Prevalence and risk factors for pulmonary artery systolic hypertension among sickle cell disease patients in Nigeria

Aliyu, Zakari Y.; Gordeuk, Victor R.; Sachdev, Vandana; Babadoko, Aliyu; Mamman, Aisha Indo; Akpanpe, Peter; Attah, E B; Suleiman, Yusuf; Aliyu, Nurudeen; Yusuf, Jamilu; Mendelsohn, Laurel; Kato, Gregory J.; Gladwin, Mark T.

doi:10.1002/ajh.21162

Cited by 86 publications

(118 citation statements)

References 23 publications

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“…This signature was found to be composed of both novel and established PH candidate genes as evidenced by literature mining and the PubMed search tool. For example, ADORA2B, a candidate gene known to modify the severity of SCD (20,21), was recently identified via metabolomic profiling of a transgenic SCD mouse model with excessive adenosine signaling through the ADORA2B leading to sickling and hemolysis (22), processes known to be independently correlated with the presence of PH in SCD (13,23). Furthermore, ADC, another signature gene, which decarboxylates L-arginine to agmatine, is an established PAH candidate gene (24) and is potentially involved in SCD-related PH (25).…”

Section: Discussionmentioning

confidence: 99%

A Novel Molecular Signature for Elevated Tricuspid Regurgitation Velocity in Sickle Cell Disease

Desai¹,

Zhou²,

Ahmad

et al. 2012

Am J Respir Crit Care Med

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Rationale: An increased tricuspid regurgitation jet velocity (TRV . 2.5 m/s) and pulmonary hypertension defined by right heart catheterization both independently confer increased mortality in sickle cell disease (SCD). Objectives: We explored the usefulness of peripheral blood mononuclear cell-derived gene signatures as biomarkers for an elevated TRV in SCD. Methods: Twenty-seven patients with SCD underwent echocardiography and peripheral blood mononuclear cell isolation for expression profiling and 112 patients with SCD were genotyped for single-nucleotide polymorphisms. Measurements and Main Results: Genome-wide gene and miRNA expression profiles were correlated against TRV, yielding 631 transcripts and 12 miRNAs. Support vector machine analysis identified a 10-gene signature including GALNT13 (encoding polypeptide N-acetylgalactosaminyltransferase 13) that discriminates patients with and without increased TRV with 100% accuracy. This finding was then validated in a cohort of patients with SCD without (n ¼ 10) and with pulmonary hypertension (n ¼ 10, 90% accuracy). Increased TRV-related miRNAs revealed strong in silico binding predictions of miR-301a to GALNT13 corroborated by microarray analyses demonstrating an inverse correlation between their expression. A genetic association study comparing patients with an elevated (n ¼ 49) versus normal (n ¼ 63) TRV revealed five significant single-nucleotide polymorphisms within GALNT13 (P , 0.005), four trans-acting (P , 2.1 3 10 27) and one cis-acting (P ¼ 0.6 3 10 24 ) expression quantitative trait locus upstream of the adenosine-A2B receptor gene (ADORA2B). Conclusions: These studies validate the clinical usefulness of genomic signatures as potential biomarkers and highlight ADORA2B and GALNT13 as potential candidate genes in SCD-associated elevated TRV.

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Section: Discussionmentioning

confidence: 99%

A Novel Molecular Signature for Elevated Tricuspid Regurgitation Velocity in Sickle Cell Disease

Desai¹,

Zhou²,

Ahmad

et al. 2012

Am J Respir Crit Care Med

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“…Some studies have found an association of high hemoglobin F with lower pulmonary hypertension risk, [11][12][13][14] but several others have detected no such association. 1,2,[15][16][17][18] We recently reported a prospective, multicenter study of 310 children and adolescents with sickle cell disease at steady state in which tricuspid regurgitation velocity of 2.6 m/s or higher occurred in 11% of participants and had independent associations with hemolysis and hemoglobin oxygen desaturation. 3 In addition, we have found that an elevated screening tricuspid regurgitation velocity in children and adolescents with sickle cell disease predicts functional impairment over 2 years of follow-up (V.R.G., unpublished observations, April 2009).…”

Section: Introductionmentioning

confidence: 99%

Relationship of erythropoietin, fetal hemoglobin, and hydroxyurea treatment to tricuspid regurgitation velocity in children with sickle cell disease

Gordeuk

Campbell

Rana

et al. 2009

Blood

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Hydroxyurea and higher hemoglobin F improve the clinical course and survival in sickle cell disease, but their roles in protecting from pulmonary hypertension are not clear. We studied 399 children and adolescents with sickle cell disease at steady state; 38% were being treated with hydroxyurea. Patients on hydroxyurea had higher hemoglobin concentration and lower values for a hemolytic component derived from 4 markers of hemolysis (P ≤ .002) but no difference in tricuspid regurgitation velocity compared with those not receiving hydroxyurea; they also had higher hemoglobin F (P < .001) and erythropoietin (P = .012) levels. Hemoglobin F correlated positively with erythropoietin even after adjustment for hemoglobin concentration (P < .001). Greater hemoglobin F and erythropoietin each independently predicted higher regurgitation velocity in addition to the hemolytic component (P ≤ .023). In conclusion, increase in hemoglobin F in sickle cell disease may be associated with relatively lower tissue oxygen delivery as reflected in higher erythropoietin concentration. Greater levels of erythropoietin or hemoglobin F were independently associated with higher tricuspid regurgitation velocity after adjustment for degree of hemolysis, suggesting an independent relationship of hypoxia with higher systolic pulmonary artery pressure. The hemolysis-lowering and hemoglobin F–augmenting effects of hydroxyurea may exert countervailing influences on pulmonary blood pressure in sickle cell disease.

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“…It is one of the most common monogenetic disorders in the world, affecting nearly 1 in 600 African Americans (3) and an estimated 1 to 4% of babies born in sub-Saharan Africa (4). The resulting hemolytic anemia is most severe in patients homozygous for the sickle hemoglobin (HbS) gene mutation (Hb-b; glu6val).…”

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Pulmonary Complications of Sickle Cell Disease

Gladwin

Vichinsky²

2008

N Engl J Med

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Sickle cell disease (SCD) is a common monogenetic disorder with high associated morbidity and mortality. The pulmonary complications of SCD are of particular importance, as acute chest syndrome and pulmonary hypertension have the highest associated mortality rates within this population. This article reviews the pathophysiology, diagnosis, and treatment of clinically significant pulmonary manifestations of SCD, including acute chest syndrome, asthma, and pulmonary hypertension in adult and pediatric patients. Clinicians should be vigilant in screening and treating such comorbidities to improve patient outcomes.

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Prevalence and risk factors for pulmonary artery systolic hypertension among sickle cell disease patients in Nigeria

Cited by 86 publications

References 23 publications

A Novel Molecular Signature for Elevated Tricuspid Regurgitation Velocity in Sickle Cell Disease

A Novel Molecular Signature for Elevated Tricuspid Regurgitation Velocity in Sickle Cell Disease

Relationship of erythropoietin, fetal hemoglobin, and hydroxyurea treatment to tricuspid regurgitation velocity in children with sickle cell disease

Pulmonary Complications of Sickle Cell Disease

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