Targeted Protein Degradation as a Promising Tool for Epigenetic Upregulation of Fetal Hemoglobin.
Thijs C J VerheulVan Tuan TrinhOlalla VázquezSjaak PhilipsenPublished in: ChemMedChem (2020)
The level of fetal hemoglobin (HbF) is an important disease modifier for β-thalassemia and sickle cell disease patients. Indeed, genetic tinkering with the HbF repression machinery has demonstrated great potential for disease mitigation. Such genetic treatments are costly and the high incidence of β-hemoglobinopathies in low-income countries, therefore, calls for the development of affordable, off-the-shelf, oral treatments. The use of PROTAC (PRoteolysis TArgeting Chimeras) technology to influence the epigenetic mechanisms involved in HbF suppression may provide a solution. In this minireview, we briefly explain the HbF repression network highlighting the epigenetic factors that could be targeted for degradation by PROTACs. We hope that this review will inspire clinicians, molecular and chemical biologists to collaborate and contribute to this fascinating field, which should ultimately deliver drugs that reactivate HbF expression with high specificity and low toxicity.
Keyphrases
- sickle cell disease
- dna methylation
- cancer therapy
- gene expression
- poor prognosis
- end stage renal disease
- genome wide
- ejection fraction
- newly diagnosed
- chronic kidney disease
- peritoneal dialysis
- copy number
- prognostic factors
- cell proliferation
- palliative care
- red blood cell
- drug delivery
- risk assessment
- long non coding rna
- small molecule
- amino acid
- drug induced
- patient reported
- network analysis