The hematologic characteristics of sickle cell anemia bearing the Bantu haplotype: the relationship between G gamma and HbF level

Nagel, Ronald L.; Rao, Srinivas K; Dunda-Belkhodja, O; Connolly, Mary M.; Fabry, Mary E.; Georges, Alan; Krishnamoorthy, Rajagopal; Labie, Dominique

doi:10.1182/blood.v69.4.1026.1026

Cited by 96 publications

(29 citation statements)

References 11 publications

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“…HbF level is partly controlled by genetic variation at the HBB cluster, although the exact responsible functional cis elements remain largely unknown (Dover et al, 1981;Nagel et al, 1985Nagel et al, , 1987Steinberg, 2005;Lettre et al, 2008;Galarneau et al, 2010). We found a clear connection between HbF level and SNP-defined b S -haplotypes in children with SCA.…”

Section: Discussionmentioning

confidence: 53%

Acute chest syndrome is associated with single nucleotide polymorphism‐defined beta globin cluster haplotype in children with sickle cell anaemia

et al. 2013

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Summary Genetic diversity at the human β-globin locus has been implicated as a modifier of sickle cell anaemia (SCA) severity. However, haplotypes defined by restriction fragment length polymorphism sites across the β-globin locus have not been consistently associated with clinical phenotypes. To define the genetic structure at the β-globin locus more thoroughly, we performed high-density single nucleotide polymorphism (SNP) mapping in 820 children who were homozygous for the sickle cell mutation (HbSS). Genotyping results revealed very high linkage disequilibrium across a large region spanning the locus control region and the HBB (β-globin gene) cluster. We identified three predominant haplotypes accounting for 96% of the βS-carrying chromosomes in this population that could be distinguished using a minimal set of common SNPs. Consistent with previous studies, fetal haemoglobin level was significantly associated with βS-haplotypes. After controlling for covariates, an association was detected between haplotype and rate of hospitalization for acute chest syndrome (ACS) (incidence rate ratio 0.51, 95% confidence interval 0.29–0.89) but not incidence rate of vaso-occlusive pain or presence of silent cerebral infarct (SCI). Our results suggest that these SNP-defined βS-haplotypes may be associated with ACS, but not pain or SCI in a study population of children with SCA.

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Section: Discussionmentioning

confidence: 53%

Acute chest syndrome is associated with single nucleotide polymorphism‐defined beta globin cluster haplotype in children with sickle cell anaemia

et al. 2013

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“…The association of b-globin-like gene cluster haplotype with the severity of sickle cell anaemia must be cautiously interpreted and the prognostic value of knowing the haplotype in an individual is very limited. Studies of several different ethnic groups of patients with sickle cell anaemia with distinct haematological characteristics suggested that the b-globin gene cluster haplotype may be useful as one predictor of disease severity (Labie et al, 1985;Hattori et al, 1986;Kulozik et al, 1986Kulozik et al, , 1987Nagel et al, 1987;Ragusa et al, 1988;Sharon et al, 1988;Srinivas et al, 1988;Labie et al, 1989;Schroeder et al, 1989;Month et al, 1990;Ballas et al, 1991;Dimovski et al, 1991;Powars, 1991a,b;Nagel & Fleming, 1992;Zago et al, 1992;Ö ner et al, 1992). In the first studies of Africans and Indian patients, most patients were homozygous for a haplotype and genetically homogeneous compared with their descendants in developed countries studied subsequently.…”

Section: Fetal Haemoglobinmentioning

confidence: 99%

Predicting clinical severity in sickle cell anaemia

2005

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Summary The ability to predict the phenotype of an individual with sickle cell anaemia would allow a reliable prognosis and could guide therapeutic decision making. Some risk factors for individual disease complications are known but are insufficiently precise to use for prognostic purposes; predicting the global disease severity is not yet possible. Genetic association studies, which attempt to link gene polymorphisms with selected disease subphenotypes, may eventually provide useful methods of foretelling the likelihood of certain complications and allow better individualized treatment.

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“…Comparison with other series suggests that the natural history of SCA in Guadeloupe is more similar to that in Jamaica with regard to those reported in Europe and the United States, suggesting a potential impact of environmental factors on the clinical course of the disease. haplotype (8)(9)(10)(11). Both affect the primary event of the SCA pathophysiological process, namely the intracellular polymerization of deoxyhemoglobin S which leads the red blood cell to sickle.…”

mentioning

confidence: 99%

Sickle cell anemia in Guadeloupean children: pattern and prevalence of acute clinical events

Tarer

Etienne‐Julan

Diara

et al. 2006

European J of Haematology

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We analyzed the records of 153 Guadeloupean children with sickle cell anemia (SCA), for whom clinical and laboratory data were prospectively collected (mean follow-up duration 8.4 +/- 4.6 yr). Prevalence and age-specific frequencies of acute clinical events were determined and correlations between complications, hematological parameters and potential modulating factors investigated. Painful crisis and acute chest syndrome (ACS) were the two most common complications, affecting 65.4% and 58.8% of the patients, respectively. The frequency of acute anemia was 49.7% (acute splenic sequestration 24.8%; acute aplastic anemia 15.0%). Prevalences of septicemia-meningitis and osteomyelitis were 15.7% and 16.3%, respectively. A higher incidence of infections, painful crises and acute anemia was detected in patients who developed ACS. The well-documented protective effect of HbF level on the overall disease expression was observed with higher HbF level in asymptomatic than in symptomatic patients (17.5% +/- 8% vs. 9.9% +/- 6.4%, P = 0.01) with similar ages and sex ratio. It was also confirmed on ACS and, for the first time, further extended to acute anemic events and septicemia. Besides its effect on hematological parameters, alpha-thalassemia seems to have little impact on the prevalence of complications, as do beta(S)-globin haplotypes. Comparison with other series suggests that the natural history of SCA in Guadeloupe is more similar to that in Jamaica with regard to those reported in Europe and the United States, suggesting a potential impact of environmental factors on the clinical course of the disease.

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The hematologic characteristics of sickle cell anemia bearing the Bantu haplotype: the relationship between G gamma and HbF level

Cited by 96 publications

References 11 publications

Acute chest syndrome is associated with single nucleotide polymorphism‐defined beta globin cluster haplotype in children with sickle cell anaemia

Acute chest syndrome is associated with single nucleotide polymorphism‐defined beta globin cluster haplotype in children with sickle cell anaemia

Predicting clinical severity in sickle cell anaemia

Sickle cell anemia in Guadeloupean children: pattern and prevalence of acute clinical events

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