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Hemoglobin
international journal for hemoglobin research
Volume 43, 2019 - Issue 1
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Original Article

Role of Genomic Biomarkers in Increasing Fetal Hemoglobin Levels Upon Hydroxyurea Therapy and in β-Thalassemia Intermedia: A Validation Cohort Study

Alexandra KolliopoulouUniversity of Patras, Medical Faculty, Laboratory of General Biology, Patras, Greece; View further author information
,
Stavroula SiamoglouSchool of Health Sciences, Department of Pharmacy, Laboratory of Pharmacogenomics and Individualized Therapy, University of Patras, Greece; View further author information
,
Anne JohnUnited Arab Emirates University, College of Medicine and Health Sciences, Department of Pathology, Al-Ain, United Arab Emirates; View further author information
,
Argyro SgourouSchool of Science and Technology, Biology Laboratory, Hellenic Open University, Patras, Greece; View further author information
,
Alexandra KourakliThalassemia and Hemoglobinopathies Unit, Hematology Division, Department of Internal Medicine, University of Patras Medical School, University Hospital, Patras, Greece; View further author information
,
Argiris SymeonidisMedical School, Hematology Division, Department of Internal Medicine, University of Patras, University of Patras, Greece; View further author information
,
Efthymia VlachakiAdults Thalassemia Unit, ‘Hippokration’ General Hospital of Thessaloniki, Greece; View further author information
,
Panagiota ChalkiaThalassemia and Sickle Cell Unit, University General Hospital of Thessaloniki, Greece; View further author information
,
Stamatia TheodoridouAdults Thalassemia Unit, ‘Hippokration’ General Hospital of Thessaloniki, Greece; View further author information
,
Bassam R. AliUnited Arab Emirates University, College of Medicine and Health Sciences, Department of Pathology, Al-Ain, United Arab Emirates; View further author information
,
Theodora KatsilaSchool of Health Sciences, Department of Pharmacy, Laboratory of Pharmacogenomics and Individualized Therapy, University of Patras, Greece; View further author information
,
George P. PatrinosSchool of Health Sciences, Department of Pharmacy, Laboratory of Pharmacogenomics and Individualized Therapy, University of Patras, Greece; ;United Arab Emirates University, College of Medicine and Health Sciences, Department of Pathology, Al-Ain, United Arab Emirates; ;United Arab Emirates University, Zayed Center of Health Sciences, Al-Ain, United Arab EmiratesView further author information
&
Adamantia PapachatzopoulouUniversity of Patras, Medical Faculty, Laboratory of General Biology, Patras, Greece; Correspondence[email protected]
View further author information
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Pages 27-33 | Received 08 Feb 2019, Accepted 01 Mar 2019, Published online: 30 Apr 2019
 
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Abstract

Hemoglobinopathies exhibit a remarkable phenotypic diversity in terms of disease severity, while individual genetic background plays a key role in differential response to drug treatment. In the last decade, genomic variants in genes located within, as well as outside the human β-globin cluster have been shown to be significantly associated with Hb F increase, in relation to hydroxyurea (HU) therapy in patients with these diseases. Here, we aim to determine the effect of genomic variants located in genes, such as MAP3K5, ASS1, NOS2A, TOX, PDE7B, NOS1, FLT1 and ARG2, previously shown to modulate fetal hemoglobin (Hb F) levels in patients with β type hemoglobinopathies and reflecting disease severity and response to HU therapy in an independent cohort of Greek patients with these diseases. We recruited and genotyped 45 β-thalassemia patients (β-thal), either transfusion-dependent (TDT) or non transfusion-dependent (NTDT), 42 Hb S (HBB: c.20A>T)-β-thal compound heterozygotes, who were treated with HU, as well as 53 healthy individuals, all of Hellenic origin. Our study showed that genomic variants of the MAP3K5, NOS2A and ARG2 gene are associated with HU therapy efficacy in Hb S-β-thal compound heterozygotes. We have also shown that FLT1 and ARG2 genomic variants are associated with the mild phenotype of NTDT patients. Our findings provide evidence that MAP3K5, NOS2A, ARG2 and FLT1 genomic variants could be considered as genomic biomarkers to predict HU therapy efficacy in Hb S-β-thal compound heterozygotes and also to describe disease severity in patients with β type hemoglobinopathies.

Acknowledgments

A. Kolliopoulou was a recipient of a General Secretariat for Research and Technology (GSRT) and the Hellenic Foundation for Research and Innovation (HFRI) doctoral fellowship.

Disclosure statement

The authors report no conflicts of interest. The authors alone are responsible for the content and writing of this article.

Additional information

Funding

This study was partly supported by European Commission grant [H2020-668353] to G.P. Patrinos.

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