Abstract 700P
Background
Immunotherapies targeting the PD-1/PD-L1 pathway with therapeutic antibodies have shown remarkable anti-tumor effects. Comparing to antibodies, small molecules render lower immunogenic risk and convenience in administration. ABSK043 is an oral small molecule PD-L1 inhibitor that potently blocks PD-1 and PD-L1 interaction. Here, we report the preliminary results from the first-in-human (FIH) study of ABSK043.
Methods
The FIH study evaluated the safety, tolerability, PK, PD, and preliminary efficacy of ABSK043. Dose escalation adopted the BOIN design, and ABSK043 was given orally QD or BID in patients with advanced solid tumors. PD assessments included PD-L1 inhibition and T-cell function.
Results
As of February 2023, 19 pts were enrolled in 5 doses from 200mg QD to 800mg BID in Australia. No DLT was observed and MTD was not reached. The most common (≥10%) TRAEs were rash (10.5%) and decreased appetite (10.5%). No peripheral neuropathy was reported. A grade 3 treatment-related thyroiditis with hyperthyroidism was reported in one patient (400mg BID) who recovered after steroid therapy. No grade 4 or 5 AEs occurred. Among 7 response evaluable pts in BID dosing, two were genomic instability, one endometrial carcinoma with MSI-H/dMMR (600mg BID) and one breast cancer with Lynch syndrome (400mg BID), both achieved partial response and were IO-naïve. ABSK043 depleted over 90% of surface PD-L1 on ex vivo stimulated whole blood in a dose dependent manner. BID dosing enhanced PD-L1 inhibition. Furthermore, ABSK043 decreased soluble PD-L1 levels in serum. Increases in IL-2 with ex vivo stimulation, CXCL9, and IFN-γ levels were observed post-treatment, indicating the activation of T cells.
Conclusions
ABSK043 was well tolerated up to 800 mg BID with no DLT reported. On-target PD effects were consistent with PD-L1 inhibition and data reported by anti-PD-(L)1 mAbs. Preliminary anti-tumor activity was observed, and further studies are warranted to explore the efficacy in a larger number of patients.
Clinical trial identification
NCT04964375.
Editorial acknowledgement
Legal entity responsible for the study
Abbisko Therapeutics Australia Pty. Ltd.
Funding
Abbisko Therapeutics Australia Pty. Ltd.
Disclosure
M. Hong: Non-Financial Interests, Institutional, Invited Speaker: Novartis. L.L. Meng, B. Shen, H. Li, L. Yao, M. Zhang: Financial Interests, Personal, Full or part-time Employment: Abbisko. All other authors have declared no conflicts of interest.
Resources from the same session
97P - Neoadjuvant durvalumab plus gemcitabine and cisplatin (D+GemCis) versus gemcis alone for localized biliary tract cancer (BTC): Results of a randomized, multicenter, open-label, phase II trial (DEBATE)
Presenter: Changhoon Yoo
Session: Poster session 17
101P - Quality of life (QoL) outcomes in patients (pts) with zanidatamab (zani)-treated HER2-positive (HER2+) biliary tract cancer (BTC) in the phase IIb HERIZON-BTC-01 study
Presenter: Harpreet Wasan
Session: Poster session 17
102P - Potentially prognostic factors of overall survival in advanced biliary tract cancer in the randomised phase III TOPAZ-1 study
Presenter: Aiwu Ruth He
Session: Poster session 17
103P - Individual patient data (IPD) meta-analysis of randomised trials to compare efficacy of second-line fluoropyrimidine-based chemotherapy in advanced biliary tract cancer (BTC)
Presenter: Jaewon Hyung
Session: Poster session 17
104P - Final analysis of the prospective, randomized phase II STAMP trial: Adjuvant gemcitabine plus cisplatin (GemCis) versus capecitabine (CAP) in node-positive extrahepatic cholangiocarcinoma (CCA)
Presenter: Hyehyun Jeong
Session: Poster session 17
105P - A phase II study of SHR-1316 plus IBI310 in patients with advanced intrahepatic cholangiocarcinoma after failure of first-line therapy
Presenter: Jia Fan
Session: Poster session 17