posted on 2023-04-03, 19:02authored byRachel J. Evans, Douglas W. Perkins, Joanna Selfe, Anna Kelsey, Gavin P. Birch, Janet M. Shipley, Koen Schipper, Clare M. Isacke
Composition and drug to antibody ratio of A5/158 and the isotype control antibody conjugated to vc-MMAE. This figure additionally shows that that conjugation of A5/158 and the isotype control antibody to vc-MMAE does not induce antibody aggregation or disrupt Endo180 protein recognition.
Funding
Breast Cancer Now (BCN)
Cancer Research UK (CRUK)
European Molecular Biology Organization (EMBO)
Chris Lucas Trust
Talan's Trust
History
ARTICLE ABSTRACT
Although the 5-year survival rates for sarcoma patients have improved, the proportion of patients relapsing after first-line treatment remains high, and the survival of patients with metastatic disease is dismal. Moreover, the extensive molecular heterogeneity of the multiple different sarcoma subtypes poses a substantial challenge to developing more personalized treatment strategies. From the IHC staining of a large set of 625 human soft-tissue sarcomas, we demonstrate strong tumor cell staining of the Endo180 (MRC2) receptor in a high proportion of samples, findings echoed in gene-expression data sets showing a significantly increased expression in both soft-tissue and bone sarcomas compared with normal tissue. Endo180 is a constitutively recycling transmembrane receptor and therefore an ideal target for an antibody–drug conjugate (ADC). An anti-Endo180 monoclonal antibody conjugated to the antimitotic agent, MMAE via a cleavable linker, is rapidly internalized into target cells and trafficked to the lysosome for degradation, causing cell death specifically in Endo180-expressing sarcoma cell lines. In a sarcoma tumor xenograft model, the Endo180-vc-MMAE ADC, but not an isotype-vc-MMAE control or the unconjugated Endo180 antibody, drives on-target cytotoxicity resulting in tumor regression and a significant impairment of metastatic colonization of the lungs, liver and lymph nodes. These data, together with the lack of a phenotype in mice with an Mrc2 genetic deletion, provide preclinical proof-of-principle evidence for the future development of an Endo180-ADC as a therapeutic strategy in a broad range of sarcoma subtypes and, importantly, with potential impact both on the primary tumor and in metastatic disease.