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Scientists discover new approach to gene therapy

2025-06-18
(Press-News.org) Researchers have found a promising new method for gene therapy. They successfully restarted inactive genes by bringing them closer to genetic switches on the DNA called enhancers. The intermediate piece of DNA was cut out using CRISPR-Cas9 technology. This strategy opens up new possibilities for treating genetic diseases. The team specifically shows the technology’s potential for the treatment of sickle cell disease and beta-thalassemia, two genetic blood diseases. In these conditions, a faulty gene could potentially be compensated by reactivating a helpful but normally inactive one. This ‘delete-to-recruit’ method works by simply changing the spacing—without adding new genes or foreign elements. The discovery, made by researchers from the Hubrecht Institute (De Laat group), Erasmus MC and Sanquin, was published in the journal Blood.

The genes in our DNA carry instructions for making proteins, which perform a range of functions in our cells. But not all genes are active at all times. For instance, some proteins are only needed when specific nutrients need to be broken down. Others only carry out functions during embryonic development and are inactive later in life. For our cells to function properly, it is therefore important that gene activity is precisely regulated. One way to do this is through enhancers: stretches of DNA capable of turning genes on, like a genetic switch.

Bringing it closer
Enhancers can be located next to the gene they control, but can also be far away on the DNA. “In this study, we discovered that it’s possible to activate a gene by bringing it closer to an enhancer,” says Anna-Karina Felder, one of the study’s first authors. Felder and her colleagues Sjoerd Tjalsma, Han Verhagen and Rezin Majied achieved this by using CRISPR-Cas9, a technology acting as molecular scissors that can be guided very precisely to cut the DNA. “We directed the scissors to cut out a piece of DNA between an enhancer and its gene, bringing them closer together,” Felder explains. “In adult cells, this successfully reactivated genes that are normally only active during embryonic development”. The team refers to this entirely new way of reactivating genes as ‘delete-to-recruit’.

Faulty hemoglobin
The new strategy offers hope for patients with sickle cell disease and beta-thalassemia. In these genetic blood diseases, the adult globin gene is broken. This causes the protein hemoglobin, responsible for carrying oxygen in our red blood cells, to not form properly. As a result, red blood cells are broken down too quickly and patients suffer serious lifelong symptoms such as anemia, fatigue and, eventually, organ damage. Blood transfusions are often necessary.

Restarting the backup engine
Delete-to-recruit technology could be used to treat these patients by harnessing the fetal globin gene. This gene is naturally active before birth, and part of the hemoglobin produced within the fetus. Once the child is born, it is switched off. “In people with sickle cell disease or beta-thalassemia, it’s the adult globin gene—the main engine that powers red blood cells—that is broken. But fetal globin is like a backup engine. By switching it back on, we can repower the red blood cells and possibly cure these patients,” Felder says.

The team collaborated with researchers at Erasmus MC (Philipsen) and Sanquin (Van den Akker) to show that this strategy works in cells from human healthy donors and patients with sickle cell disease. Particularly important is that the team confirmed its efficacy in blood stem cells. These cells are responsible for producing the variety of blood cells in our body, including red blood cells. By reactivating fetal globin in blood stem cells, these cells can give rise to healthy red blood cells instead of broken ones.

New possibilities
“While we’re still in the early stages, this research lays important groundwork for the development of new gene therapies,” Felder says. This goes beyond the scope of genetic blood diseases, as the new method could also be applied to other diseases where insufficient amounts of healthy proteins can be compensated by restarting a ‘backup engine gene’. The broader field of gene therapy could thus benefit from delete-to-recruit technology, because it uses a different approach than currently available therapies. “Editing the distance to an enhancer, instead of the genes themselves could offer a versatile therapeutic approach,” Felder concludes.

For patients with sickle cell disease and thalassemia, the new approach could—in the future—provide an alternative to the currently available gene therapy. While the existing gene therapy was approved for use in Europe in 2024, it is very expensive, which limits its accessibility. Moreover, this treatment modifies a globin repressor gene, which indeed causes reactivation of fetal globin, but may well have effects on other genes as well, with unknown consequences for the patient. Delete-to-recruit may circumvent both problems.

Publication
Reactivation of developmentally silenced globin genes through forced linear recruitment of remote enhancers. Anna-Karina Felder†, Sjoerd J.D. Tjalsma†, Han J.M.P. Verhagen†, Rezin Majied†, Marjon J.A.M. Verstegen, Thijs C.J. Verheul, Jeffrey van Haren, Rebecca Mohnani, Richard Gremmen, Peter H.L. Krijger, Sjaak Philipsen*, Emile van den Akker*, Wouter de Laat*. Blood, 2025.

† These authors contributed equally.
* Corresponding authors.

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About Wouter de Laat
Wouter de Laat was group leader at the Hubrecht Institute from 2008 to 2024. He is currently Head of Research at the Department of Genetics at UMC Utrecht, professor of Biomedical Genomics at the UMC Utrecht and Investigator at Oncode Institute.

About Emile van den Akker
Emile van den Akker is group leader at Sanquin Research. He is an investigator of the ZonMw PSIDER consortium TRACER (treating hereditary anemias through stem cell research).

About Sjaak Philipsen
Sjaak Philipsen is group leader at the Erasmus MC Department of Developmental Biology. He is coordinator of the ZonMw PSIDER consortium TRACER (treating hereditary anemias through stem cell research) and an investigator of the EU Pathfinder consortium EdiGenT (new prime editing and non-viral delivery strategies for gene therapy).

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About the Hubrecht Institute
The Hubrecht Institute is a research institute focused on developmental and stem cell biology. Because of the dynamic character of the research, the institute as a variable number of research group, around 20, that do fundamental, multidisciplinary research on healthy and diseased cells, tissues and organisms. The Hubrecht Institute is a research institute of the Royal Netherlands Academy of Arts and Sciences (KNAW), situated on Utrecht Science Park. Since 2008, the institute is affiliated with the UMC Utrecht, advancing the translation of research to the clinic. The Hubrecht Institute has a partnership with the European Molecular Biology Laboratory (EMBL). For more information, visit www.hubrecht.eu. 

About Sanquin
Sanquin provides blood services in the Netherlands on a not-for-profit basis. Sanquin is the knowledge institute in the field of blood, and conducts scientific research in the fields of blood transfusion medicine and immunology, applying this knowledge to the development and production of a range of pharmaceutical and diagnostic services. For more information, visit www.sanquin.nl/en.

About Erasmus MC
Erasmus MC is a university medical center based in Rotterdam, the Netherlands. Its three core tasks are patient care, education, and research, with a commitment to achieving a healthy population and pursuing excellence in healthcare through research and teaching. At Erasmus MC, cutting-edge, world class international medical research is performed to help understand, predict, treat, and prevent diseases and health conditions. For more information, visit www.erasmusmc.nl/en.

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[Press-News.org] Scientists discover new approach to gene therapy