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2. Thalassaemia in Sri Lanka: A molecular basis

Author

Fisher, CA, Premawardhena, A, De Silva, S, Perera, G, Lamabadasuriya, SP, Peto, TEA, Clegg, JB, Olivieri, NF, Weatherall, DJ, Old, JM, and Study, SLT

Published
2016

3. Diamond-Blackfan anemia: expansion of erythroid progenitors in vitro by IL-9, but exclusion of a significant pathogenetic role for the IL-9 gene and the hematopoietic gene cluster on chromosome 5q

Author

DIANZANI I, GARELLI E, CRESCENZIO N, TIMEUS F, MORI PG, VAROTTO S, BRANDALISE S, OLIVIERI NF, GABUTTI V, RAMENGHI U., NOBILI, Bruno, Dianzani, I, Garelli, E, Crescenzio, N, Timeus, F, Mori, Pg, Varotto, S, Nobili, Bruno, Brandalise, S, Olivieri, Nf, Gabutti, V, and Ramenghi, U.

Subjects
Male, Stem Cell Factor, Adolescent, Genetic Linkage, Interleukin-9, Chromosome Mapping, Infant, Hematopoietic Cell Growth Factors, Hematopoiesis, Fanconi Anemia, Chromosomes, Human, Pair 5, Humans, Female, Interleukin-3, Child, Erythropoietin, Microsatellite Repeats
Abstract

Diamond-Blackfan anemia (DBA) is a congenital pure red blood cell aplasia that often requires lifelong transfusional therapy. Autosomal dominant and recessive inheritance have both been reported, suggesting genetic heterogeneity, but most cases occur sporadically. The origin of impaired erythropoiesis is unknown. Several erythroid growth factors have been thought to have a role in the pathogenesis of DBA. However, there is neither molecular nor clinical evidence for the involvement of erythropoietin (EPO), its receptor, stem cell factor (SCF), or interleukin (IL)-3, even if the addition of SCF to IL-3 and EPO does significantly increase the growth of erythroid progenitors in in vitro cultures in most patients. In this work we evaluated the possible role of another early-acting erythroid growth factor, IL-9. We found that the addition of IL-9 to SCF, IL-3, and EPO further increases burst-forming unit-erythroid growth in in vitro cultures of those DBA patients who responded to SCF. To investigate the role of the IL-9 gene, we evaluated its segregation in 22 families with members who have DBA by using a polymorphic microsatellite located within its intron 4. Lod score analysis ruled out any statistically significant involvement of the IL-9 gene in the pathogenesis of DBA. Moreover, linkage analysis with 11 highly polymorphic markers spanning 5q31.1-q33.2 excluded this region, which is included in the major cluster of genes active in hematopoiesis of the human genome.

Published
1997

7. BETA-S HAPLOTYPES IN VARIOUS WORLD POPULATIONS

Author

ONER, C DIMOVSKI, AJ OLIVIERI, NF SCHILIRO, G and CODRINGTON, JF FATTOUM, S ADEKILE, AD ONER, R YUREGIR, GT ALTAY, C GURGEY, A GUPTA, RB JOGESSAR, VB and KITUNDU, MN LOUKOPOULOS, D TAMAGNINI, GP RIBEIRO, MLS and KUTLAR, F GU, LH LANCLOS, KD HUISMAN, THJ

Abstract

We have determined the beta(S) haplotypes in 709 patients with sickle cell anemia, 30 with SC disease, 91 with S-beta-thalassemia, and in 322 Hb S heterozygotes from different countries. The methodology concerned the detection of mutations in the promoter sequences of the (G)gamma- and (A)gamma-globin genes through dot blot analysis of amplified DNA with P-32-labeled probes, and an analysis of isolated Hb F by reversed phase high performance liquid chromatography to detect the presence of the (A)gamma(T) chain [(A)gamma-75 (E19) Ile –> Thr] that is characteristic for haplotype 17 (Cameroon). The results support previously published data obtained with conventional methodology that indicates that the beta(S) gene arose separately in different locations. The present methodology has the advantage of being relatively inexpensive and fast, allowing the collection of a vast body of data in a short period of time. It also offers the opportunity of identifying unusual beta(S) haplotypes that may be associated with a milder expression of the disease. The numerous blood samples obtained from many SS patients living in different countries made it possible to compare their hematological data. Such information is included (as average values) for 395 SS patients with haplotype 19/19, for 2 with haplotype 17/17, for 50 with haplotype 20/20, for 2 with haplotype 3/3, and for 37 with haplotype 31/31. Some information on haplotype characteristics of normal beta(A) chromosomes is also presented.

Published
1992

8. Identification of microdeletions spanning the Diamond-Blackfan anemia locus on 19q13 and evidence for genetic heterogeneity.

Author

Gustavsson, P, Garelli, E, Draptchinskaia, N, Ball, S, Willig, TN, Tentler, D, Dianzani, I, Punnett, HH, Shafer, FE, Cario, H, Ramenghi, U, Glomstein, A, Pfeiffer, RA, Goringe, A, Olivieri, NF, Smibert, E, Tchernia, G, Elinder, G, Dahl, N, Gustavsson, P, Garelli, E, Draptchinskaia, N, Ball, S, Willig, TN, Tentler, D, Dianzani, I, Punnett, HH, Shafer, FE, Cario, H, Ramenghi, U, Glomstein, A, Pfeiffer, RA, Goringe, A, Olivieri, NF, Smibert, E, Tchernia, G, Elinder, G, and Dahl, N

Published
1998

23. An alpha-globin gene initiation codon mutation in a black family with HbH disease

Author

Olivieri, NF, Chang, LS, Poon, AO, Michelson, AM, and Orkin, SH

Abstract

The molecular basis of hemoglobin H disease in a Black family of Canadian origin was investigated. Affected individuals had a combination of deletion and nondeletion alpha-thalassemia mutations on different chromosomes. Cloning and sequencing of the DNA of one member with the nondeletion form revealed a new thalassemia mutation, an A---- G substitution, in the initiation codon of the remaining alpha-globin gene of a rightward (-alpha 3.7) deletion chromosome. This mutation abolished an Ncol restriction site and therefore is detectable in genomic DNA by Southern blot analysis.

Published
1987
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25. Leg Ulcers: A Report in Patients with Hemoglobin E Beta Thalassemia and Review of the Literature in Severe Beta Thalassemia.

Author

Mehta V, Kirubarajan A, Sabouhanian A, Jayawardena SM, Chandrakumaran P, Thangavelu N, Cader R, Mettananda S, Bandara D, Khan S, Weatherall DJ, Allen A, Premawardhena AP, and Olivieri NF

Subjects
Humans, Wound Healing, Hemoglobin E, Leg Ulcer complications, Leg Ulcer therapy, Thalassemia complications, beta-Thalassemia complications, beta-Thalassemia therapy
Abstract

Background: Leg ulcers are a frequent complication in patients with the inherited hemoglobin disorders. In thalassemia, the literature is limited, and factors associated with the development of leg ulcers in hemoglobin E (HbE) beta thalassemia, the most common form of severe beta-thalassemia worldwide, have not previously been reported., Methods: We reviewed all available medical records of patients with HbE beta thalassemia to document the onset of leg ulcers at the 2 largest treatment centers in Sri Lanka. We reviewed the literature to identify studies reporting outcomes of interventions for ulcers in severe thalassemia., Results: Of a total of 255 actively registered patients with HbE thalassemia in the 2 centers, 196 patient charts were evaluable. A leg ulcer with a documented date of onset was recorded in 45 (22%) of 196 evaluable patients, aged (mean ± SEM) 22.2 ± 1.4 years. Most had been irregularly transfused; steady-state hemoglobin was 6.4 ± 0.2 g/dL. Treatment achieving healing in 17 patients included transfusions, antibiotics, oral zinc, wound toileting, and skin grafting., Conclusion: Leg ulcers may be more common in HbE beta thalassemia than in other forms of thalassemia. A systematic approach to treatment will be needed to document the prevalence and factors placing such patients at risk for leg ulcers. Controlled trials to evaluate the optimal treatment of this common complication are indicated., (© 2021 The Author(s). Published by S. Karger AG, Basel.)

Published
2022
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26. Survival and complications in patients with haemoglobin E thalassaemia in Sri Lanka: a prospective, longitudinal cohort study.

Author

Premawardhena AP, Ediriweera DS, Sabouhanian A, Allen A, Rees D, de Silva S, Perera W, Katugaha N, Arambepola M, Yamashita RC, Mettananda S, Jiffry N, Mehta V, Cader R, Bandara D, St Pierre T, Muraca G, Fisher C, Kirubarajan A, Khan S, Allen S, Lamabadusuriya SP, Weatherall DJ, and Olivieri NF

Subjects
Adolescent, Adult, Blood Transfusion statistics & numerical data, Chelation Therapy methods, Chelation Therapy statistics & numerical data, Child, Female, Ferritins blood, Hemoglobin E analysis, Hemoglobins, Humans, Kaplan-Meier Estimate, Longitudinal Studies, Male, Middle Aged, Proportional Hazards Models, Prospective Studies, Splenectomy statistics & numerical data, Sri Lanka epidemiology, Young Adult, beta-Thalassemia complications, beta-Thalassemia mortality
Abstract

Background: Worldwide, haemoglobin E β-thalassaemia is the most common genotype of severe β-thalassaemia. The paucity of long-term data for this form of thalassaemia makes evidence-based management challenging. We did a long-term observational study to define factors associated with survival and complications in patients with haemoglobin E thalassaemia., Methods: In this prospective, longitudinal cohort study, we included all patients with haemoglobin E thalassaemia who attended the National Thalassaemia Centre in Kurunegala, Sri Lanka, between Jan 1, 1997, and Dec 31, 2001. Patients were assessed up to three times a year. Approaches to blood transfusions, splenectomy, and chelation therapy shifted during this period. Survival rates between groups were evaluated using Kaplan-Meier survival function estimate curves and Cox proportional hazards models were used to identify risk factors for mortality., Findings: 109 patients (54 [50%] male; 55 [50%] female) were recruited and followed up for a median of 18 years (IQR 14-20). Median age at recruitment was 13 years (range 8-21). 32 (29%) patients died during follow-up. Median survival in all patients was 49 years (95% CI 45-not reached). Median survival was worse among male patients (hazard ratio [HR] 2·51, 95% CI 1·16-5·43), patients with a history of serious infections (adjusted HR 8·49, 2·90-24·84), and those with higher estimated body iron burdens as estimated by serum ferritin concentration (adjusted HR 1·03, 1·01-1·06 per 100 units). Splenectomy, while not associated with statistically significant increases in the risks of death or serious infections, ultimately did not eliminate a requirement for scheduled transfusions in 42 (58%) of 73 patients. Haemoglobin concentration less than or equal to 4·5 g/dL (vs concentration >4·5 g/dL), serum ferritin concentration more than 1300 μg/L (vs concentration ≤1300 μg/L), and liver iron concentration more than 5 mg/g dry weight of liver (vs concentration ≤5 mg/g) were associated with poorer survival., Interpretation: Patients with haemoglobin E thalassaemia often had complications and shortened survival compared with that reported in high-resource countries for thalassaemia major and for thalassaemia intermedia not involving an allele for haemoglobin E. Approaches to management in this disorder remain uncertain and prospective studies should evaluate if altered transfusion regimens, with improved control of body iron, can improve survival., Funding: Wellcome Trust, Medical Research Council, US March of Dimes, Anthony Cerami and Ann Dunne Foundation for World Health, and Hemoglobal., Competing Interests: Declaration of interests TSP reports a grant from Novartis, a discount on services and consultancy funds to his institution from Resonance Health, and patents issued to Resonance Health for experimental methods (US6605943 and US2004222792), outside the submitted work. All other authors declare no competing interests., (Copyright © 2022 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY-NC-ND 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published
2022
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27. Consequences to Patients, Clinicians, and Manufacturers When Very Serious Adverse Drug Reactions Are Identified (1997-2019): A Qualitative Analysis from the Southern Network on Adverse Reactions (SONAR).

Author

Lubaczewski CR, Olivieri NF, Hrushesky WR, and Bennett CL

Subjects
Humans, Drug-Related Side Effects and Adverse Reactions etiology
Abstract

Adverse drug/device reactions (ADRs) serious enough to lead to box warnings on drug labels or drug withdrawals occur in about one fifth of all new molecular entities., (© 2022. The Author(s), under exclusive license to Springer Nature Switzerland AG.)

Published
2022
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29. Single-center retrospective study of the effectiveness and toxicity of the oral iron chelating drugs deferiprone and deferasirox.

Author

Olivieri NF, Sabouhanian A, and Gallie BL

Subjects
Anemia, Diamond-Blackfan therapy, Blood Transfusion, Deferiprone administration & dosage, Deferiprone adverse effects, Female, Humans, Iron Overload etiology, Male, Retrospective Studies, beta-Thalassemia therapy, Administration, Oral, Deferasirox administration & dosage, Deferasirox adverse effects, Electronic Health Records, Iron Chelating Agents administration & dosage, Iron Chelating Agents adverse effects, Iron Overload drug therapy, Transfusion Reaction drug therapy
Abstract

Background: Iron overload, resulting from blood transfusions in patients with chronic anemias, has historically been controlled with regular deferoxamine, but its parenteral requirement encouraged studies of orally-active agents, including deferasirox and deferiprone. Deferasirox, licensed by the US Food and Drug Administration in 2005 based upon the results of randomized controlled trials, is now first-line therapy worldwide. In contrast, early investigator-initiated trials of deferiprone were prematurely terminated after investigators raised safety concerns. The FDA declined market approval of deferiprone; years later, it licensed the drug as "last resort" therapy, to be prescribed only if first-line drugs had failed. We undertook to evaluate the long-term effectiveness and toxicities of deferiprone and deferasirox in one transfusion clinic., Methods and Findings: Under an IRB-approved study, we retrospectively inspected the electronic medical records of consented iron-loaded patients managed between 2009 and 2015 at The University Health Network (UHN), Toronto. We compared changes in liver and heart iron, adverse effects and other outcomes, in patients treated with deferiprone or deferasirox., Results: Although deferiprone was unlicensed in Canada, one-third (n = 41) of locally-transfused patients had been switched from first-line, licensed therapies (deferoxamine or deferasirox) to regimens of unlicensed deferiprone. The primary endpoint of monitoring in iron overload, hepatic iron concentration (HIC), increased (worsened) during deferiprone monotherapy (mean 10±2-18±2 mg/g; p < 0.0003), exceeding the threshold for life-threatening complications (15 mg iron/g liver) in 50% patients. During deferasirox monotherapy, mean HIC decreased (improved) (11±1-6±1 mg/g; p < 0.0001). Follow-up HICs were significantly different following deferiprone and deferasirox monotherapies (p < 0.0000002). Addition of low-dose deferoxamine (<40 mg/kg/day) to deferiprone did not result in reductions of HIC to <15 mg/g (baseline 20±4 mg/g; follow-up, 18±4 mg/g; p < 0.2) or in reduction in the proportion of patients with HIC exceeding 15 mg/g (p < 0.2). During deferiprone exposure, new diabetes mellitus, a recognized consequence of inadequate iron control, was diagnosed in 17% patients, most of whom had sustained HICs exceeding 15 mg/g for years; one woman died after 13 months of a regimen of deferiprone and low-dose deferasirox. During deferiprone exposure, serum ALT increased over baseline in 65% patients. Mean serum ALT increased 6.6-fold (p < 0.001) often persisting for years. During deferasirox exposure, mean ALT was unchanged (p < 0.84). No significant differences between treatment groups were observed in the proportions of patients estimated to have elevated cardiac iron., Conclusions: Deferiprone showed ineffectiveness and significant toxicity in most patients. Combination with low doses of first-line therapies did not improve the effectiveness of deferiprone. Exposure to deferiprone, over six years while the drug was unlicensed, in the face of ineffectiveness and serious toxicities, demands review of the standards of local medical practice. The limited scope of regulatory approval of deferiprone, worldwide, should restrict its exposure to the few patients genuinely unable to tolerate the two effective, first-line therapies., Competing Interests: Dr. Nancy F. Olivieri led two investigator-initiated trials of deferiprone begun in 1989 (partially funded by Apotex Inc. from 1993) at Toronto’s Hospital for Sick Children and the University of Toronto. In 1995, she identified concerns regarding long-term effectiveness and safety of deferiprone. In 1996, both Toronto trials were terminated abruptly and prematurely, and Dr. Olivieri was threatened with legal remedies should she make concerns public. Dr. Brenda L. Gallie, an independent researcher at The Hospital for Sick Children and the University, was involved directly in all related events over the subsequent decade of legal proceedings. An independent description of the first five years of this controversy provides additional details (Thompson J, Baird P, Downie J. The Olivieri Report: The complete text of the report of the independent committee of inquiry commissioned by the Canadian Association of University Teachers. Toronto: James Lorimer & Co. Publishers; 2001). In 2014, a final settlement respecting all legal matters was mediated between Dr. Olivieri and Apotex. This does not alter the authors' adherence to all PLOS ONE policies on sharing data and materials.

Published
2019
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30. Dysregulated arginine metabolism and cardiopulmonary dysfunction in patients with thalassaemia.

Author

Morris CR, Kim HY, Klings ES, Wood J, Porter JB, Trachtenberg F, Sweeters N, Olivieri NF, Kwiatkowski JL, Virzi L, Hassell K, Taher A, Neufeld EJ, Thompson AA, Larkin S, Suh JH, Vichinsky EP, and Kuypers FA

Subjects
Adult, Arginase blood, Arginase metabolism, Case-Control Studies, Cross-Sectional Studies, Echocardiography, Doppler, Female, Humans, Hypertension, Pulmonary diagnosis, Male, Middle Aged, Thalassemia diagnosis, Young Adult, Arginine metabolism, Hypertension, Pulmonary etiology, Hypertension, Pulmonary physiopathology, Thalassemia complications, Thalassemia metabolism
Abstract

Pulmonary hypertension (PH) commonly develops in thalassaemia syndromes, but is poorly characterized. The goal of this study was to provide a comprehensive description of the cardiopulmonary and biological profile of patients with thalassaemia at risk for PH. A case-control study of thalassaemia patients at high versus low PH-risk was performed. A single cross-sectional measurement for variables reflecting cardiopulmonary status and biological pathophysiology were obtained, including Doppler-echocardiography, 6-min-walk-test, Borg Dyspnoea Score, New York Heart Association functional class, cardiac magnetic resonance imaging (MRI), chest-computerized tomography, pulmonary function testing and laboratory analyses targeting mechanisms of coagulation, inflammation, haemolysis, adhesion and the arginine-nitric oxide pathway. Twenty-seven thalassaemia patients were evaluated, 14 with an elevated tricuspid-regurgitant-jet-velocity (TRV) ≥ 2·5 m/s. Patients with increased TRV had a higher frequency of splenectomy, and significantly larger right atrial size, left atrial volume and left septal-wall thickness on echocardiography and/or MRI, with elevated biomarkers of abnormal coagulation, lactate dehydrogenase (LDH) levels and arginase concentration, and lower arginine-bioavailability compared to low-risk patients. Arginase concentration correlated significantly to several echocardiography/MRI parameters of cardiovascular function in addition to global-arginine-bioavailability and biomarkers of haemolytic rate, including LDH, haemoglobin and bilirubin. Thalassaemia patients with a TRV ≥ 2·5 m/s have additional echocardiography and cardiac-MRI parameters suggestive of right and left-sided cardiac dysfunction. In addition, low arginine bioavailability may contribute to cardiopulmonary dysfunction in β-thalassaemia., (© 2015 John Wiley & Sons Ltd.)

Published
2015
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31. Hepcidin is suppressed by erythropoiesis in hemoglobin E β-thalassemia and β-thalassemia trait.

Author

Jones E, Pasricha SR, Allen A, Evans P, Fisher CA, Wray K, Premawardhena A, Bandara D, Perera A, Webster C, Sturges P, Olivieri NF, St Pierre T, Armitage AE, Porter JB, Weatherall DJ, and Drakesmith H

Subjects
Adolescent, Adult, Carrier State, Case-Control Studies, Child, Child, Preschool, Erythropoiesis genetics, Female, Gene Expression Regulation, Genotype, Hemoglobin E metabolism, Hepcidins metabolism, Humans, Iron metabolism, Iron Overload etiology, Iron Overload metabolism, Iron Overload pathology, Linear Models, Male, Middle Aged, Mutation, Phenotype, Severity of Illness Index, Sri Lanka, Transfusion Reaction, beta-Globins metabolism, beta-Thalassemia metabolism, beta-Thalassemia pathology, beta-Thalassemia therapy, Hemoglobin E genetics, Hepcidins genetics, Iron Overload genetics, beta-Globins genetics, beta-Thalassemia genetics
Abstract

Hemoglobin E (HbE) β-thalassemia is the most common severe thalassemia syndrome across Asia, and millions of people are carriers. Clinical heterogeneity in HbE β-thalassemia is incompletely explained by genotype, and the interaction of phenotypic variation with hepcidin is unknown. The effect of thalassemia carriage on hepcidin is also unknown, but it could be relevant for iron supplementation programs aimed at combating anemia. In 62 of 69 Sri Lankan patients with HbE β-thalassemia with moderate or severe phenotype, hepcidin was suppressed, and overall hepcidin inversely correlated with iron accumulation. On segregating by phenotype, there were no differences in hepcidin, erythropoiesis, or hemoglobin between severe or moderate disease, but multiple linear regression showed that erythropoiesis inversely correlated with hepcidin only in severe phenotypes. In moderate disease, no independent predictors of hepcidin were identifiable; nevertheless, the low hepcidin levels indicate a significant risk for iron overload. In a population survey of Sri Lankan schoolchildren, β-thalassemia (but not HbE) trait was associated with increased erythropoiesis and mildly suppressed hepcidin, suggesting an enhanced propensity to accumulate iron. In summary, the influence of erythropoiesis on hepcidin suppression associates with phenotypic disease variation and pathogenesis in HbE β-thalassemia and indicates that the epidemiology of β-thalassemia trait requires consideration when planning public health iron interventions., (© 2015 by The American Society of Hematology.)

Published
2015
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32. Sildenafil therapy in thalassemia patients with Doppler-defined risk of pulmonary hypertension.

Author

Morris CR, Kim HY, Wood J, Porter JB, Klings ES, Trachtenberg FL, Sweeters N, Olivieri NF, Kwiatkowski JL, Virzi L, Singer ST, Taher A, Neufeld EJ, Thompson AA, Sachdev V, Larkin S, Suh JH, Kuypers FA, and Vichinsky EP

Subjects
Adult, Echocardiography, Doppler methods, Female, Humans, Hypertension, Pulmonary epidemiology, Male, Middle Aged, Pilot Projects, Purines therapeutic use, Risk Factors, Sildenafil Citrate, Thalassemia epidemiology, Hypertension, Pulmonary diagnostic imaging, Hypertension, Pulmonary drug therapy, Piperazines therapeutic use, Sulfones therapeutic use, Thalassemia diagnostic imaging, Thalassemia drug therapy, Vasodilator Agents therapeutic use
Abstract

Pulmonary hypertension is a common but often overlooked complication associated with thalassemia syndromes. There are limited data on the safety and efficacy of selective pulmonary vasodilators in this at-risk population. We, therefore, designed a 12-week, open-label, phase 1/2, pilot-scale, proof-of-principle trial of sildenafil therapy in 10 patients with β-thalassemia and at increased risk of pulmonary hypertension based on an elevated tricuspid regurgitant jet velocity >2.5 m/s on Doppler-echocardiography. Variables compared at baseline and after 12 weeks of sildenafil treatment included Doppler-echocardiographic parameters, 6-minute walked distance, Borg Dyspnea Score, New York Heart Association functional class, pulmonary function, and laboratory parameters. Treatment with sildenafil resulted in a significant decrease in tricuspid regurgitant jet velocity by 13.3% (3.0±0.7 versus 2.6±0.5 m/s, P=0.04), improved left ventricular end systolic/diastolic volume, and a trend towards a improved New York Heart Association functional class. No significant change in 6-minute walked distance was noted. Sildenafil was well tolerated, although minor expected adverse events were commonly reported. The total dose of sildenafil (mg) was strongly correlated with percent change in nitric oxide metabolite concentration in the plasma (ρ=0.80, P=0.01). There were also significant increases in plasma and erythrocyte arginine concentrations. Our study suggests that sildenafil is safe and may improve pulmonary hemodynamics in patients at risk of pulmonary hypertension; however, it was not demonstrated to improve the distance walked in 6 minutes. Clinical trials are needed to identify the best treatment strategy for pulmonary hypertension in patients with β-thalassemia. (clinicaltrials.gov identifier: NCT00872170).

Published
2013
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33. Management of the thalassemias.

Author

Olivieri NF and Brittenham GM

Subjects
Benzoates economics, Benzoates therapeutic use, Blood Transfusion, Deferasirox, Deferiprone, Deferoxamine economics, Deferoxamine therapeutic use, Ferritins blood, Humans, Iron metabolism, Iron Chelating Agents economics, Iron Chelating Agents therapeutic use, Iron Overload therapy, Liver metabolism, Myocardium metabolism, Pancreas metabolism, Pituitary Gland, Anterior metabolism, Pyridones economics, Pyridones therapeutic use, Triazoles economics, Triazoles therapeutic use, Thalassemia therapy
Abstract

During the last 30 years, in addition to the considerable progress made in control and prevention of thalassemias(3), there have also been major advances in their symptomatic management, at least in wealthier countries where appropriate facilities are available. Remarkable improvements in survival in the severe forms of thalassemia have followed the more judicious use of blood transfusion and, in particular, the ability to manage the iron accumulation resulting from transfusion with its severe and ultimately lethal effects on endocrine and cardiac function.

Published
2013
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34. Treatment strategies for hemoglobin E beta-thalassemia.

Author

Olivieri NF

Subjects
Blood Transfusion, Humans, Iron Chelating Agents therapeutic use, Splenectomy, Hemoglobin E genetics, beta-Thalassemia genetics, beta-Thalassemia therapy
Abstract

Hemoglobin E beta (ß)-thalassemia (HbE thalassemia) is a very common form of β-thalassemia that exhibits a heterogeneous clinical presentation and variable clinical course. The reasons for this extraordinary clinical heterogeneity are not completely understood. A number of factors, both genetic and environmental, appear to modify the severity of HbE thalassemia. There is also an emerging understanding that the HbE thalassemia phenotype may be unstable, which may reflect changes in adaptation to anemia and, possibly, attenuation of the erythropoietin response over time. These factors make it difficult to develop broad treatment guidelines. It is now generally appreciated that steady-state hemoglobin concentration may be of limited value to determine which patients need regular transfusions. Therefore, periodic reassessment of the need for transfusion therapy is recommended, and intermittent transfusion therapy may now be explored as an approach in this disorder., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published
2012
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35. Chelation use and iron burden in North American and British thalassemia patients: a report from the Thalassemia Longitudinal Cohort.

Author

Kwiatkowski JL, Kim HY, Thompson AA, Quinn CT, Mueller BU, Odame I, Giardina PJ, Vichinsky EP, Boudreaux JM, Cohen AR, Porter JB, Coates T, Olivieri NF, and Neufeld EJ

Subjects
Cohort Studies, Female, Humans, Liver metabolism, London, Longitudinal Studies, Magnetic Resonance Imaging, Male, North America, Thalassemia metabolism, Young Adult, Iron analysis, Iron Chelating Agents therapeutic use, Liver chemistry, Thalassemia drug therapy
Abstract

Morbidity and mortality in thalassemia are associated with iron burden. Recent advances in organ-specific iron imaging and the availability of oral deferasirox are expected to improve clinical care, but the extent of use of these resources and current chelation practices have not been well described. In the present study, we studied chelation use and the change in iron measurements in 327 subjects with transfusion-dependent thalassemia (mean entry age, 22.1 ± 2.5 years) from 2002-2011, with a mean follow-up of 8.0 years (range, 4.4-9.0 years). The predominant chelator currently used is deferasirox, followed by deferoxamine and then combination therapies. The use of both hepatic and cardiac magnetic resonance imaging increased more than 5-fold (P < .001) during the study period, leading to an 80% increase in the number of subjects undergoing liver iron concentration (LIC) measurements. Overall, LIC significantly improved (median, 10.7 to 5.1 mg/g dry weight, P < .001) with a nonsignificant improvement in cardiac T2* (median, 23.55 to 34.50 ms, P = .23). The percentage of patients with markers of inadequate chelation (ferritin > 2500 ng/mL, LIC > 15 mg/g dry weight, and/or cardiac T2* < 10 ms) also declined from 33% to 26%. In summary, increasing use of magnetic resonance imaging and oral chelation in thalassemia management has likely contributed to improved iron burden.

Published
2012
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36. Risk factors and mortality associated with an elevated tricuspid regurgitant jet velocity measured by Doppler-echocardiography in thalassemia: a Thalassemia Clinical Research Network report.

Author

Morris CR, Kim HY, Trachtenberg F, Wood J, Quinn CT, Sweeters N, Kwiatkowski JL, Thompson AA, Giardina PJ, Boudreaux J, Olivieri NF, Porter JB, Neufeld EJ, and Vichinsky EP

Subjects
Adolescent, Adult, Child, Child, Preschool, Cohort Studies, Echocardiography, Doppler, Female, Humans, Male, Middle Aged, Prevalence, Risk Factors, Thalassemia epidemiology, Thalassemia mortality, Tricuspid Valve Insufficiency epidemiology, Tricuspid Valve Insufficiency mortality, Young Adult, Thalassemia complications, Thalassemia diagnostic imaging, Tricuspid Valve Insufficiency complications, Tricuspid Valve Insufficiency diagnostic imaging
Abstract

An elevated tricuspid regurgitant jet velocity (TRV) is associated with hemolysis and early mortality in sickle cell disease, yet risk factors, clinical parameters, and mortality associated with this biomarker in thalassemia are poorly defined. This report summarizes the prevalence of an elevated TRV in 325 patients screened by Doppler echocardiography in the Thalassemia Clinical Research Network. A documented TRV was reported in 148 of 325 (46%) of patients. Average age was 25.9 years (range, 5-56 years) and 97% were transfusion-dependent. Mean TRV was 2.3 ± 0.4 m/s (range, 0.2-3.5 m/s). An abnormal TRV ≥ 2.5 m/s was identified in 49 of 148 (33%) of patients with a documented TRV, 5% (8/148), with a TRV ≥ 3.0 m/s, suggesting significant PH risk. Older age was strongly associated with a high TRV; however, 16% of children had a TRV ≥ 2.5 m/s. A history of splenectomy, hepatitis C, smoking, or high white blood cell count was associated with TRV elevation. In summary, an elevated TRV is noted in one-third of transfusion-dependent thalassemia patients with a documented value and develops in both children and adults. Age, splenectomy, hepatitis C, and smoking are significant univariate risk factors, with splenectomy surfacing as the dominant risk factor over time. Mortality was low in this cohort. Prospective longitudinal studies are needed. This study is registered at http://www.clinicaltrials.gov as NCT00661804.

Published
2011
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37. Hb E/beta-thalassaemia: a common & clinically diverse disorder.

Author

Olivieri NF, Pakbaz Z, and Vichinsky E

Subjects
Blood Transfusion, Erythropoietin blood, Fetal Hemoglobin genetics, Genotype, Humans, Malaria blood, Phenotype, Polymorphism, Genetic, Splenectomy adverse effects, alpha-Thalassemia blood, alpha-Thalassemia genetics, Hemoglobin E genetics, beta-Thalassemia diagnosis, beta-Thalassemia genetics
Abstract

Haemoglobin E-beta thalassaemia (Hb E/β-thalassaemia) is the genotype responsible for approximately one-half of all severe beta-thalassaemia worldwide. The disorder is characterized by marked clinical variability, ranging from a mild and asymptomatic anaemia to a life-threatening disorder requiring transfusions from infancy. The phenotypic variability of Hb E/β-thalassaemia and the paucity of long-term clinical data, present challenges in providing definitive recommendations for the optimal management of patients. Genetic factors influencing the severity of this disorder include the type of beta-thalassaemia mutation, the co-inheritance of alpha-thalassaemia, and polymorphisms associated with increased production of foetal haemoglobin. Other factors, including a variable increase in serum erythropoietin in response to anaemia, previous or ongoing infection with malaria, previous splenectomy and other environmental influences, may be involved. The remarkable variation, and the instability, of the clinical phenotype of Hb E beta-thalassaemia suggests that careful tailoring of treatment is required for each patient, and that therapeutic approaches should be re-assessed over-time.

Published
2011

38. A pilot study of subcutaneous decitabine in β-thalassemia intermedia.

Author

Olivieri NF, Saunthararajah Y, Thayalasuthan V, Kwiatkowski J, Ware RE, Kuypers FA, Kim HY, Trachtenberg FL, and Vichinsky EP

Subjects
Adult, Azacitidine administration & dosage, Cell Differentiation drug effects, DNA (Cytosine-5-)-Methyltransferase 1, DNA (Cytosine-5-)-Methyltransferases deficiency, DNA Methylation drug effects, Decitabine, Erythrocytes drug effects, Female, Hemoglobins metabolism, Humans, Injections, Subcutaneous, Male, Middle Aged, Pilot Projects, Prognosis, Young Adult, beta-Thalassemia genetics, Antimetabolites, Antineoplastic administration & dosage, Azacitidine analogs & derivatives, Gene Expression Regulation drug effects, beta-Thalassemia drug therapy, gamma-Globins genetics
Abstract

Ineffective erythropoiesis, the hallmark of β-thalassemia, is a result of α/non-α globin chain imbalance. One strategy to redress globin-chain imbalance is to induce γ-globin gene (HBG) expression. Repression of HBG in adult erythroid cells involves DNA methylation and other epigenetic changes. Therefore, the cytosine analog decitabine, which can deplete DNA methyltransferase 1 (DNMT1), can potentially activate HBG. In 5 patients with β-thalassemia intermedia, a dose and schedule of decitabine intended to deplete DNMT1 without causing significant cytotoxicity (0.2 mg/kg subcutaneous 2 times per week for 12 weeks) increased total hemoglobin from 7.88 ± 0.88 g/dL to 9.04 ± 0.77 g/dL (P = .004) and absolute fetal hemoglobin from 3.64 ± 1.13 g/dL to 4.29 ± 1.13 g/dL (P = .003). Significant favorable changes also occurred in indices of hemolysis and red blood cell densitometry. Consistent with a noncytotoxic, differentiation altering mechanism of action, the major side effect was an asymptomatic increase in platelet counts without erythrocyte micronucleus or VDJ recombination assay evidence of genotoxicity. This study was registered at www.clinicaltrials.gov as #NCT00661726.

Published
2011
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39. HbE/β-thalassemia: basis of marked clinical diversity.

Author

Olivieri NF, Pakbaz Z, and Vichinsky E

Subjects
Fetal Hemoglobin genetics, Genetic Heterogeneity, Humans, Polymorphism, Genetic, alpha-Thalassemia genetics, Hemoglobin E genetics, Mutation, beta-Thalassemia genetics
Abstract

Hemoglobin E thalassemia accounts for about one-half of all cases of severe beta thalassemia. There is marked variability in its clinical severity ranging from an asymptomatic to a transfusion-dependent phenotype. The phenotypic variability and inadequate longitudinal data present challenges in determining the optimal management of patients. This article summarizes findings on the natural history of Hemoglobin E thalassemia and some factors responsible for its clinical heterogeneity. Major genetic factors include the type of beta thalassemia mutation, the co-inheritance of alpha thalassemia, and polymorphisms associated with increased synthesis of fetal hemoglobin. Other factors, including response to anemia, and the influence of infection with malaria and other environmental influences, may be important. The remarkable variation and instability of clinical phenotypes in Hemoglobin E thalassemia require individual management plans for each patient, which should be reassessed over time., (Copyright © 2010. Published by Elsevier Inc.)

Published
2010
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40. Emerging insights in the management of hemoglobin E beta thalassemia.

Author

Olivieri NF, Thayalsuthan V, O'Donnell A, Premawardhena A, Rigobon C, Muraca G, Fisher C, and Weatherall DJ

Subjects
Blood Transfusion, Humans, beta-Thalassemia physiopathology, Hemoglobin E, beta-Thalassemia therapy
Abstract

Globally, hemoglobin (Hb) E beta thalassemia accounts for approximately half the severe forms of beta thalassemia. Because of its wide clinical diversity and the ability of patients with this condition to adapt unusually well to low hemoglobin levels, the management of Hb E beta thalassemia, particularly the decision to instigate regular blood transfusion, is particularly difficult. Here, we present a summary of our work in patients with this condition, which attempts to define clinical, adaptive, and genetic factors of possible value in determining the early management of this condition.

Published
2010
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41. Interaction of malaria with a common form of severe thalassemia in an Asian population.

Author

O'Donnell A, Premawardhena A, Arambepola M, Samaranayake R, Allen SJ, Peto TE, Fisher CA, Cook J, Corran PH, Olivieri NF, and Weatherall DJ

Subjects
Adolescent, Adult, Antibodies, Protozoan immunology, Antigens, Protozoan immunology, Case-Control Studies, Child, Environmental Exposure, Humans, Malaria epidemiology, Malaria immunology, Phenotype, Pilot Projects, Prevalence, Splenectomy, Sri Lanka epidemiology, beta-Thalassemia immunology, Asian People, Malaria complications, beta-Thalassemia complications, beta-Thalassemia pathology
Abstract

In many Asian populations, the commonest form of severe thalassemia results from the coinheritance of HbE and beta thalassemia. The management of this disease is particularly difficult because of its extreme clinical diversity; although some genetic and adaptive factors have been identified as phenotypic modifiers, the reasons remain unclear. Because the role of the environment in the course of severe thalassemia has been neglected completely and because malaria due to both Plasmodium falciparum and Plasmodium vivax has been prevalent in Sri Lanka, we carried out a pilot study of patients with HbE beta thalassemia that showed high frequencies of antibodies to both parasite species and that 28.6% of the children had DNA-based evidence of current infection with P. vivax. Malarial antibodies then were assessed in patients with HbE beta thalassemia compared with those in age-matched controls. There was a significant increase in the frequency of antibodies in the thalassemic patients, particularly against P. vivax and in young children. There was also a higher frequency in those who had been splenectomized compared with those with intact spleens, although in the latter it was still higher than that in the controls. The thalassemic patients showed significant correlations between malaria antibody status and phenotype. Patients with HbE beta thalassemia may be more prone to malaria, particularly P. vivax, which is reflected in their clinical severity. Because P. vivax malaria is widespread in Asia, further studies of its interaction with HbE beta thalassemia and related diseases are required urgently as a part of ongoing thalassemia control programs.

Published
2009
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42. Hemoglobin H-constant spring in North America: an alpha thalassemia with frequent complications.

Author

Singer ST, Kim HY, Olivieri NF, Kwiatkowski JL, Coates TD, Carson S, Neufeld E, Cunningham MJ, Giardina PJ, Mueller BU, Quinn CT, Fung E, and Vichinsky E

Subjects
Adolescent, Child, Child, Preschool, Humans, North America epidemiology, Young Adult, alpha-Thalassemia epidemiology, alpha-Thalassemia therapy, Hemoglobins, Abnormal, alpha-Thalassemia complications
Published
2009
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43. Disparity in the management of iron overload between patients with sickle cell disease and thalassemia who received transfusions.

Author

Fung EB, Harmatz PR, Milet M, Balasa V, Ballas SK, Casella JF, Hilliard L, Kutlar A, McClain KL, Olivieri NF, Porter JB, and Vichinsky EP

Subjects
Adolescent, Adult, Canada, Child, Cross-Sectional Studies, Female, Ferritins blood, Humans, Iron Overload etiology, Male, United Kingdom, United States, Young Adult, Anemia, Sickle Cell therapy, Erythrocyte Transfusion adverse effects, Iron Overload therapy, Thalassemia therapy
Abstract

Background: Transfusion therapy is frequently used to prevent morbidity in sickle cell disease (SCD), and subsequent iron overload is common. The objective of this study was to evaluate the current standard of care in monitoring iron overload and related complications in patients with SCD compared to thalassemia (Thal)., Study Design and Methods: A cross-sectional study was conducted at 31 hematology clinics in the United States, Canada, or the United Kingdom. Patients who received transfusions with a mean serum ferritin level of least 2000 ng per mL were eligible. A total of 199 patients with SCD (113 female; 24.9 +/- 13.2 years) and 142 with Thal (66 female; 25.8 +/- 8.1 years) were recruited, and data were collected between 2001 and 2003 by interview and medical record review., Results: Although both groups were recruited on the basis of significant iron overload, the likelihood of performing a liver biopsy for routine iron monitoring was significantly higher (odds ratio [OR], 3.4; 95% confidence interval [CI], 2.2-5.3) in Thal than SCD. Thal patients were also more likely to be screened for iron-related organ injury including an echocardiograph for cardiomyopathy (OR, 2.6; p < 0.001; 95% CI, 1.6-4.2), alanine aminotransferase for liver function (OR, 8.3; CI, 1.05-64.4), and thyroid-stimulating hormone for hypothyroidism (OR, 12.3; CI, 7.0-21.5). For adult SCD patients, those maintained on simple transfusion with a serum ferritin level of greater than 2500 ng per mL were the least likely to have a liver biopsy (p < 0.03)., Conclusions: These data highlight the unsystematic monitoring of iron and related organ injury in SCD. Until the relationship between iron and related comorbidities is better understood, routine monitoring of iron overload in SCD patients who receive transfusions should be considered a standard part of clinical care.

Published
2008
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44. Studies in haemoglobin E beta-thalassaemia.

Author

Olivieri NF, Muraca GM, O'Donnell A, Premawardhena A, Fisher C, and Weatherall DJ

Subjects
Adolescent, Adult, Child, Child, Preschool, Humans, Middle Aged, Phenotype, Practice Guidelines as Topic, Sri Lanka epidemiology, beta-Thalassemia complications, beta-Thalassemia epidemiology, beta-Thalassemia therapy, Hemoglobin E genetics, beta-Thalassemia genetics
Abstract

Haemoglobin E beta-thalassaemia is the commonest form of severe thalassaemia in many Asian countries, but little is known about its natural history, the reasons for its clinical diversity, or its optimal management. Despite its frequency, haemoglobin E beta-thalassaemia is often managed in an ill-defined and haphazard way, usually by demand transfusion. We studied a cohort of Sri Lankan patients with haemoglobin E beta-thalassaemia over 5 years, and identified several genetic and environmental factors possibly contributing to the phenotypic diversity of the disorder. These included modifiers of haemoglobin F production, malaria and age-related changes in adaptation to anaemia. Our findings suggest that in many patients, haemoglobin E beta-thalassaemia can be managed without transfusion, even with low haemoglobin levels. Age-related changes in the pattern of adaptation to anaemia suggest that more cost-effective approaches to management should be explored.

Published
2008
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45. Age-related changes in adaptation to severe anemia in childhood in developing countries.

Author

O'Donnell A, Premawardhena A, Arambepola M, Allen SJ, Peto TE, Fisher CA, Rees DC, Olivieri NF, and Weatherall DJ

Subjects
Adolescent, Adult, Age Distribution, Anemia complications, Animals, Child, Child, Preschool, Erythropoietin blood, Humans, Infant, Malaria, Falciparum complications, Malaria, Falciparum epidemiology, Malaria, Falciparum parasitology, Middle Aged, beta-Thalassemia blood, beta-Thalassemia epidemiology, beta-Thalassemia physiopathology, Adaptation, Physiological physiology, Aging physiology, Anemia physiopathology, Developing Countries statistics & numerical data
Abstract

Severe forms of anemia in children in the developing countries may be characterized by different clinical manifestations at particular stages of development. Whether this reflects developmental changes in adaptation to anemia or other mechanisms is not clear. The pattern of adaptation to anemia has been assessed in 110 individuals with hemoglobin (Hb) E beta-thalassemia, one of the commonest forms of inherited anemia in Asia. It has been found that age and Hb levels are independent variables with respect to erythropoietin response and that there is a decline in the latter at a similar degree of anemia during development. To determine whether this finding is applicable to anemia due to other causes, a similar study has been carried out on 279 children with severe anemia due to Plasmodium falciparum malaria; the results were similar to those in the patients with thalassemia. These observations may have important implications both for the better understanding of the pathophysiology of profound anemia in early life and for its more logical and cost-effective management.

Published
2007
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46. Changes in the epidemiology of thalassemia in North America: a new minority disease.

Author

Vichinsky EP, MacKlin EA, Waye JS, Lorey F, and Olivieri NF

Subjects
Adolescent, Adult, Age Distribution, Child, Child, Preschool, Genotype, Humans, Infant, Infant, Newborn, Middle Aged, North America epidemiology, Phenotype, Thalassemia ethnology, Thalassemia genetics, Thalassemia epidemiology
Abstract

Objective: Changing patterns of immigration to North America, along with improved treatment, have altered the clinical spectrum of thalassemia, one of the world's most common genetic diseases. The new demography of the disease, with its widely variable phenotypes, has implications for its diagnosis, counseling, and management. Characterization of the new spectrum of this ancient disease, now predominated by minority groups, is essential for optimizing survival., Methods: The National Institutes of Health-sponsored North American Thalassemia Clinical Research Network (TCRN) conducted a cross-sectional study of 721 patients with thalassemia syndromes. A detailed chart review was undertaken to define the relationships between ethnic origins, genotype, and phenotype. These results were compared with 3 previous surveys of similar regions. To determine if the TCRN patient epidemiology is representative of North American patients, 87 additional programs were reviewed, and hemoglobinopathy programs from the 2 largest thalassemia regions, Ontario and California, were analyzed., Results: A total of 721 patients completed analysis in the TCRN study, including 389 (54%) patients with beta-thalassemia major, 105 (15%) patients with beta-thalassemia intermedia, 95 (13%) patients with hemoglobin E-beta-thalassemia, and 132 (18%) patients with alpha-thalassemia. beta-Thalassemia predominated in Eastern North America. Hemoglobin E-beta-thalassemia and alpha-thalassemia were common on the Western continent. Genotype broadly correlated with the clinical phenotype. However, there was marked heterogeneity in clinical phenotype among patients with similar globin mutations. In beta-thalassemia disorders, coinheritance of the alpha-thalassemia trait, triplication of alpha-thalassemia genes, and heterozygosity for the dominant beta-thalassemia allele affected the clinical phenotype. In alpha-thalassemia disorders, structural mutations such as hemoglobin H-Constant Spring resulted in a severe hemoglobin H phenotype. Sixty percent of patients received regular transfusions, and 86% received regular iron-chelation therapy. Increased survival and decreasing birth rates of Mediterranean patients resulted in an aging Greek/Italian population being replaced by a young Asian/Middle Eastern population. Now, Asian patients account for >50% of the thalassemia population. Evidence of increasing survival is reflected in an advancing mean age of white patients with thalassemia major (25 years, up from 11 years in 1974). The results of the non-TCRN thalassemia survey confirm these observations and describe a young multiethnic thalassemia population distributed throughout North America. Newborn-screening results suggest that thalassemia births in North America are increasing and reflect the change in genotype and phenotype observed in the TCRN populations., Conclusions: The epidemiology of thalassemia in North America reflects a heterogeneous group of diseases with new ethnicities, genotypes, and phenotypes. In these communities, physicians will need to provide education, prenatal diagnosis, counseling, and management of this newly diverse group of patients.

Published
2005
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47. A novel molecular basis for beta thalassemia intermedia poses new questions about its pathophysiology.

Author

Premawardhena A, Fisher CA, Olivieri NF, de Silva S, Sloane-Stanley J, Wood WG, and Weatherall DJ

Subjects
Adolescent, Child, Preschool, Genotype, Globins genetics, Hemoglobins genetics, Humans, Infant, beta-Thalassemia classification, beta-Thalassemia genetics, beta-Thalassemia physiopathology
Abstract

During a study of the molecular basis for severe forms of beta thalassemia in Sri Lanka, 2 patients were found to be heterozygous for beta thalassemia mutations. Further analysis revealed that one of them has a previously unreported molecular basis for severe thalassemia intermedia, homozygosity for quadruplicated alpha globin genes in combination with heterozygous beta thalassemia. The other is homozygous for a triplicated alpha globin gene arrangement and heterozygous for beta thalassemia. Their differences in clinical phenotype are explainable by the interaction of other genetic factors and, in particular, their early management. The clinical course of the 2 propositi underlines the importance of full genotyping and a long period of observation before treatment is instituted, particularly in patients with beta thalassemia intermedia associated with extended alpha globin gene arrangements. The hemoglobin (Hb) F levels in these patients with severe beta thalassemia intermedia, compared with other forms of this condition in the Sri Lankan population and elsewhere, are unusually low, a consistent finding in extended alpha globin gene interactions and in dominant beta thalassemia, raising the possibility that increased levels of HbF production in beta thalassemia may require mutations at both beta globin gene loci.

Published
2005
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48. Fetal haemoglobin augmentation in E/beta(0) thalassaemia: clinical and haematological outcome.

Author

Singer ST, Kuypers FA, Olivieri NF, Weatherall DJ, Mignacca R, Coates TD, Davies S, Sweeters N, and Vichinsky EP

Subjects
Adolescent, Blood Transfusion, Child, Drug Therapy, Combination, Erythrocyte Aging drug effects, Erythropoiesis drug effects, Erythropoietin therapeutic use, Female, Hemoglobins metabolism, Humans, Hydroxyurea adverse effects, Iron Overload, Male, Phenylbutyrates therapeutic use, Prospective Studies, Recombinant Proteins, Treatment Outcome, beta-Thalassemia blood, beta-Thalassemia therapy, Fetal Hemoglobin metabolism, Hydroxyurea therapeutic use, beta-Thalassemia drug therapy
Abstract

Patients with E/beta(0) thalassaemia, the most common haemoglobinopathy in many Asian countries, might benefit from drugs that increase fetal and total haemoglobin and thereby decrease the need for transfusions. The long-term clinical efficacy and safety of such therapy is unknown, limiting its use in countries where resources for safe and regular transfusion are scarce. In this study, 45 patients were treated with hydroxyurea (18-20 mg/kg) for 24+/-9 months, hydroxyurea with sodium phenyl butyrate (n=8) and hydroxyurea with erythropoietin (n=9), each for approximately 6 months, and followed for 3 years from study exit. Hydroxyurea had minimal toxicity, resulted in a mean 1.3 g/dl steady-state increase in haemoglobin in 40% of patients, and a milder response (

Published
2005
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49. Hemoglobin E-beta-thalassemia: Progress report from the International Study Group.

Author

Premawardhena A, De Silver S, Arambepola M, Olivieri NF, Vichinsky EP, Merson L, Muraco G, Allen A, Fisher C, Peto T, and Weatherall DJ

Subjects
Adolescent, Adult, Blood Transfusion statistics & numerical data, Case Management, Child, Child, Preschool, Combined Modality Therapy, Erythropoietin blood, Female, Hemoglobins analysis, Humans, Infant, International Cooperation, Iron Overload epidemiology, Iron Overload etiology, Longitudinal Studies, Male, Middle Aged, Phenotype, Pregnancy, Pregnancy Complications, Hematologic, Severity of Illness Index, Splenectomy, Sri Lanka epidemiology, Transfusion Reaction, beta-Thalassemia blood, beta-Thalassemia classification, beta-Thalassemia genetics, beta-Thalassemia therapy, Genetic Heterogeneity, Hemoglobin E genetics, beta-Thalassemia epidemiology
Abstract

A long-term observational study of Hb E-beta-thalassemia in Sri Lanka is beginning to define some of the genetic and environmental factors that are responsible for its remarkable phenotypic variability. In this population there is a very small difference between the steady-state hemoglobin levels between the mild and severe phenotypes, and it has been possible to stop transfusion in many of those who have been on long-term treatment of this kind. These preliminary observations, made over the last 7 years, provide directions for future research into this increasingly important disease.

Published
2005
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50. Single and combination drug therapy for fetal hemoglobin augmentation in hemoglobin E-beta 0-thalassemia: Considerations for treatment.

Author

Singer ST, Kuypers FA, Olivieri NF, Weatherall DJ, Mignacca R, Coates TD, Davies S, Sweeters N, and Vichinsky EP

Subjects
Blood Transfusion, Combined Modality Therapy, Drug Therapy, Combination, Erythropoietin administration & dosage, Facial Bones diagnostic imaging, Facial Bones physiopathology, Fetal Hemoglobin genetics, Genotype, Hematopoiesis, Extramedullary drug effects, Humans, Hydroxyurea administration & dosage, Phenylbutyrates administration & dosage, Radiography, Recombinant Proteins, Splenectomy, Splenomegaly, Treatment Outcome, beta-Thalassemia genetics, beta-Thalassemia surgery, beta-Thalassemia therapy, Erythropoiesis drug effects, Erythropoietin therapeutic use, Fetal Hemoglobin biosynthesis, Gene Expression drug effects, Globins genetics, Hemoglobin E genetics, Hydroxyurea therapeutic use, Phenylbutyrates therapeutic use, beta-Thalassemia drug therapy
Abstract

Patients with hemoglobin E (Hb E)-beta 0-thalassemia, one of the most common hemoglobinopathies worldwide, could benefit from drugs that increase fetal and total hemoglobin levels and thereby decrease the need for transfusions. The long-term clinical outcome of such therapy, its hematologic effects, and which patients are likely to benefit from treatment are unknown. Consequently, the use of such drugs for Hb E-beta 0-thalassemia is limited, and countries where resources for safe and regular transfusion are scarce cannot benefit from them. In a multicenter trial of 42 patients treated with hydroxyurea for two years, almost half the patients demonstrated a significant increase in steady-state hemoglobin level. Drug toxicity was minimal. Combined treatment of hydroxyurea with erythropoietin benefited selected patients, but the addition of sodium phenyl butyrate was ineffective. After 5 years of follow-up, a subset of patients remained off transfusions. Hydroxyurea should be considered for a subset of Hb E-beta 0-thalassemia patients.

Published
2005
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