D J Weatherall

Publications (221)2669.4 Total impact

• Article: The population genetics and dynamics of the thalassemias.

  D J Weatherall, T N Williams, S J Allen, A O'Donnell
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  ABSTRACT: The inherited disorders of hemoglobin, including the thalassemias, are by far the commonest monogenic diseases. Although several factors are responsible for their very high frequency, the major mechanism seems to be natural selection mediated by heterozygote protection against severe forms of malaria. Recent work has highlighted the complexity of the interplay among the different hemoglobin variants themselves and among different levels of malaria resistance, and is helping to explain the extraordinary heterogeneity in the distribution of the hemoglobin disorders even within short geographical distances. Some progress has also been made toward understanding the cellular and immune mechanisms that may underlie heterozygote protection against malaria in these conditions. In addition to providing valuable information about human evolutionary biology, work in this field has an increasingly important influence on the development of programs for the better management of the hemoglobin disorders, particularly in the poorer countries of the tropical world.
  Hematology/oncology clinics of North America 12/2010; 24(6):1021-31. · 2.05 Impact Factor
• Source

  Available from: pnas.org

  Article: Interaction of malaria with a common form of severe thalassemia in an Asian population.

  A O'Donnell, A Premawardhena, M Arambepola, R Samaranayake, S J Allen, T E A Peto, C A Fisher, J Cook, P H Corran, Nancy F Olivieri, D J Weatherall
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  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.
  Proceedings of the National Academy of Sciences 11/2009; 106(44):18716-21. · 9.68 Impact Factor
• Article: The sequence of the Aγ globin gene in a Gγβ+ type of hereditary persistence of fetal haemoglobin

  R. W. Jones, S. E. Y. Goodbourn, J. M. Old, D. J. Weatherall
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  ABSTRACT: The sequence of the Aγ globin gene from the affected chromosome of an individual heterozygous for the Gγβ+ type of hereditary persistence of fetal haemoglobin (Gγβ+ HPFH) is reported. With two exceptions, it is identical to one of the two allelic Aγ globin genes already sequenced and there is therefore no change which could explain the absence of its expression in the face of the persistent Gγ globin expression which is a feature of this condition.
  British Journal of Haematology 07/2008; 59(2):357 - 362. · 4.94 Impact Factor
• Article: Thalassaemia intermedia in Cyprus: the interaction of α and β thalassaemia

  J. S. Wainscoat, E. Kanavakis, W. G. Wood, E. A. Letsky, E. R. Huehns, G. W. Marsh, D. R. Higgs, J. B. Clegg, D. J. Weatherall
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  ABSTRACT: Restriction endonuclease analysis has been performed on the and β globin gene clusters of 57 Cypriots homozygous for β thalassaemia, 30 with the transfusion dependent form of the condition (thalassaemia major) and 27 who are less severely affected (thalassaemia intermedia). There was a significant difference in the incidence of thalassaemia between the two groups: 14/27 of the patients with thalassaemia intermedia also had deletion forms of a thalassaemia, while only 4/30 of the patients with thalassaemia major were similarly affected. Thus in Cypriot patients who are homozygous for β thalassaemia the co-inheritance of a thalassaemia is an important factor in determining the clinical course.
  British Journal of Haematology 07/2008; 53(3):411 - 416. · 4.94 Impact Factor
• Article: Is the beta thalassaemia trait of clinical importance?

  A Premawardhena, M Arambepola, N Katugaha, D J Weatherall
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  ABSTRACT: Although the beta thalassaemia trait affects millions of people worldwide, there have been no controlled studies to determine whether it is associated with any clinical disability or abnormal physical signs. To address this question, 402 individuals were studied: 217 with beta thalassaemia trait, of whom 154 were aware of the diagnosis and 63 were unaware until after the completion of the study; 89 normal controls; and 96 controls with mild hypochromic anaemia. There was a significant increase in symptoms ascribable to anaemia and episodes of pyrexia in those with the beta thalassaemia trait that were not influenced by prior knowledge that they had this condition. There was no difference in physical findings, notably splenomegaly, between those with beta thalassaemia trait and either control group.
  British Journal of Haematology 06/2008; 141(3):407-10. · 4.94 Impact Factor
• Article: A Comparison of the Homozygous States for Gγ and GγAγδβ Thalassaemia

  A. B. Amin, N. L. Pandya, P. P. Diwin, P. D. Darbre, C. Kattamis, A. Metaxatou-Mavromati, J. M. White, W. G. Wood, J. B. Clegg, D. J. Weatherall
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  ABSTRACT: One Arabic and two Indian patients with thalassaemia intermedia produce only Hb F of the Gγ type. Haemoglobin synthesis studies and genetic analysis indicate that they are homozygous for Gγδβ thalassaemia. The findings in these patients and their heterozygous relatives are compared with those in an individual homozygous for GγAγδβ thalassaemia. From this analysis, and from previously reported data on GγAγδβ thalassaemia, the phenotypic expression of the two varieties of δβ thalassaemia is defined. The relationship between the clinical expression and molecular pathology of these forms of δβ thalassaemia is discussed.
  British Journal of Haematology 03/2008; 43(4):537 - 548. · 4.94 Impact Factor
• Article: Characterization of an Indian (δβ)° thalassaemia

  J. S. Wainscoat, J. M. Old, W. G. Wood, R. J. Trent, D. J. Weatherall
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  ABSTRACT: The molecular basis of δβ thalassaemia in an Indian family is shown here to be due to a previously undescribed deletion within the β globin gene complex. Starting 3 kilobases from the 3’ end of the Aγ gene, the deletion removes the δ and β globin genes and continues to an unknown extent in the 3’ direction. Heterozygotes for this deletion have about 25% Hb F with a Gγ: Aγ ratio of 70:30 while interaction with β+ thalassaemia results in the clinical picture of thalassaemia intermedia.
  British Journal of Haematology 03/2008; 58(2):353 - 360. · 4.94 Impact Factor
• Source

  Available from: pnas.org

  Article: Age-related changes in adaptation to severe anemia in childhood in developing countries.

  Angela O'Donnell, A Premawardhena, M Arambepola, S J Allen, T E A Peto, C A Fisher, D C Rees, Nancy F Olivieri, D J Weatherall
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  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.
  Proceedings of the National Academy of Sciences 06/2007; 104(22):9440-4. · 9.68 Impact Factor
• Article: Alpha+ -thalassaemia and pregnancy in a malaria endemic region of Papua New Guinea.

  A O'Donnell, A Raiko, J B Clegg, D J Weatherall, S J Allen
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  ABSTRACT: The effect of maternal alpha+ -thalassaemia on pregnancy was assessed in the north coastal region of Papua New Guinea (PNG), where malaria is hyperendemic and alpha+ -thalassaemia is extremely common. In a prospective study of 987 singleton hospital deliveries, we correlated maternal alpha-globin genotype with markers of reproductive fitness (age in primigravidae, gravidity, pregnancy interval and the number of miscarriages and stillbirths), Plasmodium falciparum(P. falciparum) infection of the mother and placenta, maternal haemoglobin, preterm delivery and birthweight. The frequency of the -alpha genotype in mothers was 0.61. Markers of reproductive fitness were similar in women with and without alpha+ -thalassaemia. Median haemoglobin concentration during pregnancy and after delivery was about 1.0 g/dl lower in homozygous alpha+ -thalassaemia than in women with a normal alpha- globin genotype (P < or = 0.001). The frequency of placental P. falciparum infection and systemic malaria infection after delivery showed no consistent relationship to alpha-globin genotype. The frequency of preterm delivery and low birthweight did not vary significantly according to maternal alpha-globin genotype. Maternal alpha+ -thalassaemia does not affect reproductive fitness or susceptibility to malaria during pregnancy. Although median haemoglobin concentration was significantly lower in mothers homozygous for alpha+ -thalassaemia than those with a normal alpha-globin genotype, this did not result in an adverse outcome of pregnancy.
  British Journal of Haematology 11/2006; 135(2):235-41. · 4.94 Impact Factor
• Article: Muscle cell injury, haemolysis and dark urine in children with falciparum malaria in Papua New Guinea.

  A O'Donnell, D J Weatherall, A M Taylor, J C Reeder, S J Allen
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  ABSTRACT: During a prospective study of red cell variants and severe malaria in children, a surprising observation was the occurrence of dark urine. Children were grouped according to urine findings: 22 had dark urine that contained a haem protein (Group I), 93 had urine of normal colour that contained a haem protein (Group II) and 236 had normal urine (Group III). To investigate the cause of dark urine, haemolysis and muscle cell injury were assessed. Intravascular haemolysis was greater in Group I than in Groups II and III. However, anaemia was more severe in Group III and is likely to have resulted mainly from extravascular haemolysis. Median plasma myoglobin concentrations were greater in Groups I and II than Group III (P = 0.00060). Plasma myoglobin was greater in children with cerebral malaria, hyperlactataemia and those who died but was not associated with acidosis. Urine myoglobin was greater in Group I than Groups II and III (P = 0.00054). It is likely that both haemoglobin and myoglobin contributed to dark urine. The association between muscle cell injury and coma suggests sequestration of parasitized red cells as a common underlying pathology. In malaria, hyperlactataemia may result directly from breakdown of muscle protein as well as tissue hypoxia.
  Transactions of the Royal Society of Tropical Medicine and Hygiene 10/2006; 100(9):817-25. · 2.16 Impact Factor
• Source

  Available from: ksu.edu.sa

  Article: Phenotype/genotype relationships in sickle cell disease: a pilot twin study.

  M W Weatherall, D R Higgs, H Weiss, D J Weatherall, G R Serjeant
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  ABSTRACT: The roles of genetic and non-genetic factors in the haematology, growth and clinical features of sickle cell disease have been studied in nine identical twin pairs (six homozygous sickle cell disease, three sickle cell-haemoglobin C disease). A comparison group of 350 age-gender matched sibling pairs, selected to have an age difference of <5 years, was used for assessing the concordance of numerical data. Attained height, weight at attained height, fetal haemoglobin, total haemoglobin, mean cell volume, mean cell haemoglobin and total bilirubin levels showed significantly greater correlation in identical twins than in siblings. Twins showed similarities in the prevalence and degree of splenomegaly, susceptibility to priapism, and in onset of menarche, but other clinical complications were discordant in prevalence and severity. These findings suggest that physical growth and many haematological characteristics are subject to genetic influences, but that non-genetic factors contribute to the variance in disease manifestations.
  Clinical & Laboratory Haematology 12/2005; 27(6):384-90. · 1.11 Impact Factor
• Article: Recent advances in understanding haemochromatosis: a transition state.

  K J H Robson, A T Merryweather-Clarke, E Cadet, V Viprakasit, M G Zaahl, J J Pointon, D J Weatherall, J Rochette
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  ABSTRACT: Mutations in the hepcidin gene HAMP and the hemojuvelin gene HJV have recently been shown to result in juvenile haemochromatosis (JH). Hepcidin is an antimicrobial peptide that plays a key role in regulating intestinal iron absorption. Hepcidin levels are reduced in patients with haemochromatosis due to mutations in the HFE and HJV genes. Digenic inheritance of mutations in HFE and HAMP can result in either JH or hereditary haemochromatosis (HH) depending upon the severity of the mutation in HAMP. Here we review these findings and discuss how understanding the different types of haemochromatosis and our increasing knowledge of iron metabolism may help to elucidate the host's response to infection.
  Journal of Medical Genetics 11/2004; 41(10):721-30. · 6.36 Impact Factor
• Article: Deferiprone versus desferrioxamine in thalassaemia, and T2* validation and utility.

  G M Brittenham, D G Nathan, N F Olivieri, M J Pippard, D J Weatherall
  The Lancet 02/2003; 361(9352):183; author reply 183-4. · 38.28 Impact Factor
• Article: Genetic determinants of jaundice and gallstones in haemoglobin E beta thalassaemia.

  A Premawardhena, C A Fisher, F Fathiu, S de Silva, W Perera, T E Peto, N F Olivieri, D J Weatherall
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  ABSTRACT: Chronic hyperbilirubinaemia, gallstone formation, and gall bladder disease are unusually common in people with haemoglobin E beta thalassaemia in Sri Lanka. To determine whether this has a genetic basis we compared the bilirubin levels and frequency of gallstones in patients with different alleles of the UGT*1 gene. There was a significantly higher bilirubin level in those with the 7/7 genotypes compared with 6/6 and 6/7 genotype (p=0.032 and 0.0015 respectively), who also appeared more prone to gallstone formation. These results suggest that the UGT*1 genotpe is of importance in the genesis of gallstones in this population of patients.
  The Lancet 07/2001; 357(9272):1945-6. · 38.28 Impact Factor
• Article: Deferiprone for thalassaemia.

  M J Pippard, D J Weatherall
  The Lancet 11/2000; 356(9239):1444-5. · 38.28 Impact Factor
• Article: Thalassaemia in Sri Lanka: implications for the future health burden of Asian populations. Sri Lanka Thalassaemia Study Group.

  S de Silva, C A Fisher, A Premawardhena, S P Lamabadusuriya, T E Peto, G Perera, J M Old, J B Clegg, N F Olivieri, D J Weatherall
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  ABSTRACT: Thalassaemias pose an increasing problem for the Indian subcontinent and many Asian countries. We analysed the different types of thalassaemia in the Sri Lankan population, surveyed gene frequencies in schoolchildren, and estimated the burden of disease and requirements for its control. We analysed blood samples from patients attending clinics in nine hospitals and defined the different types of beta thalassaemia by high-performance liquid chromatography (HPLC) and DNA analysis. The range of mutations was obtained by analysis of beta-globin genes. Capillary blood was obtained from schoolchildren from different parts of the island and analysed by HPLC to provide an approximate assessment of the carrier frequency of beta thalassaemia and haemoglobin E (HbE). To estimate the frequency of alpha thalassaemia the alpha-globin genotypes were also analysed when it was possible. Blood samples were obtained from 703 patients with beta thalassaemia and from 1600 schoolchildren. The thalassaemia mutations were unevenly spread. Although 23 different beta-thalassaemia mutations were found, three accounted for the thalassaemia phenotype in about 70% of the patients, most whom are homozygotes or compound heterozygotes for IVS1-5 (G-->C) or IVS1-1 (G-->A). The third common mutation, codon 26 (G-->A), which produces HbE, interacts with one or other of these mutations to produce HbE/beta thalassaemia; this comprises 13.0-30.9% of cases in the main centres. Samples from 472 patients were analysed to determine the alpha-globin genotype. Overall, 15.5% patients were carriers for deletion forms of alpha+ thalassaemia. Average gene frequencies showed that there will be more than 2000 patients requiring treatment at any one time, in the future, of whom those with HbE/beta thalassaemia will account for about 40%. In Sri Lanka, interactions of the two common beta-thalassaemia alleles will nearly always result in a transfusion-dependent disorder. However, about 40% of patients will have HbE/beta thalassaemia, which has a variable course. The management of these disorders could require about 5% of the total health budget. We need to learn more about the natural history and appropriate management of HbE/beta thalassaemia if resources are to be used effectively.
  The Lancet 03/2000; 355(9206):786-91. · 38.28 Impact Factor
• Article: Rapid detection of alpha-thalassaemia deletions and alpha-globin gene triplication by multiplex polymerase chain reactions.

  Y T Liu, J M Old, K Miles, C A Fisher, D J Weatherall, J B Clegg
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  ABSTRACT: We describe a sensitive, reliable and reproducible method, based on three multiplex PCR assays, for the rapid detection of seven common alpha-thalassaemia deletions and one alpha-globin gene triplication. The new assay detects the alpha0 deletions - -SEA, - (alpha)20.5, - -MED, - -FIL and - -THAI in the first multiplex PCR, the second multiplex detects the -alpha3.7 deletion and alphaalphaalphaanti3.7 variant, the third multiplex detects the -alpha4.2 deletion. This simple multiplex method should greatly facilitate the genetic screening and molecular diagnosis of these determinants in populations where alpha-thalassaemias are prevalent.
  British Journal of Haematology 03/2000; 108(2):295-9. · 4.94 Impact Factor
• Article: Why are hemoglobin F levels increased in HbE/beta thalassemia?

  D C Rees, J B Porter, J B Clegg, D J Weatherall
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  ABSTRACT: To try to further define the mechanisms that increase the levels of hemoglobin F (HbF) in the blood of patients with severe forms of beta thalassemia, we have studied two comparable populations of hemoglobin E (HbE)/beta thalassemics, one regularly transfused and one receiving only occasional blood transfusions. Regular transfusion was associated with a significant decrease in soluble transferrin receptor and erythropoietin levels. Globin chain synthesis studies also show a highly significant decrease in HbF synthesis relative to HbE in the transfused patients. This effect was confirmed by sequential data on one patient, studied before and after the commencement of regular blood transfusion; blood transfusion was followed by a marked increase in the alpha/gamma, beta(E)/gamma, and HbE/HbF ratios. These data suggest that the high HbF levels in HbE/beta thalassemia, and other beta thalassemia syndromes, result from increased erythropoietin levels leading to bone marrow expansion, and possibly increased F-cell production, combined with ineffective erythropoiesis giving a survival advantage to F cells. This study also suggests that alteration in blood transfusion regimes must be taken into account when interpreting changes in HbF levels seen in trials of HbF-promoting drugs.
  Blood 12/1999; 94(9):3199-204. · 9.90 Impact Factor
• Source

  Available from: Tim E Peto

  Article: Prevention of cerebral malaria in children in Papua New Guinea by southeast Asian ovalocytosis band 3.

  S J Allen, A O'Donnell, N D Alexander, C S Mgone, T E Peto, J B Clegg, M P Alpers, D J Weatherall
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  ABSTRACT: Southeast Asian ovalocytosis (SAO) occurs at high frequency in malarious regions of the western Pacific and may afford a survival advantage against malaria. It is caused by a deletion of the erythrocyte membrane band 3 gene and the band 3 protein mediates the cytoadherence of parasitized erythrocytes in vitro. The SAO band 3 variant may prevent cerebral malaria but it exacerbates malaria anemia and may also increase acidosis, a major determinant of mortality in malaria. We undertook a case-control study of children admitted to hospital in a malarious region of Papua New Guinea. The SAO band 3, detected by the polymerase chain reaction, was present in 0 of 68 children with cerebral malaria compared with six (8.8%) of 68 matched community controls (odds ratio = 0, 95% confidence interval = 0-0.85). Median hemoglobin levels were 1.2 g/dl lower in malaria cases with SAO than in controls (P = 0.035) but acidosis was not affected. The remarkable protection that SAO band 3 affords against cerebral malaria may offer a valuable approach to a better understanding of the mechanisms of adherence of parasitized erythrocytes to vascular endothelium, and thus of the pathogenesis of cerebral malaria.
  The American journal of tropical medicine and hygiene 07/1999; 60(6):1056-60. · 2.59 Impact Factor
• Source

  Available from: David C Rees

  Article: Reduced soluble transferrin receptor concentrations in acute malaria in Vanuatu.

  T N Williams, K Maitland, D C Rees, T E Peto, D K Bowden, D J Weatherall, J B Clegg
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  ABSTRACT: Soluble transferrin receptor (sTfR) concentration is a sensitive index of iron deficiency when used in conjunction with ferritin measurements in adults. One advantage of this assay is that unlike ferritin it does not appear to be affected by a range of infectious and inflammatory conditions or by pregnancy, rendering it a promising adjunct to the diagnosis of iron deficiency in tropical populations. We have measured plasma sTfR concentrations in a group of malaria patients (n = 21) and asymptomatic (18) and aparasitemic (76) controls in Vanuatu. Plasma sTfR concentration was significantly reduced in individuals with acute malaria (P = 0.003). While this observation provides evidence that erythropoeitic suppression may be an important etiologic component in malarial anemia, it also suggests that malaria may be a confounding factor when interpreting sTfR concentrations in such populations. The role of sTfR in the diagnosis of iron deficiency in tropical populations remains to be established.
  The American journal of tropical medicine and hygiene 06/1999; 60(5):875-8. · 2.59 Impact Factor