Frontiers in Medicine (May 2020)

Delta-Globin Gene Expression Is Enhanced in vivo by Interferon Type I

  • Maria Francesca Manchinu,
  • Michela Simbula,
  • Cristian Antonio Caria,
  • Ester Musu,
  • Lucia Perseu,
  • Susanna Porcu,
  • Maristella Steri,
  • Daniela Poddie,
  • Jessica Frau,
  • Eleonora Cocco,
  • Laura Manunza,
  • Susanna Barella,
  • Maria Serafina Ristaldi

DOI
https://doi.org/10.3389/fmed.2020.00163
Journal volume & issue
Vol. 7

Abstract

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Beta hemoglobinopathies are widely spread monogenic lethal diseases. Delta-globin gene activation has been proposed as a possible approach for curing these pathologies. The therapeutic potential of delta-globin, the non-alpha component of Hemoglobin A2 (α2δ2; HbA2), has been demonstrated in a mouse model of beta thalassemia, while its anti-sickling effect, comparable to that of gamma globin, was established some time ago. Here we show that the delta-globin mRNA level is considerably increased in a Deoxyribonuclease II-alpha knockout mouse model in which type 1 interferon (interferon beta, IFNb) is activated. IFNb activation in the fetal liver improves the delta-globin mRNA level, while the beta-globin mRNA level is significantly reduced. In addition, we show that HbA2 is significantly increased in patients with multiple sclerosis under type 1 interferon treatment. Our results represent a proof of principle that delta-globin expression can be enhanced through the use of molecules. This observation is potentially interesting in view of a pharmacological approach able to increase the HbA2 level.

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