In vivo evaluation of the effect of sickle cell hemoglobin S, C and therapeutic transfusion on erythrocyte metabolism and cardiorenal dysfunction

D’Alessandro, Angelo; Nouraie, Mehdi; Zhang, Yingze; Cendali, Francesca; Gamboni, Fabia; Reisz, Julie A.; Zhang, Xu; Bartsch, Kyle W; Galbraith, Matthew D.; Gladwin, Mark T.

doi:10.1002/ajh.26923

Cited by 14 publications

(23 citation statements)

References 80 publications

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“…As a result, we identified multiple signatures associated with cardiorenal dysfunction and hazard ratios, including alterations in tryptophan/kynurenine/indole metabolism, bile acid deconjugation, acyl-carnitine and S1P metabolism, glutaminolysis and mitochondrial dysfunction and L-arginine metabolism to citrulline and creatinine (Figure 7). Results are relevant in that they confirm and expand upon previous findings in the literature, linking metabolic differences 23 to clinically relevant outcomes and providing a metabolic window on clinical efficacy of common interventions like transfusion of packed RBCs and treatment with hydroxyurea. 39 For example, previous smaller scale studies had documented a beneficial effect of transfusion events in SCD in the circulating plasma and RBC metabolome, 40 though the scale of these studies was limited to a handful of recipients with no characterization of clinical relevant covariates.…”

Section: Discussionsupporting

confidence: 81%

“…Principal component analyses (PCA) and hierarchical clustering analyses (HCA) of all the metabolomics data showed a significant separation of plasma samples from individuals with SS genotypes compared to the other groups (Supplementary Figure 1.A-B). As previously noted, 23 despite double randomization of the samples and blinding of the analytical team, plasma creatinine levels measured via mass spectrometry significantly correlated with clinical measurement for this metabolite (Supplementary Figure 1.C).…”

Section: A) Results Extensively Reported Insupporting

confidence: 64%

“…An extended version of this section is provided in Supplementary Methods Extended, and our previous metabolomics report on RBC samples from the same cohort. 23 Ethical statement, blood collection, processing and storage A total of 596 SCD patients with available plasma samples were recruited as part of the Walk-PHaSST clinical trial (NCT00492531 at ClinicalTrials.gov and HLB01371616a BioLINCC study) under protocols approved by the University of Pittsburgh 9,24-28 . Clinical covariates were collected prior to plasma metabolomics analysis, including hemolysis, tricuspid regurgitation velocity (TRV), 29 parameters indicative of kidney function such as estimated glomerular filtration rate (eGFR), creatinine.…”

Section: Methodsmentioning

confidence: 99%

“…Clinical and plasma metabolomics data in this study, and RBC metabolomics data from our previous study 23 were collated into an online portal for real time data processing and figure generation. The portal, open and accessible at https://mirages.shinyapps.io/SCD2023/ serves as a repository for the data generated as part of this study, and as a tool to perform real time analyses and export of results upon correlation analyses between metabolites and clinical covariates, with the opportunity to modify filters (e.g.…”

Section: The Sickle Cell Disease Online Portal For Real Time Processi...mentioning

confidence: 99%

“…To bridge this gap, here we performed a metabolomics study of plasma from 596 SCD patients, for which extensive information on patients' demographics (sex, age, BMI), genotypes, hematological and clinical characteristics, as well as therapeutic interventions (transfusion events, as inferred from HbA %; hydroxyurea treatment) were available. Results from analyses in plasma were compared against the recently characterized RBC metabolome in this cohort 23 , identifying compartment-specific metabolic signatures associated with potential novel strategies for metabolic interventions in SCD.…”

Section: Introductionmentioning

confidence: 99%

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Metabolic signatures of cardiorenal dysfunction in plasma from sickle cell patients, as a function of therapeutic transfusion and hydroxyurea treatment

D’Alessandro

Nouraie

Zhang

et al. 2023

Preprint

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Metabolomics studies in sickle cell disease (SCD) have been so far limited to tens of samples, owing to technical and experimental limitations. To overcome these limitations, we performed plasma metabolomics analyses on 596 samples from patients with sickle cell sickle cell disease (SCD) enrolled in the WALK PHaSST study. Clinical covariates informed the biological interpretation of metabolomics data, including genotypes (hemoglobin SS, hemoglobin SC), history of recent transfusion (HbA%), response to hydroxyurea treatment (HbF%). We investigated metabolic correlates to the degree of hemolysis, cardiorenal function, as determined by tricuspid regurgitation velocity (TRV), estimated glomerular filtration rate (eGFR), and overall hazard ratio (unadjusted or adjusted by age). Recent transfusion events or hydroxyurea treatment were associated with elevation in plasma free fatty acids and decreases in acyl-carnitines, urate, kynurenine, indoles, carboxylic acids, and glycine- or taurine-conjugated bile acids. High levels of these metabolites, along with low levels of plasma S1P and L-arginine were identified as top markers of hemolysis, cardiorenal function (TRV, eGFR), and overall hazard ratio. We thus uploaded all omics and clinical data on a novel online portal that we used to identify a potential mechanism of dysregulated red cell S1P synthesis and export as a contributor to the more severe clinical manifestations in patients with the SS genotype compared to SC. In conclusion, plasma metabolic signatures, including low S1P, arginine and elevated kynurenine, acyl-carnitines and bile acids - are associated with clinical manifestation and therapeutic efficacy in SCD patients, suggesting new avenues for metabolic interventions in this patient population.

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Section: Discussionsupporting

confidence: 81%

Section: A) Results Extensively Reported Insupporting

confidence: 64%

Section: Methodsmentioning

confidence: 99%

Section: The Sickle Cell Disease Online Portal For Real Time Processi...mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Metabolic signatures of cardiorenal dysfunction in plasma from sickle cell patients, as a function of therapeutic transfusion and hydroxyurea treatment

D’Alessandro

Nouraie

Zhang

et al. 2023

Preprint

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Metabolic blood profile and response to treatment with the pyruvate kinase activator mitapivat in patients with sickle cell disease

van Dijk,

Ruiter,

van der Veen

et al. 2024

HemaSphere

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Mitapivat is an investigational, oral, small‐molecule allosteric activator of pyruvate kinase (PK). PK is a regulatory glycolytic enzyme that is key in providing the red blood cell (RBC) with sufficient amounts of adenosine triphosphate (ATP). In sickle cell disease (SCD), decreased 2,3‐DPG levels increase the oxygen affinity of hemoglobin, thereby preventing deoxygenation and polymerization of sickle hemoglobin. The PK activator mitapivat has been shown to decrease levels of 2,3‐DPG and increase levels of ATP in RBCs in patients with SCD. In this phase 2, investigator‐initiated, open‐label study (https://www.clinicaltrialsregister.eu/ NL8517; EudraCT 2019‐003438‐18), untargeted metabolomics was used to explore the overall metabolic effects of 8‐week treatment with mitapivat in the dose‐finding period. In total, 1773 unique metabolites were identified in dried blood spots of whole blood from ten patients with SCD and 42 healthy controls (HCs). The metabolic phenotype of patients with SCD revealed alterations in 139/1773 (7.8%) metabolites at baseline when compared to HCs (false discovery rate‐adjusted p < 0.05), including increases of (derivatives of) polyamines, purines, and acyl carnitines. Eight‐week treatment with mitapivat in nine patients with SCD altered 85/1773 (4.8%) of the total metabolites and 18/139 (12.9%) of the previously identified altered metabolites in SCD (unadjusted p < 0.05). Effects were observed on a broad spectrum of metabolites and were not limited to glycolytic intermediates. Our results show the relevance of metabolic profiling in SCD, not only to unravel potential pathophysiological pathways and biomarkers in multisystem diseases but also to determine the effect of treatment.

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A novel composition of endogenous metabolic modulators improves red blood cell properties in sickle cell disease

van Dijk,

Traets,

van Oirschot

et al. 2024

eJHaem

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The most common forms of sickle cell disease (SCD) are sickle cell anemia (SCA; HbSS) and HbSC disease. In both, especially the more dense, dehydrated and adherent red blood cells (RBCs) with reduced deformability are prone to hemolysis and sickling, and thereby vaso‐occlusion. Based on plasma amino acid profiling in SCD, a composition of 10 amino acids and derivatives (RCitNacQCarLKHVS; Axcella Therapeutics, USA), referred to as endogenous metabolic modulators (EMMs), was designed to target RBC metabolism. The effects of ex vivo treatment with the EMM composition on different RBC properties were studied in SCD (n = 9 SCA, n = 5 HbSC disease). Dose‐dependent improvements were observed in RBC hydration assessed by hemocytometry (MCV, MCHC, dense RBCs) and osmotic gradient ektacytometry (Ohyper). Median (interquartile range [IQR]) increase in Ohyper compared to vehicle was 4.9% (4.0%–5.5%), 7.5% (6.9%–9.4%), and 12.8% (11.5%–14.0%) with increasing 20×, 40×, and 80X concentrations, respectively (all p < 0.0001). RBC deformability (EImax using oxygen gradient ektacytometry) increased by 8.1% (2.2%–12.1%; p = 0.0012), 9.6% (2.9%–15.1%; p = 0.0013), and 13.3% (5.7%–25.5%; p = 0.0007), respectively. Besides, RBC adhesion to subendothelial laminin decreased by 43% (6%–68%; p = 0.4324), 58% (48%–72%; p = 0.0185), and 71% (49%–82%; p = 0.0016), respectively. Together, these results provide a rationale for further studies with the EMM composition targeting multiple RBC properties in SCD.

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In vivo evaluation of the effect of sickle cell hemoglobin S, C and therapeutic transfusion on erythrocyte metabolism and cardiorenal dysfunction

Cited by 14 publications

References 80 publications

Metabolic signatures of cardiorenal dysfunction in plasma from sickle cell patients, as a function of therapeutic transfusion and hydroxyurea treatment

Metabolic signatures of cardiorenal dysfunction in plasma from sickle cell patients, as a function of therapeutic transfusion and hydroxyurea treatment

Metabolic blood profile and response to treatment with the pyruvate kinase activator mitapivat in patients with sickle cell disease

A novel composition of endogenous metabolic modulators improves red blood cell properties in sickle cell disease

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