CEA expression heterogeneity and plasticity confer resistance to the CEA-targeting bispecific immunotherapy antibody cibisatamab (CEA-TCB) in patient-derived colorectal cancer organoids.
Reyes Gonzalez-ExpositoMaria SemiannikovaBeatrice GriffithsKhurum KhanLouise J BarberAndrew WoolstonGeorgia SpainKatharina von LogaBen ChallonerRadhika PatelMichael RanesAmanda SwainJanet ThomasAnnette BryantClaire SafferyNicos FotiadisSebastian GuettlerDavid MansfieldAlan MelcherThomas PowlesSheela RaoDavid WatkinsIan ChauNik MatthewsFredrik WallbergNaureen StarlingDavid CunninghamMarco GerlingerPublished in: Journal for immunotherapy of cancer (2019)
Based on these preclinical findings, heterogeneity and plasticity of CEA expression appear to confer low cibisatamab sensitivity in PDOs, supporting further clinical evaluation of their predictive effect in CRC. Pharmacological inhibition of the WNT/β-catenin pathway may be a rational combination to sensitize CRCs to cibisatamab. Our novel PDO and T cell co-culture immunotherapy models enable pre-clinical discovery of candidate biomarkers and combination therapies that may inform and accelerate the development of immuno-oncology agents in the clinic.