| Literature DB >> 29067496 |
Timothy S Fisher1,2,3, Andrea T Hooper4,5, Justin Lucas4,5, Tracey H Clark6, Allison K Rohner4,5, Bryan Peano4,5, Mark W Elliott4,5, Konstantinos Tsaparikos4,5, Hui Wang4,5, Jonathan Golas4,5, Maria Gavriil4,5, Nahor Haddish-Berhane6,7, Lioudmila Tchistiakova6, Hans-Peter Gerber4,5,8, Adam R Root6, Chad May4,5,8.
Abstract
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.Entities:
Keywords: Bispecific; Immunotherapy; P-cadherin; Solid tumor
Mesh:
Substances:
Year: 2017 PMID: 29067496 DOI: 10.1007/s00262-017-2081-0
Source DB: PubMed Journal: Cancer Immunol Immunother ISSN: 0340-7004 Impact factor: 6.968