Individualizing fetal hemoglobin augmenting therapy for β-type hemoglobinopathies patients

Author:

Gravia Aikaterini1,Chondrou Vasiliki1,Sgourou Argyro2,Papantoni Ioanna1,Borg Joseph34,Katsila Theodora1,Papachatzopoulou Adamantia5,Patrinos George P1

Affiliation:

1. University of Patras, School of Health Sciences, Department of Pharmacy, University Campus, Rion, GR-265 04, Patras, Greece

2. Hellenic Open University, School of Science & Technology, Patras, Greece

3. University of Malta, Faculty of Health Sciences, Department of Applied Biomedical Science, Msida, Malta

4. Erasmus University Medical Center, Department of Cell Biology, Rotterdam, The Netherlands

5. University of Patras, Faculty of Medicine, Laboratory of General Biology, Patras, Greece

Abstract

Individual genetic composition is an important cause of variations in the response and tolerance to drug treatment. Pharmacogenomics is a modern discipline aiming to delineate individual genomic profiles and drug response. To date, there are several medical disciplines where pharmacogenomics is readily applicable, while in others its usefulness is yet to be demonstrated. Recent experimental evidence suggest that besides genomic variation within the human β-globin gene cluster, other variants in modifier genes residing outside the human β-globin gene cluster are significantly associated with response to hydroxyurea treatment in β-type hemoglobinopathies patients, deducted from the increase in fetal hemoglobin levels. This article aims to provide an update and to discuss future challenges on the application of pharmacogenomics for β-type hemoglobinopathies therapeutics in relation to the current pharmacological treatment modalities for those disorders.

Publisher

Future Medicine Ltd

Subject

Pharmacology,Genetics,Molecular Medicine

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