Do Difficulties In Swallowing Medication Impede The Use Of Hydroxyurea In Children?

Abstract Introduction Barriers to hydroxyurea (HU) use exist for children with sickle cell disease (SCD). Anecdotally, some parents report that their children struggle to swallow HU capsules. We hypothesized that difficulties in swallowing capsules and other forms of daily medication may be a barrier to pediatric HU use. Methods A self-administered survey of parents of children with SCD ages 5-17 years was conducted in pediatric SCD clinics at four different sites (see author affiliations). Parents submitted one survey for each eligible child. We assessed views on their child's medication regimen, including HU; how medications were swallowed; whether swallowing difficulties were perceived as barriers to medication adherence and whether children taking HU had fewer difficulties taking medication. Respondents were grouped by whether children were on HU therapy. Data were analyzed using descriptive statistics, chi square and Fisher exact tests. Results A total of 122 adults completed the survey, with 27-35 surveys obtained from each site. Of survey respondents, 98% were parents and 95% reported being the child's primary caregiver. Half of all children were ages 8-13 years, and 23% were 7 or younger. Groups were evenly divided by whether children were taking HU (n=61 in both groups). There were no significant differences between groups regarding parent or child age, number of children living in the home or choice of the Spanish version of the survey. Parents of children in the group taking HU had a higher level of education (p=0.04). We found 24% of all parents thought that swallowing medications was “hard to do”. Most (85%) parents reported that swallowing difficulties did not preclude daily medication use, with no differences by HU use. All (98%) children could swallow liquid medication, with two thirds reported as able to do so by age 1. In contrast, 76% of children could swallow pills, with 40% able to do so by age 4. No differences by HU use were found in overall ability or age to swallow pills, although more in the HU group could swallow large pills (78.4 vs. 54.2%, p=0.03). No differences between groups were found in ability to swallow capsules. Across all age groups, 26.5% of children could not swallow capsules. Only 20% of all children could swallow capsules by age 4. Of children taking HU, 71.4% used the capsule form. Only 17% of those children open the capsules to mix with a liquid or soft food to aid in swallowing. Few (11%) children in both groups had received training for medication swallowing; most of their parents perceived the training as helpful to their child. While 96% of the children were prescribed medication, children taking HU were more likely than the others to be taking any medication (100 vs. 85%, p=0.001), and twice as likely to take medication on a daily basis (98.4 vs. 51.6%, p=0.001). Parents of children taking HU more often reported that their children took multiple medications (<0.001), including more pills daily (p=0.02). Children on HU had a medication regimen of more than once daily (61.7 vs. 28.6%, p<0.001). Conclusions Based on self-report, the majority of parents of children with SCD did not view medication swallowing as an impediment to daily use of medications, including HU. Children in the HU group reported less difficulty swallowing large pills, but were not different in their ability to ingest capsules, small pills or liquid medication. These data suggest that difficulty swallowing medication is not a barrier to HU use for most children. Nonetheless, a substantial proportion of children ages 5-17 cannot swallow capsules; children under 5 are especially challenged. Therefore, coaching for swallowing to improve HU uptake could be targeted to the modest proportion of children who need assistance. Moreover, a reliable source of liquid HU is still needed for children who cannot swallow capsules. Our findings also suggest that HU use is more likely in families committed to daily medication use and more complex medication schedules, or for children with medical needs requiring therapy beyond once daily HU. Clinicians should continue to educate families about the benefits of HU and address potential impediments such as swallowing HU capsules and complex medication regimens. This study received support from NIH 1R21NR013745 (Green and Smaldone, PIs). Disclosures: Off Label Use: Hydroxyurea for treating children with sickle cell disease is off-label use.

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Comparison of the Safety Profile of Sickle Cell Disease Patients Treated with Hydroxycarbamide in Off-Label Versus in-Label Prescriptions in the Escort-HU Non Interventional, Prospective, Observational Open-Label Cohort Study

Blood ◽

10.1182/blood.v128.22.2497.2497 ◽

2016 ◽

Vol 128 (22) ◽

pp. 2497-2497

Author(s):

Ersi Voskaridou ◽

Stephan Lobitz ◽

Uwe Kordes ◽

Regine Grosse ◽

Valentine Brousse ◽

...

Keyword(s):

Immune System ◽

Sickle Cell Disease ◽

Sickle Cell ◽

Safety Profile ◽

Research Funding ◽

Therapeutic Indication ◽

Off Label Use ◽

Cell Disease ◽

Off Label ◽

Label Use

Abstract ESCORT-HU (European Sickle Cell Disease (SCD) COhoRT - HydroxyUrea) is a multicenter prospective non interventional study implemented in Europe, following the European Medical Agency's request to collect more information focused on long-term safety profile of hydroxycarbamide (HU) in SCD patients treated with HU. Primary endpoint of the study is to determine the frequency of adverse events (AEs) under HU treatment Secondary endpoints include the efficacy of HU in labeled indications (prevention of vaso-occlusive complications and of acute thoracic syndrome), frequency of hospitalizations due to SCD events and frequency of blood transfusions. Data collection on the reason for HU initiation permitted to identify in-label (in the therapeutic indication of the European marketing authorization, group 1, G1) and off-label (other therapeutic indication, group 2, G2) prescriptions of HU. Frequency of AEs (including not related to SCD and infections) was compared between adults and children, both in G1 and G2, with focus on the following subclasses: blood and lymphatic system disorders, fever, gastrointestinal disorders, infection, nervous system disorders, skin and subcutaneous tissue disorders and others. As of 6th June 2016 (cut-off date), a cohort of 1047 sickle cell patients have been enrolled in 3 European countries (Greece, 11.4%, Germany, 13.4%, and France, 75.2%). Of the 1047 patients, 845 (80.7%) have an in-label prescription (478 adults and 367 children), 170 (16.2%) an off-label prescription (61 adults and 109 children), and 32 reported unknown or no indication (Table 1a). As usually observed in any disease, the off-label use is more frequent in children compared to adults (p=0.01). Main reasons for off-label prescription were anemia (31%) (n=9 in adults and n=44 in children), abnormal Transcranial Doppler (TCD) values/cerebral vasculopathy (15%) (n=2 in adults and n=24 in children) and sickle cell organopathy including renal impairment (15%) (n=14 in adults and n=12 in children) (Table 1b). These three indications follow recommendations issued by European clinicians and are in accordance with the last version of US guidelines (JAMA 2014). Mean HU daily doses at initiation were respectively 18 mg/kg (G1) and 17.3 mg/kg (G2) in children, and 16.2 mg/kg (G1) and 13.5 mg/kg (G2) in adults. Not SCD-related AEs were respectively reported in 25% and 27.6% of patients in G1 and G2 groups (Table 2a). Focusing on the number of not-SCD related AE reported in each group, 355 AE have been reported in 211 patients in G1 and 73 AE have been reported in 47 patients in G2. Within G1 group, more AEs were reported in adults (30.8%) vs. children (17.4%) (p < 0.01) (Table 2b) but not in G2 group (NS) (Table 2c). When compared by AE type in G1, significant differences appeared between children and adults for the following AE subclasses (p < 0.01): infections more frequent in children as usually observed, renal & urinary disorders, immune system disorders more common in adults. Regarding neoplasms benign, immune system disorders, no malignancy has been reported, but mainly cysts (1 ovary, 2 breast), 1 renal tumor and 1 cutaneous lesion (histological types not provided), 1 other (location not reported) (Table 3). All AEs were more frequent in adults except infections. In conclusion, the current ESCORT-HU data confirm the more frequent off-label use of HU in children, a similar frequency of patients reporting not SCD-related AE between the in-label and off-label groups despite a higher number of AE reported in the in-label group, and a significant difference between children and adults in frequency of AEs in the in-label group. Disclosures De Montalembert: Addmedica: Research Funding; Novartis: Research Funding, Speakers Bureau. Ribeil:Bluebirdbio: Consultancy; Addmedica: Research Funding.

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Pharmacological Induction of FOXO3 Is a Potential Treatment for Sickle Cell Disease

Blood ◽

10.1182/blood.v126.23.282.282 ◽

2015 ◽

Vol 126 (23) ◽

pp. 282-282

Author(s):

Yankai Zhang ◽

Jacy R Crosby ◽

Eric Boerwinkle ◽

Betty Pace ◽

Vivien A. Sheehan

Keyword(s):

Sickle Cell Disease ◽

Sickle Cell ◽

Therapeutic Target ◽

Off Label Use ◽

Cell Disease ◽

Off Label ◽

Positive Regulator ◽

Hbf Induction ◽

Erythroid Maturation ◽

Label Use

Abstract Sickle cell disease (SCD) affects >100,000 Americans and millions more worldwide. Symptoms and sequelae of SCD can be ameliorated by increasing fetal hemoglobin (HbF, α2γ2) levels. Unfortunately, up to 50% of adult SCD patients treated with hydroxyurea, the only FDA-approved and widely used HbF inducer, do not have a clinically meaningful response to the drug. Additional oral HbF inducing agents, especially those that require less intense laboratory monitoring, are urgently needed. Development of such drugs has been stymied by an incomplete understanding of γ-globin regulation. We hypothesized that natural human genetic variation can be used to identify genes that may be drug targets for HbF induction. To test this hypothesis, we performed whole exome sequencing on 171 pediatric SCD patients to identify variants associated with endogenous HbF levels. Gene-based analysis identified seven unique non-synonymous variations in a Forkhead box O transcription factor, FOXO3, as significantly associated with lower HbF (p=5.6x10-4, β-value of log transformed (ln) HbF= -0.66). Two variants in the α2 subunit of AMPK, a FOXO3 activator, were also associated with reduced HbF (p=1.56x10-4, β-value ln%HbF=-1.5). We then performed functional studies to verify the association between FOXO3 and endogenous HbF levels in an ex vivo model of erythroid differentiation from CD34+ cells isolated from peripheral blood of normal human blood donors. Lentiviral short hairpin RNA (shRNA) knockdown of FOXO3 reduced γ-globin expression from 1 to 0.4, p= 0.0005. While γ-globin expression and protein levels were reduced by FOXO3 knockdown, β-globin levels remained unchanged. These results suggest that FOXO3 is a positive regulator of γ-globin. Morphologic and flow cytometry analysis of primary erythroid culture with and without FOXO3 knockdown indicates that knockdown of FOXO3 delays erythroid maturation, while reducing γ-globin production. We therefore conclude that FOXO3 appears to regulate γ-globin through a specific mechanism rather than through alteration of erythroid maturation kinetics. FOXO3 is a viable therapeutic target for the treatment of individuals with SCD as well as those with quantitative hemoglobinopathies like β-thalassemia, who do not benefit from hydroxyurea due to its delay of erythropoiesis. FOXO3 expression is known to be increased by three drugs, metformin, phenformin, and resveratrol. We found that these drugs also cause FOXO3 to accumulate in the nucleus, where it is active, rather than in the cytoplasm, where FOXO3 is degraded. We have investigated the effects of these agents on FOXO3 and γ-globin expression in K562 cells. Metformin, phenformin and resveratrol increased FOXO3 and γ-globin transcription levels in a dose-dependent manner. We then treated primary erythroid culture cells with a range of metformin doses (20-200µM), with and without a stable dose of 30 µM hydroxyurea. Alone, metformin had a modest effect (1.5 fold) on γ-globin induction at all concentrations. In combination with hydroxyurea, 50 µM metformin increased γ-globin expression 3.7-fold compared to 2.5-fold with hydroxyurea alone when analyzed by RT-qPCR. β-globin levels were unchanged by hydroxyurea or metformin. γ-globin induction persisted through terminal maturation of the culture when measured serially every 5 days. Taken together, our results indicate that not only is FOXO3 is a positive regulator of γ-globin expression, but it is an excellent therapeutic target for HbF induction. Metformin, a well-studied, well tolerated oral agent, will be investigated in combination with hydroxyurea in a phase II trial as an adjunctive agent to increase HbF induction. Disclosures Off Label Use: This presentation will discuss off-label use of metformin as a possible HbF inducing agent..

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Hydroxyurea Therapy Requires HbF Induction for Clinical Benefit in a Sickle Cell Mouse Model.

Blood ◽

10.1182/blood.v114.22.817.817 ◽

2009 ◽

Vol 114 (22) ◽

pp. 817-817

Author(s):

Jeffrey D. Lebensburger ◽

Tamara I Pestina ◽

Kelli Boyd ◽

Russell E. Ware ◽

Derek Persons

Keyword(s):

Gene Therapy ◽

Sickle Cell ◽

Pediatric Patients ◽

Organ Damage ◽

Off Label Use ◽

Cell Disease ◽

Off Label ◽

Cell Gene ◽

Stem Cell Gene ◽

Hydroxyurea Therapy

Abstract Abstract 817 PURPOSE: To evaluate whether there are clinical benefits from chronic hydroxyurea administration that are independent of HbF induction using a murine SCD model in which fetal hemoglobin (HbF) cannot be induced. METHODS: Cohorts of sex- and aged-matched SCD mice were generated by transplanting lethally irradiated C57/BL6 mice with bone marrow from BERK mice. Only mice fully engrafted with SCD hematopoiesis were used for study. Transplanted SCD mice were injected by intraperitoneal route five days per week. SCD mice with high levels of HbF were generated by stem cell gene transfer using a gamma-globin lentiviral vector followed by transplantation. RESULTS: We identified a dose of hydroxyurea (50 mg/kg) that would lead to a stable, well-tolerated reduction in neutrophil count, much like what is done to titrate dosage in human patients with SCD. Hydroxyurea dosed at 25 mg/kg produced no difference in blood counts compared to control mice, while 75 mg/kg and 100 mg/kg both produced critical pancytopenia. As expected, cellulose acetate gel electrophoresis and HPLC analysis showed that HbF was undetectable in both hydroxyurea-treated and saline-treated mice. Based on this dose-finding data, we treated SCD mice with 50 mg/kg hydroxyurea (n=20) and saline (n=13) five days/week for 20 weeks in order to determine whether chronic hydroxyurea therapy could improve both the anemia and organ damage of SCD. Blood counts obtained after 10 weeks again demonstrated a reduction in white blood cells (26.1 vs. 31.2 ×109/L, p<0.005), absolute neutrophil counts (2.9 vs. 4.6 ×109/L, p<0.005), platelets (780 vs 870 × 109/L, p<0.05), without improvement in the anemia (6.7 vs 6.6 g/dL). Consistent with this data, the serum LDH and total bilirubin values remained elevated, similar to control mice, suggesting no improvement in the rate of hemolysis. Necropsy and pathologic analyses of major organs were performed on six mice from each group after 18-20 weeks of hydroxyurea therapy. Hydroxyurea-treated mice showed no improvement in the severe, multi-organ damage, compared to saline-treated, control mice. In contrast, six SCD mice with high levels of HbF resulting from stem cell gene transfer but not treated with hydroxyurea had a significant correction of their anemia (10.8 g/dL) along with a reduction in both total white blood cell (11.7 ×109/L) and absolute neutrophil counts (2.6 × 109/L). The reduction in the neutrophil count secondary to the correction of the anemia by gene therapy was similar to the levels demonstrated with hydroxyurea administration (hydroxyurea ANC 2.9 × 109/L vs. gene therapy ANC 2.6 × 109/L). Importantly, the SCD mice with high HbF demonstrated no significant organ damage. CONCLUSIONS: Despite causing a significant reduction in the leukocytosis and thrombocytosis, hydroxyurea treatment did not improve the severe anemia and multi-organ disease pathology in SCD mice. In contrast, SCD mice with high levels of HbF resulting from stem cell gene therapy showed resolution of both the anemia and organ pathology. These data suggest that induction of HbF is a necessary and major contributor to the beneficial effects of hydroxyurea in SCD. Disclosures: Off Label Use: Hydroxyurea use in pediatric patients sickle cell disease. This abstract does not discuss the off label use of Hydroxyurea in pediatric patients with sickle cell disease. However, discussion of this abstract would likely result in referencing the off label use of hydroxyurea in pediatric patients with sickle cell disease.

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Medication Use in the Neonatal Intensive Care Unit: Current Patterns and Off-Label Use of Parenteral Medications

The Journal of Pediatrics ◽

10.1016/j.jpeds.2007.07.050 ◽

2008 ◽

Vol 152 (3) ◽

pp. 412-415.e1 ◽

Cited By ~ 56

Author(s):

Praveen Kumar ◽

Jennifer K. Walker ◽

Kristin M. Hurt ◽

Kimberly M. Bennett ◽

Neal Grosshans ◽

...

Keyword(s):

Intensive Care Unit ◽

Intensive Care ◽

Neonatal Intensive Care Unit ◽

Neonatal Intensive Care ◽

Medication Use ◽

Off Label Use ◽

Off Label ◽

Label Use

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The Importance of the Pharmacist’s Role and the Quality of Pharmacy Services in Nursing Home Care

Innovation in Aging ◽

10.1093/geroni/igab046.2099 ◽

2021 ◽

Vol 5 (Supplement_1) ◽

pp. 550-550

Author(s):

Geoffrey Joyce ◽

Seth Seabury ◽

Victoria Shier ◽

Neeraj Sood ◽

Yuna Bae-Shaaw

Keyword(s):

Fixed Effects ◽

Inappropriate Medication ◽

Medication Use ◽

Nursing Home Care ◽

Pharmacy Services ◽

Medication Regimen ◽

Rehospitalization Rate ◽

Off Label ◽

Facility Level

Abstract The Centers for Medicare & Medicaid Services requires nursing homes (NHs) to provide pharmacy services to ensure the safety of medication use, such as minimizing off-label medication use for residents with dementia. This study examined NH’s response to this requirement and its relationship to medication-related outcomes. The contemporaneous relationship between the quality of pharmacy services and outcome measures were modeled using facility-level longitudinal data from 2011-2017 and facility fixed-effects. The results revealed that deficiency in pharmacy services increased medication-related issues by: 11% in inappropriate medication regimen, 5% in medication error rate >5%, and 3% in any serious medication errors. Additionally, deficiency in pharmacy services was associated with small but statistically significant increases in antipsychotic use, residents with daily pain, number of hospitalizations and rehospitalization rate. The results suggest that pharmacy services have a direct and immediate impact on medication outcomes. The results underscore the importance of pharmacy services in NHs.

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More Rapid Delivery of Parenteral Analgesia By Adding Intranasal Fentanyl to the Management of Sickle Cell Disease Vaso-Occlusive Pain Episodes at a Pediatric Emergency Department

Blood ◽

10.1182/blood.v124.21.4083.4083 ◽

2014 ◽

Vol 124 (21) ◽

pp. 4083-4083

Author(s):

Bolanle T Akinsola ◽

Robert Hagbom ◽

April Zmitrovich ◽

Patricia Kavanagh ◽

Ashley Ashkouti ◽

...

Keyword(s):

Pain Score ◽

Admission Rate ◽

Parent Satisfaction ◽

Clinical Settings ◽

Off Label Use ◽

Cell Disease ◽

Off Label ◽

Admission Rates ◽

Pain Scores ◽

Historical Controls

Abstract Background: Vaso-occlusive episodes (VOE) are the leading cause of hospitalizations & emergency department (ED) visits in sickle cell disease (SCD), & are associated with increased mortality. Intranasal fentanyl (INF) provides rapid & powerful parenteral analgesia, with an onset of action of 5-10 minutes, & peak effect in 30 minutes. INF is a safe & effective method of pain management for children in the ED & other settings, yet it is underutilized in SCD. Objective: To study the impact of the addition of INF to standard ED management for SCD VOE on time to parenteral opioid, pain scores, ED length of stay (LOS) & admission rate. Methods: This quality improvement initiative was conducted at a tertiary pediatric ED at Children's Healthcare of Atlanta from November 2013-May 2014. Patients with all genotypes of SCD ages ≥2 years old who presented with VOE & pain score >6/10 were offered INF within 15 minutes of triage. 2 INF doses (1.5mcg/kg/dose; max 100mcg/dose) were given 5 minutes apart. Patients then continued on institutional standard protocol treatment for VOE (±PO hydrocodone, ±IV ketorolac, & ± IV morphine or IV hydromorphone). Pain scores were documented at frequent intervals by nursing staff. Patient/parent satisfaction data were obtained using a satisfaction questionnaire. Outcomes included: Time from arrival to 1st parenteral opioid, pain scores, ED LOS (time from arrival to disposition), admission rates & patient/parent satisfaction. We compared patients in this study to those who did not receive INF during the study period (n=48) & historical controls from Jan-Dec 2012 (n=231) for the 1st three outcomes. Results: 248 visits for VOE met inclusion criteria, of whom 228 received parenteral opioids (92%) & 180/228 (79 %) received INF. Mean age was 11.7±4.5 years. The majority were female (56%), 65% HbSS, 14% HbSC & 21% had other genotype. 48 patients did not receive INF; 36 were not offered INF without explanation for protocol deviation &12 patients refused. They had similar gender & Hb genotype, but were older than INF+ patients (13.5±4.0 years, p=0.01). The mean time from arrival to 1st parenteral opioid decreased significantly in the INF+ group compared to historical controls, and was remarkably shorter than those not treated with INF. There was minimal difference in LOS between INF+ group & historical controls, but LOS was shorter in the group that did not receive INF. Admission rates were significantly higher in those who did not receive INF when compared to those treated with INF & historical controls. (See Table 1) Table 1 INF+(n =180) INF-(n =48) Historical Data (n=231) P-value Time to 1st Parenteral Opioid (minutes) 29 ±15 77 ±44 35±18 p < 0.0001 LOS (minutes) 215± 86 197± 67 231±95 p = 0.028 Admission Rate (%) 48% 71% 45% p = 0.004 Mean baseline pain score was 8.5±1.5, 1st reassessment pain score after INF was 7.8±2.4 & last ED pain score prior to disposition was 5.5±3.4. Pain scores were similar in all groups. 98 families completed the patient satisfaction questionnaire, 79 (81%) of whom received INF. 65% of patients who received INF were satisfied & would like to receive the treatment again in the ED. Conclusions: The addition of INF to the management of SCD VOE significantly improved time to receipt of 1st parenteral analgesia & was well tolerated. Admission rates were significantly higher in patients who did not receive INF during our study period. The associated delay in time to receipt of 1st parenteral analgesia may have contributed to the increased admission rate. However, causality of INF on admission rates cannot be determined without further study. INF did not impact ED LOS compared to historical controls, however rapid admission turn-around time likely decreased LOS in the INF- group. INF is a safe & effective strategy to provide rapid pain relief in children with SCD & VOE. Disclosures Off Label Use: Intranasal Fentanyl (INF). Widely accepted as off label use in pediatric ED's and a variety of other clinical settings for the management of pain. It is a synthetic narcotic analgesic with a rapid onset and short duration of action. Current evidence suggests that INF is a safe and effective method of pain management for children in a variety of clinical settings..

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Optimism Predicting Daily Pain Medication Use in Adolescents with Sickle Cell Disease

Journal of Pain and Symptom Management ◽

10.1016/j.jpainsymman.2006.08.010 ◽

2007 ◽

Vol 33 (3) ◽

pp. 302-309 ◽

Cited By ~ 26

Author(s):

Laura Pence ◽

Cecelia R. Valrie ◽

Karen M. Gil ◽

Rupa Redding-Lallinger ◽

Charles Daeschner

Keyword(s):

Sickle Cell Disease ◽

Sickle Cell ◽

Medication Use ◽

Pain Medication ◽

Cell Disease ◽

Daily Pain

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Successful Use of Pegylated Carboxyhemoglobin Bovine As an Emergency Treatment for Severe Anemia in a Patient with Sickle Cell Disease and Hyperhemolysis: A Case Report

Blood ◽

10.1182/blood.v124.21.4928.4928 ◽

2014 ◽

Vol 124 (21) ◽

pp. 4928-4928 ◽

Cited By ~ 1

Author(s):

Candice M Nalley ◽

Abe Abuchowski ◽

Steven Hsu ◽

Sophie Lanzkron

Keyword(s):

Case Report ◽

Sickle Cell Disease ◽

Sickle Cell ◽

Emergency Treatment ◽

Investigational Drug ◽

Severe Anemia ◽

Oxygen Carriers ◽

Cell Disease ◽

Free Hemoglobin ◽

Once Daily

Abstract Introduction: Modern biotechnology has long sought the development of a safe and effective red cell alternative. For patients with sickle cell disease and alloimmunization who develop severe anemia, few treatments exist to improve oxygen-carrying capacity. PEGylated carboxyhemoglobin bovine (PEG-Hb) may offer a novel treatment modality in such situations. Here we describe the use of the investigational drug PEG-Hb as an emergency treatment for severe anemia in a patient with sickle cell anemia (HbSS) who developed life-threatening hyperhemolysis following packed red blood cell transfusion. Case Report: A 28-year-old female with HbSS, not on hydroxyurea therapy, with complications including alloimmunization, multiple past episodes of acute chest syndrome, and avascular necrosis of the bilateral femoral heads, presented with severe pain in her back, legs, and hips, reported as the worst she had ever felt. Her urine was dark in color, and her hemoglobin dropped from 7 to 4.7 g/dL within 12 hours of presentation. She was diagnosed with acute hyperhemolysis following the transfusion of one unit of phenotypically matched red blood cells six days prior, with precipitated vaso-occlusive crisis. The patient received steroids and IVIG to mitigate the immune response, and erythropoietin or darbepoietin to stimulate erythropoiesis. It was felt that giving additional phenotypically matched red cells would lead to further hemolysis and bone marrow suppression. On hospital day 2, she developed a fever to 39.5 C and was tachycardic to 138 BPM. By hospital day 3, she was severely anemic with hemoglobin 3.5 g/dL, hematocrit 9.8%. On hospital day 5, she required 50% FiO2 to maintain her oxygen saturation above 95%. The patient’s absolute reticulocyte count dropped from 316k to 113.9k and nadired at 24.5K. Her ongoing hypoxemia, reticulocytopenia, and marked anemia were leading to severe tachycardia, fatigue, and depressed sensorium. To compensate for this severely symptomatic anemia, the investigational biologic PEGylated carboxyhemoglobin bovine (PEG-Hb) 40 mg/mL for intravenous infusion was requested from the manufacturer and granted under an emergency investigational new drug (IND) approval. By hospital day 6, following two once-daily infusions (500 mL each = approximately 400 mg/kg/dose) of PEG-Hb, the patient reported feeling well with no pain and no shortness of breath. Anemia remained severe (hemoglobin 2.5 g/dL, hematocrit 10%). Additional investigational drug was requested, and the patient received six additional once-daily 500 mL infusions of PEG-Hb with continued improvement in exertional ability and tachycardia, though with mild dyspnea upon exertion. No adverse effects were noted with the infusions; there were no changes in renal function or episodes of hypertension. The patient was discharged home on day 32 with a hemoglobin of 4.1 g/dL. Discussion: Hemoglobin-based oxygen carriers have, in general, met problems including increased mortality and myocardial infarctions when compared with controls (Natanson C et al. JAMA. 2008;299(19):2304). This is postulated to be due to systemic vasoconstriction secondary to the nitric-oxide scavenging properties of cell-free hemoglobin (Buehler PW, et al. Transfusion. 2004;44(10):1516). In patients with sickle cell disease who already have elevated levels of circulating free heme (Uzunova W, et al. Biophys J. Sep 22, 2010; 99(6): 1976–1985), the potential additional free hemoglobin contributed by hemoglobin-based oxygen carriers may not confer a significant increase in risk. For patients with sickle cell disease and severe anemia for whom transfusion is not an option, PEG-Hb may present a viable alternative to transfusion. This is the first reported case of the use of PEG-Hb in a patient with sickle cell disease and profound anemia from hyperhemolysis. This therapy is thought to have been lifesaving for this patient. Further research into the use of PEGylated carboxyhenoglobin bovine in patients with severe anemia secondary to sickle cell disease is warranted. Disclosures Off Label Use: Pegylated Carboxyhemoglobin Bovine was used to improve oxygen delivery. Abuchowski:Prolong Pharmaceuticals: Employment. Lanzkron:NHLBI: Research Funding.

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Medication-Use Evaluation of Recombinant Human Factor VIIa

Global Journal on Quality and Safety in Healthcare ◽

10.36401/jqsh-19-41 ◽

2020 ◽

Vol 3 (2) ◽

pp. 38-43 ◽

Cited By ~ 1

Author(s):

Abrar Al-Subhi ◽

Mansoor Ahmed Khan ◽

Mohammed A. Aseeri

Keyword(s):

Human Factor ◽

Hemophilia A ◽

Factor Viia ◽

Medication Use ◽

Off Label Use ◽

Off Label ◽

Medical City ◽

One Year ◽

The Cost ◽

Label Use

ABSTRACT Introduction Medication-use evaluation (MUE) is a performance improvement method used to achieve optimal patient outcomes. The recombinant human factor VIIa (rFVIIa) (NovoSeven) is an expensive agent approved by the U.S. Food and Drug Administration (FDA) for specific indications. However, in clinical practice, rFVIIa is often used for conditions unrelated to the one approved, with limited evidence. The use of rFVIIa has been associated with expenditures of more than Saudi riyal (SR)30 million ($8 million) annually at King Abdul-Aziz Medical City-Western Region (KAMC-WR). Therefore, we planned a MUE of rFVIIa. The primary purpose was to determine the off-label use of rFVIIa, and the secondary purpose was to evaluate the cost impact of off-label use of rFVIIa at KAMC-WR. Methods This was an observational retrospective cohort study conducted to assess the off-label usage pattern and the direct cost of rFVIIa for one year. Results A total of 27 patients who received rFVIIa were included. Two out of the 27 patients had hemophilia A with inhibitors (7%), and 23 of the 27 patients received rFVIIa with off-label indications (85%). The total cost associated with the use of rFVIIa was SR18.61 million ($4.96 million). The cost of the rFVIIa used for the appropriate purpose was SR17.83 million ($4.75 million), which represented 95.8% of the expenditures. Conclusions Recombinant FVIIa is one of the most expensive medications in our hospital. It has been used mostly in patients having hemophilia A with inhibitors.

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Off-label Medication Use in the NICU

Neonatal Network The Journal of Neonatal Nursing ◽

10.1891/0730-0832.29.4.253 ◽

2010 ◽

Vol 29 (4) ◽

pp. 253-255 ◽

Cited By ~ 2

Author(s):

Susan Givens Bell

Keyword(s):

Medication Use ◽

Pediatric Research ◽

Off Label Use ◽

Off Label ◽

Label Use

MANY INFANTS CARED FOR IN the NICU receive at least one drug that is used off label.1 This column explains what off-label use means, describes the Best Pharmaceuticals for Children Act and the Pediatric Research Equity Act, and discusses implications for practice.

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