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Start Over Author "Alina Sadaf" Publisher american society of hematology
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2. Pharmacokinetics of L-Glutamine (Endari) in Pediatric and Adult Sickle Cell Disease Patients: A Phase 4, Open-Label, Single-Center Study

Author

Amanda Pfeiffer, Charles T. Quinn, Teresa Latham, Russell E. Ware, Min Dong, Alina Sadaf, and Alexander A. Vinks

Subjects
business.industry, Immunology, Cell, Cell Biology, Hematology, Disease, Pharmacology, Single Center, Biochemistry, medicine.anatomical_structure, Pharmacokinetics, Phase (matter), L-glutamine, Medicine, Open label, business
Abstract

Introduction: L-glutamine (Endari ®, Emmaus Medical, Inc.) is an amino acid approved for the treatment of sickle cell disease (SCD) by the United States Food and Drug Association (FDA) after 2 clinical trials demonstrated a reduction in painful episodes and hospitalizations. L-glutamine has many roles, including de novo synthesis of intracellular glutathione that may protect sickle erythrocytes from oxidant injury. Despite its licensure, the pharmacokinetics (PK) of multi-dose oral L-glutamine for SCD have not been studied. Methods: We conducted a dose-escalation PK trial from January to June 2021 (NCT04684381) on 3 cohorts with 4 participants each: pediatric SCD patients (0 - 18 y, cohort 1), adult SCD patients (>18 y, cohort 2), and adult healthy volunteers (>18 y, cohort 3). There were 4 weekly study visits to assess 3 ascending dose levels (Figure 1). For each visit, participants arrived in the research clinic after an overnight fast. Plasma L-glutamine and other amino acid levels were obtained before and after oral L-glutamine doses at each visit and quantified by ion exchange chromatography. On study visit 1, a dose of 0.1 g/kg of L-glutamine was administered and amino acids were measured at 30±5, 60±10, 120±15, 180±15 and 240±20 minutes after the dose. The procedure was repeated in the afternoon after a standardized meal. On study visit 2, the dose was increased to 0.3 g/kg twice daily (approximate FDA-approved dosing). On study visit 3, a single oral dose of 0.6 g/kg (once daily dosing) was given for fasting PK levels, and on study visit 4 the 0.6 g/kg dose was given with a standardized meal. After the first 3 study visits, participants continued L-glutamine at the corresponding dose level at home and completed a daily phone survey to document adherence and adverse events. Results: Baseline characteristics are summarized in Table 1. Baseline L-glutamine levels similar across the three study cohorts (Table 1). One participant from cohort 1 withdrew during study visit 1 and was replaced. Another participant from cohort 2 was withdrawn due to hospitalization for severe anemia and was replaced. One participant from cohort 3 did not complete visit 4 due to dyspepsia. Non-compartmental PK analysis (NCA) was conducted using Phoenix WinNonlin® Professional Version 8.4 (Certara, NJ, US; Figure 2). After oral administration, L-glutamine plasma levels peaked (T max) at an average (mean ± SD) of 1.2 ± 0.9 hours. Compared to doses 0.1 g/kg and 0.3 g/kg, the T max was later for 0.6 g/kg (p The most common grade 2 adverse events were dyspepsia and headache (3 instances each). There was no significant elevation in ammonia levels, and plasma concentrations of the metabolite L-glutamate was similar to L-glutamine (Figure 2). Conclusions: This is the first multi-dose PK study of L-glutamine (Endari) for SCD. Daily dosing was overall well-tolerated, with rapid absorption of 0.1 and 0.3 g/kg doses and no drug accumulation. The highest 0.6 g/kg dose was limited by palatability and featured slower and saturable absorption, so further dose escalation is likely not feasible. Ongoing analyses include possible food-drug interactions and PK-pharmacodynamic (PK-PD) studies to identify salutary effects on erythrocytes. Our findings will help inform the proper dosing of L-glutamine for patients with SCD, and potentially permit individualized PK-guided dosing to maximize treatment benefits. This was an investigator-initiated trial funded by Emmaus Medical, Inc. Figure 1 Figure 1. Disclosures Sadaf: Emmaus Medical, Inc: Research Funding. Ware: Bristol Myers Squibb: Research Funding; Addmedica: Research Funding; Hemex Health: Research Funding; Nova Laboratories: Research Funding; Novartis: Other: DSMB Chair; Editas: Other: DSMB Chair. Quinn: Emmaus Medical: Research Funding; Novo Nordisk: Consultancy; Aruvant: Research Funding; Forma Therapeutics: Consultancy. OffLabel Disclosure: Endari (L-glutamine) is FDA approved for the treatment of Sickle Cell Disease at a dose of 0.3 g/kg. However, in our pharmacokinetic study we tested doses 0.1, 0.3 and 0.6 g/kg.

Published
2021
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3. Rapid and Automated Quantitation of Dense Red Blood Cells: A Robust Biomarker of Therapeutic Response to Early Initiation of Hydroxyurea in Young Children with Sickle Cell Anemia

Author

Alina Sadaf, Theodosia A. Kalfa, Russell E. Ware, Charles T. Quinn, Amanda Pfeiffer, Punam Malik, Jennifer Korpik, Patrick T. McGann, Mary Reynaud, and Omar Niss

Subjects
business.industry, Immunology, Cancer research, Medicine, Biomarker (medicine), Cell Biology, Hematology, business, medicine.disease, Biochemistry, Early initiation, Sickle cell anemia
Abstract

Introduction: Hydroxyurea has well-described clinical and laboratory benefits in sickle cell anemia (SCA). Traditionally, hemoglobin concentration (Hb) and fetal hemoglobin (HbF) are used to assess treatment response, but these aggregate parameters do not fully capture the range of erythrocyte abnormalities in SCA. Dense red blood cells (DRBCs) are defined as RBCs with density >1.11 g/mL as measured by density-gradient fractionation methods, which are tedious and require technical expertise. This subpopulation of dehydrated RBCs has been associated with increased SCA severity but has not been extensively studied in children. Here we describe the utility of rapid, automated DRBC quantitation and show that the percent of DRBCs (%DRBCs) is a robust biomarker of hydroxyurea response in children with SCA. Methods: The Therapeutic Response Evaluation and Adherence Trial (TREAT, NCT02286154) was a single-center prospective study that demonstrated individualized, pharmacokinetic (PK)-guided hydroxyurea dosing in young patients (mean age 12.1 months at initiation) results in robust and sustained HbF levels >30-40% for most adherent patients. The longitudinal follow-up phase of TREAT aims to comprehensively evaluate hematologic parameters and organ function to demonstrate the long-term benefits of this treatment strategy. During clinic visits (every 3-6 months), TREAT participants had complete blood counts (CBCs) with the ADVIA® 2120i system. This automated analyzer quantifies hyperchromic RBCs within seconds by directly measuring cell hemoglobin concentration, where DRBCs are known to correspond to RBCs with a measured MCHC >41 g/dL. Data were analyzed at baseline and after at least 6 months of hydroxyurea therapy (M≥6). α- and β-globin genotypes were determined for all patients. Results: Thirty-three TREAT participants had ADVIA data available for analysis (Table). All had homozygous SCA except one with sickle-β0-thalasemia; 17 (51.5%) were male. The median age at hydroxyurea initiation was 10.3 months (mean 26.1 months; range 6 months - 17 years). The median duration of hydroxyurea therapy was 27.7 months (mean 31.5). At baseline, median %DRBCs was 2.1%. Baseline %DRBCs were directly correlated with age at initiation of hydroxyurea (p=0.022) and inversely correlated with baseline HbF (p=0.001). After initiation of hydroxyurea (M≥6), there was a 47.6% reduction in %DRBCs (p=0.001). Median %DRBCs at M≥6 was directly correlated with absolute reticulocyte (ARC) (p=0.002), absolute neutrophil (ANC) (p=0.003) and platelet counts (p Conclusions: DRBCs can be rapidly quantified without the tedium of classical density-gradient fractionation methods using the automated ADVIA 2120i hematology analyzer, which directly measures hyperchromic RBCs. These data from TREAT demonstrate the feasibility of serial %DRBC measurements in clinical trials and clinical practice. TREAT participants had low baseline DRBCs compared to untreated adult SCA patients (reported mean ≈12%), reflecting the young age of these patients. Nevertheless, there was a significant decline in %DRBCs with treatment that correlated strongly with the known laboratory benefits of hydroxyurea. In conclusion, automated DRBC measurements are a robust biomarker that can be incorporated in a panel of laboratory measurements of response to hydroxyurea (and severity of SCA). A larger, multicenter study of PK-guided hydroxyurea therapy (HOPS, NCT03789591) is currently underway in 11 US sickle cell centers and will provide generalizable data on DRBC responses with optimal hydroxyurea therapy. Disclosures Malik: Aruvant Sciences, Forma Therapeutics, Inc.: Consultancy; Aruvant Sciences, CSL Behring: Patents & Royalties. Kalfa:Agios Pharmaceuticals, Inc: Consultancy, Research Funding; Forma Therapeutics, Inc: Research Funding.

Published
2020
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