A new study in HemaSphere from an international team of collaborators from Yale School of Medicine and their partner institutions in Ghana, through the SickleGenAfrica Network reports that serum heme oxygenase-1 (HO-1), an enzyme that degrades free heme and counters hemolysis-related toxicity, is markedly elevated in patients with sickle cell disease, with the strongest responses in children.
The lead author, Anna Sowa, MD, MHS, clinical associate (hematology/oncology) and PhD candidate at the Investigative Medicine Program at Yale, noted that this first large study of HO-1 in sickle cell disease, analyzing over 2,300 patients from Ghana, found that circulating HO-1 levels were about 20 times higher in patients with sickle cell disease compared to levels reported in healthy populations. Notably, this protective enzyme was also nearly threefold higher in children than in adults with sickle cell disease, a pattern consistent across sickle cell subtypes.
With these findings, Sowa says the next steps for the SickleGenAfrica Network are to better define the role and mechanisms of HO-1 in people with sickle cell disease, including its genetic regulation. These insights would open the door to therapeutic strategies that boost HO-1 expression or activity, or deliver synthetic HO, in hopes to reduce complications in sickle cell disease.