Selective haematological cancer eradication with preserved haematopoiesis

Author:

Garaudé SimonORCID,Marone RominaORCID,Lepore RosalbaORCID,Devaux AnnaORCID,Beerlage AstridORCID,Seyres DenisORCID,Dell’ Aglio Alessandro,Juskevicius Darius,Zuin JessicaORCID,Burgold ThomasORCID,Wang Sisi,Katta VarunORCID,Manquen GarretORCID,Li YichaoORCID,Larrue Clément,Camus AnnaORCID,Durzynska Izabela,Wellinger Lisa C.,Kirby Ian,Van Berkel Patrick H.ORCID,Kunz Christian,Tamburini Jérôme,Bertoni FrancescoORCID,Widmer Corinne C.ORCID,Tsai Shengdar Q.ORCID,Simonetta Federico,Urlinger Stefanie,Jeker Lukas T.ORCID

Abstract

AbstractHaematopoietic 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.

Publisher

Springer Science and Business Media LLC

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