miRNA profile and disease severity in patients with sickle cell anemia

Abstract A single point mutation in the β hemoglobin gene causes sickle cell disease (SCD), but patients have extremely variable phenotypes. Hemolysis-related complications include pulmonary hypertension (PHT), priapism, stroke and leg ulceration; blood viscosity and sickle vasoocclusion are associated with painful episodes, acute chest syndrome and osteonecrosis. Predicting who is at highest risk of death would be useful therapeutically and prognostically. Applying Bayesian network modeling that describes complex interactions among many variables by factorizing their joint probability distribution into modules, to data from 3380 SCD patients, we constructed a disease severity score (DSS: 0, least severe; 1, most severe), defining severity as risk of death within 5 years. A network of 24 variables described complex associations among clinical and laboratory complications of SCD. The analysis was validated in 140 patients whose SCD severity was assessed by expert clinicians and 210 adults where severity was also assessed by the echocardiographic diagnosis of PHT and death. Information about PHT allowed a comparison of the DSS with the tricuspid regurgitant jet velocity (TRJV), an objective marker of PHT and an independent risk factor for death. DSS and three indices of clinical severity (severity ranking of individuals by expert clinicians; objective measurement of the presence and severity of PHT; risk of prospective death) were correlated. Among living subjects, the median score was 0.57 in 135 patients without PHT, 0.64 in 40 patients with mild PHT and 0.86 in 15 patients with severe PHT. The difference in average score between living patients with and without PHT is significant. The same increasing trend was noticeable in the subjects who died during follow-up: 0.60 in subjects without PHT; 0.68 in subjects with mild PHT; 0.79 in subjects with severe PHT. The utility of the DSS is also supported by the ability to assign a score to subjects for whom the TRJV cannot be measured. Surprisingly, besides known risk factors like renal insufficiency and leukocytosis, we identified the intensity of hemolytic anemia and clinical events associated with hemolytic anemia as contributing to risk for death. Priapism, an excellent reflection of the hemolytic anemia-related complications of SCD, is associated with PHT and its association with death was unexpected. Laboratory variables predictive of disease severity included LDH and reticulocytes that reflect the intensity of hemolytic anemia. Elevated systolic blood pressure increased the odds of death by 3.4, consistent with hypertension as a marker of early death in SCD. Subjects with sickle cell anemia are at greatest risk compared with subjects with sickle cell anemia-α thalassemia and with subjects with HbSC disease. Our model suggests that the intensity of hemolytic anemia, estimated by LDH, reticulocyte count and AST, and shown previously to be associated with PHT, priapism, leg ulceration and possibly stroke, is an important contributor to death. This model can be used to compute a personalized measure of disease severity that might be useful for guiding therapeutic decisions and designing clinical trials.

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The relationship between fetal hemoglobin and disease severity in children with sickle cell anemia

American Journal of Medical Genetics ◽

10.1002/ajmg.1320270305 ◽

1987 ◽

Vol 27 (3) ◽

pp. 525-535 ◽

Cited By ~ 24

Author(s):

Daniel J. Odenheimer ◽

Sharada A. Sarnaik ◽

Charles F. Whitten ◽

Donald L. Rucknagel ◽

Charles F. Sing ◽

...

Keyword(s):

Disease Severity ◽

Sickle Cell ◽

Sickle Cell Anemia ◽

Fetal Hemoglobin ◽

The Relationship

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The HBG2 rs7482144 (C > T) Polymorphism is Linked to HbF Levels but not to the Severity of Sickle Cell Anemia

Journal of Pediatric Genetics ◽

10.1055/s-0041-1733950 ◽

2021 ◽

Author(s):

Bhaskar V. K. S. Lakkakula ◽

Smaranika Pattnaik

Keyword(s):

Disease Severity ◽

Sickle Cell ◽

Sickle Cell Anemia ◽

High Performance ◽

Complete Blood Count ◽

Small Sample Size ◽

Severe Disease ◽

Small Sample ◽

Total Leucocyte Count ◽

Severity Scores

AbstractSickle cell anemia (SCA) is a severe disease characterized by anemia, acute clinical complications, and a relatively short life span. In this disease, abnormal hemoglobin makes the red blood cells deformed, rigid, and sticky. Fetal hemoglobin (HbF) is one of the key modulators of SCA morbidity and mortality. Interindividual HbF variation is a heritable trait that is controlled by polymorphism in genes linked and unlinked to the hemoglobin β gene (HBB). The genetic polymorphisms that determine HbF levels are known to ameliorate acute clinical events. About 190 well-characterized homozygous SCA patients were included in this study. Complete blood count (CBC), high-performance liquid chromatography (HPLC), and clinical investigations were obtained from patient's records. Severity scores were determined by using the combination of anemia, complications, total leucocyte count, and transfusion scores. HBG2 rs7482144 polymorphism was genotyped by using the polymerase chain reaction and restriction fragment length polymorphism. The association between HBG2 rs7482144 polymorphism and HbF levels as well as the disease severity of SCA were assessed. SCA patients carrying TT genotype were found to have higher HbF levels. In addition, SCA patients with increased severity showed significantly lower levels of hemoglobin, HbF, and hematocrit values. However, the genotypes of HBG2 rs7482144 polymorphism were not found to be associated with the risk of disease severity. In summary, this study demonstrated that HBG2 rs7482144 polymorphism is linked with HbF levels, but it does not affect disease severity. The sample sizes used and the pattern of association deduced from our small sample size prevents us from extrapolating our findings further.

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Therapeutic Intervention and Decision-Making by Parents of Children with Severe Sickle Cell Anemia.

Blood ◽

10.1182/blood.v106.11.3193.3193 ◽

2005 ◽

Vol 106 (11) ◽

pp. 3193-3193

Author(s):

Jane Hankins ◽

Sara Day ◽

Yvonne Carroll ◽

Paula Naidu ◽

Pam Hinds ◽

...

Keyword(s):

Decision Making ◽

Disease Severity ◽

Sickle Cell ◽

Sickle Cell Anemia ◽

Treatment Preference ◽

Medical Decision ◽

Risk Of Death ◽

Time Commitment ◽

Risks And Benefits ◽

Factors Influencing

Abstract Recurrent vaso-occlusive events in children with sickle cell anemia (SCA) prompt consideration of intervention with one of 3 treatments: hydroxyurea (HU), chronic red cell transfusion (CT) or stem cell transplant (SCT). Differing risks and benefits and a lack of randomized trials make it difficult to determine the best strategy. The preference of parents/caregivers (PC) is an important element in the decision process. To address these issues, we have completed a study with the following objectives: 1) To explore factors that influence PC decision-making (DM) regarding interventions, 2) To examine relationships between treatment preference and health-related quality of life (HRQOL). Severe SCA was defined as ≥3 pain events requiring ER visits or hospitalization within 12 months, or ≥2 acute chest syndrome events within 24 months, or a combination. PC were given literature in layman’s language describing the treatments and later participated in a standardized discussion about treatment risks and benefits with an educator. PC then completed a 10-minute survey, which explored factors influencing treatment preference, and the HRQOL Peds QL 4.0 inventory. The survey had 40 questions grouped in different categories, including efficacy, safety, emotional factors, and practicability. HRQOL included physical, emotional, social and school functioning domains. Thirty PC were interviewed, 83% were female with a median age of 36 years (range 24–50); all were African-American. Twenty-two (73 %) PC felt they received enough information to make a choice and 26 (87%) thought their children needed treatment. Twenty-one (70%) PC expressed preference for HU, 3 (10%) for SCT, 5 (17%) for CT, one (3%) was undecided, and none preferred no treatment (p<0.001). The most common factors influencing PC choice were efficacy (n=29, 97%), and safety (n=24, 80%). Among the possible factors influencing preference, those significantly different among treatment groups are shown in the table. Motivation for Treatment Preference Factor* HU(%) SCT(%) CT(%) * p<.05 for differences among groups Safer 19(90) 2(67) 3(60) Fewer side effects 18(86) 3(100) 3(60) Less time commitment 5(24) 0 0 Less family impact 13(62) 3(100) 3(60) Concerns with disease severity 13(62) 2(67) 3(60) Concerns with death risk 9(43) 2(67) 3(60) “ Treatment is the best for my child” 16(76) 3(100) 2(40) Patient’s fear 5(24) 2(67) 3(60) The HRQOL median scores, on a 0 to 100 scale, were 51 (range: 28–91), 66 (range: 64–90), and 56 (range: 53–77) among the HU, SCT, and CT groups respectively (p=0.2). We conclude that: HU was the most often preferred treatment option of PC of children with severe SCA. Efficacy and safety were the most common concerns influencing treatment preference, PC preferring SCT appear to have a distinct profile, with more concerns regarding disease severity and risk of death, greater endorsement of the “good parent concept”, and a perception of lower toxicity with the treatment. This may seem incongruent given the higher toxicity of SCT, but may reflect a perception of less long-term SCA-related complications (due to a possible cure). HU-preferring PC appear to have greater appreciation of treatment safety and time-commitment, and less concerns with the risk of death and patients’ fears. There were no differences in HRQOL among the groups. Improved understanding of caregivers’ preferences and their DM process will aid in the design of future clinical trials and medical decision-making.

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A Repertoire of Genes Modifying the Risk of Death in Sickle Cell Anemia.

Blood ◽

10.1182/blood.v110.11.150.150 ◽

2007 ◽

Vol 110 (11) ◽

pp. 150-150

Author(s):

Paola Sebastiani ◽

Ling Wang ◽

Thomas Perls ◽

Dellara F. Terry ◽

Monty Montano ◽

...

Keyword(s):

Disease Severity ◽

Sickle Cell ◽

Sickle Cell Anemia ◽

Severity Score ◽

Association Studies ◽

Acute Chest Syndrome ◽

Risk Of Death ◽

Genome Wide ◽

Laboratory Variables ◽

Individual Disease

Abstract Phenotypic heterogeneity is a well known characteristic of sickle cell anemia. Patients have different rates of hemolysis-related complications, like pulmonary hypertension, priapism and leg ulceration, and viscosity/vasoocclusion-related complications, like painful episodes, acute chest syndrome and osteonecrosis; they also have variation in levels of HbF and hematocrit. To integrate individual disease variables into a global measure of severity, we developed a Bayesian network model that described the complex associations of 25 clinical and laboratory variables, deriving a score that we used to define disease severity (0, least severe to 1, most severe) as the risk of death within 5 years (Sebastiani et al, Blood 2007). This initial network, validated in 2 unrelated patient populations, did not incorporate the genetic heterogeneity that is likely to modulate its components. Accordingly, we studied the association of single nucleotide polymorphisms (964 SNPs) in candidate genes (315 genes) using a Bayesian beta regression model of the severity score in 741 HBB glu6val homozygotes, aged more than 18 years. Forty-three SNPs in about 25 genes were associated with disease severity. Some associated SNPs tag genes that affect nitric oxide and oxidative biology and the endothelium, such as NOS1, ASS, KL, HMOX1, ECE1, KDR, FLT1. Homozygosity for an intronic SNP in ECE1 is associated with a increase of severity (OR=3.5). As expected, some associations were consistent with our previous findings. For example, the same SNP in ECE1 and TGFBR3, that was highly predictive of severity, was also strongly associated with sickle cell stroke (Sebastiani et al, Nature Genet 2005). Also, the association with severity of genes in the TGF-beta signaling pathway, including BMP6 and TGFBR3, were also associated with individual disease complications. Other associated genes play a less obvious role in the pathobiology of disease, e.g., HAO2, but are very strongly associated with the phenotype of severity (probability of a chance association, for HAO2, 10−6). Several of the genes associated with severity, including KL, PRKCA, FLT1 and MET have been related to aging, as suggested by gene expression profiling and studies in model organisms for aging. In genome-wide studies of the genetic basis of exceptional longevity, we found associations with some of the same genes that were associated with severity in sickle cell anemia. Perhaps increased oxidative stress, and the relentless progression of vasculopathy in sickle cell anemia, cause accelerated tissue damage that is modulated by a set of genes similar to those involved in the normal aging process. We suggest that the disease severity score can be used as a phenotype integrating many features of the disease, for genetic association studies. As we add the results of unbiased genome-wide association studies to capture polymorphisms not included in candidate gene studies, we can develop a predictive network with even greater reliability than one using only clinical and laboratory variables. Such networks might also identify pathways that could be targeted to alter the course of disease.

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Spleen Function in Infants with Sickle Cell Anemia: Baseline Data from the BABY HUG Trial.

Blood ◽

10.1182/blood.v112.11.1416.1416 ◽

2008 ◽

Vol 112 (11) ◽

pp. 1416-1416 ◽

Cited By ~ 2

Author(s):

Zora R. Rogers ◽

Renee C. Rees ◽

Beatrice Files ◽

Rathi V. Iyer ◽

Barry L. Shulkin ◽

...

Keyword(s):

Disease Severity ◽

Sickle Cell ◽

Sickle Cell Anemia ◽

Surrogate Markers ◽

Spleen Volume ◽

Sulfur Colloid ◽

Splenic Sequestration ◽

History Of ◽

Splenic Uptake ◽

99Mtc Sulfur Colloid

Abstract The Pediatric Hydroxyurea [HU] Phase III Clinical Trial [BABY HUG], an NHLBI and NICHD sponsored double-blind placebo-controlled 14 center trial (NCT00006400), was designed to critically assess the efficacy of HU in preventing chronic organ damage in infants with sickle cell anemia [SCA]. The spleen is among the first organs damaged in SCA, but loss of function is variable among patients and difficult to measure. Pretreatment splenic filtrative function as determined by uptake on 99mTc sulfur colloid liver-spleen [LS] scan was compared to surrogate markers of spleen function: pocked erythrocyte [PIT] counts and flow cytometric quantitation of Howell-Jolly Bodies [HJB]. Splenic uptake of 99mTc sulfur-colloid was qualitatively interpreted by structured consensus of 3 pediatric nuclear medicine physicians. Results were correlated with age, total hemoglobin [Hb], fetal hemoglobin[HbF], white blood cell [WBC], platelet [PLT], absolute neutrophil count [ANC], reticulocyte count [RETIC], spleen volume [SVOL] on ultrasound, maximum TCD velocity [TCD], glomerular filtration rate determined by 99mTc-DTPA [GFR], steady state oxygen saturation [O2], as well as clinical features of SCA (presence of a palpable spleen at screening, history of splenic sequestration, dactylitis, other vaso-occlusive event or transfusion). A logarithmic transformation was applied to each parameter (except age) to improve linearity with other variables and stabilize the variance of the transformed data. LS scans were available for 205 (89 male; mean age 13 mos, range 8–18 mos) of the 233 subjects who were recruited without regard to disease severity. To date 170 scans have been adjudicated into 1 of 3 categories of uptake: normal (n=21, 12.4%), reduced (n=124, 72.9%) and absent (n=25, 14.7%). Both surrogate markers of spleen function, PIT and HJB, increased with decreasing splenic function [p<.001] and correlated well with each other [R2=.57, p<.001]. Patients with absent splenic uptake had a significantly higher mean age (14.6 mos) than those with normal (12.3 mos) or reduced uptake (12.5 mos) [p=.001]. Higher PIT, HJB, WBC, RETIC, TCD and lower Hb or HbF values were significantly associated with decreased LS scan uptake [p<.001]. PLT [p=.002] and ANC [p=.02] were also differentiated by categorical spleen function, while DTPA and O2 were not. SVOL was also not associated with spleen function as assessed by LS scan, PIT, or HJB, but was associated with a palpable spleen at screening [p=.001]. Patients with diminished spleen function on LS scan were more likely to have a history of splenic sequestration [p=.027], dactylitis [p=.025], transfusion [p=.014], and vaso-occlusive events [p=.005]. Higher PIT and HJB values were associated with a history of splenic sequestration [p≤.001], palpable spleen at screening [p≤.003] and transfusion [p<.001]. No child with a normal spleen scan had a palpable spleen at screening or a history of splenic sequestration or transfusion. This is the largest structured assessment of spleen function in SCA reported to date. Baseline data from the BABY HUG trial confirms that loss of spleen function begins in the first year of life and is associated with indicators of disease severity such as lower Hb and HbF, higher WBC, and history of splenic enlargement. We conclude that a palpable spleen may not be a functional one, and that spleen volume is unrelated to function. Surrogate assessments, PIT and HJB, correlate well with LS scan results and may obviate the need for radionuclide exposure to determine splenic function. With these 3 methods to assess spleen function the BABY HUG trial is well positioned to determine whether HU impacts the loss of spleen function and the utility of surrogate markers to monitor that effect.

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Circulating Endothelial Cells: A Potential Parameter of Organ Damage in Sickle Cell Anemia?

Blood ◽

10.1182/blood.v112.11.4798.4798 ◽

2008 ◽

Vol 112 (11) ◽

pp. 4798-4798

Author(s):

Michiel Strijbos ◽

Precious Landburg ◽

Erfan Nur ◽

Bart J. Biemond ◽

Frank Leebeek ◽

...

Keyword(s):

Endothelial Cells ◽

Disease Severity ◽

Sickle Cell ◽

Sickle Cell Anemia ◽

Endothelial Activation ◽

Organ Damage ◽

Circulating Endothelial Cells ◽

Laboratory Markers ◽

Leukocyte Counts ◽

Painful Crisis

Abstract Traditional laboratory markers of disease severity (Hb concentrations, HbF%, LDH concentrations and leukocyte counts) are not powerful enough to identify individuals with sickle cell disease (SCD) at high risk of complications. In several disease states, the number of circulating endothelial cells (CEC) is indicative of the extent of vascular disease and several small studies employing cumbersome techniques have shown increased CEC to occur in SCD as well. In this pilot study we determined if, by employing the CellSearch system, elevated CEC can be detected in SCD and whether the CEC count is related to the presence of organ damage, painful crisis frequency, traditional laboratory markers of disease severity as well as markers of endothelial activation. Peripheral blood was collected from 15 sickle cell patients and 15 healthy sex, age and race matched HbAA controls. Cells positive for CD146 (present on endothelial cells) are immuno-magnetically isolated and stained with nuclear DAPI and anti-CD105 (present on endothelial cells) and anti-CD45 (pan-leukocyte marker). Within the CD146 enriched cell suspension, cells meeting the DAPI+/CD146+/CD105+/CD45− criteria after image cytometry are designated CEC. CEC counts were significantly higher in sickle cell patients (12 cells/mL, IQR 8–29) as compared to controls (4 cells/mL, 3–10) (p=0.007). CEC counts were significantly higher in patients with pulmonary hypertension (PHT) (p=0.02), and increased with the presence of number of affected organs as well (0–4 involved organs, p=0.03), with the number of affected organs being the most important determinant of increased CEC numbers in SCD (R2=0.72, P=0.001). No statistically significant correlation was detected between CEC counts and markers of endothelial activation (serum sVCAM-1 and plasma VWF:Ag levels). CEC counts did not differ between patients on hydroxyurea and those who did not use hydroxyurea. No statistically significant correlations were detected between CEC counts and painful crisis frequency, Hb, HbF%, leukocyte counts, LDH concentrations. In conclusion, elevated CEC’s can be demonstrated in the clinically asymptomatic state in patients with sickle cell anemia with a validated and automated technique and, for the first time, a relation of CEC counts to SCD related organ damage is demonstrated. Furthermore, the extent of EC activation (as assessed by sVCAM-1 and VWF:Ag levels) is not necessarily related to the extent of EC damage (as assessed by CEC counts).

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