Author
Listed:
- Simon Garaudé
(Basel University Hospital and University of Basel
Basel University Hospital)
- Romina Marone
(Basel University Hospital and University of Basel
Basel University Hospital)
- Rosalba Lepore
(Basel University Hospital and University of Basel
Basel University Hospital
Cimeio Therapeutics)
- Anna Devaux
(Basel University Hospital and University of Basel
Basel University Hospital)
- Astrid Beerlage
(Basel University Hospital and University of Basel
Basel University Hospital
Basel University Hospital)
- Denis Seyres
(Basel University Hospital and University of Basel
Basel University Hospital)
- Alessandro Dell’ Aglio
(Basel University Hospital and University of Basel
Basel University Hospital)
- Darius Juskevicius
(Diagnostic Hematology, Basel University Hospital)
- Jessica Zuin
(Basel University Hospital and University of Basel
Basel University Hospital)
- Thomas Burgold
(Basel University Hospital and University of Basel
Basel University Hospital)
- Sisi Wang
(Geneva University Hospitals)
- Varun Katta
(St. Jude Children’s Research Hospital)
- Garret Manquen
(St. Jude Children’s Research Hospital)
- Yichao Li
(St. Jude Children’s Research Hospital)
- Clément Larrue
(University of Geneva
Université de Toulouse, Inserm, CNRS)
- Anna Camus
(Cimeio Therapeutics)
- Izabela Durzynska
(Ridgeline Discovery)
- Lisa C. Wellinger
(Ridgeline Discovery)
- Ian Kirby
(ADC Therapeutics (UK))
- Patrick H. Berkel
(ADC Therapeutics (UK))
- Christian Kunz
(Ridgeline Discovery)
- Jérôme Tamburini
(University of Geneva)
- Francesco Bertoni
(USI
Ente Ospedaliero Cantonale)
- Corinne C. Widmer
(Basel University Hospital
Diagnostic Hematology, Basel University Hospital)
- Shengdar Q. Tsai
(St. Jude Children’s Research Hospital)
- Federico Simonetta
(Geneva University Hospitals
University of Geneva)
- Stefanie Urlinger
(Cimeio Therapeutics)
- Lukas T. Jeker
(Basel University Hospital and University of Basel
Basel University Hospital
Basel University Hospital)
Abstract
Haematopoietic stem cell (HSC) transplantation (HSCT) is the only curative treatment for a broad range of haematological malignancies, but the standard of care relies on untargeted chemotherapies and limited possibilities to treat malignant cells after HSCT without affecting the transplanted healthy cells1. Antigen-specific cell-depleting therapies hold the promise of much more targeted elimination of diseased cells, as witnessed in the past decade by the revolution of clinical practice for B cell malignancies2. However, target selection is complex and limited to antigens expressed on subsets of haematopoietic cells, resulting in a fragmented therapy landscape with high development costs2–5. Here we demonstrate that an antibody–drug conjugate (ADC) targeting the pan-haematopoietic marker CD45 enables the antigen-specific depletion of the entire haematopoietic system, including HSCs. Pairing this ADC with the transplantation of human HSCs engineered to be shielded from the CD45-targeting ADC enables the selective eradication of leukaemic cells with preserved haematopoiesis. The combination of CD45-targeting ADCs and engineered HSCs creates an almost universal strategy to replace a diseased haematopoietic system, irrespective of disease aetiology or originating cell type. We propose that this approach could have broad implications beyond haematological malignancies.
Suggested Citation
Simon Garaudé & Romina Marone & Rosalba Lepore & Anna Devaux & Astrid Beerlage & Denis Seyres & Alessandro Dell’ Aglio & Darius Juskevicius & Jessica Zuin & Thomas Burgold & Sisi Wang & Varun Katta & , 2024.
"Selective haematological cancer eradication with preserved haematopoiesis,"
Nature, Nature, vol. 630(8017), pages 728-735, June.
Handle:
RePEc:nat:nature:v:630:y:2024:i:8017:d:10.1038_s41586-024-07456-3
DOI: 10.1038/s41586-024-07456-3
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