作者
Johanna Theruvath,Marie Ménard,Benjamin Smith,Miles H. Linde,Garry L. Coles,Guillermo Nicolás Dalton,Wei Wu,Louise Kiru,Alberto Delaidelli,Elena Sotillo,John L. Silberstein,Anna C. Geraghty,Allison Banuelos,Molly Radosevich,Shaurya Dhingra,Sabine Heitzeneder,Aidan M. Tousley,John Lattin,Peng Xu,Jing Huang,Nicole Nasholm,Andy He,Tracy C. Kuo,Emma Sangalang,Jaume Pons,Amira Barkal,Rachel Brewer,Kristopher D. Marjon,José G. Vilches-Moure,Payton L. Marshall,Ricardo A. Fernandes,Michelle Monje,Jennifer R. Cochran,Poul H. Sorensen,Heike E. Daldrup‐Link,Irving L. Weissman,Julien Sage,Ravindra Majeti,Carolyn R. Bertozzi,William A. Weiss,Crystal L. Mackall,Robbie G. Majzner
摘要
The disialoganglioside GD2 is overexpressed on several solid tumors, and monoclonal antibodies targeting GD2 have substantially improved outcomes for children with high-risk neuroblastoma. However, approximately 40% of patients with neuroblastoma still relapse, and anti-GD2 has not mediated significant clinical activity in any other GD2+ malignancy. Macrophages are important mediators of anti-tumor immunity, but tumors resist macrophage phagocytosis through expression of the checkpoint molecule CD47, a so-called 'Don't eat me' signal. In this study, we establish potent synergy for the combination of anti-GD2 and anti-CD47 in syngeneic and xenograft mouse models of neuroblastoma, where the combination eradicates tumors, as well as osteosarcoma and small-cell lung cancer, where the combination significantly reduces tumor burden and extends survival. This synergy is driven by two GD2-specific factors that reorient the balance of macrophage activity. Ligation of GD2 on tumor cells (a) causes upregulation of surface calreticulin, a pro-phagocytic 'Eat me' signal that primes cells for removal and (b) interrupts the interaction of GD2 with its newly identified ligand, the inhibitory immunoreceptor Siglec-7. This work credentials the combination of anti-GD2 and anti-CD47 for clinical translation and suggests that CD47 blockade will be most efficacious in combination with monoclonal antibodies that alter additional pro- and anti-phagocytic signals within the tumor microenvironment.