Early safety and efficacy from a phase I open-label clinical study of LVGN7409 (CD40 agonist antibody) in patients with advanced or metastatic malignancies.

e14501 Background: LVGN7409 is a recombinant monoclonal antibody against CD40. The modified Fc fragment binds FcγRIIB selectively. LVGN7409 activates CD40 in Fc-FcγRIIB cross-link dependent manner and thus optimally in CD40 and FcγRIIB enriched tumor microenvironment. LVGN7409 demonstrated more robust antitumor efficacy and superior safety profile than published CD40 agonist antibodies in preclinical models. An open-label, first in human phase 1 study of LVGN7409 as a single agent, combined with LVGN3616 (anti-PD-1 antibody), and combined with LVGN3616 and LVGN6051 (CD137 agonist antibody) is ongoing. Methods: LVGN7409 was given intravenously every 3 weeks. For single agent dose-finding, LVGN7409 accelerated doses from 0.01 to 0.1mg/kg, and then conventional “3 + 3” design from 0.3 mg/kg. The objectives evaluate LVGN7409 safety, RP2D in a single agent and combination therapy, PK, immunogenicity, preliminary antitumor activity, and exploratory PD biomarkers. Results: As date on January 24, 2022, 12 patients (5 males, 7 females; median age 56, range 29-76; all ECOG 1 at screening; median 6 lines of prior therapies, range 2-14) have been treated with LVGN7409 monotherapy into 6 cohorts (0.01-0.03mg/kg n=1, 0.1-0.3mg/kg n=3, 1mg/kg n=6, 2mg/kg n=2). They received a median of 3 (range 1-10) treatment cycles. No DLT event was observed up to 2mg/kg of LVGN7409. Treatment-related adverse events (TRAEs) of any grade occurred in 10 out of 12 patients (n=10) including infusion related reaction (n=7), amylase increased (n=5), lipase increased (n=5), ALT increased (n=5), AST increased (n=5), bilirubin increased (n=1), WBC or neutrophil decreased (n=1), nausea (n=1), and cytokine release syndrome (n=1). Two patients experienced grade 3 TRSAEs: amylase/lipase increased (n=1) and ALT/AST increased (n=1). Most TRAEs were transient, asymptomatic, self-limited, and occurred in the initial cycle without recurrence upon rechallenge. Four of nine evaluable patients (44%) hadstabledisease by RECIST1.1 and iRECIST, with one active patient being treated for more than 8 months. CD40 receptor occupancy was achieved at the dose of 0.3 mg/kg and above; preliminary pharmacodynamic marker changes were observed. Conclusions: Preliminary evidence showed LVGN7409 monotherapy was well tolerated up to 2mg/kg. Approximately 44% of stable diseases were observed in these heavily treated patients. The favorable safety profile and preliminary antitumor activity warrant further evaluation of LVGN7409 as a single agent and in combination with other cancer therapeutics in patients with advanced malignancies. Clinical trial information: NCT04635995.