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Tumor-targeted 4-1BB agonists for combination with T cell bispecific antibodies as off-the-shelf therapy.

Christina ClausClaudia FerraraWei XuJohannes SamSabine LangFranziska UhlenbrockRosmarie AlbrechtSylvia HerterRamona SchlenkerTamara HüsserSarah DiggelmannJohn ChallierEkkehard MössnerRalf J HosseThomas HoferPeter BrünkerCatherine JosephJörg BenzPhilippe RinglerHenning StahlbergMatthias LauerMario PerroStanford ChenChristine KüttelPreethi L Bhavani MohanValeria NicoliniMartina Carola BirkAmandine OngaroChristophe PrinceReto GianottiGregory DuganChristopher T WhitlowKiran Kumar Solingapuram SaiDavid L CaudellArmando G Burgos-RodriguezJ Mark ClineMichael HettichMaurizio CeppiAnna Maria GiustiFlavio CrameriWouter DriessenPeter N MorcosAnne Freimoser-GrundschoberVictor LevitskyMaria AmannSandra Grau-RichardsThomas von HirschheydtStella TournavitiMichael MølhøjTanja FautiViola Heinzelmann-SchwarzVolker TeichgräberSara ColombettiMarina BacacAlfred ZippeliusChristiane NeumannPablo Umaña
Published in: Science translational medicine (2020)
Endogenous costimulatory molecules on T cells such as 4-1BB (CD137) can be leveraged for cancer immunotherapy. Systemic administration of agonistic anti-4-1BB antibodies, although effective preclinically, has not advanced to phase 3 trials because they have been hampered by both dependency on Fcγ receptor-mediated hyperclustering and hepatotoxicity. To overcome these issues, we engineered proteins simultaneously targeting 4-1BB and a tumor stroma or tumor antigen: FAP-4-1BBL (RG7826) and CD19-4-1BBL. In the presence of a T cell receptor signal, they provide potent T cell costimulation strictly dependent on tumor antigen-mediated hyperclustering without systemic activation by FcγR binding. We could show targeting of FAP-4-1BBL to FAP-expressing tumor stroma and lymph nodes in a colorectal cancer-bearing rhesus monkey. Combination of FAP-4-1BBL with tumor antigen-targeted T cell bispecific (TCB) molecules in human tumor samples led to increased IFN-γ and granzyme B secretion. Further, combination of FAP- or CD19-4-1BBL with CEA-TCB (RG7802) or CD20-TCB (RG6026), respectively, resulted in tumor remission in mouse models, accompanied by intratumoral accumulation of activated effector CD8+ T cells. FAP- and CD19-4-1BBL thus represent an off-the-shelf combination immunotherapy without requiring genetic modification of effector cells for the treatment of solid and hematological malignancies.
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