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A CD3-bispecific molecule targeting P-cadherin demonstrates T cell-mediated regression of established solid tumors in mice

Cancer Immunology, Immunotherapy, ISSN: 1432-0851, Vol: 67, Issue: 2, Page: 247-259
2018
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Article Description

Strong evidence exists supporting the important role T cells play in the immune response against tumors. Still, the ability to initiate tumor-specific immune responses remains a challenge. Recent clinical trials suggest that bispecific antibody-mediated retargeted T cells are a promising therapeutic approach to eliminate hematopoietic tumors. However, this approach has not been validated in solid tumors. PF-06671008 is a dual-affinity retargeting (DART)-bispecific protein engineered with enhanced pharmacokinetic properties to extend in vivo half-life, and designed to engage and activate endogenous polyclonal T cell populations via the CD3 complex in the presence of solid tumors expressing P-cadherin. This bispecific molecule elicited potent P-cadherin expression-dependent cytotoxic T cell activity across a range of tumor indications in vitro, and in vivo in tumor-bearing mice. Regression of established tumors in vivo was observed in both cell line and patient-derived xenograft models engrafted with circulating human T lymphocytes. Measurement of in vivo pharmacodynamic markers demonstrates PF-06671008-mediated T cell activation, infiltration and killing as the mechanism of tumor inhibition.

Bibliographic Details

Fisher, Timothy S; Hooper, Andrea T; Lucas, Justin; Clark, Tracey H; Rohner, Allison K; Peano, Bryan; Elliott, Mark W; Tsaparikos, Konstantinos; Wang, Hui; Golas, Jonathan; Gavriil, Maria; Haddish-Berhane, Nahor; Tchistiakova, Lioudmila; Gerber, Hans-Peter; Root, Adam R; May, Chad

Springer Science and Business Media LLC

Medicine; Immunology and Microbiology; Biochemistry, Genetics and Molecular Biology

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