- Soto, Maira;
- Filbert, Erin L;
- Yang, Hai;
- Starzinski, Stephanie;
- Starzinski, Alec;
- Gin, Marissa;
- Chen, Brandon K;
- Le, Phi;
- Li, Tony;
- Bol, Brandon;
- Cheung, Alexander;
- Zhang, Li;
- Hsu, Frank J;
- Ko, Andrew H;
- Fong, Lawrence;
- Keenan, Bridget P
Sotigalimab is an agonistic anti-CD40 monoclonal antibody that can modulate anti-tumor immune responses. In a phase II clinical trial of sotigalimab combined with neoadjuvant chemoradiation (CRT) in locally advanced esophageal/gastroesophageal junction (E/GEJ) cancer with the primary outcome of efficacy as measured by pathologic complete response (pCR) rate, the combination induced pCR in 38% of treated patients. We investigated the mechanism of action of sotigalimab in samples obtained from this clinical trial. Tumor biopsies and peripheral blood samples were collected at baseline, following an initial dose of sotigalimab, and at the time of surgery after CRT completion from six patients. High dimensional single cell techniques were used, including combined single cell RNA sequencing and proteomics (CITEseq) and multiplexed ion beam imaging (MIBI), to analyze immune responses. Sotigalimab dramatically re-modeled the immune compartment in the periphery and within the tumor microenvironment (TME), increasing expression of molecules related to antigen processing and presentation and altering metabolic pathways in myeloid cells. Concomitant with these changes in myeloid cells, sotigalimab treatment primed new T cell clonotypes and increased the density and activation of T cells with enhanced cytotoxic function. Sotigalimab treatment also induced a decrease in the frequency of Tregs in the TME. These findings indicate that a single dose of sotigalimab leads to enhanced antigen presentation that can activate T cells and induce new T cell clones. This restructuring of the TME provides elements which are critical to the development of effective antitumor immune responses and improved clinical outcomes.