by these cells to sites of infection. In vitro and in vivo models have demonstrated that azithromycin is taken up, transported and released at the sites of infection by phagocytic cells such as polymorphonuclear neutrophils and macrophages. Uptake is not saturable; therefore delivery of the total dose of azithromycin as a 1- or 3-day regimen should lead to increased uptake and delivery of the drug to sites of infection.

Published
2004

133. Efficacy of single-dose azithromycin in treatment of acute otitis media in children after a baseline tympanocentesis

Author

Judy A. Krogstad, Jean Chow, Chandra Khurana, P. Fernández, Richard H. Schwartz, Mary M. Aspin, Michael W. Dunne, Adib Rodriguez, Sergio L. Vargas, Paz Emparanza, Irmeli Roine, Adriano Arguedas Mohs, John K. Podgore, Samuel Mclinn, Jeffrey L. Blumer, Antonio Arrieta, Mark M. Blatter, Garth D. Ehrlich, and Willis M. Gooch

Subjects
Male, Cure rate, medicine.medical_specialty, Acute otitis media, Azithromycin, Clinical Therapeutics, Body weight, medicine.disease_cause, Haemophilus influenzae, Internal medicine, Streptococcus pneumoniae, Tympanocentesis, Medicine, Humans, Pharmacology (medical), Pharmacology, business.industry, Dosing regimen, Infant, Combined Modality Therapy, Surgery, Anti-Bacterial Agents, Otitis Media, Infectious Diseases, Child, Preschool, Drainage, Female, business, medicine.drug
Abstract

Children with acute otitis media underwent tympanocentesis and were given a single dose of 30 mg of azithromycin/kg of body weight. At day 28, the overall clinical cure rate was 206 of 242 (85%). Clinical cure rates for patients infected with Streptococcus pneumoniae (67 of 76; 88%) and Haemophilus influenzae (28 of 44; 64%) were consistent with historical rates for the 5-day dosing regimen.

Published
2003

134. Intravenous and oral itraconazole versus intravenous and oral fluconazole for long-term antifungal prophylaxis in allogeneic hematopoietic stem-cell transplant recipients. A multicenter, randomized trial

Author

Gerhard J. Leitz, Mitchell Goldman, Pranatharthi H. Chandrasekar, Mary C. Territo, Drew J. Winston, Hillard M. Lazarus, Jeffrey L. Blumer, and Richard T. Maziarz

Subjects
Adult, Male, medicine.medical_specialty, Antifungal Agents, Adolescent, Itraconazole, medicine.medical_treatment, Administration, Oral, Hematopoietic stem cell transplantation, Opportunistic Infections, Gastroenterology, law.invention, Pharmacotherapy, Randomized controlled trial, law, Internal medicine, Internal Medicine, medicine, Humans, Adverse effect, Fluconazole, Chemotherapy, business.industry, Hematopoietic Stem Cell Transplantation, General Medicine, Middle Aged, Survival Analysis, Surgery, Transplantation, Mycoses, Injections, Intravenous, Female, business, medicine.drug
Abstract

Allogeneic hematopoietic stem-cell transplant recipients often receive fluconazole or an amphotericin B preparation for antifungal prophylaxis. Because of concerns about fungal resistance with fluconazole and toxicity with amphotericin B, alternative prophylactic regimens have become necessary.To compare the efficacy and safety of intravenous and oral itraconazole with the efficacy and safety of intravenous and oral fluconazole for long-term prophylaxis of fungal infections.Open-label, multicenter, randomized trial.Five transplantation centers in the United States.140 patients undergoing allogeneic hematopoietic stem-cell transplantation.Itraconazole (200 mg intravenously every 12 hours for 2 days followed by 200 mg intravenously every 24 hours or a 200-mg oral solution every 12 hours) or fluconazole (400 mg intravenously or orally every 24 hours) from day 1 until day 100 after transplantation.Proven invasive or superficial fungal infection, drug-related side effects, mortality from fungal infection, and overall mortality.Proven invasive fungal infections occurred in 6 of 71 itraconazole recipients (9%) and in 17 of 67 fluconazole recipients (25%) during the first 180 days after transplantation (difference, -16 percentage points [95% CI, -29.2 to -4.7 percentage points]; P = 0.01). Superficial fungal infections occurred in 3 of 71 itraconazole recipients (4%) and in 2 of 67 fluconazole recipients (3%). In a multivariable analysis using factors known to affect the risk for invasive fungal infection after hematopoietic stem-cell transplantation, prophylaxis with itraconazole was still associated with fewer invasive fungal infections (odds ratio, 0.300 [CI, 0.111 to 0.814]; P = 0.02) caused by either yeasts or molds. More fungal pathogens were found to be resistant to fluconazole than to itraconazole. Except for more frequent gastrointestinal side effects (nausea, vomiting, diarrhea, or abdominal pain) in patients given itraconazole (24% vs. 9%; difference, 15 percentage points [CI, 2.9 to 27.0 percentage points]; P = 0.02), both itraconazole and fluconazole were well tolerated. The overall mortality rate was similar in each group (32 of 71 patients in the itraconazole group [45%] vs. 28 of 67 patients in the fluconazole group [42%]; difference, 3 percentage points [CI, -13.2 to 19.8 percentage points]; P0.2), but fewer deaths were related to fungal infection in patients given itraconazole (6 of 71 [9%]) than in patients given fluconazole (12 of 67 [18%]) (difference, 9 percentage points [CI, -20.6 to 1.8 percentage points]; P = 0.13).Itraconazole is more effective than fluconazole for long-term prophylaxis of invasive fungal infections after allogeneic hematopoietic stem-cell transplantation. Except for gastrointestinal side effects, itraconazole is well tolerated.

Published
2003

135. Pharmacokinetic Characteristics of Caspofungin in Two Pediatric Liver Transplant Patients

Author

Michael Neely and Jeffrey L. Blumer

Subjects
Pharmacology, Volume of distribution, medicine.medical_specialty, business.industry, Brief Report, Antifungal drug, biochemical phenomena, metabolism, and nutrition, bacterial infections and mycoses, Gastroenterology, Surgery, Transplantation, chemistry.chemical_compound, Pharmacokinetics, chemistry, Internal medicine, Concomitant, medicine, polycyclic compounds, Pharmacology (medical), Caspofungin, Adverse effect, business, skin and connective tissue diseases, Perfusion
Abstract

Background: The pharmacokinetic characteristics of the antifungal drug caspofungin have not been reported in children. Objective: The aim of this study was to report limited caspofungin pharmacokinetic data for pediatric liver transplant patients. Methods: Two pediatric liver transplant patients, aged 5 years (not dialyzed) and 9 months (dialyzed), were assessed. Using a novel, validated, liquid-phase extraction with high-performance liquid chromatography, we measured plasma caspofungin concentrations from blood samples obtained within a 24-hour period after the patients were given 1 mg/kg IV of caspofungin. Results: Noncompartmental analysis for the nondialyzed patient showed an elimination half-life of 10.7 hours, a volume of distribution of 0.11 L/kg, and a systemic clearance of 0.12 mL/min/kg. Liver enzyme activities increased briefly; the increase may have been due to concomitant graft rejection. For the dialyzed patient, the half-life was 11.7 hours, with an adjusted volume of distribution of 0.18 L/kg and a systemic clearance of 0.24 mL/min/kg. No clinically relevant treatment-related adverse events were noted. Conclusions: Pharmacokinetic data found in the 2 patients in this study are similar to those reported in adults. Until more thorough data are published, caspofungin 1 mg/kg may be considered a reasonable, tolerable dose for children.

Published
2003

136. Developing strategies for psychopharmacological studies in preschool children

Author

David Shaffer, Christopher J. Kratochvil, Kayla Pope, Kimberly Hoagwood, Jeffrey L. Blumer, Howard Abikoff, Peter S. Jensen, Celia B. Fisher, Benedetto Vitiello, Theodore A. Petti, Laurence L. Greenhill, Thomas Laughren, Benjamin B. Lahey, James F. Leckman, Joseph DeVeaugh-Geiss, and Charles H. Zeanah

Subjects
N of 1 trial, Research design, medicine.medical_specialty, Adolescent, MEDLINE, Clinical trials, Diagnosis, Ethics, Preschool children, Child, Child Psychiatry, Child, Preschool, Clinical Trials as Topic, Guidelines as Topic, Humans, Mental Disorders, Psychotropic Drugs, Research, Psychiatry and Mental Health, Developmental and Educational Psychology, Interpersonal communication, Child and adolescent psychiatry, Medicine, Medical prescription, Psychiatry, Preschool, Medical education, business.industry, Aggression, Clinical trial, medicine.symptom, business
Abstract

Objective To identify the obstacles and special challenges—ethical, practical, scientific, and regulatory—faced by investigators who attempt to conduct psychopharmacological studies in preschoolers. Method In a workshop held at the 47th Annual Meeting of the American Academy of Child and Adolescent Psychiatry, featuring interactive sessions designed to elicit discussion of the theory and feasibility of research in this young population, several key domains were identified: diagnosis and assessment, ethics, research design, special considerations for preschoolers, regulatory/industry issues, and education/training. Results A Pediatric Psychopharmacology Initiative is needed to consolidate recommendations from this and other workshops and current federal, research, and regulatory committees. A scholarly review and a guide for institutional review boards and investigators should be prepared on issues related to preschoolers. Developmental specialists provide valuable expertise that can strengthen studies of pediatric psychopharmacology. “N of 1” case studies can provide valuable information to clinicians. Only preschoolers with severe symptoms that occur in several interpersonal contexts should be entered into trials. Indications for the study of symptom complexes (e.g., aggression) rather than specific diagnoses should be examined and considered for regulatory activities. Psychopharmacology practice parameters for preschoolers are needed. Conclusions With preschoolers being increasingly treated with psychopharmacological agents, the need for investigations to address the safety and efficacy of these medications is becoming a central issue for researchers from many disciplines.

Published
2003

137. Antibiotics and breast-feeding: a critical review of the literature

Author

Michael D. Reed, Allison M. Chung, and Jeffrey L. Blumer

Subjects
Milk, Human, medicine.drug_class, business.industry, Antibiotics, Infant, Newborn, Clindamycin, Physiology, Biological Availability, Pharmacology, Breast milk, medicine.disease, Mastitis, Anti-Bacterial Agents, Breast Feeding, Nitrofurantoin, Pediatrics, Perinatology and Child Health, medicine, Vancomycin, Humans, Pharmacology (medical), Female, business, Breast feeding, Postpartum period, medicine.drug
Abstract

Continuous breast-feeding, an integral component of the postpartum period, is often threatened upon maternal initiation of antibiotics. The real risk of antibiotic use while breast-feeding must be carefully analysed with regard to all the variables that influence the extent of antibiotic distribution into breast milk, including breast milk composition, physicochemical properties of the antibiotic (molecular weight, lipid solubility, pH, protein binding), length of feeding, and maternal disposition. In addition, infant disposition, including ability to absorb, metabolize, eliminate, and tolerate any amounts of antibiotic, must also be considered prior to maternal administration of antibiotic. The milk to plasma (M/P) ratio is a frequently quoted parameter used to predict drug distribution into breast milk. However, its utility is questionable and often fraught with misinterpretation. An alternative approach when the amount of antibiotic concentration in breast milk is known (through clinical trials) is to calculate an estimated or expected infant drug exposure factoring in known/expected milk consumption, drug concentration and bioavailability. In this review, the following antibiotic classes and current literature regarding their distribution into breast milk are critically reviewed: beta-lactam antibiotics, fluoroquinolones, sulfonamides, macrolides, aminoglycosides, tetracyclines, nitrofurantoin, metronidazole, vancomycin, clindamycin and chloramphenicol. In the majority of instances, these antibiotics do not distribute into breast milk in sufficient concentrations to be of any clinical consequence in the breast-feeding infant.

Published
2002

138. 3-O-methyldobutamine, a major metabolite of dobutamine in humans

Author

Jeffrey L. Blumer, Leslie T. Webster, and Maohe Yan

Subjects
Male, medicine.medical_specialty, S-Adenosylmethionine, Magnetic Resonance Spectroscopy, Metabolite, Pharmaceutical Science, In Vitro Techniques, Catechol O-Methyltransferase, chemistry.chemical_compound, Pharmacokinetics, Internal medicine, Dobutamine, medicine, Humans, Child, Pharmacology, Metabolism, Adrenergic beta-Agonists, medicine.disease, Endocrinology, chemistry, Heart failure, Shock (circulatory), Catecholamine, Leukocytes, Mononuclear, medicine.symptom, Ionotropic effect, medicine.drug
Abstract

Dobutamine is a synthetic ionotropic catecholamine commonly used to treat heart failure and shock. The catabolic fate of dobutamine in humans has yet to be reported, although formation of 3-O-methyldobutamine represents the principal pathway of dobutamine disposition in the dog. Herein, we describe the isolation and identification of 3-O-methyldobutamine in the urine of children receiving infusions of racemic dobutamine. In a 9-year-old child with heart failure approximately 80% of dobutamine administered intravenously at steady state was detected in the urine. Forty-seven percent of infused dobutamine was identified as 3-O-methyldobutamine and its acid-hydrolyzed derivatives, the latter mostly conjugated with sulfate (33%). Thirty-two percent consisted of acid-hydrolyzed dobutamine metabolites, primarily conjugated with sulfate (16%). Sonicates of human blood mononuclear cells catalyzed the formation of 3-O-methyldobutamine from dobutamine and S-adenosylmethionine in vitro. These findings indicate that formation of 3-O-methyldobutamine constitutes a major pathway of dobutamine metabolism in humans.

Published
2002

139. Pemoline ingestion in children: a report of five cases and review of the literature

Author

Michael D. Reed, Jeffrey L. Blumer, and Hidefumi Nakamura

Subjects
Male, Adolescent, medicine.drug_class, Sinus tachycardia, medicine.medical_treatment, Pemoline, Poison control, Hyperkinesis, Irritability, Benzodiazepines, Tachycardia, medicine, Ingestion, Humans, Pharmacology (medical), Gastric Lavage, Pharmacology, Benzodiazepine, business.industry, Infant, medicine.disease, Gastric lavage, Anesthesia, Charcoal, Child, Preschool, Hypertension, Central Nervous System Stimulants, Female, medicine.symptom, Drug Overdose, business, Rhabdomyolysis, medicine.drug
Abstract

The authors describe five pediatric cases of excessive pemoline ingestion. Based on their experience compared with previously reported cases in the literature, they describe the clinical presentation and rational treatment recommendations for acute pemoline ingestion. Overall, patients experienced a relatively benign clinical course following pemoline ingestion. Symptoms of pemoline ingestion appear to be primarily an accentuation of the drug's pharmacological effects on the central nervous and cardiovascular systems with sinus tachycardia, hypertension, hyperactivity, choreoathetoid movements, and hallucinations being most commonly observed. These findings are consistent with previously reported cases. Possible rhabdomyolysis manifested by evaluation of serum CPK was also observed in 3 of 4 patients in whom this laboratory parameter was measured and appears to be a common finding in acute pemoline poisoning. After acute ingestion, symptoms occurred within 6 hours, lasting up to 48 hours in all patients. Gastric lavage and/or activated charcoal would be effective decontamination measures, whereas ipecac-induced emesis should be avoided after massive ingestion due to the possibility of seizures. Aggressive use of a benzodiazepine appears a reasonable first choice to treat associated involuntary movements, tremor, hyperactivity, irritability, and agitation. Phenothiazines or butyrophenones may also be used especially for serious life-threatening symptoms, including hypertensive crisis and severe hyperthermia, although these serious complications of stimulant overdose have not been reported after pemoline ingestion. If a patient should experience pemoline-induced hypertensive crisis, individual dose titration of labetalol or sodium nitroprusside would appear reasonable pharmacologic approaches for rapid stabilization of blood pressure.

Published
2002

140. Nosocomial acquisition and transmission of antibiotic-resistant gram-negative organisms in the pediatric intensive care unit

Author

Jeffrey L. Blumer and Philip Toltzis

Subjects
Microbiology (medical), medicine.medical_specialty, medicine.drug_class, Antibiotics, Drug resistance, Intensive Care Units, Pediatric, law.invention, Antibiotic resistance, law, medicine, Humans, Intensive care medicine, Gram, Antibacterial agent, Pediatric intensive care unit, Cross Infection, Infection Control, business.industry, Drug Resistance, Microbial, Intensive care unit, Anti-Bacterial Agents, Infectious Diseases, Transmission (mechanics), Pediatrics, Perinatology and Child Health, business, Gram-Negative Bacterial Infections
Published
2001

141. The pharmacokinetics of colistin in patients with cystic fibrosis

Author

Michael D. Reed, Robert C. Stern, Jeffrey L. Blumer, and Mary Ann O'Riordan

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, Cystic Fibrosis, medicine.drug_class, Antibiotics, Cystic fibrosis, Nephrotoxicity, Pharmacokinetics, Medicine, Humans, Pharmacology (medical), Adverse effect, Child, Antibacterial agent, Pharmacology, Volume of distribution, business.industry, Colistin, Middle Aged, medicine.disease, Surgery, Anti-Bacterial Agents, Anesthesia, lipids (amino acids, peptides, and proteins), Female, business, medicine.drug
Abstract

The safety and pharmacokinetics of colistin were determined after first dose (n = 30) and again under steady-state conditions (n = 27) in 31 patients with cystic fibrosis receiving the drug as a component of their treatment for an acute pulmonary exacerbation of their disease. Patients ranged in age from 14 to 53 years and received colistin for 6 to 35 days. Each patient was started on colistin 5 to 7 mg/kg/day administered intravenously in three equally divided doses. Elimination half-life (t1/2), mean residence time (MRT), steady-state volume of distribution (Vdss), total body clearance (Cl), and renal clearance (Clr) after first-dose administration averaged 3.4 hours, 4.4 hours, 0.09 l/kg, and 0.35 and 0.24 ml/min/kg, respectively. No differences in colistin disposition characteristics between first-dose and steady-state evaluations were observed. Sputum sampling was incomplete and confounded by previous aerosol administration but revealed colistin concentrations that markedly exceeded observed plasma concentrations. Twenty-one patients experienced one or more side effects attributed to colistin administration. The most common reactions involved reversible neurologic manifestations, including oral and perioral paresthesias (n = 16), headache (n = 5), and lower limb weakness (n = 5). All of these apparent colistin-induced neurologic adverse effects, though bothersome, were benign and reversible. Intermittent proteinuria was observed on urinalysis in 14 patients, and 1 patient developed reversible, colistin-induced nephrotoxicity. No relationship between the occurrence of any colistin-associated adverse effect and plasma colistin concentration or colistin pharmacokinetic parameter estimate was observed. These data provide no basis for routine monitoring of colistin plasma concentrations to guide dosing for patient safety and suggest slow upward dose titration to minimize the incidence and severity of associated side effects.

Published
2001

142. Safety of antihistamines in children

Author

Michael D. Reed, Jeffrey L. Blumer, and Andrew P. Ten Eick

Subjects
Adult, Ebastine, medicine.medical_treatment, Sedation, Cobra Cardiotoxin Proteins, Loratadine, Toxicology, Torsades de Pointes, medicine, Potassium Channel Blockers, Humans, Pharmacology (medical), Terfenadine, Child, Pharmacology, Fexofenadine, business.industry, Learning Disabilities, Infant, Arrhythmias, Cardiac, History, Medieval, Astemizole, Anesthesia, Histamine H1 Antagonists, Antihistamine, Sleep Stages, medicine.symptom, Drug Overdose, business, Algorithms, medicine.drug, Mizolastine
Abstract

The histamine H1 receptor antagonists (antihistamines) are an important class of medications used for the relief of common symptoms associated with hyperhistaminic conditions occurring in children and adults. This group of drugs may be subdivided into 3 classes, or generations, based upon their propensity to induce sedation and cardiotoxicity. The first generation (classical) antihistamines are highly effective in treating hyperhistaminic conditions. However, they frequently induce sedation and may adversely affect a child’s learning ability. First generation antihistamine—induced sedation has been described to occur in more than 50% of patients receiving therapeutic dosages. Serious adverse events are unusual following overdoses of first generation antihistamines although life-threatening adverse events have been described. When the so-called ‘second generation’ antihistamines terfenadine and astemizole were introduced they were widely embraced and quickly used by clinicians of all specialities, including paediatricians, as nonsedating alternatives to the first generation compounds. These new agents were found to be equally or more effective than first generation antihistamines in relieving symptoms associated with hyperhistaminic conditions without the soporific effects of the first generation agents. Unfortunately, after approximately 10 years of widespread clinical use, disturbing reports of potentially life-threatening dysrhythmias, specifically torsades de pointes, were described. Both terfenadine and astemizole have been shown in vitro to inhibit several ion channels, and in particular the delayed outward rectifier potassium channel in the myocardium, predisposing the heart to dysrhythmias. The potential life-threatening cardiotoxicities of the second generation antihistamines led to the search for noncardiotoxic and nonsedating agents. Loratadine, fexofenadine, mizolastine, ebastine, azelastine and cetirizine are the first of the new third generation antihistamines. These drugs have been shown to be efficacious with few adverse events including no clinically relevant cytochrome P450 mediated metabolic—based drug-drug interactions or QT interval prolongation/cardiac dysrhythmias. Appropriate treatment of an antihistamine overdose depends upon which class of compound has been ingested. There is no specific antidote for antihistamine overdose and treatment is supportive particularly for ingestions of first generation compounds. Ingestion of excessive doses of terfenadine or astemizole requires immediate medical attention. Children who accidentally ingest excessive doses of a third generation compound may usually be adequately managed at home. However, patients ingesting large amounts (approximately >3 to 4 times the normal therapeutic daily dose) should receive medical attention. These patients should be monitored for 2 to 3 hours after the ingestion and patients ingesting cetirizine should be advised about the potential for sedation. The availability of newer generation antihistamine compounds has clearly added to the clinical effectiveness and patient tolerance of a widely prescribed class of drugs. These advances have also been accompanied by improved safety profiles, particularly in the case of third generation antihistamine overdose.

Published
2001

143. Randomized, double-blind, multicenter trial comparing clinafloxacin with imipenem as empirical monotherapy for febrile granulocytopenic patients

Author

Ronald Feld, Ruth Horn, Roy A. Beveridge, Hillard M. Lazarus, Anthony W. Chow, Jeffrey L. Blumer, James W. Hathorn, Mary C. Territo, Thomas J. Louie, Kenneth J. Tack, Rasim Gucalp, Reuben Ramphal, Winston G. Ho, and Drew J. Winston

Subjects
Microbiology (medical), Adult, Male, medicine.medical_specialty, Imipenem, Canada, Adolescent, medicine.drug_class, Nausea, Antibiotics, Microbial Sensitivity Tests, Neutropenia, Gastroenterology, chemistry.chemical_compound, Anti-Infective Agents, Double-Blind Method, Internal medicine, Multicenter trial, Medicine, Humans, Antibacterial agent, Aged, Aged, 80 and over, business.industry, Middle Aged, medicine.disease, Rash, United States, Surgery, Blood Cell Count, Infectious Diseases, Treatment Outcome, chemistry, Female, Thienamycins, medicine.symptom, Clinafloxacin, business, medicine.drug, Agranulocytosis, Fluoroquinolones
Abstract

In a double-blind, multicenter trial, 541 febrile granulocytopenic patients were randomized to receive either intravenous (iv) clinafloxacin (200 mg every 12 h) or i.v. imipenem (500 mg every 6 h) as empirical monotherapy. More baseline pathogens were susceptible to clinafloxacin (259 [99%] of 262 organisms) than to imipenem (253 [95%] of 265; P=.03). Initial favorable clinical response rates for clinafloxacin (88 [32%] of 272 patients) and imipenem (89 [33%] of 269) were similar. After addition of other antimicrobial agents, overall response rates were 259 (95%) of 272 for clinafloxacin and 251 (93%) of 269 for imipenem. During the study, only 13 clinafloxacin (5%) and 18 imipenem (7%) recipients died. Both drugs were generally well tolerated. Drug-related skin rash occurred more often with clinafloxacin (11% vs. 6%; P=.07), whereas nausea (2% vs. 5%; P=.16), Clostridium-difficile-associated diarrhea (3% vs. 8%; P=.02), and seizures (0% vs. 2%; P=.06) occurred more often with imipenem. These results suggest that clinafloxacin and imipenem have similar efficacy as empirical monotherapy in febrile granulocytopenic patients.

Published
2001

144. Early Weight Gain in Adolescents on Depot Medroxyprogesterone Acetate: Have We Been Ignoring a Biologic Mechanism?

Author

Barbara A. Cromer, Andrea Bonny, Mary Ann O'Riordan, Jeffrey L. Blumer, Michael D. Reed, Sam Mesiano, and Bram R. Kaufman

Subjects
medicine.medical_specialty, Mechanism (biology), business.industry, Depot, Obstetrics and Gynecology, General Medicine, Endocrinology, Internal medicine, Pediatrics, Perinatology and Child Health, medicine, Medroxyprogesterone acetate, medicine.symptom, business, Weight gain, medicine.drug
Published
2010
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145. Pharmacology of inotropic agents in infants and children

Author

Jeffrey L. Blumer, Samir Latifi, and Karen Lidsky

Subjects
Inotrope, Lusitropy, Digoxin, business.industry, Pharmacology, Amrinone, Therapeutic index, Pharmacokinetics, Pharmacodynamics, Pediatrics, Perinatology and Child Health, Medicine, Milrinone, Cardiology and Cardiovascular Medicine, business, medicine.drug
Abstract

Inotropic agents are drugs which increase the stroke work of the heart at a given pre-load and after-load. All of these agents work through a final common pathway involving the modulation of calcium interactions with various myocardial contractile proteins. The agents employed with pediatric patients include the cardial glycosides, catecholamine β-agonists and the selective phosphodiesterase III inhibitors. Digoxin is the prototypic cardiac glycoside which has a long history of safe and effective use in infants and children. Its utility in improving right ventricular dysfunction in patients with cor pulmonale leading to biventricular dysfunction makes it ideally suited to the pediatric population. Monitoring digoxin pharmacokinetics in infants is confounded by the presence of an endogenous digoxin-like substance. Nevertheless, the drug is well suited for subacute and chronic myocardial support. In contrast, the catecholamines are the drugs of choice for acute intervention. Their pharmacokinetics permit rapid dosing titration. In infants and children the greatest experience has been accrued with dopamine, a mixed α- and β-agonist but both epinephreine and norepinephrine are being used with increasing frequency as the need for drugs with increased potency and pressor activity becomes more common. The phosphodiesterase inhibitors amrinone and milrinone are the newest additions to our therapeutic armamentarium. In addition to their modest inotropic effects, amrinone and to a greater extent, milrinone offer significant pulmonary vasodilatation as part of their therapeutic package. These effects occur with little or any impact on myocardial oxygen consumpton while their lusitropic effects enhance relaxation in hypertrophied ventricular muscle. Of the two agents milrinone is probably preferred due to its greater therapeutic index and shorter elimination half-life. All of these agents remain important tools in the care of critically ill infants and children. The rational use of these drugs based upon their pharmacokinetic and pharmacodynamic properties is essential to achieve their optimal effects.

Published
2000

146. Prognostic markers in sepsis: the role of leukotrienes

Author

Jeffrey L. Blumer and Michael R. Anderson

Subjects
Leukotriene C4, Critical Care, business.industry, Inflammation, Critical Care and Intensive Care Medicine, medicine.disease, Prognosis, Shock, Septic, Predictive factor, Sepsis, Survival Rate, chemistry.chemical_compound, Text mining, chemistry, Shock (circulatory), Immunology, medicine, Immune Tolerance, Leukocytes, Humans, medicine.symptom, business, Biomarkers
Published
2000

147. A double-blind pilot study of risperidone in the treatment of conduct disorder

Author

Nora K. McNamara, Robert L. Findling, Mark D. Schluchter, Jeffrey L. Blumer, Lisa A. Branicky, and Eloise Lemon

Subjects
Conduct Disorder, Male, medicine.medical_specialty, Pediatrics, Adolescent, medicine.medical_treatment, Pilot Projects, Placebo, Double blind, Double-Blind Method, Developmental and Educational Psychology, medicine, Humans, Antipsychotic, Psychiatry, Child, Morning, Psychiatric Status Rating Scales, Risperidone, Dose-Response Relationship, Drug, Dopamine antagonist, medicine.disease, Aggression, Psychiatry and Mental health, Treatment Outcome, El Niño, Conduct disorder, Female, Psychology, medicine.drug, Antipsychotic Agents
Abstract

Objective To examine whether risperidone is superior to placebo in the treatment of youths with conduct disorder. Method This was a 10-week, randomized, double-blind, placebo-controlled study with 2 parallel arms. Ten youths were randomly assigned to receive placebo and 10 youths were randomly assigned to receive risperidone. Patients were seen weekly throughout the trial. Medications could be increased at weekly intervals during the first 6 weeks of the study from an initial dose of 0.25 mg or 0.50 mg each morning, depending on patient weight. Patients weighing less than 50 kg had a maximum total daily dose of risperidone of 1.5 mg. Patients weighing 50 kg or greater had a maximum total daily dose of risperidone of 3.0 mg. The primary outcome measure was the Rating of Aggression Against People and/or Property Scale. Results Risperidone was superior to placebo in ameliorating aggression on most measures. Risperidone was reasonably well tolerated, with none of the risperidone-treated patients developing extrapyramidal side effects. Conclusions These data provide preliminary evidence that risperidone may have efficacy in the treatment of youths with conduct disorder. Because of the small sample size and the brief length of this study, further research is necessary to confirm these findings.

Published
2000

148. Acute encephalopathy due to aluminum toxicity successfully treated by combined intravenous deferoxamine and hemodialysis

Author

Jeffrey L. Blumer, Peter G. Rose, Michael D. Reed, and Hidefumi Nakamura

Subjects
medicine.medical_specialty, medicine.medical_treatment, Encephalopathy, Acute encephalopathy, Deferoxamine, complex mixtures, Bladder Irrigation, Injections, Intramuscular, Pharmacokinetics, Renal Dialysis, Medicine, Humans, Pharmacology (medical), Aged, Pharmacology, Aged, 80 and over, Chemotherapy, business.industry, Delirium, medicine.disease, Surgery, Toxicity, Acute Disease, Injections, Intravenous, Alum Compounds, Female, Hemodialysis, business, medicine.drug
Abstract

Acute aluminum intoxication is uncommon in clinical practice but can be fatal. This limited experience is reflected in the paucity of data assessing a viable approach to the treatment of these patients. In this report, the authors describe the clinical course and successful, pharmacokinetic-based deferoxamine-hemodialysis treatment regimen of a patient with severe aluminum encephalopathy following alum bladder irrigation. The combined use of deferoxamine and appropriately timed hemodialysis appears to be a very reasonable means of treating patients with severe acute aluminum intoxication.

Published
2000

149. Pharmacokinetics and safety of meropenem in young infants with intra-abdominal infections

Author

Michael Cohen-Wolkowiez, Robert L. Schelonka, Robert M. Ward, Varsh Bhatt-Mehta, Neil Finer, Lisa Castro, John N. van den Anker, William MacKendrick, Brian Smith, Daniel K. Benjamin, Edmund V. Capparelli, Antonio Arrieta, Margarita Bidegain, Kelly C. Wade, William W. Hope, Jeffrey L. Blumer, and Gloria B. Valencia

Subjects
Volume of distribution, medicine.medical_specialty, education.field_of_study, business.industry, Population, Obstetrics and Gynecology, Gestational age, Gastroenterology, Meropenem, Surgery, NONMEM, Pharmacokinetics, Internal medicine, Pediatrics, Perinatology and Child Health, medicine, Dosing, education, Adverse effect, business, medicine.drug
Abstract

Background: Meropenem is approved for treatment of complicated abdominal infections in pediatric patients and adults. The primary objective of this study is to characterize meropenem multiple-dose PK and preliminary safety in young infants. Design and population: Infants Material and methods: Population and individual subject (Bayesian) PK parameters were estimated using NONMEM. Results: Data including 99 meropenem concentrations on the first 22 infants enrolled are presented. Dosing was based on both gestational age and postnatal age: 3 infants received 20 mg/kg q12 h, 13 received 20 mg/kg q8 h, 1 received 30 mg/kg q8 h, and 1 received 40 mg/kg q8 h. Median gestational age at birth and post-natal age were 27 weeks and 18 days, respectively. Median plasma clearance (CL), volume of distribution, and elimination T½ were 0.12 L/kg/h, 0.54 L/kg, and 2.9 h, respectively. A significant, positive association was observed between CL and postconceptional age. All infants had predicted meropenem concentrations above an MIC of 2 µg/mL for > 75% of the dosing interval. No serious adverse events related to meropenem were observed. Conclusions: Meropenem doses of 20 mg/kg q12 h to 40 mg/kg q8 h were well tolerated and produced drug plasma concentrations above an MIC that inhibits most susceptible pathogens.

Published
2009
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150. Fundamental basis for rational therapeutics in acute otitis media

Author

Jeffrey L. Blumer

Subjects
Microbiology (medical), medicine.medical_specialty, business.industry, Acute otitis media, Middle ear disease, Drug Resistance, Microbial, Surgery, Anti-Bacterial Agents, Otitis Media, Infectious Diseases, Pediatrics, Perinatology and Child Health, Acute Disease, medicine, Humans, Intensive care medicine, business, Child
Published
1999

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