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Therapeutic strategies for sickle cell disease: towards a multi-agent approach
by
Vercellotti, Gregory M
, Malik, Punam
, Telen, Marilyn J
in
Anemia
/ Blood
/ Blood platelets
/ Cell adhesion & migration
/ Endothelium
/ Gene therapy
/ Hematology
/ Hemoglobin
/ Kinases
/ Life expectancy
/ Oxidative stress
/ Polymerization
/ Proteins
/ Sickle cell disease
2019
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Therapeutic strategies for sickle cell disease: towards a multi-agent approach
by
Vercellotti, Gregory M
, Malik, Punam
, Telen, Marilyn J
in
Anemia
/ Blood
/ Blood platelets
/ Cell adhesion & migration
/ Endothelium
/ Gene therapy
/ Hematology
/ Hemoglobin
/ Kinases
/ Life expectancy
/ Oxidative stress
/ Polymerization
/ Proteins
/ Sickle cell disease
2019
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
Therapeutic strategies for sickle cell disease: towards a multi-agent approach
by
Vercellotti, Gregory M
, Malik, Punam
, Telen, Marilyn J
in
Anemia
/ Blood
/ Blood platelets
/ Cell adhesion & migration
/ Endothelium
/ Gene therapy
/ Hematology
/ Hemoglobin
/ Kinases
/ Life expectancy
/ Oxidative stress
/ Polymerization
/ Proteins
/ Sickle cell disease
2019
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Therapeutic strategies for sickle cell disease: towards a multi-agent approach
Journal Article
Therapeutic strategies for sickle cell disease: towards a multi-agent approach
2019
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Overview
For over 100 years, clinicians and scientists have been unravelling the consequences of the A to T substitution in the β-globin gene that produces haemoglobin S, which leads to the systemic manifestations of sickle cell disease (SCD), including vaso-occlusion, anaemia, haemolysis, organ injury and pain. However, despite growing understanding of the mechanisms of haemoglobin S polymerization and its effects on red blood cells, only two therapies for SCD — hydroxyurea and l-glutamine — are approved by the US Food and Drug Administration. Moreover, these treatment options do not fully address the manifestations of SCD, which arise from a complex network of interdependent pathophysiological processes. In this article, we review efforts to develop new drugs targeting these processes, including agents that reactivate fetal haemoglobin, anti-sickling agents, anti-adhesion agents, modulators of ischaemia–reperfusion and oxidative stress, agents that counteract free haemoglobin and haem, anti-inflammatory agents, anti-thrombotic agents and anti-platelet agents. We also discuss gene therapy, which holds promise of a cure, although its widespread application is currently limited by technical challenges and the expense of treatment. We thus propose that developing systems-oriented multi-agent strategies on the basis of SCD pathophysiology is needed to improve the quality of life and survival of people with SCD.
Publisher
Nature Publishing Group
Subject
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