The role of anaemia in oxidative and genotoxic damage in transfused β-thalassaemic patients
Articolo
Data di Pubblicazione:
2017
Abstract:
OBJECTIVES:
Redox imbalance and genotoxic damage are commonly observed in β thalassaemic patients. The aim of this study was to assess the role of anaemia in oxidative and genotoxic damage in regularly transfused thalassaemic patients, undergoing iron chelation therapy.
METHODS:
We studied the relationships of haematological, biochemical and clinical parameters with oxidative (reactive oxygen species and 8-oxo-7,8-dihydro-2'-deoxyguanosine) and genotoxic biomarkers (Comet assay and cytokinesis-block micronucleus test) in blood samples from 105 patients. To reduce the early effect of redox-active iron, samples were collected when pharmacokinetics of the iron chelators ensured their maximum effectiveness. The transfusion regimen, cardiac and hepatic magnetic resonance imaging T2* were evaluated to characterize the patient cohort. Labile plasma iron (LPI) was also assayed.
RESULTS:
Haemoglobin level had a significant effect on ROS, %DNA in the tail and micronuclei-micronucleated cell frequency (p < 0.05). Higher Hb values reduced redox imbalance. LPI, detectable in 50.5% of patients, was related to the number of apoptotic and necrotic lymphocytes (p = 0.03), demonstrating the cytotoxic effect of iron.
DISCUSSION:
The results highlight that an adequate transfusion regimen is essential to limit oxidative and genotoxic damage in β-thalassemic patients undergoing chelation therapy.
CONCLUSION:
Owing to the higher risk of cancer in the thalassaemic cohorts, specific genotoxicity/oxidative biomarkers should be monitored in order to ameliorate and formulate more personalized disease management.
Redox imbalance and genotoxic damage are commonly observed in β thalassaemic patients. The aim of this study was to assess the role of anaemia in oxidative and genotoxic damage in regularly transfused thalassaemic patients, undergoing iron chelation therapy.
METHODS:
We studied the relationships of haematological, biochemical and clinical parameters with oxidative (reactive oxygen species and 8-oxo-7,8-dihydro-2'-deoxyguanosine) and genotoxic biomarkers (Comet assay and cytokinesis-block micronucleus test) in blood samples from 105 patients. To reduce the early effect of redox-active iron, samples were collected when pharmacokinetics of the iron chelators ensured their maximum effectiveness. The transfusion regimen, cardiac and hepatic magnetic resonance imaging T2* were evaluated to characterize the patient cohort. Labile plasma iron (LPI) was also assayed.
RESULTS:
Haemoglobin level had a significant effect on ROS, %DNA in the tail and micronuclei-micronucleated cell frequency (p < 0.05). Higher Hb values reduced redox imbalance. LPI, detectable in 50.5% of patients, was related to the number of apoptotic and necrotic lymphocytes (p = 0.03), demonstrating the cytotoxic effect of iron.
DISCUSSION:
The results highlight that an adequate transfusion regimen is essential to limit oxidative and genotoxic damage in β-thalassemic patients undergoing chelation therapy.
CONCLUSION:
Owing to the higher risk of cancer in the thalassaemic cohorts, specific genotoxicity/oxidative biomarkers should be monitored in order to ameliorate and formulate more personalized disease management.
Tipologia CRIS:
14.a.1 Articolo su rivista
Keywords:
anaemia, Comet assay; cytokinesis-block micronucleus, Genotoxicity, iron chelators, iron overload; oxidative damage, transfusion therapy, Adult; Anemia; Biomarkers, Blood Transfusion, Comet Assay, Female; Humans, Iron, Iron Overload; Liver, Lymphocytes, Male; Micronucleus Tests, Middle Aged; Reactive Oxygen Species, beta-Thalassemia, DNA Damage, Oxidative Stress, Medicine (all), Hematology
Elenco autori:
Ferro, Elisa; Visalli, Giuseppa; LA ROSA, maria angela; Civa, Rosa; Papa, Gaetano Randazzo; D’Ascola, Domenico Giuseppe; Roccamo, Gaetano; Piraino, Basilia; SALPIETRO DAMIANO, Carmelo; DI PIETRO, Angela
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