Researcher Contact
Annarita Miccio
Inserm researcher
Leader of the Chromatin and Gene Regulation During Development team
Inserm unit 1163 Imagine Institute
Sickle-shaped red blood cells (sickle cell disease) © Inserm/Anne-Marie Chevance de Boisfleury
Both sickle cell disease and beta-thalassemia are genetic disorders that affect hemoglobin, and as such are categorized as beta-hemoglobinopathies. A team of scientists from Inserm, Université Paris Cité and the Paris Public Hospitals Group AP-HP at the Imagine Institute has shown the efficacy of a gene therapy approach to treat these two disorders. The principle is to reactivate in patients the production of fetal hemoglobin, a protein whose expression usually ceases after birth. In a study published in Nature Communications, the research team describes a promising approach for future therapeutic applications.
Sickle cell disease and beta-thalassemia are genetic disorders known as beta-hemoglobinopathies. They are caused by mutations on chromosome 11 of the gene responsible for the production of beta globin, a constituent protein of hemoglobin which is the main component of red blood cells.
In the 1970s, researchers observed that rare individuals with mutations specific to each of these conditions did not develop the disease. What was it they had in common? They were all carriers of compensatory mutations on another chromosome 11 gene, which stimulated the production of fetal hemoglobin (gamma globin). This protein that usually ceases to be produced at the end of fetal life is able to advantageously replace the defective adult beta globin to form healthy hemoglobin, thereby ensuring the production of perfectly functional red blood cells in sufficient quantities.
A research team led by Annarita Miccio, Inserm researcher at the Imagine Institute (Inserm/Université Paris Cité/Paris Public Hospitals Group AP-HP) conducted a series of in vitro experiments to determine the most effective strategy for stimulating fetal hemoglobin production, using gene therapy to reproduce these beneficial mutations for treatment purposes. The most effective approach was to insert a genetic mutation that generates, in red blood cells, a molecular mechanism with the dual advantage of stimulating fetal hemoglobin production and blocking the mechanism that naturally inhibits that production.
Furthermore, the researchers have shown in animals that this strategy is effective over the long term, which is a very important finding in the context of therapeutic application.
“There is still a long way to go before this new gene therapy approach can be used in a clinical setting,” explains Panagiotis Antoniou, first author of the study, for example, we need to optimize the protocol in order to genetically modify more red blood cells, as only 60% are done so with the current protocol. Nevertheless, our research is paving the way for the clinical development of a safe and innovative treatment for patients with beta-hemoglobinopathies, with the objective of improving their quality of life,” concludes the researcher.
Annarita Miccio
Inserm researcher
Leader of the Chromatin and Gene Regulation During Development team
Inserm unit 1163 Imagine Institute
Base-editing-mediated dissection of a γ-globin cis-regulatory element for the therapeutic reactivation of fetal hemoglobin expression
Panagiotis Antoniou1, Giulia Hardouin1,2,3, Pierre Martinucci1, Giacomo Frati1, Tristan Felix1, Anne Chalumeau1, Letizia Fontana1, Jeanne Martin1, Cecile Masson4, Megane Brusson1, Giulia Maule5, Marion Rosello6, Carine Giovannangeli7, Vincent Abramowski8, Jean-Pierre de Villartay8, Jean-Paul Concordet7, Filippo Del Bene6, Wassim El Nemer9,10, Mario Amendola11,12, Marina Cavazzana3,13,14, Anna Cereseto5, Oriana Romano15 & Annarita Miccio1
1 Université Paris Cité, Imagine Institute, Laboratory of chromatin and gene regulation during development, Inserm UMR1163, 75015 Paris, France.
2 Université Paris Cité, Imagine Institute, Laboratory of Human Lymphohematopoiesis, Inserm UMR 1163, 75015 Paris, France.
3 Biotherapy Department and Clinical Investigation Center, Assistance Publique Hôpitaux de Paris, Inserm, 75015 Paris, France.
4 Bioinformatics Platform, Imagine Institute, 75015 Paris, France.
5 CIBIO, University of Trento, 38100 Trento, Italy.
6 Sorbonne Université, Inserm, CNRS, Institut de la Vision, 75015 Paris, France.
7 Inserm U1154, CNRS UMR7196, Museum National d’Histoire Naturelle, Paris, France.
8 Université Paris Cité, Imagine Institute, Laboratory of genome dynamics in the immune system, Inserm UMR 1163, 75015 Paris, France.
9 Établissement Français du Sang, UMR 7268, 13005 Marseille, France.
10 Laboratoire d’Excellence GR-Ex, 75015 Paris, France.
11 Genethon, 91000 Evry, France.
12 Université Paris-Saclay, Univ Evry, Inserm, Genethon, Integrare research unit UMR_S951, 91000 Evry, France.
13 Université Paris Cité, 75015 Paris, France.
14 Imagine Institute, 75015 Paris, France.
15 Department of Life Sciences, University of Modena and Reggio Emilia, 41125 Modena, Italy.
Nature Communications : https://doi.org/10.1038/s41467-022-34493-1